ABSTRACT
Peptidomimitism is applied to the medicinal chemistry in order to synthesize drugs that devoid of the disadvantages of peptides. AT1 antagonists constitute a new generation of drugs for the treatment of hypertension designed and synthesized to mimic the C-terminal segment of Angiotensin II and to block its binding action on AT1 receptor. An effort was made to understand the molecular basis of hypertension by studying the conformational analysis of Ang II and its derivatives as well as the AT1 antagonists belonging to SARTANs class of molecules. Such studies offer the possibility to reveal the stereoelectronic factors responsible for bioactivity of AT1 antagonists and to design and synthesize new analogs. An example will be given which proves that drugs with better pharmacological and financial profiles may arise based on this rational design.
Subject(s)
Angiotensin II Type 1 Receptor Blockers , Angiotensin II/analogs & derivatives , Antihypertensive Agents/chemistry , Drug Design , 1-Sarcosine-8-Isoleucine Angiotensin II/analogs & derivatives , 1-Sarcosine-8-Isoleucine Angiotensin II/chemistry , Angiotensin II/chemistry , Angiotensin II/pharmacology , Antihypertensive Agents/chemical synthesis , Antihypertensive Agents/pharmacology , Humans , Hypertension/drug therapy , Losartan/analogs & derivatives , Losartan/chemistry , Magnetic Resonance Spectroscopy , Molecular Conformation , Molecular Mimicry , Peptides/chemistry , Peptides/pharmacology , Structure-Activity RelationshipABSTRACT
One of the major systems which interferes with the disease of hypertension, is the Renin Angiotensin Aldosterone System (RAS). The octapeptide hormone angiotensin II is the active product of RAS which causes vasoconstriction when binds to the AT(1) receptor. In the last years, there has been a development of drugs which block the Angiotensin II from binding the AT(1) receptor and are called AT(1) antagonists. In an effort to comprehend their stereoelectronic features, a study has been initiated to compare the conformational properties of drugs already marketed for the treatment of hypertension and others which are designed and synthesized in our laboratory possessing structural characteristics necessary for antihypertensive activity. In this study, two synthetic non-peptide AT(1) antagonists, are structurally elucidated and their conformational properties and bioactivity are compared to the prototype and first approved drug of this category in the market; losartan (trade name: COZAAR).
Subject(s)
Angiotensin II Type 1 Receptor Blockers , Angiotensin II/metabolism , Antihypertensive Agents/pharmacology , Benzyl Compounds/pharmacology , Losartan/pharmacology , Animals , Antihypertensive Agents/chemistry , Benzyl Compounds/chemistry , Blood Pressure/drug effects , Dose-Response Relationship, Drug , Losartan/analogs & derivatives , Losartan/chemistry , Magnetic Resonance Spectroscopy , Male , Models, Molecular , Molecular Conformation , Rabbits , Receptor, Angiotensin, Type 1/chemistryABSTRACT
The novel amide linked Angiotensin II (ANG II) cyclic analogue cyclo(3, 5) -[Sar(1)-Lys(3)-Glu(5)-Ile(8)] ANG II (18) has been designed, synthesized and bioassayed in anesthetized rabbits. The constrained cyclic analogue with a lactam amide bridge linking a Lys-Glu pair at positions 3 and 5 and possessing Ile at position 8, was synthesized by solution procedure using the maximum protection strategy. This analogue was found to be inhibitor of Angiotensin II. NMR spectroscopy coupled with computational analysis showed clustering between the side chains of the key aminoacids Tyr(4)-His(6)-Ile(8) similar to that observed with ANG II. The obtained data show that only pi*--pi* interactions observed in ANG II or its superagonist Sar(1) [ANG II] are missing. Therefore, it can be concluded that these interactions are essential for agonist activity. Conformational analysis comparisons between AT(1) antagonists losartan, eprosartan and irbesartan with C-terminal segment of cyclic compound 18 revealed structural similarities.
Subject(s)
Angiotensin II/antagonists & inhibitors , Angiotensin II/chemistry , Angiotensin II/pharmacology , Peptides, Cyclic/chemistry , Peptides, Cyclic/pharmacology , Thiophenes , Acrylates/chemistry , Acrylates/pharmacology , Angiotensin II/analogs & derivatives , Angiotensin II/chemical synthesis , Animals , Antihypertensive Agents/chemistry , Antihypertensive Agents/pharmacology , Biochemistry/methods , Biphenyl Compounds/chemistry , Biphenyl Compounds/pharmacology , Drug Design , Imidazoles/chemistry , Imidazoles/pharmacology , Irbesartan , Losartan/chemistry , Losartan/pharmacology , Magnetic Resonance Spectroscopy , Male , Models, Molecular , Peptides, Cyclic/chemical synthesis , Rabbits , Structure-Activity Relationship , Tetrazoles/chemistry , Tetrazoles/pharmacologyABSTRACT
The novel amide linked Angiotensin II potent cyclic analogue, c-[Sar1,Lys3,Glu5] ANG II 19 has been designed and synthesized in an attempt to test the aromatic ring clustering and the charge relay bioactive conformation we have recently suggested for ANG II. This constrained cyclic analogue was synthesized by connecting the Lys3 amino and Glu5 carboxyl side chain groups, and it was found to be potent in the rat uterus assay and in anesthetized rabbits. The central part of the molecule is fixed covalently in the conformation predicted according to the backbone bend conformational model proposed for Angiotensin II. The obtained results using a combination of 2D NMR, 1D NOE spectroscopy and molecular modeling revealed a similar Tyr4-Ile5-His6 bend, a His6-Pro7 trans configuration and a side chain aromatic ring cluster of the key aminoacids Tyr4, His6, Phe8 for c-[Sar1,Lys3,Glu5] ANG II as it has been found for ANG II (Matsoukas, J. H.; Hondrelis, J.; Keramida, M.; Mavromoustakos, T.; Markriyannis, A.; Yamdagni, R.; Wu, Q.; Moore, G. J. J. Biol. Chem. 1994, 269, 5303). Previous study of the conformational properties of the Angiotensin II type I antagonist [Hser(gamma-OMe)8] ANG II (Matsoukas, J. M.; Agelis, G.; Wahhab, A.; Hondrelis, J.; Panagiotopoulos. D.; Yamdagni, R.; Wu, Q.; Mavromoustakos, T.; Maia, H.; Ganter, R.; Moore, G. J. J. Med. Chem. 1995, 38, 4660) using 1-D NOE spectroscopy coupled with the present study of the same type of lead antagonist Sarilesin revealed that the Tyr4-Ile5-His6 bend, a conformational property found in Angiotensin II is not present in type I antagonists. The obtained results provide an important conformational difference between Angiotensin II agonists and type I antagonists. It appears that our synthetic attempt to further support our proposed model was successful and points out that the charge relay system and aromatic ring cluster are essential stereoelectronic features for Angiotensin II to exert its biological activity.
Subject(s)
Angiotensin II/chemical synthesis , Peptides, Cyclic/chemistry , Receptors, Angiotensin/chemistry , Angiotensin II/chemistry , Angiotensin II/pharmacology , Animals , Female , Nuclear Magnetic Resonance, Biomolecular , Peptides, Cyclic/pharmacology , Protein Conformation , Rats , Receptors, Angiotensin/metabolism , Uterus/drug effectsABSTRACT
Analogues of sarilesin (type I AT1 antagonists), and sarmesin (type II AT1 antagonists) with homoserine (hSer) at position 8 were prepared and bioassayed. The presence of a Tyr4-Ile5-His6 bend found in sarmesin but not in sarilesin was identified. The obtained results coupled with conformational analysis studies, using a combination of NMR spectroscopy and computational chemistry, propose important conformational and stereoelectronic properties for agonist and antagonist activity at AT1 receptors.
Subject(s)
Angiotensin II/analogs & derivatives , Angiotensin II/metabolism , Angiotensin I/metabolism , Angiotensin Receptor Antagonists , Angiotensin II/chemical synthesis , Angiotensin II/chemistry , Angiotensin II/pharmacology , Animals , Drug Design , Female , Magnetic Resonance Spectroscopy , Models, Molecular , Rats , Receptors, Angiotensin/metabolism , Structure-Activity Relationship , Uterus/drug effectsABSTRACT
Losartan is the first recently approved drug against hypertension disease that competes with the biological action of angiotensin II (AII) at the AT1 receptor. Its design was based on the mimicry of the C-terminal segment of AII. Due to the biological significance of Losartan, its structure elucidation and conformational properties are reported as determined by NMR spectroscopy and computational analysis. In addition, molecular modeling of the peptide Sarmesin [Sar1Tyr(OMe)4AII], a competitive antagonist of AII, was also developed based on NMR and computational analysis data. Sarmesin's C-terminal was used as a template for superimposition with specific molecular features of interest in the structure of Losartan such as the conformation of biphenyltetrazole, the n-butyl chain, and the orientation of hydroxymethylimidazole relative to the biphenyl template. The major conclusions derived from this study are the following: (a) Sarmesin, like the AII superagonist [Sar1]AII, adopts a conformation which keeps in close proximity the key amino acids Sar1 (or Arg2)-Tyr(OMe)4-His6-Phe8. (b) Losartan favors a low-energy conformation in which imidazole and tetrazole rings are placed in the opposite site relative to the spacer phenyl ring plane; the hydroxymethyl group is placed away from the spacer phenyl ring, the alkyl chain is oriented above the spacer phenyl ring, and the two phenyl rings deviate approximately 60 degrees from being coplanar. (c) Overlay of the C-terminal region of Sarmesin with Losartan using equivalent groups revealed an excellent match. (d) Interestingly, the matching between enantiomeric structures of Losartan was not equivalent, proposing that the chirality of this molecule is significant in order to exert its biological activity. These findings open a new avenue for synthetic chemists to design and synthesize peptidomimetic drugs based on the C-terminal segment of the proposed model of Sarmesin. The new candidate drug molecules are not restricted to structurally resemble Losartan as the design is hitherto focused.
Subject(s)
Angiotensin II/analogs & derivatives , Antihypertensive Agents/chemistry , Hypertension/etiology , Losartan/chemistry , Angiotensin II/antagonists & inhibitors , Angiotensin II/chemistry , Angiotensin Receptor Antagonists , Magnetic Resonance Spectroscopy , Models, Molecular , Molecular Conformation , Monte Carlo Method , Protein ConformationABSTRACT
Experimental allergic encephalomyelitis (EAE) is induced in susceptible animals by immunodominant determinants of myelin basic protein (MBP). Analogs of these disease-associated peptides have been identified with disease progression upon coimmunization. Usage of peptides, with disease-specific immunomodulatory capacity in vivo is limited, however, due to their sensitivity to proteolytic enzymes. Alternative approaches include the development of mimetic molecules which maintain the biological function of an original peptide, yet are stable and able to elicit their response in pharmacological quantities. A novel technique was employed to design a series of semi-mimetic peptides, based on the guinea pig MBP72-85 peptide used to induce EAE in Lewis rats. We used isonipecotic (iNip) and aminocaproic (Acp) acids as templates. Acp-MBP72-85 peptide derived analogues were effective in inducing EAE compared to iNip-peptide analogues which were ineffective at 350 micrograms. These findings suggest that the design and synthesis of semi-mimetic peptide molecules with immunomodulatory potential is possible and that eventually these molecules may form the basis for the development of novel and more effective disease-specific therapeutic agents.
Subject(s)
Aminocaproates/chemistry , Isonipecotic Acids/chemistry , Molecular Mimicry , Myelin Basic Protein/chemistry , Peptides/chemical synthesis , Amino Acid Sequence , Animals , Drug Design , Encephalomyelitis, Autoimmune, Experimental/chemically induced , Encephalomyelitis, Autoimmune, Experimental/metabolism , Female , Guinea Pigs , Models, Chemical , Molecular Sequence Data , Protein Conformation , Rats , Rats, Inbred Lew , Templates, GeneticABSTRACT
Thrombin, the most potent physiological platelet agonist interacts with cells through a specific G protein-coupled receptor which has been cloned and sequenced. Synthetic thrombin receptor peptides (TRAPs) comprising the first 5 amino acids (SFLLR and SFLLR-NH2) of the new N-terminus tethered ligand of the thrombin receptor that is generated by thrombin's proteolytic activity were found to cause full platelet aggregation. During the screening of novel thrombin receptor derived non-peptide mimetics in the platelet aggregation assay we found that 1-phenylacetyl-4-(6-guanidohexanoyl)-piperazine (1) and 1-(6-guanidohexanoyl)-4-(phenylacetylamidomethyl)-piperidine (2) exerted in vitro antagonist activities (56% and 40% correspondingly) as it is depicted by the platelet aggregation assay. Using Molecular Modeling, the synthetic compounds were overlayed with SFFLR. All three superimposed low energy structures had Phe and Arg amino acids in spatial close proximity. The superimposition results revealed that 1 resembled more the stereoelectronic environment of SFLLR than 2. This difference may be related to their different antagonist efficacy.
