Patent application title: Vaccine
Inventors:
Günther Staffler (Vienna, AT)
Petra Lührs (Vienna, AT)
Andreas Mairhofer (Vienna, AT)
Frank Mattner (Vienna, AT)
Frank Mattner (Vienna, AT)
Walter Schmidt (Vienna, AT)
Walter Schmidt (Vienna, AT)
Andrea Dolischka (Vienna, AT)
Assignees:
AFFIRIS AG
IPC8 Class: AA61K39385FI
USPC Class:
4241851
Class name: Drug, bio-affecting and body treating compositions antigen, epitope, or other immunospecific immunoeffector (e.g., immunospecific vaccine, immunospecific stimulator of cell-mediated immunity, immunospecific tolerogen, immunospecific immunosuppressor, etc.) amino acid sequence disclosed in whole or in part; or conjugate, complex, or fusion protein or fusion polypeptide including the same
Publication date: 2014-09-11
Patent application number: 20140255435
Abstract:
Vaccine comprising a peptide bound to a pharmaceutically acceptable
carrier, said peptide having the amino acid sequence
TABLE-US-00001
(SEQ ID NO: 1)
(X1)m (X2)n (X3)o X4 X5 H P
X6 (Formula I),
for treating and/or preventing a physical disorder associated with the
renin-activated angiotensin system, wherein X1 is G or D, X2
is A, P, M, G, or R, X3 is G, A, H, or V, X4 is S, A, D, or
Y, X5 is A, D, H, S, N, or I, X6 is A, L or F, wherein m, n
and o are independently 0 or 1 under the premise that when o is 0 m and n
are 0 and when n is 0 m is 0, and wherein the peptide is not DRVYIHPF
(SEQ ID NO:4).Claims:
1. A pharmaceutical composition for inducing an immune response
comprising a peptide bound to a pharmaceutically acceptable carrier,
wherein said peptide has the amino acid sequence
TABLE-US-00008
(SEQ ID NO: 1)
(X1)m (X2)n (X3)o X4 X5 HP X6
(Formula I),
wherein X1 is G or D, X2 is A, P, M, G, or R, X3 is G, A, H, or V, X4 is 5, A, D, or Y, X5 is A, D, H, S, N, or I, X6 is A, L or F, wherein m, n and o are independently 0 or 1 under the premise that when o is 0 m and n are 0 and when n is 0 m is 0, and wherein the peptide is not DRVYIHPF (SEQ ID NO:4), and wherein said pharmaceutical composition is for treating and/or preventing a physical disorder associated with the rennin-activated angiotensin system.
2. The pharmaceutical composition according to claim 1, wherein the peptide is selected from the group consisting of GRVYIHPF (SEQ ID NO:6), DPVYIHPF (SEQ ID NO:7), DMVYIHPF (SEQ ID NO:8), DGVYIHPF (SEQ ID NO:9), DAVYIHPF (SEQ ID NO:10), DRGYIHPF (SEQ ID NO:11), DRAYIHPF (SEQ ID NO:12), DRHYIHPF (SEQ ID NO:13), DRVAIHPF (SEQ ID NO:14), DRVSIHPF (SEQ ID NO:15), DRVDIHPF (SEQ ID NO:16), DRVYAHPF (SEQ ID NO: 17), DRVYNHPF (SEQ ID NO:18), DRVYDHPF (SEQ ID NO:19), DRVYHHPF (SEQ ID NO:20), DRVYSHPF (SEQ ID NO:21), DRVYIHPA (SEQ ID NO:23), DRVYIHPL (SEQ ID NO:25), DAAYIHPF (SEQ ID NO:27), DRAAIHPF (SEQ ID NO:28), DRVAAHPF (SEQ ID NO:29), DRAYAHPF (SEQ ID NO:30), DRAAAHPF (SEQ ID NO:31), DAAAIHPF (SEQ ID NO:34), DAGYIHPF (SEQ ID NO:37), DAHYIHPF (SEQ ID NO:38), DPGYIHPF (SEQ ID NO:39), DPAYIHPF (SEQ ID NO:40), DMGYIHPF (SEQ ID NO:41), DMAYIHPF (SEQ ID NO:42), DMHYIHPF (SEQ ID NO:43), DGGYIHPF (SEQ ID NO:44), DGAYIHPF (SEQ ID NO:45), DGHYIHPF (SEQ ID NO:46), DPVAIHPF (SEQ ID NO:47), DMVAIHPF (SEQ ID NO:49), DMVSIHPF (SEQ ID NO:50), DRGAIHPF (SEQ ID NO:51), DRHAIHPF (SEQ ID NO:52), DRGYAHPF (SEQ ID NO:53), DRGYDHPF (SEQ ID NO:54), DRGYHHPF (SEQ ID NO:55), DRGYSHPF (SEQ ID NO:56), DRGYNHPF (SEQ ID NO:57), DRAYDHPF (SEQ ID NO:58), DRAYHHPF (SEQ ID NO:59), DRAYSHPF (SEQ ID NO:60), DRAYNHPF (SEQ ID NO:61), DRHYAHPF (SEQ ID NO:62), DRHYSHPF (SEQ ID NO:63), DRHYNHPF (SEQ ID NO:64), DRHYDHPF (SEQ ID NO:65), DRHYHHPF (SEQ ID NO:66), DRGADHPF (SEQ ID NO:68), DRVAHHPF (SEQ ID NO:70), DRHADHPF (SEQ ID NO:71), GRGAIHPF (SEQ ID NO:72), DPGAIHPF (SEQ ID NO:75), DPGSIHPF (SEQ ID NO:77), DMGAIHPF (SEQ ID NO:78), DMGSIHPF (SEQ ID NO:79), GPGYIHPF (SEQ ID NO:80), GPGSIHPF (SEQ ID NO:82), GMGSIHPF (SEQ ID NO:83), DRGSIHPF (SEQ ID NO:84), DPHAIHPF (SEQ ID NO:85), DMHAIHPF (SEQ ID NO:86), GPHAIHPF (SEQ ID NO:87), GMHSIHPF (SEQ ID NO:90), PVYIHPF (SEQ ID NO: 91), MVYIHPF (SEQ ID NO: 92), GVYIHPF (SEQ ID NO: 93), AVYIHPF (SEQ ID NO: RGYIHPF (SEQ ID NO: 95), RAYIHPF (SEQ ID NO: 96), RHYIHPF (SEQ ID NO: 97), RVAIHPF (SEQ ID NO: 98), RVSIHPF (SEQ ID NO: 99), RVDIHPF (SEQ ID NO: 100), RVYAHPF (SEQ ID NO: 101), RVYNHPF (SEQ ID NO: 102), RVYDHPF (SEQ ID NO: 103), RVYHHPF (SEQ ID NO: 104), RVYSHPF (SEQ ID NO: 105), RVYIHPA (SEQ ID NO:107), RVYIHPL (SEQ ID NO: 109), AAYIHPF (SEQ ID NO: 111), RAAIHPF (SEQ ID NO: 112), RVAAHPF (SEQ ID NO: 113), RAYAHPF (SEQ ID NO: 114), RAAAHPF (SEQ ID NO: 115), AAAIHPF (SEQ ID NO: 118), AGYIHPF (SEQ ID NO: 121), AHYIHPF (SEQ ID NO: 122), PGYIHPF (SEQ ID NO:164), PAYIHPF (SEQ ID NO: 124), MGYIHPF (SEQ ID NO:125), MAYIHPF (SEQ ID NO: 126), MHYIHPF (SEQ ID NO: 127), GGYIHPF (SEQ ID NO: 128), GAYIHPF (SEQ ID NO: 129), GHYIHPF (SEQ ID NO: 130), PVAIHPF (SEQ ID NO: 131), PVSIHPF (SEQ ID NO: 132), MVAIHPF (SEQ ID NO: 133), MVSIHPF (SEQ ID NO: 134), RGAIHPF (SEQ ID NO:156), RHAIHPF (SEQ ID NO: 136), RGYAHPF (SEQ ID NO: 137), RGYDHPF (SEQ ID NO: 138), RGYHHPF (SEQ ID NO: 139), RGYSHPF (SEQ ID NO: 140), RGYNHPF (SEQ ID NO: 141), RAYDHPF (SEQ ID NO: 142), RAYHHPF (SEQ ID NO: 143), RAYSHPF (SEQ ID NO: 144), RAYNHPF (SEQ ID NO: 145), RHYAHPF (SEQ ID NO: 146), RHYSHPF (SEQ ID NO: 147), RHYNHPF (SEQ ID NO: 148), RHYDHPF (SEQ ID NO: 149), RHYHHPF (SEQ ID NO: 150), RGADHPF (SEQ ID NO: 152), RGAHHPF (SEQ ID NO: 153), RHADHPF (SEQ ID NO: 155), RHSIHPF (SEQ ID NO:157), PGAIHPF (SEQ ID NO:159), RHAIHPF (SEQ ID NO: 136), PGSIHPF (SEQ ID NO:161), MGAIHPF (SEQ ID NO:162), MGSIHPF (SEQ ID NO:163), RGSIHPF (SEQ ID NO:166), PHAIHPF (SEQ ID NO:167), MHAIHPF (SEQ ID NO:168), PHSIHPF (SEQ ID NO:169), MHSIHPF (SEQ ID NO:170), GYIHPF (SEQ ID NO:171), AYIHPF (SEQ ID NO:172), HYIHPF (SEQ ID NO:190), VYAHPF (SEQ ID NO:176), VYNHPF (SEQ ID NO:177), VYDHPF (SEQ ID NO:178), VYHHPF (SEQ ID NO:179), VYSHPF (SEQ ID NO:180), VYIHPA (SEQ ID NO:182), VYIHPL (SEQ ID NO:184), AAIHPF (SEQ ID NO:186), AYAHPF (SEQ ID NO:188), HYIHPF (SEQ ID NO:190), GAIHPF (SEQ ID NO:192), HAIHPF (SEQ ID NO:193), GYAHPF (SEQ ID NO:194), GYDHPF (SEQ ID NO:195), GYHHPF (SEQ ID NO:196), GYSHPF (SEQ ID NO:197), GYNHPF (SEQ ID NO:198), AYDHPF (SEQ ID NO:199), AYHHPF (SEQ ID NO:200), AYSHPF (SEQ ID NO:201), AYNHPF (SEQ ID NO:202), HYAHPF (SEQ ID NO:203), HYSHPF (SEQ ID NO:204), HYNHPF (SEQ ID NO:205), HYDHPF (SEQ ID NO:206), HYHHPF (SEQ ID NO:207), GAIHPF (SEQ ID NO:192), HSIHPF (SEQ ID NO:214), GSIHPF (SEQ ID NO:216), HAIHPF (SEQ ID NO:193), AIHPF (SEQ ID NO:218), SIHPF (SEQ ID NO:219), DIHPF (SEQ ID NO:220), YAHPF (SEQ ID NO:221), YNHPF (SEQ ID NO:222), YDHPF (SEQ ID NO:223), YHHPF (SEQ ID NO:224) and YSHPF (SEQ ID NO:225).
3. The pharmaceutical composition Vaccine according to claim 1, wherein at least one cysteine residue is bound to the N-terminus of the amino acid sequence according to Formula I.
4. The pharmaceutical composition according to claim 1, wherein said carrier is a protein carrier.
5. The pharmaceutical composition according to claim 4, wherein said protein carrier is selected from the group consisting of keyhole limpet haemocyanin (KLH), tetanus toxoid (TT) and diphtheria toxin (DT).
6. The pharmaceutical composition according to claim 1, wherein said composition further comprises an adjuvant.
7. The pharmaceutical composition according to claim 1, wherein said physical disorder associated with the renin-activated angiotensin system is selected from the group consisting of hypertension, stroke, infarction, kidney failure, congestive heart failure, atherosclerosis, vascular damage, retinal hemorrhage, and autoimmune diseases, and multiple sclerosis.
8. (canceled)
9. The pharmaceutical composition according to claim 6, wherein said adjuvant is alum.
10. A method for treating a patient having or being at risk of a physical disorder associated with the renin-activated angiotensin system, wherein an efficient amount of a composition according to any one of claim 1 is administered to said patient.
11. The method according to claim 10, wherein said physical disorder associated with the renin-activated angiotensin system is hypertension or a hypertension-associated disease.
12. The method according to claim 10, wherein said physical disorder associated with the renin-activated angiotensin system is selected from the group consisting of hypertension, stroke, infarction, kidney failure, congestive heart failure, atherosclerosis, vascular damage, retinal hemorrhage and an autoimmune disease wherein the autoimmune disease is multiple sclerosis.
Description:
CROSS REFERENCE TO RELATED APPLICATIONS
[0001] This application is a continuation of U.S. application Ser. No. 13/386,603, which is the U.S. National Stage Application under U.S.C. §371 of International Application No. PCT/AT2010/000271, with an international filing date of Jul. 23, 2010. The content of the aforesaid application is relied upon and incorporated by reference in its entirety.
REFERENCE TO A SEQUENCE LISTING SUBMITTED ELECTRONICALLY VIA EFS-WEB
[0002] The content of the sequence listing (Name: r56221-2010-07-23-seq_list_ST25, Size: 46,620 bytes; and Date of Creation: Dec. 21, 2011) electronically submitted via EFS-Web is incorporated by reference in its entirety.
[0003] The present invention relates to a medicament to be used in the fields of medicine, immunology, molecular biology and virology preferentially to prevent and/or treat physical disorders associated with the renin-activated angiotensin system, preferably hypertension and hypertension-associated cardiovascular diseases (CVD).
[0004] The renin angiotensin system (RAS), also known as renin angiotensin aldosteron system (RAAS), is a hormone system that regulates different physiological processes in the body. RAS activity is initiated by the cleavage of the peptide angiotensinogen to the decapeptide angiotensin I (Ang I) by the enzyme renin. The key product of the renin system is the octapeptide hormone angiotensin II (Ang II), which is formed from Ang I by the angiotensin-converting enzyme (ACE). RAS plays a key role in volume regulation and the maintenance of blood pressure. However, excessive activity of the renin system is associated with hypertension and target organ damage.
[0005] In recent years it became clear that the renin angiotensin system (RAS) extends well beyond their classical role in blood pressure regulation and salt-water balance. Beside regulating the physiological and pathophysiological processes of cardiovascular and renin tissue, the RAS has been described to act on a number of additional tissues, including, brain, endocrine, sensory, fat and immune cells. Thus the RAS plays an important role in physiological and pathophysiological processes of these tissues as well.
[0006] Since physiological and pathophysiological implications of the RAS are extremely broad medications targeting the RAS have become key clinical tools in the treatment of cardiovascular and renal diseases, such as hypertension, heart failure and diabetic nephropthy. Moreover different studies show that blocking the RAS does not only influence cardiovascular diseases connected to high blood pressure but can also reduce cardiovascular events linked to inflammatory processes such as atherosclerosis. These basic research and animal studies strongly support angiotensin II as a proinflammatory mediator, which directly induces atherosclerotic plaque development and heart remodeling.
[0007] In addition, RAS seems to be central not only to the inflammatory aspects of atherosclerosis but also of autoimmune diseases such as multiple sclerosis.
[0008] Furthermore, evidence suggests that blockade of the renin-angiotensin system decreases the occurrence of new-onset diabetes and reduces the risk of diabetic complications. Other studies provide an overview of the effects of Ang II leading to the development of insulin resistance and its implications for diabetes. Components of the renin-angiotensin system have a complex interaction with insulin action and the development and progression of metabolic diseases.
[0009] RAS, Inflammatory Disorders and Autoimmune Disorders (Atherosclerosis and Multiple Sclerosis)
[0010] Atherosclerosis is a chronic inflammatory disease, which involves vascular cells, immune system, and several organs. Although leukocytes, endothelial and smooth muscle cells have been shown to play a crucial role in atherosclerotic inflammation, recent evidence also supports a direct activity for cytokines and chemokines, factors that have been shown to modulate inflammatory processes. Recent studies now suggest new inflammatory activities for the peptide hormone angiotensin II. The renin-angiotensin system serves an important role in promoting inflammation, since angiotensin II induces proatherosclerotic cytokine secretion and increases endothelial dysfunction. Angiotensin II regulates not only cytokine, chemokine, and growth factor secretion within the arterial wall but regulates also the expression of adhesion molecules (VCAM-1, ICAM-1, P-selectin). Beside this it has been shown that the renin-angiotensin system can modulate the activation of complement system in both atherosclerosis and renal injury. This inflammatory cascade activates the vascular inflammatory response by increasing inflammatory cell recruitment to intima. Recruited cells can produce angiotensin II, resulting in a positive feedback response, which can maintain this inflammatory vicious circle.
[0011] Recently different publications show that the intersection between chronic inflammatory diseases like multiple sclerosis (MS) and the most common of all of the human chronic diseases, atherosclerosis, may go far beyond the root "sclerosis", which is shared in both their names. They showed that the RAS also plays a major role in autoimmunity, exemplified by multiple sclerosis (MS) and its animal model, experimental autoimmune encephalomyelitis (EAE). Using proteomics, the authors observed that RAS is up-regulated in brain lesions of MS. Blocking angiotensin II production with ACE inhibitors or inhibiting angiotensin II signaling with angiotensin II receptor blockers suppressed autoreactive TH1 and TH17 cells and promoted antigen-specific CD4_FoxP3_ regulatory T cells (Treg cells). Treatment with ACE inhibitors induces abundant CD4 FoxP3 T cells with sufficient potency to reverse paralytic EAE. Therefore, authors concluded that modulation of the RAS is an attractive therapeutic strategy for application to human autoimmune diseases.
[0012] RAS and Cardiovascular Diseases--Hypertension
[0013] Cardiovascular disease (CVD) is the leading cause of death throughout the world. According to the World Health Organization (WHO) approximately 30% of all global deaths can be attributed to CVD. CVD is caused by disorders of the heart and blood vessels and encompasses various manifestations. These include myocardial infarction, stroke, heart failure, and end stage renal disease. The most prevalent risk factor for CVD is hypertension. More than a quarter of the world's adult population had hypertension in 2000 and if appropriate action is not taken, this numbers will increase continuously.
[0014] Hypertension, commonly referred to as high blood pressure is defined as chronically elevated blood pressure with a systolic blood pressure above 140 mmHg and/or a diastolic blood pressure above 90 mmHg. Guidelines defined by the "Joint National Committee on Prevention, Detection, Evaluation, and Treatment of High Blood Pressure" suggest that persons with a blood pressure between 120 and 139 mmHg systolic and/or a blood pressure between 80 and 89 mmHg diastolic should be considered pre-hypertensive and require health-promoting changes to prevent CVD. Therefore, lowering the blood pressure is an important strategy to prevent CVD. As first step, blood pressure reduction can be achieved by changes in life style targeting the primary factors like unhealthy diet, physical inactivity, and smoking. However, treatment of essential hypertension requires specific therapies. A key regulator of the blood pressure is the renin-angiotensin system (RAS) which has become an attractive target for therapeutic intervention. Therefore pharmaceuticals that specifically act on components of the RAS have become important clinical tools in the treatment of hypertension.
[0015] The RAS pathway is a cascade beginning with the cleavage of angiotensinogen by renin. Renin is an aspartyl protease synthesized and stored primarily in the granules of juxtaglomerular cells in the kidney and has high substrate specificity for angiotensinogen. Angiotensinogen is mainly formed and constitutively secreted into the circulation by hepatic cells. It is cleaved at the N-terminus by renin to form the decapeptide Angiotensin I (Ang I; the 1-10 peptide) which is rapidly converted into the biological active octapeptide angiotensin II (Ang II; the 1-8 peptide). In contrast to Ang II, Ang I appears to have no biological activity and exists solely as a precursor for Ang II. Cleavage of Ang I is mediated basically, but not exclusively by the angiotensin-converting enzyme (ACE). This membrane-bound metalloproteinase is expressed on the surface of endothelial cells with the highest concentrations found on the vascular epithelium in the lung. Besides ACE chymase has been shown to produce Ang II. Ang II can also directly be generated from angiotensinogen by enzymes like tonin and cathepsin. In addition, other Ang I- and Ang II-derived, functional peptides can be found in the circulation. These are generated by amino-, carboxy- or endopeptidases and include Ang(1-9), Ang(1-7), Ang III (the 2-8 peptide) and Ang IV (the 3-8 peptide). A carboxypeptidase, known as angiotensin-converting enzyme II (ACE2), acts on Ang I as well as Ang II. ACE2 generates Ang1-9 from Ang I and Ang1-7 from Ang II. Ang1-9 can then be further converted to Ang1-7 by ACE. In contrast to Ang II, which elevates blood pressure and appears to be the major mediator of vascular remodeling in hypertension, Ang1-7 peptide promotes vasodilation and by that may counteract the potentially detrimental actions of Ang II. The peptide Ang1-7 acts via its receptor the mas oncogen product (MAS).
[0016] Ang II and Ang 1-7 are considered as the main effector peptides of the RAS, while Ang III and Ang IV have some lesser activity (approximately 40% of the activity of Ang II). The actions of Ang II are mediated predominantly by two seven transmembrane receptors termed Ang II receptors, type 1 (AT1; subtypes 1a and 1b) and type 2 (AT2). The AT1 and AT2 subtypes bind Ang II similarly, but have a different cellular localization and are differentially expressed in diverse tissues. Most of the Ang II hypertensinogenic actions are attributed to the AT1 receptor.
[0017] Throughout the body Ang II is a potent vasoconstrictor. In the kidneys it constricts glomerular arterioles thereby increasing systemic arterial blood pressure and decreasing blood flow. In the adrenal cortex, it causes the release of aldosterone which in turn causes the tubules in the kidneys to reabsorb more sodium and water from the urine. It also acts on the central nervous system to increase a person's appetite for salt and to make them feel thirsty. Additionally, Ang II stimulates the release of Anti Diuretic Hormone (ADH).
[0018] The classical role of components of the RAS is to act as endocrine factors in order to maintain blood pressure and electrolyte as well as fluid balance. In addition to this circulating RAS a local angiotensin-generating cascade exists in several tissues. The so-called tissue RAS can act locally as a paracrine and/or autocrine factor and can operate, in whole or in part, independently of the circulating counterpart.
[0019] Currently several drugs are on the market to treat hypertension. These encompass for example diuretics and calcium-channel blockers and include numerous pharmaceuticals that specifically target components of the RAS. The latter include ACE inhibitors which act by binding to the active side of ACE and interfering with the ability of the enzyme to bind and cleave its substrates. Characteristic side effects of ACE inhibitors are dry cough and first dose hypotension/angioneurotic oedema. Another class of pharmaceuticals that target the RAS is angiotensin receptor (AT1) blockers (ARBs). ARBs specifically interfere with the function of Ang II by blocking the binding of angiotensin II to the AT1 receptor. Recently, a new compound targeting the RAS, namely Aliskerin a drug which inhibits renin has been released on the market.
[0020] In the art it is also suggested to use antagonists for Ang II which show a higher binding affinity to AT1 receptor than Ang II. In document WO 2005/044313 A compounds are disclosed which can be used in the treatment of heart diseases, diseases associated with fibrosis and atherosclerosis. The compounds disclosed in WO 2005/044313 A comprise an octapeptide having the general formula X1X2VYIHPX3 whereby X1 may be any amino acid residue, X2 arginine or N-alkylated arginine or a mimetic of arginine, and X3 may be an amino acid residue containing a hydrophobic side chain. These compounds have a higher binding affinity to the AT1 receptor than angiotensin II (antagonistic activity).
[0021] In GB 2001653 A a compound being derived from angiotensin II and having the general formula XRVYIHPY is disclosed, wherein X represents an α-aminooxy aliphatic acyl group and Y may be leucin, isoleuin, alanin or threonin. Such a compound can be used in the treatment of renal hypertension.
[0022] WO 2002/087504 A, WO 2001/043761 A, WO 2001/098325 A and WO 2000/002905 A provide compounds which function as angiotensin II analogues.
[0023] Although different drugs to treat hypertension are available on the market, hypertension still remains inadequately handled. Poor overall treatment success lies on the one hand in the asymptomatic nature of hypertension and on the other side in the necessity for long-term treatment with medications that requires at least once daily self-administration.
[0024] Recently, active immunotherapy has become of increasing interest as a potential new strategy to treat hypertension and associated disorders.
[0025] The practicability of vaccination against components of the RAS to treat hypertension has been shown in different animal models (Michel-J B et al., Am Heart J. 1989; 117:756). In one of the first approaches it has been shown that vaccination against renin was effective in lowering blood pressure. However, this approach has not been pursued in following years since animals started to suffer from autoimmune nephritis (Michel-J B et al., Circulation. 1990; 81(6):1899-910). Other approaches aimed at inducing an immune response against components of the RAS that are expressed as transmembrane proteins on the cell surface, such as ACE and AT1R. Several research groups have investigated active immunization against AT1R. Although some studies report that antibodies against the N-terminus of the AT1R can attenuate the development of hypertension in spontaneously hypertensive rats, most approaches had no significant effect on blood pressure. Data on active immunization against ACE is very limited. One report describes the vaccination of rabbits but only 1 out of 50 animals made detectable anti ACE antibodies (Soffer-R L et al., Fed. Proc. 1983; 42(19):2735-9). No reports are available on active immunization against angiotensinogen, however several studies explored the feasibility of vaccination against angiotensin I and angiotensin II.
[0026] Vaccination with Ang I conjugated to carrier proteins (e.g. keyhole limpet haemocyanin (KLH)) led to the induction of high antigen-specific humoral immune responses. In experimental settings using different animal models the vaccination-induced antibodies against angiotensin I appeared to be functional, since (i) they were able to bind angiotensin I as revealed by Western blot analysis and (ii) the blood pressure was significantly reduced, indicating that the effects of angiotensin on the RAS were blocked (Downham et al., Br J Clin Pharmacol. 2003; 56:505-12.). By contrast, in human healthy volunteers the blood pressure lowering effect was not seen (Downham et al., 2003). This finding was further confirmed in a study with hypertensive patients who were treated with a 12 amino acid analogue of Ang I covalently linked to KLH and adsorbed to Alum (referred to as PMD3117) (Brown et al., Clin Sci. 2004; 107:167-73). Importantly, this treatment regimen was well tolerated and induced a long lasting, antigen-specific humoral immune response. Additionally, this treatment showed an effect on the renin system as detected by changes in renin and aldosterone levels. However, vaccination with PMD3117 showed no influence on the blood pressure as compared to the placebo control group (Brown et al., 2004). In contrast, a slightly different further development of this Ang I vaccine which was developed by Protherics and replaced Alum by a new adjuvant, namely Co Vaccine HT® did show an effect. Administration of this new vaccine formulation resulted in a 10-fold increase in anti-angiotensin antibody titers in a preclinical setting and human healthy subjects showed changes in systolic and diastolic blood pressure. However, blood pressure was only slightly reduced and this only during rest periods but not during phases of activity which would be of more importance.
[0027] Other approaches to induce antibodies that are able to block the RAS used angiotensin II-derived peptides as antigens. In contrast to a previous study where injection of Ang II-carrier protein conjugates did not result in lowering blood pressure, vaccination with Ang II coupled to virus-like particles (VLP) led to the induction of a high anti-angiotensin specific humoral immune response, that was paralleled with a statistically significant reduction of blood pressure (Ambuhl et al., J Hypertension. 2007; 25:63-72.). In a recent clinical study however, this blood pressure lowering effect could not be monitored upon vaccination using angiotensin II coupled to virus like particles, indicating that the induced humoral immune response induced by this peptide vaccine might not be optimal or sufficient. Therefore, there remains a need in the art to provide new and more effective vaccines targeting angiotensin peptides.
[0028] It is an object of the present invention to provide a medication to prevent and treat conditions associated with elevated levels of angiotensin II produced by the RAS on the basis of a vaccine.
[0029] It turned out that a vaccine comprising a peptide bound to a pharmaceutically acceptable carrier, said peptide having the amino acid sequence
TABLE-US-00002 (SEQ ID NO: 1) (X1)m (X2)n (X3)o X4 X5 H P X6 (Formula I),
wherein
[0030] X1 is G or D,
[0031] X2 is A, P, M, G, or R,
[0032] X3 is G, A, H, or V,
[0033] X4 is S, A, D, or Y,
[0034] X5 is A, D, H, S, N, or I,
[0035] X6 is A, L or F,
wherein m, n and o are independently 0 or 1 under the premise that when o is 0 m and n are 0 and when n is 0 m is 0, and wherein the peptide is not DRVYIHPF (SEQ ID NO:4) can be suitably used for treating and/or preventing a physical disorder associated with the renin-activated angiotensin system.
[0036] Not only peptides having the amino acid sequence according to Formula I can be used for treating and/or preventing a physical disorder associated with the renin-activated angiotensin system, but also peptides having the amino acid sequences according to Formula II and III. Therefore, another aspect of the present invention relates to a vaccine comprising a peptide bound to a pharmaceutically acceptable carrier, said peptide having the amino acid sequence
TABLE-US-00003 (SEQ ID NO: 2) (X1)m (X2)n (X3)o X4 X5 X6 P X7 (Formula II),
for treating and/or preventing a physical disorder associated with the renin-activated angiotensin system, wherein
[0037] X1 is G, A or D,
[0038] X2 is A, P, M, G, or R,
[0039] X3 is G, A, H, or V,
[0040] X4 is S, A, D, or Y,
[0041] X5 is A, D, H, S, N, or I,
[0042] X6 is Y or H,
[0043] X7 is A, V, L, I or F,
wherein m, n and o are independently 0 or 1 under the premise that when o is 0 m and n are 0 and when n is 0 m is 0, and wherein the peptide is not DRVYIHPF (SEQ ID NO:4).
[0044] According to a particularly preferred embodiment of the present invention the vaccine comprises a peptide having the amino acid sequence
TABLE-US-00004 (SEQ ID NO: 3) X1X2X3X4X5X6PX7 (Formula III)
which can be used for treating and/or preventing physical disorders associated with the renin-activated angiotensin system, preferably hypertension and hypertension-associated diseases, wherein
[0045] X1 is G, A or D,
[0046] X2 is A, P, M, G, or R,
[0047] X3 is G, A, H, or V,
[0048] X4 is S, A, D, or Y,
[0049] X5 is A, D, H, S, N, or I,
[0050] X6 is Y or H,
[0051] X7 is A, V, L, I or F.
wherein the peptide is not DRVYIHPF (SEQ ID NO:4).
[0052] The vaccine of the present invention is able to induce specifically the formation of antibodies directed to angiotensin I or angiotensin II when coupled to a carrier protein (or to a peptide containing a T cell epitope) and administered to a mammal. The peptides as outlined in Formulas I to III, may induce antibodies that recognize Ang II with higher specificity than Ang I. Vaccines comprising a peptide having the sequence as outlined in Formulas I to III and having H, and L on their C-terminus X1X2X3X4X5X6PX7HL (both amino acids derived from Ang I), for instance, induce antibodies that may recognize Ang I with higher specificity than Ang II. This allows the specific targeting of either only one species of angiotensin peptides or a combination thereof. Due to the binding of these antibodies to angiotensinogen-derived peptides in said mammals the level of angiotensin peptides can be influenced significantly, and thus these immunogens can be used in an immunotherapeutic approach to combat conditions associated with elevated levels of angiotensin II produced by the RAS or by other proteases (e.g. chymase). Without intending to be limited to any particular theory of mode of molecular action, the peptide variants of the present invention will act as immunogens that can induce antibodies which bind to more than one angiotensin peptide species, thus neutralizing all relevant species of angiotensin peptides at the same time. Alternatively, the induced antibodies can specifically bind to the C-terminus of angiotensin II. Under these conditions the induced antibodies will additionally block the binding of angiotensin II to its receptor, the AT1R.
[0053] The amino acid residues identified in Formulas I to III can be exchanged by the respective amino acid residues indicated above. The amino acid sequence obtained by said variation may comprise one, two, three, four, five, six or seven amino acid residues which are not identical to the original Angiotensin II sequence (DRVYIHPF) (SEQ ID NO:4). Most preferably Formulas I to III may vary from the Angiotensin II sequence by at least one, more preferably by at least two, amino acid residues and by a maximum of seven, preferably by a maximum of six, more preferably by a maximum of five, more preferably by a maximum of four, even more preferably by a maximum of three amino acid residues.
[0054] The peptides of the above identified Formulas may also comprise five, six, seven or eight amino acid residues (starting from X1 or X2 or X3 to the terminal amino acid residue).
[0055] The peptide according to the present invention may be a peptide with 5, 6, 7 or 8 to 20, preferably with 5, 6, 7 or 8 to 15, in particular with 5, 6, 7, 8 or 9, amino acid residues. The peptide of the present invention may also be part of a polypeptide or protein having up to 300, preferably up to 200, more preferably up to 150, even more preferably up to 100, amino acid residues.
[0056] The peptides of the present invention are not identical to the naturally occurring angiotensin II (DRVYIHPF) (SEQ ID NO:4). The vaccine of the present invention will elicit an immunological response in a host that is reactive to angiotensin peptides.
[0057] The peptides of the present invention can be synthetically produced by chemical synthesis methods which are well known in the art, either as an isolated peptide or as a part of another peptide or polypeptide. Alternatively, the peptide can be produced in a microorganism which produces the peptide which is then isolated and if desired, further purified. The peptide variant can be produced in microorganisms such as bacteria, yeast or fungi, in eukaryote cells such as a mammalian or an insect cell, or in a recombinant virus vector such as adenovirus, poxvirus, herpesvirus, Simliki forest virus, baculovirus, bacteriophage, sindbis virus or sendai virus. Suitable bacteria for producing the compound/peptide include E. coli, B. subtilis or any other bacterium that is capable of expressing peptides. Suitable yeast types for expressing said compound/peptide include Saccharomyces cerevisiae, Schizosaccharomyces pombe, Candida, Pichia pastoris or any other yeast capable of expressing peptides. Corresponding methods are well known in the art. Also methods for isolating and purifying recombinantly produced peptides are well known in the art and include e.g. as gel filtration, affinity chromatography, ion exchange chromatography etc.
[0058] To facilitate isolation of the peptide, a fusion polypeptide may be made wherein the peptide is translationally fused (covalently linked) to a heterologous polypeptide which enables isolation by affinity chromatography. Typical heterologous polypeptides are His-Tag (e.g. His6; 6 histidine residues), GST-Tag (Glutathione-S-transferase) etc. The fusion polypeptide facilitates not only the purification of the peptide but may also prevent the degradation of said peptide during purification. If it is desired to remove the heterologous polypeptide after purification, the fusion polypeptide may comprise a cleavage site at the junction between the peptide and the heterologous polypeptide. The cleavage site consists of an amino acid sequence that is cleaved with an enzyme specific for the amino acid sequence at the site (e.g. proteases).
[0059] "Peptide bound to a pharmaceutically acceptable carrier" and "peptide bound to a carrier", as used herein refers to a peptide which is fused to, or conjugated to a carrier. If the peptide of the present invention is fused or conjugated (e.g. via carboxyl, amino, sulfhydryl, hydroxyl, imidazolyl, guanidyl or indolyl groups) to a protein carrier, a linker may be provided between the peptide and the protein carrier.
[0060] According to a particularly preferred embodiment of the present invention the substituents of Formula I may be as follows:
[0061] X1 is G or D,
[0062] X2 is G, R, A, P or M
[0063] X3 is A, V or G
[0064] X4 is Y, A or S
[0065] X5 is N, I, D, S or A and/or
[0066] X6 is F.
[0067] According to a preferred embodiment of the present invention the peptide derived from Formula I is selected from the group consisting of GRVYIHPF (SEQ ID NO:6), DPVYIHPF (SEQ ID NO:7), DMVYIHPF (SEQ ID NO:8), DGVYIHPF (SEQ ID NO:9), DAVYIHPF (SEQ ID NO:10), DRGYIHPF (SEQ ID NO:11), DRAYIHPF (SEQ ID NO:12), DRHYIHPF (SEQ ID NO:13), DRVAIHPF (SEQ ID NO:14), DRVSIHPF (SEQ ID NO:15), DRVDIHPF (SEQ ID NO:16), DRVYAHPF (SEQ ID NO:17), DRVYNHPF (SEQ ID NO:18), DRVYDHPF (SEQ ID NO:19), DRVYHHPF (SEQ ID NO:20), DRVYSHPF (SEQ ID NO:21), DRVYIHPA (SEQ ID NO:23), DRVYIHPL (SEQ ID NO:25), DAAYIHPF (SEQ ID NO:27), DRAAIHPF (SEQ ID NO:28), DRVAAHPF (SEQ ID NO:29), DRAYAHPF (SEQ ID NO:30), DRAAAHPF (SEQ ID NO:31), DAAAIHPF (SEQ ID NO:34), DAGYIHPF (SEQ ID NO:37), DAHYIHPF (SEQ ID NO:38), DPGYIHPF (SEQ ID NO:39), DPAYIHPF (SEQ ID NO:40), DMGYIHPF (SEQ ID NO:41), DMAYIHPF (SEQ ID NO:42), DMHYIHPF (SEQ ID NO:43), DGGYIHPF (SEQ ID NO:44), DGAYIHPF (SEQ ID NO:45), DGHYIHPF (SEQ ID NO:46), DPVAIHPF (SEQ ID NO:47), DMVAIHPF (SEQ ID NO:49), DMVSIHPF (SEQ ID NO:50), DRGAIHPF (SEQ ID NO:51), DRHAIHPF (SEQ ID NO:52), DRGYAHPF (SEQ ID NO:53), DRGYDHPF (SEQ ID NO:54), DRGYHHPF (SEQ ID NO:55), DRGYSHPF (SEQ ID NO:56), DRGYNHPF (SEQ ID NO:57), DRAYDHPF (SEQ ID NO:58), DRAYHHPF (SEQ ID NO:59), DRAYSHPF (SEQ ID NO:60), DRAYNHPF (SEQ ID NO:61), DRHYAHPF (SEQ ID NO:62), DRHYSHPF (SEQ ID NO:63), DRHYNHPF (SEQ ID NO:64), DRHYDHPF (SEQ ID NO:65), DRHYHHPF (SEQ ID NO:66), DRGADHPF (SEQ ID NO:68), DRVAHHPF (SEQ ID NO:70), DRHADHPF (SEQ ID NO:71), GRGAIHPF (SEQ ID NO:72), DPGAIHPF (SEQ ID NO:75), DPGSIHPF (SEQ ID NO:77), DMGAIHPF (SEQ ID NO:78), DMGSIHPF (SEQ ID NO:79), GPGYIHPF (SEQ ID NO:80), GPGSIHPF (SEQ ID NO:82), GMGSIHPF (SEQ ID NO:83), DRGSIHPF (SEQ ID NO:84), DPHAIHPF (SEQ ID NO:85), DMHAIHPF (SEQ ID NO:86), GPHAIHPF (SEQ ID NO:87), GMHSIHPF (SEQ ID NO:90), PVYIHPF (SEQ ID NO:91), MVYIHPF (SEQ ID NO:92), GVYIHPF (SEQ ID NO:93), AVYIHPF (SEQ ID NO:94), RGYIHPF (SEQ ID NO:95), RAYIHPF (SEQ ID NO:96), RHYIHPF (SEQ ID NO:97), RVAIHPF (SEQ ID NO:98), RVSIHPF (SEQ ID NO:99), RVDIHPF (SEQ ID NO:100), RVYAHPF (SEQ ID NO:101), RVYNHPF (SEQ ID NO:102), RVYDHPF (SEQ ID NO:103), RVYHHPF (SEQ ID NO:104), RVYSHPF (SEQ ID NO:105), RVYIHPA (SEQ ID NO:107), RVYIHPL (SEQ ID NO:109), AAYIHPF (SEQ ID NO:111), RAAIHPF (SEQ ID NO:112), RVAAHPF (SEQ ID NO:113), RAYAHPF (SEQ ID NO:114), RAAAHPF (SEQ ID NO:115), AAAIHPF (SEQ ID NO:118), AGYIHPF (SEQ ID NO:121), AHYIHPF (SEQ ID NO: 122), PGYIHPF (SEQ ID NO:123), PAYIHPF (SEQ ID NO:124), MGYIHPF (SEQ ID NO:125), MAYIHPF (SEQ ID NO:126), MHYIHPF (SEQ ID NO:127), GGYIHPF (SEQ ID NO:128), GAYIHPF (SEQ ID NO:129), GHYIHPF (SEQ ID NO:130), PVAIHPF (SEQ ID NO:131), PVSIHPF (SEQ ID NO: 132), MVAIHPF (SEQ ID NO:133), MVSIHPF (SEQ ID NO:134), RGAIHPF (SEQ ID NO:135), RHAIHPF (SEQ ID NO: 136), RGYAHPF (SEQ ID NO:137), RGYDHPF (SEQ ID NO:138), RGYHHPF (SEQ ID NO:139), RGYSHPF (SEQ ID NO:140), RGYNHPF (SEQ ID NO:141), RAYDHPF (SEQ ID NO:142), RAYHHPF (SEQ ID NO:143), RAYSHPF (SEQ ID NO:144), RAYNHPF (SEQ ID NO:145), RHYAHPF (SEQ ID NO:146), RHYSHPF (SEQ ID NO:147), RHYNHPF (SEQ ID NO:148), RHYDHPF (SEQ ID NO:149), RHYHHPF (SEQ ID NO:150), RGADHPF (SEQ ID NO: 152), RGAHHPF (SEQ ID NO:153), RHADHPF (SEQ ID NO:155), RHSIHPF (SEQ ID NO:157), PGAIHPF (SEQ ID NO:159), RHAIHPF (SEQ ID NO: 136), PGSIHPF (SEQ ID NO:161), MGAIHPF (SEQ ID NO:162), MGSIHPF (SEQ ID NO:163), RGSIHPF (SEQ ID NO:166), PHAIHPF (SEQ ID NO:167), MHAIHPF (SEQ ID NO:168), PHSIHPF (SEQ ID NO:169), MHSIHPF (SEQ ID NO:170), GYIHPF (SEQ ID NO:171), AYIHPF (SEQ ID NO:172), HYIHPF (SEQ ID NO:173), VYAHPF (SEQ ID NO:176), VYNHPF (SEQ ID NO:177), VYDHPF (SEQ ID NO:178), VYHHPF (SEQ ID NO:179), VYSHPF (SEQ ID NO:180), VYIHPA (SEQ ID NO:182), VYIHPL (SEQ ID NO:184), AAIHPF (SEQ ID NO:186), AYAHPF (SEQ ID NO:188), HYIHPF (SEQ ID NO:173), GAIHPF (SEQ ID NO:192), HAIHPF (SEQ ID NO:193), GYAHPF (SEQ ID NO:194), GYDHPF (SEQ ID NO:195), GYHHPF (SEQ ID NO:196), GYSHPF (SEQ ID NO:197), GYNHPF (SEQ ID NO:198), AYDHPF (SEQ ID NO:199), AYHHPF (SEQ ID NO:200), AYSHPF (SEQ ID NO:201), AYNHPF (SEQ ID NO:202), HYAHPF (SEQ ID NO:203), HYSHPF (SEQ ID NO:204), HYNHPF (SEQ ID NO:205), HYDHPF (SEQ ID NO:206), HYHHPF (SEQ ID NO:207), GAIHPF (SEQ ID NO:192), HSIHPF (SEQ ID NO:214), GSIHPF (SEQ ID NO:216), HAIHPF (SEQ ID NO:193), AIHPF (SEQ ID NO:218), SIHPF (SEQ ID NO:219), DIHPF (SEQ ID NO:220), YAHPF (SEQ ID NO:221), YNHPF (SEQ ID NO:222), YDHPF (SEQ ID NO:223), YHHPF (SEQ ID NO:224) and YSHPF (SEQ ID NO:225).
[0068] Particularly preferred peptides are DPVYIHPF (SEQ ID NO:7), DMVYIHPF (SEQ ID NO:8), DGVYIHPF (SEQ ID NO:9), DAVYIHPF (SEQ ID NO:10), DRGYIHPF (SEQ ID NO:11), DRAYIHPF (SEQ ID NO:12), DRHYIHPF (SEQ ID NO:13), DRVAIHPF (SEQ ID NO:14), DRVYAHPF (SEQ ID NO: 17), DRVYNHPF (SEQ ID NO:18), DRVYDHPF (SEQ ID NO:19), DRVYSHPF (SEQ ID NO:21), DRVYIHPL (SEQ ID NO:25), DAAYIHPF (SEQ ID NO:27), DRAAIHPF (SEQ ID NO:28), DRVAAHPF (SEQ ID NO:29), DRAYAHPF (SEQ ID NO:30), DAGYIHPF (SEQ ID NO:37), DAHYIHPF (SEQ ID NO:38), DPGYIHPF (SEQ ID NO:39), DPAYIHPF (SEQ ID NO:40), DMGYIHPF (SEQ ID NO:41), DMAYIHPF (SEQ ID NO:42), DMHYIHPF (SEQ ID NO:43), DGGYIHPF (SEQ ID NO:44), DGAYIHPF (SEQ ID NO:45), DGHYIHPF (SEQ ID NO:46), DMVSIHPF (SEQ ID NO:50), DRGAIHPF (SEQ ID NO:51), DRGYAHPF (SEQ ID NO:53), DRGYDHPF (SEQ ID NO:54), DRGYSHPF (SEQ ID NO:56), DRGYNHPF (SEQ ID NO:57), DRAYDHPF (SEQ ID NO:58), DRAYSHPF (SEQ ID NO:60), DRAYNHPF (SEQ ID NO:61), DRHYAHPF (SEQ ID NO:62), DRHYSHPF (SEQ ID NO:63), DRHYNHPF (SEQ ID NO:64), DRHYDHPF (SEQ ID NO:65), GPGYIHPF (SEQ ID NO:80), GPGSIHPF (SEQ ID NO:82), DRGSIHPF (SEQ ID NO:84), PVYIHPF (SEQ ID NO:91), GVYIHPF (SEQ ID NO:93), AVYIHPF (SEQ ID NO: 94), RGYIHPF (SEQ ID NO: 95), RAYIHPF (SEQ ID NO: 96), RHYIHPF (SEQ ID NO:97), RVAIHPF (SEQ ID NO:98), RVSIHPF (SEQ ID NO:99), RVDIHPF (SEQ ID NO:100), RVYAHPF (SEQ ID NO:101), RVYNHPF (SEQ ID NO:102), RVYDHPF (SEQ ID NO:103), RVYSHPF (SEQ ID NO:105), RVYIHPL (SEQ ID NO:109), AAYIHPF (SEQ ID NO:111), RAAIHPF (SEQ ID NO:112), RVAAHPF (SEQ ID NO:113), RAYAHPF (SEQ ID NO:114), AGYIHPF (SEQ ID NO:121), AHYIHPF (SEQ ID NO:122), PGYIHPF (SEQ ID NO:123), PAYIHPF (SEQ ID NO:124), GGYIHPF (SEQ ID NO:128), GAYIHPF (SEQ ID NO:129), GHYIHPF (SEQ ID NO:130), PVSIHPF (SEQ ID NO:132), MVSIHPF (SEQ ID NO:134), RGAIHPF (SEQ ID NO:135), RGYAHPF (SEQ ID NO:137), RGYDHPF (SEQ ID NO:138), RGYSHPF (SEQ ID NO:140), RGYNHPF (SEQ ID NO:141), RAYDHPF (SEQ ID NO:142), RAYSHPF (SEQ ID NO:144), RAYNHPF (SEQ ID NO:145), RHYAHPF (SEQ ID NO:146), RHYSHPF (SEQ ID NO:147), RHYNHPF (SEQ ID NO:148), RHYDHPF (SEQ ID NO:149), RHSIHPF (SEQ ID NO:157), PGAIHPF (SEQ ID NO:159), RHAIHPF (SEQ ID NO:136), PGSIHPF (SEQ ID NO:161), MGAIHPF (SEQ ID NO:162), MGSIHPF (SEQ ID NO:163), MGYIHPF (SEQ ID NO:125), RGSIHPF (SEQ ID NO:166), PHAIHPF (SEQ ID NO:167), MHAIHPF (SEQ ID NO:168), PHSIHPF (SEQ ID NO:169), MHSIHPF (SEQ ID NO:170), GYIHPF (SEQ ID NO:171), AYIHPF (SEQ ID NO:172), VYAHPF (SEQ ID NO:176), VYNHPF (SEQ ID NO:177), VYDHPF (SEQ ID NO:178), VYSHPF (SEQ ID NO:180), AAIHPF (SEQ ID NO:186), AYAHPF (SEQ ID NO:188), HYIHPF (SEQ ID NO:173), GAIHPF (SEQ ID NO:192), GYAHPF (SEQ ID NO:194), GYDHPF (SEQ ID NO:195), GYSHPF (SEQ ID NO:197), GYNHPF (SEQ ID NO:198), AYDHPF (SEQ ID NO:199), AYSHPF (SEQ ID NO:201), AYNHPF (SEQ ID NO:202), GAIHPF (SEQ ID NO:192), GSIHPF (SEQ ID NO:216).
[0069] Even more preferred peptides are DPVYIHPF (SEQ ID NO:7), DMVYIHPF (SEQ ID NO:8), DGVYIHPF (SEQ ID NO:9), DAVYIHPF (SEQ ID NO:10), DRGYIHPF (SEQ ID NO:11), DRAYIHPF (SEQ ID NO:12), DRHYIHPF (SEQ ID NO:13), DRVYIHPL (SEQ ID NO:25), DAAYIHPF (SEQ ID NO:27), DRAAIHPF (SEQ ID NO:28), DRVAAHPF (SEQ ID NO:29), DRAYAHPF (SEQ ID NO:30), DAGYIHPF (SEQ ID NO:37), DAHYIHPF (SEQ ID NO:38), DPGYIHPF (SEQ ID NO:39), DPAYIHPF (SEQ ID NO:40), DMGYIHPF (SEQ ID NO:41), DMAYIHPF (SEQ ID NO:42), DMHYIHPF (SEQ ID NO:43), DGGYIHPF (SEQ ID NO:44), DGAYIHPF (SEQ ID NO:45), DGHYIHPF (SEQ ID NO:46), DMVSIHPF (SEQ ID NO:50), DRGAIHPF (SEQ ID NO:51), DRGYAHPF (SEQ ID NO:53), DRGYDHPF (SEQ ID NO:54), DRGYSHPF (SEQ ID NO:56), DRGYNHPF (SEQ ID NO:57), DRAYDHPF (SEQ ID NO:58), DRAYSHPF (SEQ ID NO:60), DRAYNHPF (SEQ ID NO:61), GPGYIHPF (SEQ ID NO:80), PVYIHPF (SEQ ID NO: 91), GVYIHPF (SEQ ID NO:93), RGYIHPF (SEQ ID NO:95), RAYIHPF (SEQ ID NO:96), RVSIHPF (SEQ ID NO:99), RVYIHPL (SEQ ID NO:109), AAYIHPF (SEQ ID NO:111), RAAIHPF (SEQ ID NO:112), RAYAHPF (SEQ ID NO:114), AGYIHPF (SEQ ID NO:121), PGYIHPF (SEQ ID NO:123), PAYIHPF (SEQ ID NO:124), GAYIHPF (SEQ ID NO:129), PVSIHPF (SEQ ID NO:132), MVSIHPF (SEQ ID NO:134), RGAIHPF (SEQ ID NO:135), RGYAHPF (SEQ ID NO:137), RGYSHPF (SEQ ID NO:140), GYIHPF (SEQ ID NO:171), whereby the most preferred peptides are DPVYIHPF (SEQ ID NO:7), DMVYIHPF (SEQ ID NO:8), DAAYIHPF (SEQ ID NO:27), DRAAIHPF (SEQ ID NO:28), DRAYAHPF (SEQ ID NO:30), DAGYIHPF (SEQ ID NO:37), DPGYIHPF (SEQ ID NO:39), DGAYIHPF (SEQ ID NO:45), DMVSIHPF (SEQ ID NO:50), DRGAIHPF (SEQ ID NO:51), DRGYDHPF (SEQ ID NO:54), DRGYSHPF (SEQ ID NO:56), PVYIHPF (SEQ ID NO:91), GVYIHPF (SEQ ID NO:93), AAYIHPF (SEQ ID NO:111), RAAIHPF (SEQ ID NO:112), RAYAHPF (SEQ ID NO: 114), PGYIHPF (SEQ ID NO:123), PVSIHPF (SEQ ID NO:132), MVSIHPF (SEQ ID NO:134), RGAIHPF (SEQ ID NO:135).
[0070] According to a preferred embodiment of the present invention
[0071] X1 of Formula II and III is G, A or D,
[0072] X2 of Formula II and III is G, A, P, M, or R
[0073] X3 of Formula II and III is G, A, H, or V
[0074] X4 of Formula II and III is S, A, D, or Y
[0075] X5 of Formula II and III is A, D, H, S, N or I
[0076] X6 of Formula II and III is Y or H
[0077] X7 of Formula II and III is A, V, L, I or F.
[0078] The amino acid residues mentioned above are particularly preferred substitutes.
[0079] The peptides of the present invention may comprise a truncation at their N-terminus, so that these peptides miss the first, second and/or third amino acid residue.
[0080] The peptide is preferably selected from the group consisting of GRVYIHPF (SEQ ID NO:6), DPVYIHPF (SEQ ID NO:7), DMVYIHPF (SEQ ID NO:8), DGVYIHPF (SEQ ID NO:9), DAVYIHPF (SEQ ID NO:10), DRGYIHPF (SEQ ID NO:11), DRAYIHPF (SEQ ID NO:12), DRHYIHPF (SEQ ID NO:13), DRVAIHPF (SEQ ID NO:14), DRVSIHPF (SEQ ID NO:15), DRVDIHPF (SEQ ID NO:16), DRVYAHPF (SEQ ID NO: 17), DRVYNHPF (SEQ ID NO:18), DRVYDHPF (SEQ ID NO:19), DRVYHHPF (SEQ ID NO:20), DRVYSHPF (SEQ ID NO:21), DRVYIYPF (SEQ ID NO:22), DRVYIHPA (SEQ ID NO:23), DRVYIHPV (SEQ ID NO:24), DRVYIHPL (SEQ ID NO:25), DRVYIHPI (SEQ ID NO:26), DAAYIHPF (SEQ ID NO:27), DRAAIHPF (SEQ ID NO:28), DRVAAHPF (SEQ ID NO:29), DRAYAHPF (SEQ ID NO:30), DRAAAHPF (SEQ ID NO:31), ARAAIHPF (SEQ ID NO:32), ARVAAHPF (SEQ ID NO:33), DAAAIHPF (SEQ ID NO:34), DAAAAHPF (SEQ ID NO:35), DAVAAHPF (SEQ ID NO:36), DAGYIHPF (SEQ ID NO:37), DAHYIHPF (SEQ ID NO:38), DPGYIHPF (SEQ ID NO:39), DPAYIHPF (SEQ ID NO:40), DMGYIHPF (SEQ ID NO:41), DMAYIHPF (SEQ ID NO:42), DMHYIHPF (SEQ ID NO:43), DGGYIHPF (SEQ ID NO:44), DGAYIHPF (SEQ ID NO:45), DGHYIHPF (SEQ ID NO:46), DPVAIHPF (SEQ ID NO:47), DPVSIHPF (SEQ ID NO:48), DMVAIHPF (SEQ ID NO:49), DMVSIHPF (SEQ ID NO:50), DRGAIHPF (SEQ ID NO:51), DRHAIHPF (SEQ ID NO:52), DRGYAHPF (SEQ ID NO:53), DRGYDHPF (SEQ ID NO:54), DRGYHHPF (SEQ ID NO:55), DRGYSHPF (SEQ ID NO:56), DRGYNHPF (SEQ ID NO:57), DRAYDHPF (SEQ ID NO:58), DRAYHHPF (SEQ ID NO:59), DRAYSHPF (SEQ ID NO:60), DRAYNHPF (SEQ ID NO:61), DRHYAHPF (SEQ ID NO:62), DRHYSHPF (SEQ ID NO:63), DRHYNHPF (SEQ ID NO:64), DRHYDHPF (SEQ ID NO:65), DRHYHHPF (SEQ ID NO:66), DRHYIYPF (SEQ ID NO:67), DRGADHPF (SEQ ID NO:68), DRGAHHPF (SEQ ID NO:69), DRVAHHPF (SEQ ID NO:70), DRHADHPF (SEQ ID NO:71), GRGAIHPF (SEQ ID NO:72), GRHSIHPF (SEQ ID NO:73), GRHADYPF (SEQ ID NO:74), DPGAIHPF (SEQ ID NO:75), GRHAIHPF (SEQ ID NO:76), DPGSIHPF (SEQ ID NO:77), DMGAIHPF (SEQ ID NO:78), DMGSIHPF (SEQ ID NO:79), GPGYIHPF (SEQ ID NO:80), GMGYIHPF (SEQ ID NO:81), GPGSIHPF (SEQ ID NO:82), GMGSIHPF (SEQ ID NO:83), DRGSIHPF (SEQ ID NO:84), DPHAIHPF (SEQ ID NO:85), DMHAIHPF (SEQ ID NO:86), GPHAIHPF (SEQ ID NO:87), GMHAIHPF (SEQ ID NO:88), GPHSIHPF (SEQ ID NO:89), and GMHSIHPF (SEQ ID NO:90).
[0081] Truncated versions missing the first N-terminal amino acid residue are preferably selected from the group consisting of PVYIHPF (SEQ ID NO:91), MVYIHPF (SEQ ID NO:92), GVYIHPF (SEQ ID NO:93), AVYIHPF (SEQ ID NO:94), RGYIHPF (SEQ ID NO:95), RAYIHPF (SEQ ID NO:96), RHYIHPF (SEQ ID NO:97), RVAIHPF (SEQ ID NO:98), RVSIHPF (SEQ ID NO:99), RVDIHPF (SEQ ID NO:100), RVYAHPF (SEQ ID NO:101), RVYNHPF (SEQ ID NO:102), RVYDHPF (SEQ ID NO:103), RVYHHPF (SEQ ID NO:104), RVYSHPF (SEQ ID NO:105), RVYIYPF (SEQ ID NO:106), RVYIHPA (SEQ ID NO:107), RVYIHPV (SEQ ID NO:108), RVYIHPL (SEQ ID NO:109), RVYIHPI (SEQ ID NO:110), AAYIHPF (SEQ ID NO:111), RAAIHPF (SEQ ID NO:112), RVAAHPF (SEQ ID NO:113), RAYAHPF (SEQ ID NO:114), RAAAHPF (SEQ ID NO:115), RAAIHPF (SEQ ID NO:112), RVAAHPF (SEQ ID NO:113), AAAIHPF (SEQ ID NO:118), AAAAHPF (SEQ ID NO:119), AVAAHPF (SEQ ID NO:120), AGYIHPF (SEQ ID NO:121), AHYIHPF (SEQ ID NO:122), PGYIHPF (SEQ ID NO:123), PAYIHPF (SEQ ID NO:124), MGYIHPF (SEQ ID NO:125), MAYIHPF (SEQ ID NO:126), MHYIHPF (SEQ ID NO:127), GGYIHPF (SEQ ID NO:128), GAYIHPF (SEQ ID NO:129), GHYIHPF (SEQ ID NO:130), PVAIHPF (SEQ ID NO:131), PVSIHPF (SEQ ID NO:132), MVAIHPF (SEQ ID NO:133), MVSIHPF (SEQ ID NO:134), RGAIHPF (SEQ ID NO:135), RHAIHPF (SEQ ID NO:136), RGYAHPF (SEQ ID NO:137), RGYDHPF (SEQ ID NO:138), RGYHHPF (SEQ ID NO:139), RGYSHPF (SEQ ID NO:140), RGYNHPF (SEQ ID NO:141), RAYDHPF (SEQ ID NO:142), RAYHHPF (SEQ ID NO:143), RAYSHPF (SEQ ID NO:144), RAYNHPF (SEQ ID NO:145), RHYAHPF (SEQ ID NO:146), RHYSHPF (SEQ ID NO:147), RHYNHPF (SEQ ID NO:148), RHYDHPF (SEQ ID NO:149), RHYHHPF (SEQ ID NO:150), RHYIYPF (SEQ ID NO:151), RGADHPF (SEQ ID NO:152), RGAHHPF (SEQ ID NO:153), RVAHHPF (SEQ ID NO:154), RHADHPF (SEQ ID NO:155), RHSIHPF (SEQ ID NO:157), RHADYPF (SEQ ID NO:158), PGAIHPF (SEQ ID NO:159), RHAIHPF (SEQ ID NO:136), PGSIHPF (SEQ ID NO:161), MGAIHPF (SEQ ID NO:162), MGSIHPF (SEQ ID NO:163), RGSIHPF (SEQ ID NO:166), PHAIHPF (SEQ ID NO:167), MHAIHPF (SEQ ID NO:168), PHSIHPF (SEQ ID NO:169), and MHSIHPF (SEQ ID NO:170).
[0082] Truncated versions missing the first two N-terminal amino acid residues are preferably selected from the group consisting of GYIHPF (SEQ ID NO:171), AYIHPF (SEQ ID NO:172), HYIHPF (SEQ ID NO:173), VAIHPF (SEQ ID NO:174), VSIHPF (SEQ ID NO:191), VDIHPF (SEQ ID NO:175), VYAHPF (SEQ ID NO:176), VYNHPF (SEQ ID NO:177), VYDHPF (SEQ ID NO:178), VYHHPF (SEQ ID NO:179), VYSHPF (SEQ ID NO:180), VYIYPF (SEQ ID NO:181), VYIHPA (SEQ ID NO:182), VYIHPV (SEQ ID NO:183), VYIHPL (SEQ ID NO:184), VYIHPI (SEQ ID NO:185), AAIHPF (SEQ ID NO:186), VAAHPF (SEQ ID NO:187), AYAHPF (SEQ ID NO:188), AAAHPF (SEQ ID NO:189), HYIHPF (SEQ ID NO:173), GAIHPF (SEQ ID NO:192), HAIHPF (SEQ ID NO:193), GYAHPF (SEQ ID NO:194), GYDHPF (SEQ ID NO:195), GYHHPF (SEQ ID NO:196), GYSHPF (SEQ ID NO:197), GYNHPF (SEQ ID NO:198), AYDHPF (SEQ ID NO:199), AYHHPF (SEQ ID NO:200), AYSHPF (SEQ ID NO:201), AYNHPF (SEQ ID NO:202), HYAHPF (SEQ ID NO:203), HYSHPF (SEQ ID NO:204), HYNHPF (SEQ ID NO:205), HYDHPF (SEQ ID NO:206), HYHHPF (SEQ ID NO:207), HYIYPF (SEQ ID NO:208), GADHPF (SEQ ID NO:209), GAHHPF (SEQ ID NO:210), VAHHPF (SEQ ID NO:211), HADHPF (SEQ ID NO:212), GAIHPF (SEQ ID NO:192), HSIHPF (SEQ ID NO:214), HADYPF (SEQ ID NO:215), GSIHPF (SEQ ID NO:216), and HAIHPF (SEQ ID NO:193).
[0083] Truncated versions missing the first three N-terminal amino acid residues are preferably selected from the group consisting of AIHPF (SEQ ID NO:218), SIHPF (SEQ ID NO:219), DIHPF (SEQ ID NO:220), YAHPF (SEQ ID NO:221), YNHPF (SEQ ID NO:222), YDHPF (SEQ ID NO:223), YHHPF (SEQ ID NO:224), YSHPF (SEQ ID NO:225), YIYPF (SEQ ID NO:226), YIHPA (SEQ ID NO:227), YIHPV (SEQ ID NO:228), YIHPL (SEQ ID NO:229), YIHPI (SEQ ID NO:230), AAHPF (SEQ ID NO:231), ADHPF (SEQ ID NO:232), AHHPF (SEQ ID NO:233), and ADYPF (SEQ ID NO:234).
[0084] According to a preferred embodiment of the present invention at least one cysteine residue is bound to the N-terminus of the amino acid sequences according to Formula I, II and/or III and all specific peptides mentioned above.
[0085] The peptide of the present invention may further comprise at least one cysteine residue at its N-terminus. This cysteine residue may serve as a reactive group in order to bind the peptide to another molecule or a carrier. For instance, this group may be used to bind the peptide to a carrier protein. The cysteine residue may alternatively be bound to the C-terminus of the peptide of the present invention.
[0086] The peptide of the present invention is bound to a carrier, preferably protein carrier.
[0087] In order to enhance the production of angiotensin peptide specific antibodies in a mammal the compound of the present invention is bound to a carrier.
[0088] According to a preferred embodiment of the present invention the carrier is selected from the group consisting of keyhole limpet haemocyanin (KLH), tetanus toxoid (TT) or diphtheria toxin (DT) or any other protein or peptide containing T cell epitopes.
[0089] According to a preferred embodiment of the present invention the peptide is coupled to a pharmaceutically acceptable carrier, preferably KLH (Keyhole Limpet Haemocyanin), tetanus toxoid, albumin-binding protein, bovine serum albumin, a dendrimer (MAP; Biol. Chem. 358: 581), peptide linkers (or flanking regions) as well as the adjuvant substances described in Singh et al., Nat. Biotech. 17 (1999), 1075-1081 (in particular those in Table 1 of that document), and O'Hagan et al., Nature Reviews, Drug Discovery 2 (9) (2003), 727-735 (in particular the endogenous immuno-potentiating compounds and delivery systems described therein), or mixtures thereof. The conjugation chemistry (e.g. via heterobifunctional compounds such as GMBS and of course also others as described in "Bioconjugate Techniques", Greg T. Hermanson) in this context can be selected from reactions known to the skilled man in the art. Moreover, the vaccine composition may be formulated with an adjuvant, preferably a low soluble aluminium composition, in particular aluminium hydroxyide. Of course, also adjuvants like MF59 aluminium phosphate, calcium phosphate, cytokines (e.g., IL-2, IL-12, GM-CSF), saponins (e.g., QS21), MDP derivatives, CpG oligos, LPS, MPL, polyphosphazenes, emulsions (e.g., Freund's, SAF), liposomes, virosomes, iscoms, cochleates, PLG microparticles, poloxamer particles, virus-like particles, heat-labile enterotoxin (LT), cholera toxin (CT), mutant toxins (e.g., LTK63 and LTR72), microparticles and/or polymerized liposomes may be used.
[0090] According to a preferred embodiment of the present invention the peptide is formulated with an adjuvant, preferably adsorbed to alum.
[0091] In a related embodiment, the invention is useful for the prevention or treatment of diseases, disorders or conditions associated with the RAS, including but not limited to hypertension, stroke, infarction, kidney failure, congestive heart failure, vascular damage or retinal hemorrhage. In addition to that immunization using peptides enclosed in the embodiment of the present invention can be used to treat or prevent atherosclerotic plaque formation, arterial thrombosis events and events associated with vascular inflammation. Beside this treatment of autoimmune diseases such as multiple sclerosis can be performed using peptides enclosed in the embodiment of the present invention.
[0092] The vaccine of the present invention may be administered subcutaneously, intramuscularly, intradermally, intravenously (see e.g. "Handbook of Pharmaceutical Manufacturing Formulations", Sarfaraz Niazi, CRC Press Inc, 2004). Depending on the route of administration, the medicament may comprise respective carriers, adjuvants and/or excipients.
[0093] The vaccine according to the present invention contains the compound according to the invention in an amount of from 0.1 ng to 10 mg, preferably 10 ng to 1 mg, in particular 100 ng to 100 μg, or, alternatively, e.g. 100 fmol to 10 μmol, preferably 10 pmol to 1 μmol, in particular 100 pmol to 100 nmol. The compound or peptide of the present invention is administered to a mammal in an amount of preferably 100 ng to 1 mg, more preferably 1 μg to 500 μg, even more preferably 10 μg to 100 μg, in particular 20 to 40 or 30 μg, per doses. Typically, the vaccine may also contain auxiliary substances, e.g. buffers, stabilizers etc.
[0094] Yet, another aspect of the present invention relates to the use of a peptide according to the present invention for the manufacture of a medicament for treating and/or preventing physical disorders associated with the renin-activated angiotensin system, preferably hypertension and hypertension-associated diseases.
[0095] The abbreviations for the amino acid residues disclosed in the present invention follow the IUPAC recommendations:
TABLE-US-00005 Amino Acid 3-Letter Code 1-Letter Code Alanine Ala A Arginine Arg R Asparagine Asn N Aspartic Asp D Cysteine Cys C Glutamic Glu E Glutamine Gln Q Glycine Gly G Histidine His H Isoleucine Ile I Leucine Leu L Lysine Lys K Methionine Met M Phenylalanine Phe F Proline Pro P Serine Ser S Threonine Thr T Tryptophan Trp W Tyrosine Tyr Y Valine Val V
[0096] The present invention is further illustrated in the following figures and examples, however, without being restricted thereto.
[0097] FIG. 1 shows the immunogenicity of peptide variants for position 1 of Ang II peptide CDRVYIHPF (SEQ ID NO:235).
[0098] FIG. 2 shows the immunogenicity of peptide variants for position 2 of Ang II peptide CDRVYIHPF (SEQ ID NO:235).
[0099] FIG. 3 shows the immunogenicity of peptide variants for position 3 of Ang II peptide CDRVYIHPF (SEQ ID NO:235).
[0100] FIG. 4 shows the immunogenicity of peptide variants for position 4 of Ang II peptide CDRVYIHPF (SEQ ID NO:235).
[0101] FIG. 5 shows the immunogenicity of peptide variants for position 5 of Ang II peptide CDRVYIHPF (SEQ ID NO:235).
[0102] FIG. 6 shows the immunogenicity of peptide variants for position 6 of Ang II peptide CDRVYIHPF (SEQ ID NO:235).
[0103] FIG. 7 shows the immunogenicity of peptide variants for position 7 of Ang II peptide CDRVYIHPF (SEQ ID NO:235).
[0104] FIG. 8 shows the immunogenicity of peptide variants for position 8 of Ang II peptide CDRVYIHPF (SEQ ID NO:235).
[0105] FIG. 9 shows the immunogenicity of peptide variants where two or more amino acids were replaced by alanine.
[0106] FIG. 10 shows the immunogenicity of peptide variants where three amino acids were replaced on different positions using favorable amino acid substitutes for these positions.
[0107] FIG. 11 shows the immunogenicity of peptide variants where two to four amino acids were replaced on different positions using favorable amino acid substitutes for these positions.
[0108] FIG. 12 shows the immunogenicity of truncated angiotensin VARIOTOPE versions missing the first N-terminal amino acid.
[0109] FIG. 13 shows the immunogenicity of truncated angiotensin VARIOTOPE versions missing the first two or three N-terminal amino acids.
[0110] In each Figure, on the X-axis sera derived from animals immunized with indicated peptides are listed. On the Y-axis relative titers of induced sera are shown. Titers derived from Ang II treated animals were set as 100%. Titers were calculated as the sera dilution giving half-maximal binding (i.e. ODmax/2). White bars indicate titers against the peptides that were used for vaccination while black bars represent titers against the Ang II peptide.
EXAMPLES
Example 1
Positional-Scanning of the Ang II Peptide
[0111] Angiotensin II (Ang II), a key component of the blood pressure regulating RAS was chosen as target for a vaccination approach. Therefore, peptides which are able to induce a humoral immune response that targets angiotensin II have been identified and selected.
[0112] The term "positional scanning" refers to a technology that systematically substitutes the amino acid (AA) residues at each position within a certain protein or peptide region with other AAs. This technology has been used and applied so far only for protein-protein interaction studies, peptide-protein interaction studies and/or for studying the functionality of peptide or protein domains.
[0113] The positional scanning technology was now transferred into and applied in the field of immunology to identify appropriate VARIOTOPEs for the octapeptide Ang II (DRVYIHPF) (SEQ ID NO:4). The aim of this example was to identify AA for each position that support or at least do not interfere with the induction of a polyclonal/oligoclonal humoral immune response that targets the Ang II peptide.
[0114] Therefore, in a first set of experiments each position in the Ang II sequence was systematically replaced by amino acids having similar or different features (see Table 1 for position 2). Subsequently all these peptides were chemically linked via an additional N-terminal cystein to the protein carrier keyhole limpet haemocyanin (KLH) and administrated to mice (BALB/c) together with Alum as adjuvant. Sera from vaccinated mice were used to analyze the immunogenicity of indicated peptides. For this purpose a peptide based ELISA assay was used to define sera titers against the injected peptide (i.e. Ang II peptide variants, VARIOTOPEs) as well as to define the binding capacity of the obtained sera against the Ang II peptide.
TABLE-US-00006 TABLE 1 Peptide variants by amino acid substitution for position 2 Position 1 2 3 4 5 6 7 8 C D R V Y I H P F Ang II SEQ ID NO: 235 C D A V Y I H P F aliphatic non-polar neutral SEQ ID NO: 236 C D E V Y I H P F opposed charge polar acidic SEQ ID NO: 237 C D F V Y I H P F aromatic non-polar neutral SEQ ID NO: 238 C D H V Y I H P F aromatic polar basic SEQ ID NO: 239 C D K V Y I H P F aliphatic polar basic SEQ ID NO: 240 C D M V Y I H P F aliphatic non-polar neutral SEQ ID NO: 241 C D V V Y I H P F aliphatic non-polar neutral SEQ ID NO: 242 C D Y V Y I H P F aromatic polar neutral SEQ ID NO: 243 C D P V Y I H P F ring non-polar neutral SEQ ID NO: 244
[0115] In the Figures (FIGS. 1 to 8 for position 1 to position 8) the results derived from these experiments are shown. On the X-axis sera derived from animals immunized with indicated peptides are listed. On the Y-axis relative titers of induced sera are shown. Titers derived from Ang II treated animals were set as 100%. Titers were calculated as the sera dilution giving half-maximal binding (i.e. ODmax/2). White bars indicate titers against the peptides that were used for vaccination while black bars represent titers against the Ang II peptide.
[0116] Although all tested Ang II peptide variants for position 1 were able to induce antibodies which bound to the injected peptide (FIG. 1), indicating that the amino acid exchange did not abrogate their immunogenicity completely, some peptide variants induced sera that showed a significantly lower titer (peptide variants having an aromatic amino acid exchange). In contrast to this, the peptide variant with G on position 1 seems to have the capacity to induce sera-titers against the injected peptide that are almost twice as high as sera-titers derived from Ang II treated animals. Reactivity against Ang II is roughly increased by 50% using this variant. Sera derived from peptide variants containing A, T, E, N, R or H on first position do not differ significantly from sera derived from Ang II peptide. Aromatic or aliphatic residue on position 1 such as L, F, Y seem to be less favorable for inducing an immune response that recognizes Ang II.
[0117] Therefore, position 1 may contain the following AA:
[0118] the original AA D
[0119] the amino acids G, A
[0120] amino acids that are polar such as E, N, R, H.
[0121] As outlined in FIG. 2 using peptides for immunization where the arginine on position 2 was replaced by P or M increased the titer and also the reactivity to Ang II. Peptides with e.g. R to A or R to K substitution evoked sera that showed the same titer as sera induced by the Ang II peptide. These results indicate that a P or M instead of an R on position 2 is more favorable for inducing a humoral immune response. A and K for example seem to be as good as R.
[0122] Position 2 may contain the following AA:
[0123] the original AA R
[0124] the non-polar and neutral AAs P, M, G and A
[0125] amino acids that are polar such as E, H, K
[0126] Position 3 may contain following AA:
[0127] the original AA V
[0128] The AAs G and H (most favorable)
[0129] non-polar and neutral AAs such as A
[0130] AA aliphatic AA such as L
[0131] amino acids that are polar such as E, H, K
[0132] On Position 4 the original AA Y can be substituted by all AA irrespective of their characteristics.
[0133] The aromatic AAs Y and W and the AA P cannot substitute the original AA I on position 5. All other AA can be used for this purpose.
[0134] The results derived from peptides where the H on position 6 was replaced by indicated amino-acids are shown in FIG. 6. Substitution of the aromatic amino-acid H by other aromatic amino acids such as W, and Y resulted in peptides that have the capacity to induce sera that seem to recognize Ang II even better than the peptide used for vaccination. For peptides with non aromatic amino-acid substitutions on position 6 the reactivity of evoked sera to Ang II is considerably diminished (up to 60%). These results indicate that on position 6 aromatic amino acid can be placed (but not F).
[0135] Position 6 may contain following AA:
[0136] the original AA H
[0137] amino acids that contain an aromatic side chain such as Y, W
[0138] Position 7 may contain following AA:
[0139] the original AA P
[0140] alternatively amino acids that contain an aromatic side chain such as F, W, H may potentially be used
[0141] Position 8 may contain following AA:
[0142] the original AA F
[0143] the AA A, L, I, V, P, M
Example 2
Combined Exchanges of Two or More AA-Positions in Ang II Sequence Using Alanine
[0144] To prove the results derived from the first in vivo experiments where the positional scanning approach was performed, and to test whether combined AA exchanges on different positions might either be additive, when neutral or favorable AA replace the original AA, or subtractive, when less favorable AA are combined, two or more amino acids in the Ang II sequence were replaced. For this purpose in a next set of experiments the amino acid alanine was used (Table 2). Alanine has been defined as a favorable-exchange AA for position 4 (FIG. 4), a neutral-exchange AA for position 1, 2, 3, 5, and for position 8 (FIGS. 1 to 3, 5, 8 and 9). For position 6 and 7 the exchange of the original AAs H and P, respectively, to alanine appeared to be less favorable (FIGS. 6, 7 and 9). Therefore, peptide variants containing alanine on position 4 (favorable exchange) in combination with 1 to 3, 5, and 8 (neutral exchange), can be expected to induce titers against Ang II that are higher or have at least the same value as titers from sera evoked by Ang II peptide. Peptide variants containing alanine on position 1 to 3, 5 and 8 should induce at least an immune response that recognizes Ang II equally well as sera evoked by Ang II peptide. Peptide variants with alanine exchanges on position 6 and 7 (less favorable exchange amino acid for these positions) can be expected to evoke sera with diminished reactivity against Ang II.
[0145] All peptides listed in Table 2 were again chemically linked via the N-terminus to KLH adsorbed to Alum and injected s.c. into experimental animals (BALB/c mice). Sera were analyzed by ELISA and antibody responses induced by the peptide variants were compared to that one induced by the original peptide.
TABLE-US-00007 TABLE 2 Example for peptide variants by amino acid substitution exchanged exchanged sequence position amino acid C-DRVYIHPF (SEQ ID NO: 235) C-DAAVIHPF 2, 3 R, V C-DRAAIHPF 3, 4 V, Y C-DRVAAHPF 4, 5 Y, I C-DRVYAAPF 5, 6 I, H C-DRVYIHAA 7, 8 P, F C-DRAAAHPF 3, 4, 5 V, Y, I C-DRAYAHPF 3, 5 V, I C-DRAAAHPA 3, 4, 5, 8 V, Y, I, F C-DAVYIAPF 2, 6 R, H C-DAVYIAAF 2, 6, 7 R, H, P C-DAVYIAAA 2, 6, 7, 8 R, H, P, F
[0146] All alanine-substituted peptide variants were able to induce antibodies which bind to the injected peptide, indicating that the amino acid exchange did not abrogate their immunogenicity (FIG. 9). But the titers of the sera induced by C-DAVYIAAF, are lower compared to the titers induced by the other antigens, indicating that the combined exchange of indicated AA by alanine is less favorable for immunogenicity of the peptides (FIG. 9).
[0147] Analyzing the reactivity of peptide variant-induced sera (Table 2) against Ang II revealed that sera induced by the following peptides showed diminished reactivity to Ang II: C-DRVYAAPF, C-DRVYIHAA, C-DRAAAHAF, C-DAVYIAPF, C-DAVYIAAF, C-DAVYIAAA, (FIG. 9). These results indicate that Ang II-peptide-variants having at least one alanine substitution at position 6 or position 7 (alanine as a non-favorable AA exchange for these positions), induce sera that show diminished reactivity to Ang II. This is in line with results obtained in positional scanning experiments.
[0148] Alanine substitutions on the position 1-5 of the Ang II molecule (for those positions A has been defined as neutral or favorable AA exchange) do not interfere with reactivity to Ang II. Alanine-substitution on these positions led to the induction of titers which were above to that obtained with Ang II. This effect was seen especially when Y at position 4 was replaced by alanine (FIG. 9).
[0149] Investigation of various alanine-modified Ang II epitopes in Wistar rats showed similar results. This indicates that the results are not only restricted to mice but can also be transferred to another species.
Example 3
Combination of Favorable AAs on Different Positions for Selection of Angiotensin VARIOTOPEs
[0150] In next experiments AA combinations of favorable and/or neutral AA for each position have been tested. As can be seen in FIGS. 10 and 11 amino acid exchanges on different positions using favorable amino acids selected during positional scanning experiments result in the formation of VARIOTOPEs that are able to induce humoral immune responses to angiotensin II that are comparable or higher to that response induced by angiotensin II.
Example 4
Truncated Angiotensin VARIOTOPE Versions Missing the First N-Terminal Amino Acid Residues
[0151] In next experiments truncated versions of angiotensin VARIOTOPEs have been tested. As can be seen in FIGS. 12 and 13 shortening angiotensin VARIOTOPEs (selected as outlined above) on their N-termini does not abrogate their capacity to induce humoral immune responses to angiotensin II that are comparable or higher to that response induced by angiotensin II.
Sequence CWU
1
1
24418PRTArtificial SequenceAngiotensin II derived peptide 1Xaa Xaa Xaa Xaa
Xaa His Pro Xaa 1 5 28PRTArtificial
SequenceAngiotensin II derived peptide 2Xaa Xaa Xaa Xaa Xaa Xaa Pro Xaa 1
5 38PRTArtificial SequenceAngiotensin II
derived peptide 3Xaa Xaa Xaa Xaa Xaa Xaa Pro Xaa 1 5
48PRTArtificial SequenceAngiotensin II derived peptide 4Asp Arg
Val Tyr Ile His Pro Phe 1 5 510PRTArtificial
SequenceAngiotensin II derived peptide 5Xaa Xaa Xaa Xaa Xaa Xaa Pro Xaa
His Leu 1 5 10 68PRTArtificial
SequenceAngiotensin II derived peptide 6Gly Arg Val Tyr Ile His Pro Phe 1
5 78PRTArtificial SequenceAngiotensin II
derived peptide 7Asp Pro Val Tyr Ile His Pro Phe 1 5
88PRTArtificial SequenceAngiotensin II derived peptide 8Asp Met
Val Tyr Ile His Pro Phe 1 5 98PRTArtificial
SequenceAngiotensin II derived peptide 9Asp Gly Val Tyr Ile His Pro Phe 1
5 108PRTArtificial SequenceAngiotensin II
derived peptide 10Asp Ala Val Tyr Ile His Pro Phe 1 5
118PRTArtificial SequenceAngiotensin II derived peptide 11Asp Arg
Gly Tyr Ile His Pro Phe 1 5 128PRTArtificial
SequenceAngiotensin II derived peptide 12Asp Arg Ala Tyr Ile His Pro Phe
1 5 138PRTArtificial SequenceAngiotensin II
derived peptide 13Asp Arg His Tyr Ile His Pro Phe 1 5
148PRTArtificial SequenceAngiotensin II derived peptide 14Asp Arg
Val Ala Ile His Pro Phe 1 5 158PRTArtificial
SequenceAngiotensin II derived peptide 15Asp Arg Val Ser Ile His Pro Phe
1 5 168PRTArtificial SequenceAngiotensin II
derived peptide 16Asp Arg Val Asp Ile His Pro Phe 1 5
178PRTArtificial SequenceAngiotensin II derived peptide 17Asp Arg
Val Tyr Ala His Pro Phe 1 5 188PRTArtificial
SequenceAngiotensin II derived peptide 18Asp Arg Val Tyr Asn His Pro Phe
1 5 198PRTArtificial SequenceAngiotensin II
derived peptide 19Asp Arg Val Tyr Asp His Pro Phe 1 5
208PRTArtificial SequenceAngiotensin II derived peptide 20Asp Arg
Val Tyr His His Pro Phe 1 5 218PRTArtificial
SequenceAngiotensin II derived peptide 21Asp Arg Val Tyr Ser His Pro Phe
1 5 228PRTArtificial SequenceAngiotensin II
derived peptide 22Asp Arg Val Tyr Ile Tyr Pro Phe 1 5
238PRTArtificial SequenceAngiotensin II derived peptide 23Asp Arg
Val Tyr Ile His Pro Ala 1 5 248PRTArtificial
SequenceAngiotensin II derived peptide 24Asp Arg Val Tyr Ile His Pro Val
1 5 258PRTArtificial SequenceAngiotensin II
derived peptide 25Asp Arg Val Tyr Ile His Pro Leu 1 5
268PRTArtificial SequenceAngiotensin II derived peptide 26Asp Arg
Val Tyr Ile His Pro Ile 1 5 278PRTArtificial
SequenceAngiotensin II derived peptide 27Asp Ala Ala Tyr Ile His Pro Phe
1 5 288PRTArtificial SequenceAngiotensin II
derived peptide 28Asp Arg Ala Ala Ile His Pro Phe 1 5
298PRTArtificial SequenceAngiotensin II derived peptide 29Asp Arg
Val Ala Ala His Pro Phe 1 5 308PRTArtificial
SequenceAngiotensin II derived peptide 30Asp Arg Ala Tyr Ala His Pro Phe
1 5 318PRTArtificial SequenceAngiotensin II
derived peptide 31Asp Arg Ala Ala Ala His Pro Phe 1 5
328PRTArtificial SequenceAngiotensin II derived peptide 32Ala Arg
Ala Ala Ile His Pro Phe 1 5 338PRTArtificial
SequenceAngiotensin II derived peptide 33Ala Arg Val Ala Ala His Pro Phe
1 5 348PRTArtificial SequenceAngiotensin II
derived peptide 34Asp Ala Ala Ala Ile His Pro Phe 1 5
358PRTArtificial SequenceAngiotensin II derived peptide 35Asp Ala
Ala Ala Ala His Pro Phe 1 5 368PRTArtificial
SequenceAngiotensin II derived peptide 36Asp Ala Val Ala Ala His Pro Phe
1 5 378PRTArtificial SequenceAngiotensin II
derived peptide 37Asp Ala Gly Tyr Ile His Pro Phe 1 5
388PRTArtificial SequenceAngiotensin II derived peptide 38Asp Ala
His Tyr Ile His Pro Phe 1 5 398PRTArtificial
SequenceAngiotensin II derived peptide 39Asp Pro Gly Tyr Ile His Pro Phe
1 5 408PRTArtificial SequenceAngiotensin II
derived peptide 40Asp Pro Ala Tyr Ile His Pro Phe 1 5
418PRTArtificial SequenceAngiotensin II derived peptide 41Asp Met
Gly Tyr Ile His Pro Phe 1 5 428PRTArtificial
SequenceAngiotensin II derived peptide 42Asp Met Ala Tyr Ile His Pro Phe
1 5 438PRTArtificial SequenceAngiotensin II
derived peptide 43Asp Met His Tyr Ile His Pro Phe 1 5
448PRTArtificial SequenceAngiotensin II derived peptide 44Asp Gly
Gly Tyr Ile His Pro Phe 1 5 458PRTArtificial
SequenceAngiotensin II derived peptide 45Asp Gly Ala Tyr Ile His Pro Phe
1 5 468PRTArtificial SequenceAngiotensin II
derived peptide 46Asp Gly His Tyr Ile His Pro Phe 1 5
478PRTArtificial SequenceAngiotensin II derived peptide 47Asp Pro
Val Ala Ile His Pro Phe 1 5 488PRTArtificial
SequenceAngiotensin II derived peptide 48Asp Pro Val Ser Ile His Pro Phe
1 5 498PRTArtificial SequenceAngiotensin II
derived peptide 49Asp Met Val Ala Ile His Pro Phe 1 5
508PRTArtificial SequenceAngiotensin II derived peptide 50Asp Met
Val Ser Ile His Pro Phe 1 5 518PRTArtificial
SequenceAngiotensin II derived peptide 51Asp Arg Gly Ala Ile His Pro Phe
1 5 528PRTArtificial SequenceAngiotensin II
derived peptide 52Asp Arg His Ala Ile His Pro Phe 1 5
538PRTArtificial SequenceAngiotensin II derived peptide 53Asp Arg
Gly Tyr Ala His Pro Phe 1 5 548PRTArtificial
SequenceAngiotensin II derived peptide 54Asp Arg Gly Tyr Asp His Pro Phe
1 5 558PRTArtificial SequenceAngiotensin II
derived peptide 55Asp Arg Gly Tyr His His Pro Phe 1 5
568PRTArtificial SequenceAngiotensin II derived peptide 56Asp Arg
Gly Tyr Ser His Pro Phe 1 5 578PRTArtificial
SequenceAngiotensin II derived peptide 57Asp Arg Gly Tyr Asn His Pro Phe
1 5 588PRTArtificial SequenceAngiotensin II
derived peptide 58Asp Arg Ala Tyr Asp His Pro Phe 1 5
598PRTArtificial SequenceAngiotensin II derived peptide 59Asp Arg
Ala Tyr His His Pro Phe 1 5 608PRTArtificial
SequenceAngiotensin II derived peptide 60Asp Arg Ala Tyr Ser His Pro Phe
1 5 618PRTArtificial SequenceAngiotensin II
derived peptide 61Asp Arg Ala Tyr Asn His Pro Phe 1 5
628PRTArtificial SequenceAngiotensin II derived peptide 62Asp Arg
His Tyr Ala His Pro Phe 1 5 638PRTArtificial
SequenceAngiotensin II derived peptide 63Asp Arg His Tyr Ser His Pro Phe
1 5 648PRTArtificial SequenceAngiotensin II
derived peptide 64Asp Arg His Tyr Asn His Pro Phe 1 5
658PRTArtificial SequenceAngiotensin II derived peptide 65Asp Arg
His Tyr Asp His Pro Phe 1 5 668PRTArtificial
SequenceAngiotensin II derived peptide 66Asp Arg His Tyr His His Pro Phe
1 5 678PRTArtificial SequenceAngiotensin II
derived peptide 67Asp Arg His Tyr Ile Tyr Pro Phe 1 5
688PRTArtificial SequenceAngiotensin II derived peptide 68Asp Arg
Gly Ala Asp His Pro Phe 1 5 698PRTArtificial
SequenceAngiotensin II derived peptide 69Asp Arg Gly Ala His His Pro Phe
1 5 708PRTArtificial SequenceAngiotensin II
derived peptide 70Asp Arg Val Ala His His Pro Phe 1 5
718PRTArtificial SequenceAngiotensin II derived peptide 71Asp Arg
His Ala Asp His Pro Phe 1 5 728PRTArtificial
SequenceAngiotensin II derived peptide 72Gly Arg Gly Ala Ile His Pro Phe
1 5 738PRTArtificial SequenceAngiotensin II
derived peptide 73Gly Arg His Ser Ile His Pro Phe 1 5
748PRTArtificial SequenceAngiotensin II derived peptide 74Gly Arg
His Ala Asp Tyr Pro Phe 1 5 758PRTArtificial
SequenceAngiotensin II derived peptide 75Asp Pro Gly Ala Ile His Pro Phe
1 5 768PRTArtificial SequenceAngiotensin II
derived peptide 76Gly Arg His Ala Ile His Pro Phe 1 5
778PRTArtificial SequenceAngiotensin II derived peptide 77Asp Pro
Gly Ser Ile His Pro Phe 1 5 788PRTArtificial
SequenceAngiotensin II derived peptide 78Asp Met Gly Ala Ile His Pro Phe
1 5 798PRTArtificial SequenceAngiotensin II
derived peptide 79Asp Met Gly Ser Ile His Pro Phe 1 5
808PRTArtificial SequenceAngiotensin II derived peptide 80Gly Pro
Gly Tyr Ile His Pro Phe 1 5 818PRTArtificial
SequenceAngiotensin II derived peptide 81Gly Met Gly Tyr Ile His Pro Phe
1 5 828PRTArtificial SequenceAngiotensin II
derived peptide 82Gly Pro Gly Ser Ile His Pro Phe 1 5
838PRTArtificial SequenceAngiotensin II derived peptide 83Gly Met
Gly Ser Ile His Pro Phe 1 5 848PRTArtificial
SequenceAngiotensin II derived peptide 84Asp Arg Gly Ser Ile His Pro Phe
1 5 858PRTArtificial SequenceAngiotensin II
derived peptide 85Asp Pro His Ala Ile His Pro Phe 1 5
868PRTArtificial SequenceAngiotensin II derived peptide 86Asp Met
His Ala Ile His Pro Phe 1 5 878PRTArtificial
SequenceAngiotensin II derived peptide 87Gly Pro His Ala Ile His Pro Phe
1 5 888PRTArtificial SequenceAngiotensin II
derived peptide 88Gly Met His Ala Ile His Pro Phe 1 5
898PRTArtificial SequenceAngiotensin II derived peptide 89Gly Pro
His Ser Ile His Pro Phe 1 5 908PRTArtificial
SequenceAngiotensin II derived peptide 90Gly Met His Ser Ile His Pro Phe
1 5 917PRTArtificial SequenceAngiotensin II
derived peptide 91Pro Val Tyr Ile His Pro Phe 1 5
927PRTArtificial SequenceAngiotensin II derived peptide 92Met Val Tyr Ile
His Pro Phe 1 5 937PRTArtificial
SequenceAngiotensin II derived peptide 93Gly Val Tyr Ile His Pro Phe 1
5 947PRTArtificial SequenceAngiotensin II derived
peptide 94Ala Val Tyr Ile His Pro Phe 1 5
957PRTArtificial SequenceAngiotensin II derived peptide 95Arg Gly Tyr Ile
His Pro Phe 1 5 967PRTArtificial
SequenceAngiotensin II derived peptide 96Arg Ala Tyr Ile His Pro Phe 1
5 977PRTArtificial SequenceAngiotensin II derived
peptide 97Arg His Tyr Ile His Pro Phe 1 5
987PRTArtificial SequenceAngiotensin II derived peptide 98Arg Val Ala Ile
His Pro Phe 1 5 997PRTArtificial
SequenceAngiotensin II derived peptide 99Arg Val Ser Ile His Pro Phe 1
5 1007PRTArtificial SequenceAngiotensin II derived
peptide 100Arg Val Asp Ile His Pro Phe 1 5
1017PRTArtificial SequenceAngiotensin II derived peptide 101Arg Val Tyr
Ala His Pro Phe 1 5 1027PRTArtificial
SequenceAngiotensin II derived peptide 102Arg Val Tyr Asn His Pro Phe 1
5 1037PRTArtificial SequenceAngiotensin II derived
peptide 103Arg Val Tyr Asp His Pro Phe 1 5
1047PRTArtificial SequenceAngiotensin II derived peptide 104Arg Val Tyr
His His Pro Phe 1 5 1057PRTArtificial
SequenceAngiotensin II derived peptide 105Arg Val Tyr Ser His Pro Phe 1
5 1067PRTArtificial SequenceAngiotensin II derived
peptide 106Arg Val Tyr Ile Tyr Pro Phe 1 5
1077PRTArtificial SequenceAngiotensin II derived peptide 107Arg Val Tyr
Ile His Pro Ala 1 5 1087PRTArtificial
SequenceAngiotensin II derived peptide 108Arg Val Tyr Ile His Pro Val 1
5 1097PRTArtificial SequenceAngiotensin II derived
peptide 109Arg Val Tyr Ile His Pro Leu 1 5
1107PRTArtificial SequenceAngiotensin II derived peptide 110Arg Val Tyr
Ile His Pro Ile 1 5 1117PRTArtificial
SequenceAngiotensin II derived peptide 111Ala Ala Tyr Ile His Pro Phe 1
5 1127PRTArtificial SequenceAngiotensin II derived
peptide 112Arg Ala Ala Ile His Pro Phe 1 5
1137PRTArtificial SequenceAngiotensin II derived peptide 113Arg Val Ala
Ala His Pro Phe 1 5 1147PRTArtificial
SequenceAngiotensin II derived peptide 114Arg Ala Tyr Ala His Pro Phe 1
5 1157PRTArtificial SequenceAngiotensin II derived
peptide 115Arg Ala Ala Ala His Pro Phe 1 5
1167PRTArtificial SequenceAngiotensin II derived peptide 116Arg Ala Ala
Ile His Pro Phe 1 5 1177PRTArtificial
SequenceAngiotensin II derived peptide 117Arg Val Ala Ala His Pro Phe 1
5 1187PRTArtificial SequenceAngiotensin II derived
peptide 118Ala Ala Ala Ile His Pro Phe 1 5
1197PRTArtificial SequenceAngiotensin II derived peptide 119Ala Ala Ala
Ala His Pro Phe 1 5 1207PRTArtificial
SequenceAngiotensin II derived peptide 120Ala Val Ala Ala His Pro Phe 1
5 1217PRTArtificial SequenceAngiotensin II derived
peptide 121Ala Gly Tyr Ile His Pro Phe 1 5
1227PRTArtificial SequenceAngiotensin II derived peptide 122Ala His Tyr
Ile His Pro Phe 1 5 1237PRTArtificial
SequenceAngiotensin II derived peptide 123Pro Gly Tyr Ile His Pro Phe 1
5 1247PRTArtificial SequenceAngiotensin II derived
peptide 124Pro Ala Tyr Ile His Pro Phe 1 5
1257PRTArtificial SequenceAngiotensin II derived peptide 125Met Gly Tyr
Ile His Pro Phe 1 5 1267PRTArtificial
SequenceAngiotensin II derived peptide 126Met Ala Tyr Ile His Pro Phe 1
5 1277PRTArtificial SequenceAngiotensin II derived
peptide 127Met His Tyr Ile His Pro Phe 1 5
1287PRTArtificial SequenceAngiotensin II derived peptide 128Gly Gly Tyr
Ile His Pro Phe 1 5 1297PRTArtificial
SequenceAngiotensin II derived peptide 129Gly Ala Tyr Ile His Pro Phe 1
5 1307PRTArtificial SequenceAngiotensin II derived
peptide 130Gly His Tyr Ile His Pro Phe 1 5
1317PRTArtificial SequenceAngiotensin II derived peptide 131Pro Val Ala
Ile His Pro Phe 1 5 1327PRTArtificial
SequenceAngiotensin II derived peptide 132Pro Val Ser Ile His Pro Phe 1
5 1337PRTArtificial SequenceAngiotensin II derived
peptide 133Met Val Ala Ile His Pro Phe 1 5
1347PRTArtificial SequenceAngiotensin II derived peptide 134Met Val Ser
Ile His Pro Phe 1 5 1357PRTArtificial
SequenceAngiotensin II derived peptide 135Arg Gly Ala Ile His Pro Phe 1
5 1367PRTArtificial SequenceAngiotensin II derived
peptide 136Arg His Ala Ile His Pro Phe 1 5
1377PRTArtificial SequenceAngiotensin II derived peptide 137Arg Gly Tyr
Ala His Pro Phe 1 5 1387PRTArtificial
SequenceAngiotensin II derived peptide 138Arg Gly Tyr Asp His Pro Phe 1
5 1397PRTArtificial SequenceAngiotensin II derived
peptide 139Arg Gly Tyr His His Pro Phe 1 5
1407PRTArtificial SequenceAngiotensin II derived peptide 140Arg Gly Tyr
Ser His Pro Phe 1 5 1417PRTArtificial
SequenceAngiotensin II derived peptide 141Arg Gly Tyr Asn His Pro Phe 1
5 1427PRTArtificial SequenceAngiotensin II derived
peptide 142Arg Ala Tyr Asp His Pro Phe 1 5
1437PRTArtificial SequenceAngiotensin II derived peptide 143Arg Ala Tyr
His His Pro Phe 1 5 1447PRTArtificial
SequenceAngiotensin II derived peptide 144Arg Ala Tyr Ser His Pro Phe 1
5 1457PRTArtificial SequenceAngiotensin II derived
peptide 145Arg Ala Tyr Asn His Pro Phe 1 5
1467PRTArtificial SequenceAngiotensin II derived peptide 146Arg His Tyr
Ala His Pro Phe 1 5 1477PRTArtificial
SequenceAngiotensin II derived peptide 147Arg His Tyr Ser His Pro Phe 1
5 1487PRTArtificial SequenceAngiotensin II derived
peptide 148Arg His Tyr Asn His Pro Phe 1 5
1497PRTArtificial SequenceAngiotensin II derived peptide 149Arg His Tyr
Asp His Pro Phe 1 5 1507PRTArtificial
SequenceAngiotensin II derived peptide 150Arg His Tyr His His Pro Phe 1
5 1517PRTArtificial SequenceAngiotensin II derived
peptide 151Arg His Tyr Ile Tyr Pro Phe 1 5
1527PRTArtificial SequenceAngiotensin II derived peptide 152Arg Gly Ala
Asp His Pro Phe 1 5 1537PRTArtificial
SequenceAngiotensin II derived peptide 153Arg Gly Ala His His Pro Phe 1
5 1547PRTArtificial SequenceAngiotensin II derived
peptide 154Arg Val Ala His His Pro Phe 1 5
1557PRTArtificial SequenceAngiotensin II derived peptide 155Arg His Ala
Asp His Pro Phe 1 5 1567PRTArtificial
SequenceAngiotensin II derived peptide 156Arg Gly Ala Ile His Pro Phe 1
5 1577PRTArtificial SequenceAngiotensin II derived
peptide 157Arg His Ser Ile His Pro Phe 1 5
1587PRTArtificial SequenceAngiotensin II derived peptide 158Arg His Ala
Asp Tyr Pro Phe 1 5 1597PRTArtificial
SequenceAngiotensin II derived peptide 159Pro Gly Ala Ile His Pro Phe 1
5 1607PRTArtificial SequenceAngiotensin II derived
peptide 160Arg His Ala Ile His Pro Phe 1 5
1617PRTArtificial SequenceAngiotensin II derived peptide 161Pro Gly Ser
Ile His Pro Phe 1 5 1627PRTArtificial
SequenceAngiotensin II derived peptide 162Met Gly Ala Ile His Pro Phe 1
5 1637PRTArtificial SequenceAngiotensin II derived
peptide 163Met Gly Ser Ile His Pro Phe 1 5
1647PRTArtificial SequenceAngiotensin II derived peptide 164Pro Gly Tyr
Ile His Pro Phe 1 5 1657PRTArtificial
SequenceAngiotensin II derived peptide 165Met Gly Tyr Ile His Pro Phe 1
5 1667PRTArtificial SequenceAngiotensin II derived
peptide 166Arg Gly Ser Ile His Pro Phe 1 5
1677PRTArtificial SequenceAngiotensin II derived peptide 167Pro His Ala
Ile His Pro Phe 1 5 1687PRTArtificial
SequenceAngiotensin II derived peptide 168Met His Ala Ile His Pro Phe 1
5 1697PRTArtificial SequenceAngiotensin II derived
peptide 169Pro His Ser Ile His Pro Phe 1 5
1707PRTArtificial SequenceAngiotensin II derived peptide 170Met His Ser
Ile His Pro Phe 1 5 1716PRTArtificial
SequenceAngiotensin II derived peptide 171Gly Tyr Ile His Pro Phe 1
5 1726PRTArtificial SequenceAngiotensin II derived peptide
172Ala Tyr Ile His Pro Phe 1 5 1736PRTArtificial
SequenceAngiotensin II derived peptide 173His Tyr Ile His Pro Phe 1
5 1746PRTArtificial SequenceAngiotensin II derived peptide
174Val Ala Ile His Pro Phe 1 5 1756PRTArtificial
SequenceAngiotensin II derived peptide 175Val Asp Ile His Pro Phe 1
5 1766PRTArtificial SequenceAngiotensin II derived peptide
176Val Tyr Ala His Pro Phe 1 5 1776PRTArtificial
SequenceAngiotensin II derived peptide 177Val Tyr Asn His Pro Phe 1
5 1786PRTArtificial SequenceAngiotensin II derived peptide
178Val Tyr Asp His Pro Phe 1 5 1796PRTArtificial
SequenceAngiotensin II derived peptide 179Val Tyr His His Pro Phe 1
5 1806PRTArtificial SequenceAngiotensin II derived peptide
180Val Tyr Ser His Pro Phe 1 5 1816PRTArtificial
SequenceAngiotensin II derived peptide 181Val Tyr Ile Tyr Pro Phe 1
5 1826PRTArtificial SequenceAngiotensin II derived peptide
182Val Tyr Ile His Pro Ala 1 5 1836PRTArtificial
SequenceAngiotensin II derived peptide 183Val Tyr Ile His Pro Val 1
5 1846PRTArtificial SequenceAngiotensin II derived peptide
184Val Tyr Ile His Pro Leu 1 5 1856PRTArtificial
SequenceAngiotensin II derived peptide 185Val Tyr Ile His Pro Ile 1
5 1866PRTArtificial SequenceAngiotensin II derived peptide
186Ala Ala Ile His Pro Phe 1 5 1876PRTArtificial
SequenceAngiotensin II derived peptide 187Val Ala Ala His Pro Phe 1
5 1886PRTArtificial SequenceAngiotensin II derived peptide
188Ala Tyr Ala His Pro Phe 1 5 1896PRTArtificial
SequenceAngiotensin II derived peptide 189Ala Ala Ala His Pro Phe 1
5 1906PRTArtificial SequenceAngiotensin II derived peptide
190His Tyr Ile His Pro Phe 1 5 1916PRTArtificial
SequenceAngiotensin II derived peptide 191Val Ser Ile His Pro Phe 1
5 1926PRTArtificial SequenceAngiotensin II derived peptide
192Gly Ala Ile His Pro Phe 1 5 1936PRTArtificial
SequenceAngiotensin II derived peptide 193His Ala Ile His Pro Phe 1
5 1946PRTArtificial SequenceAngiotensin II derived peptide
194Gly Tyr Ala His Pro Phe 1 5 1956PRTArtificial
SequenceAngiotensin II derived peptide 195Gly Tyr Asp His Pro Phe 1
5 1966PRTArtificial SequenceAngiotensin II derived peptide
196Gly Tyr His His Pro Phe 1 5 1976PRTArtificial
SequenceAngiotensin II derived peptide 197Gly Tyr Ser His Pro Phe 1
5 1986PRTArtificial SequenceAngiotensin II derived peptide
198Gly Tyr Asn His Pro Phe 1 5 1996PRTArtificial
SequenceAngiotensin II derived peptide 199Ala Tyr Asp His Pro Phe 1
5 2006PRTArtificial SequenceAngiotensin II derived peptide
200Ala Tyr His His Pro Phe 1 5 2016PRTArtificial
SequenceAngiotensin II derived peptide 201Ala Tyr Ser His Pro Phe 1
5 2026PRTArtificial SequenceAngiotensin II derived peptide
202Ala Tyr Asn His Pro Phe 1 5 2036PRTArtificial
SequenceAngiotensin II derived peptide 203His Tyr Ala His Pro Phe 1
5 2046PRTArtificial SequenceAngiotensin II derived peptide
204His Tyr Ser His Pro Phe 1 5 2056PRTArtificial
SequenceAngiotensin II derived peptide 205His Tyr Asn His Pro Phe 1
5 2066PRTArtificial SequenceAngiotensin II derived peptide
206His Tyr Asp His Pro Phe 1 5 2076PRTArtificial
SequenceAngiotensin II derived peptide 207His Tyr His His Pro Phe 1
5 2086PRTArtificial SequenceAngiotensin II derived peptide
208His Tyr Ile Tyr Pro Phe 1 5 2096PRTArtificial
SequenceAngiotensin II derived peptide 209Gly Ala Asp His Pro Phe 1
5 2106PRTArtificial SequenceAngiotensin II derived peptide
210Gly Ala His His Pro Phe 1 5 2116PRTArtificial
SequenceAngiotensin II derived peptide 211Val Ala His His Pro Phe 1
5 2126PRTArtificial SequenceAngiotensin II derived peptide
212His Ala Asp His Pro Phe 1 5 2136PRTArtificial
SequenceAngiotensin II derived peptide 213Gly Ala Ile His Pro Phe 1
5 2146PRTArtificial SequenceAngiotensin II derived peptide
214His Ser Ile His Pro Phe 1 5 2156PRTArtificial
SequenceAngiotensin II derived peptide 215His Ala Asp Tyr Pro Phe 1
5 2166PRTArtificial SequenceAngiotensin II derived peptide
216Gly Ser Ile His Pro Phe 1 5 2176PRTArtificial
SequenceAngiotensin II derived peptide 217His Ala Ile His Pro Phe 1
5 2185PRTArtificial SequenceAngiotensin II derived peptide
218Ala Ile His Pro Phe 1 5 2195PRTArtificial
SequenceAngiotensin II derived peptide 219Ser Ile His Pro Phe 1
5 2205PRTArtificial SequenceAngiotensin II derived peptide 220Asp
Ile His Pro Phe 1 5 2215PRTArtificial SequenceAngiotensin
II derived peptide 221Tyr Ala His Pro Phe 1 5
2225PRTArtificial SequenceAngiotensin II derived peptide 222Tyr Asn His
Pro Phe 1 5 2235PRTArtificial SequenceAngiotensin II
derived peptide 223Tyr Asp His Pro Phe 1 5
2245PRTArtificial SequenceAngiotensin II derived peptide 224Tyr His His
Pro Phe 1 5 2255PRTArtificial SequenceAngiotensin II
derived peptide 225Tyr Ser His Pro Phe 1 5
2265PRTArtificial SequenceAngiotensin II derived peptide 226Tyr Ile Tyr
Pro Phe 1 5 2275PRTArtificial SequenceAngiotensin II
derived peptide 227Tyr Ile His Pro Ala 1 5
2285PRTArtificial SequenceAngiotensin II derived peptide 228Tyr Ile His
Pro Val 1 5 2295PRTArtificial SequenceAngiotensin II
derived peptide 229Tyr Ile His Pro Leu 1 5
2305PRTArtificial SequenceAngiotensin II derived peptide 230Tyr Ile His
Pro Ile 1 5 2315PRTArtificial SequenceAngiotensin II
derived peptide 231Ala Ala His Pro Phe 1 5
2325PRTArtificial SequenceAngiotensin II derived peptide 232Ala Asp His
Pro Phe 1 5 2335PRTArtificial SequenceAngiotensin II
derived peptide 233Ala His His Pro Phe 1 5
2345PRTArtificial SequenceAngiotensin II derived peptide 234Ala Asp Tyr
Pro Phe 1 5 2359PRTArtificial SequenceAngiotensin II
derived peptide 235Cys Asp Arg Val Tyr Ile His Pro Phe 1 5
2369PRTArtificial SequenceAngiotensin II derived peptide
236Cys Asp Ala Val Tyr Ile His Pro Phe 1 5
2379PRTArtificial SequenceAngiotensin II derived peptide 237Cys Asp Glu
Val Tyr Ile His Pro Phe 1 5
2389PRTArtificial SequenceAngiotensin II derived peptide 238Cys Asp Phe
Val Tyr Ile His Pro Phe 1 5
2399PRTArtificial SequenceAngiotensin II derived peptide 239Cys Asp His
Val Tyr Ile His Pro Phe 1 5
2409PRTArtificial SequenceAngiotensin II derived peptide 240Cys Asp Lys
Val Tyr Ile His Pro Phe 1 5
2419PRTArtificial SequenceAngiotensin II derived peptide 241Cys Asp Met
Val Tyr Ile His Pro Phe 1 5
2429PRTArtificial SequenceAngiotensin II derived peptide 242Cys Asp Val
Val Tyr Ile His Pro Phe 1 5
2439PRTArtificial SequenceAngiotensin II derived peptide 243Cys Asp Tyr
Val Tyr Ile His Pro Phe 1 5
2449PRTArtificial SequenceAngiotensin II derived peptide 244Cys Asp Pro
Val Tyr Ile His Pro Phe 1 5
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