Your search keyword '"Jeff Soderquist"' showing total 3 results

1. New inhibitors of human renin that contain novel Leu-Val replacements

Author

Jay R. Luly, Jeff Soderquist, Thomas J. Perun, Herman H. Stein, Jacob J. Plattner, Nwe Yi, and Jerome Cohen

Subjects

Dipeptide, biology, Stereochemistry, Angiotensinogen, Epoxide, Stereoisomerism, Valine, chemistry.chemical_compound, Scissile bond, chemistry, Nucleophile, Leucine, Enzyme inhibitor, Renin, Drug Discovery, biology.protein, Side chain, Humans, Molecular Medicine, Amino Acid Sequence, Enzyme Inhibitors, Isopropyl, Histidine

Abstract

Stereoselective syntheses of several nonpeptide fragments that function as Leu10-Val11 scissile bond replacements in human angiotensinogen are presented. The opening of N-protected aminoalkyl epoxide 3 with a variety of sulfur, oxygen, nitrogen, and carbon nucleophiles is a key reaction in the preparation of these novel fragments 4-8. The coupling of these fragments to protected dipeptides that mimic positions 8 and 9 in angiotensinogen produces inhibitors of human renin even though the molecules contain no functionality beyond what is formally the Val11 side chain of angiotensinogen. R groups that closely resemble that of the Val side chain are preferable; thus, isopropyl greater than or equal to higher alkyl greater than phenyl greater than substituted phenyl. Sulfur is the best X group; oxidation leads to slight (X = SO2) and significant (X = SO) decreases in inhibitory potency. One such inhibitor, 60, has an IC50 of 13 nM when tested with purified human renin at pH 6.0. The significant activity of these small inhibitors is thought to be due in part to the hydroxyl group of the fragment functioning as a transition-state analogue. Of these, the inhibitors that contain histidine show marked selectivity toward renin over a related aspartic proteinase, pepsin.

Published

1987

2. New inhibitors of human renin that contain novel Leu-Val replacements. Examination of the P1 site

Author

Jerome Cohen, Jonathan Greer, Thomas J. Perun, Herman H. Stein, Giorgio Bolis, Joseph F. Dellaria, Jeff Soderquist, Nwe Y. Bamaung, Jacob J. Plattner, and Jay R. Luly

Subjects

Models, Molecular, Molecular model, Stereochemistry, Angiotensinogen, Structure-Activity Relationship, Scissile bond, chemistry.chemical_compound, Leucine, Renin, Drug Discovery, Humans, Amino Acid Sequence, Alanine, chemistry.chemical_classification, Binding Sites, Dipeptide, biology, Chemistry, Valine, Hydrogen-Ion Concentration, Amino acid, Enzyme inhibitor, Lipophilicity, biology.protein, Molecular Medicine, Isopropyl

Abstract

Stereoselective syntheses of several nonpeptide sulfidoethanol fragments that function as Leu10-Val11 (P1-P1') scissile bond replacements in human angiotensinogen are presented. These fragments are prepared from a variety of amino acids with formal P1 side chains varying in size and lipophilicity by converting them to their corresponding N-protected aminoalkyl epoxide 5 followed by ring opening with isopropyl mercaptan. The coupling of these fragments to either Boc-Phe-Ala-OH or Boc-Phe-His-OH produces inhibitors of human renin, 6 and 7, respectively, which are compared to a series of dipeptide-aldehyde inhibitors, 4, by molecular modeling and biochemical methods. Qualitatively, histidine-containing (P2) inhibitors 7 possess greater inhibitory potency than their corresponding alanine (P2) analogues 6, which are more potent than the corresponding aldehydic inhibitors from series 4. Within a given series, inhibitors with the cyclohexylmethyl P1 side chain are more potent than the benzyl analogues, which in turn are more potent than cyclohexyl or isobutyl derivatives. Inhibitors with parger P1 side chains (e.g. adamantylmethyl and benzhydryl) are much less active. The inhibitory potency of these compounds against human renin is discussed in terms of specific interactions with the enzyme.

Published

1988

3. Renin inhibitors. Dipeptide analogues of angiotensinogen utilizing a dihydroxyethylene transition-state mimic at the scissile bond to impart greater inhibitory potency

Author

Herman H. Stein, I Merits, Luly, Barbara A. Bopp, Hollis D. Kleinert, Anthony K. L. Fung, Jeff Soderquist, Nwe Y. Bamaung, David A. Egan, and P. A. Marcotte

Subjects

Models, Molecular, Chemical Phenomena, Stereochemistry, Metabolic Clearance Rate, Diol, Angiotensinogen, Blood Pressure, chemistry.chemical_compound, Scissile bond, Structure-Activity Relationship, Dogs, Drug Discovery, Renin–angiotensin system, Renin, Animals, chemistry.chemical_classification, Dipeptide, Binding Sites, biology, Biological activity, Hydrogen Bonding, Stereoisomerism, Dipeptides, Haplorhini, Gastricsin, Rats, Chemistry, Enzyme, Biochemistry, chemistry, Enzyme inhibitor, biology.protein, Molecular Medicine, Ethylene Glycols

Abstract

The synthesis of diol-containing renin inhibitors has revealed that a simple vicinal diol functionality corresponding to the scissile Leu-Val bond in human angiotensinogen is capable of imparting inhibitory activity at a comparable or higher level than either the corresponding aldehyde or hydroxymethyl functionality (compare inhibitors 2a-c or 3a-c). This finding has led to the further optimization of a series of small transition-state analogue inhibitors by the inclusion of a second hydroxyl group in the Leu-Val surrogate to give compounds that inhibited human renin in the 200-700-pM range (e.g. 43, 45, 63, 66). The magnitude of effect of the second hydroxyl group on potency is not only dictated by the absolute stereochemistry of the diol but also by the side chain of the P1 residue. Molecular modeling of the diol-containing inhibitors suggests that one of the hydroxyl groups hydrogen bonds to Asp 32 and Asp 215, while the second hydrogen bonds to Asp 215. These diol inhibitors are extremely selective for human renin over the related enzymes cathepsin D, pepsin, and gastricsin. At high concentrations, compounds containing a leucine or phenylalanine rather than a histidine at the P2 position gave only minor amounts of inhibition of the other enzymes. Inhibitor 43 suppressed plasma renin activity completely and lowered mean blood pressure in monkeys after both intravenous and intraduodenal administration, but the blood pressure drop lasted less than 1 h. Monitoring the blood levels of 43 by enzyme inhibition assay after intraduodenal administration to monkeys or oral administration to rats revealed low absorption and rapid clearance. While intratracheal administration to dogs gave approximately 50% bioavailability, rapid clearance was still a problem. After examination of inhibitor 45 in a sensitive primate model in which monkeys were rendered both hypertensive and hyperreninemic, the effects on lowering systolic but not diastolic pressure were apparent even after 22 h postdosing. Details on the synthesis, in vitro structure-activity relationships, molecular modeling, in vivo activity, and metabolism of these inhibitors are described.

Published

1988