Your search keyword '"Kiso Y"' showing total 41 results

1. Novel β-amyloid aggregation inhibitors possessing a turn mimic.

Author

Hamada Y, Miyamoto N, and Kiso Y

Subjects

Peptides chemical synthesis, Peptides chemistry, Amyloid beta-Peptides chemistry, Amyloid beta-Peptides metabolism, Peptides pharmacology, Protein Aggregation, Pathological drug therapy

Abstract

Amyloid β peptide, the main component of senile plaques found in the brain of Alzheimer disease (AD) patients, is a molecular target for AD therapeutic intervention. A number of potential AD therapeutics have been reported, including inhibitors of β-secretase, γ-secretase, and Aβ aggregation, and anti-amyloid agents, such as neprilysin, insulin degrading enzyme (IDE), and Aβ antibodies. Recently, we reported potent small-sized β-secretase (BACE1) inhibitors, which could serve as anti-AD drugs. However AD is a progressive disorder, where dementia symptoms gradually worsen over several decades, and therefore may require many years to get cured. One possible way to achieve a greater therapeutic effect is through simultaneous administration of multiple drugs, similar to those used in Highly Active Anti-Retroviral Therapy (HAART) used to treat AIDS. In order to overcome AD, we took a drug discovery approach to evaluate, novel β-amyloid aggregation inhibitors. Previously, we reported that a tong-type compound possessing a turn mimic as the inhibitor of HIV-1 protease dimerization. Oligomerized amyloid β peptides contain a turn structure within the molecule. Here, we designed and synthesized novel β-amyloid aggregation inhibitors with a turn-mimic template, based on the turn conformer of the oligomerized amyloid β peptides., (Copyright © 2015 Elsevier Ltd. All rights reserved.)

Published

2015

2. Non-pretreated O-acyl isopeptide of amyloid β peptide 1-42 is monomeric with a random coil structure but starts to aggregate in a concentration-dependent manner.

Author

Yoshiya T, Maruno T, Uemura T, Kubo S, Kiso Y, Sohma Y, Yoshizawa-Kumagaye K, Kobayashi Y, and Nishiuchi Y

Subjects

Protein Conformation, Amyloid beta-Peptides chemistry, Peptide Fragments chemistry

Abstract

An isopeptide of amyloid β peptide 1-42 (isoAβ42) was considered as a non-aggregative precursor molecule for the highly aggregative Aβ42. It has been applied to biological studies after several pretreatments. Here we report that isoAβ42 is monomeric with a random coil structure at 40 μM without any pretreatment. But we also found that isoAβ42 retains a slight aggregative nature, which is significantly weaker than that of the native Aβ42., (Copyright © 2014 The Authors. Published by Elsevier Ltd.. All rights reserved.)

Published

2014

3. Optimization of plasmepsin inhibitor by focusing on similar structural feature with chloroquine to avoid drug-resistant mechanism of Plasmodium falciparum.

Author

Miura T, Hidaka K, Azai Y, Kashimoto K, Kawasaki Y, Chen SE, de Freitas RF, Freire E, and Kiso Y

Subjects

Antimalarials chemical synthesis, Antimalarials chemistry, Aspartic Acid Endopeptidases metabolism, Chloroquine chemistry, Dose-Response Relationship, Drug, Molecular Structure, Parasitic Sensitivity Tests, Protease Inhibitors chemical synthesis, Protease Inhibitors chemistry, Structure-Activity Relationship, Antimalarials pharmacology, Aspartic Acid Endopeptidases antagonists & inhibitors, Chloroquine pharmacology, Drug Resistance, Multiple drug effects, Plasmodium falciparum drug effects, Protease Inhibitors pharmacology

Abstract

The plasmepsins are specific aspartic proteases of the malaria parasite and a potential target for developing new antimalarial agents. Our previously reported peptidomimetic plasmepsin inhibitor with modified 2-aminoethylamino substituent, KNI-10740, was tested against chloroquine sensitive Plasmodium falciparum, D6, to be highly potent, however, the inhibitor exhibited about 5 times less activity against multi-drug resistant parasite (TM91C235). We hypothesized the potency reduction resulted from structural similarity between 2-aminoethylamino substituent of KNI-10740 and chloroquine. Then, we modified the moiety and finally identified compound 15d (KNI-10823), that could avoid drug-resistant mechanism of TM91C235 strain., (Copyright © 2014 Elsevier Ltd. All rights reserved.)

Published

2014

4. Structure-activity relationship study of BACE1 inhibitors possessing a chelidonic or 2,6-pyridinedicarboxylic scaffold at the P(2) position.

Author

Hamada Y, Suzuki K, Nakanishi T, Sarma D, Ohta H, Yamaguchi R, Yamasaki M, Hidaka K, Ishiura S, and Kiso Y

Subjects

Amyloid Precursor Protein Secretases metabolism, Aspartic Acid Endopeptidases metabolism, Binding Sites physiology, Enzyme Inhibitors chemistry, Enzyme Inhibitors metabolism, Enzyme Inhibitors pharmacology, HEK293 Cells, Humans, Picolinic Acids, Protein Structure, Secondary, Protein Structure, Tertiary, Pyrans metabolism, Pyrans pharmacology, Pyridines metabolism, Pyridines pharmacology, Structure-Activity Relationship, Amyloid Precursor Protein Secretases antagonists & inhibitors, Aspartic Acid Endopeptidases antagonists & inhibitors, Pyrans chemistry, Pyridines chemistry

Abstract

We have previously reported potent substrate-based pentapeptidic BACE1 inhibitors possessing a hydroxymethylcarbonyl isostere as a substrate transition-state mimic. While these inhibitors exhibited potent activities in enzymatic and cellular assays (KMI-429 in particular inhibited Aβ production in vivo), these inhibitors contained some natural amino acids that seemed to be required to improve enzymatic stability in vivo and permeability across the blood-brain barrier, so as to be practical drug. Recently, we synthesized non-peptidic and small-sized BACE1 inhibitors possessing a heterocyclic scaffold at the P2 position. Herein we report the SAR study of BACE1 inhibitors possessing this heterocyclic scaffold, a chelidonic or 2,6-pyridinedicarboxylic moiety., (Copyright © 2013 Elsevier Ltd. All rights reserved.)

Published

2014

5. Comparative properties of Aβ1-42, Aβ11-42, and [Pyr¹¹]Aβ11-42 generated from O-acyl isopeptides.

Author

Sohma Y, Yamasaki M, Kawashima H, Taniguchi A, Yamashita M, Akaji K, Mukai H, and Kiso Y

Subjects

Circular Dichroism, Humans, Peptide Fragments chemical synthesis, Protein Structure, Secondary, Alzheimer Disease metabolism, Amyloid beta-Peptides chemistry, Peptide Fragments chemistry

Abstract

The use of water-soluble O-acyl isopeptides enabled us to investigate the biochemical properties of Aβ11-42 species, by preparing highly concentrated stock solutions after a pretreatment. Aβ11-42 and [Pyr(11)]Aβ11-42 showed comparable aggregation capability and cytotoxicity, suggesting that the pyroglutamate modification at Glu(11) does not have a crucial role in these events. However, given that Aβ11-42 is converted to [Pyr(11)]Aβ11-42 by a glutamyl cyclase in vivo, the potential aggregative and cytotoxic nature of [Pyr(11)]Aβ11-42 that was observed in the present study provides valuable insights into the pathological functions of pyroglutamate-modified Aβ species in Alzheimer's disease., (Copyright © 2012 Elsevier Ltd. All rights reserved.)

Published

2013

6. Novel BACE1 inhibitors possessing a 5-nitroisophthalic scaffold at the P2 position.

Author

Hamada Y, Nakanishi T, Suzuki K, Yamaguchi R, Hamada T, Hidaka K, Ishiura S, and Kiso Y

Subjects

Models, Molecular, Molecular Structure, Nitro Compounds pharmacology, Peptide Hydrolases pharmacology, Phthalic Acids pharmacology, Structure-Activity Relationship, Amyloid Precursor Protein Secretases antagonists & inhibitors, Aspartic Acid Endopeptidases antagonists & inhibitors, Nitro Compounds chemistry, Peptide Hydrolases chemical synthesis, Phthalic Acids chemistry

Abstract

Recently, we reported substrate-based pentapeptidic BACE1 inhibitors possessing a hydroxymethylcarbonyl isostere as a substrate transition-state mimic. These inhibitors showed potent inhibitory activities in enzymatic and cell assays. We also designed and synthesized non-peptidic and small-sized inhibitors possessing a heterocyclic scaffold at the P(2) position. By studying the structure-activity relationship of these inhibitors, we found that the σ-π interaction of an inhibitor with the BACE1-Arg235 side chain played a key role in the inhibition mechanism. Hence, we optimized the inhibitors with a focus on their P(2) regions. In this Letter, a series of novel BACE1 inhibitors possessing a 5-nitroisophthalic scaffold at the P(2) position are described along with the results of the related structure-activity relationship study. These small-sized inhibitors are expected improved membrane permeability and bioavailability., (Copyright © 2012 Elsevier Ltd. All rights reserved.)

Published

2012

7. Tripeptidic BACE1 inhibitors devised by in-silico conformational structure-based design.

Author

Hamada Y, Tagad HD, Nishimura Y, Ishiura S, and Kiso Y

Subjects

Amyloid Precursor Protein Secretases metabolism, Aspartic Acid Endopeptidases metabolism, Dose-Response Relationship, Drug, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors chemistry, Humans, Models, Molecular, Molecular Structure, Oligopeptides chemical synthesis, Oligopeptides chemistry, Recombinant Proteins antagonists & inhibitors, Recombinant Proteins metabolism, Stereoisomerism, Structure-Activity Relationship, Amyloid Precursor Protein Secretases antagonists & inhibitors, Aspartic Acid Endopeptidases antagonists & inhibitors, Drug Design, Enzyme Inhibitors pharmacology, Oligopeptides pharmacology

Abstract

Previously reported pentapeptidic BACE1 inhibitors, designed using a substrate-based approach, were used as lead compounds for the further design of non-peptidic BACE1 inhibitors. Although these peptidic and non-peptidic inhibitors, with a hydroxymethylcarbonyl isostere as a substrate transition-state mimic, exhibited potent BACE1 inhibitory activities, their molecular-sizes appeared a little too big (molecular weight of >600daltons) for developing practical anti-Alzheimer's disease drugs. To develop lower weight BACE1 inhibitors, a series of tripeptidic BACE1 inhibitors were devised using a design approach based on the conformation of a virtual inhibitor bound to the BACE1 active site, also called 'in-silico conformational structure-based design'. Although these tripeptidic BACE1 inhibitors contained some natural amino acid residues, they are expected to be useful as lead compounds for developing the next generation BACE1 inhibitors, due to their low molecular size and unique structural features compared with previously reported inhibitors., (Copyright © 2011 Elsevier Ltd. All rights reserved.)

Published

2012

8. Design and synthesis of several small-size HTLV-I protease inhibitors with different hydrophilicity profiles.

Author

Nguyen JT, Kato K, Hidaka K, Kumada HO, Kimura T, and Kiso Y

Subjects

Binding Sites, Catalytic Domain, Computer-Aided Design, Crystallography, X-Ray, Drug Design, HIV Protease chemistry, HIV Protease metabolism, Humans, Hydrogen Bonding, Hydrophobic and Hydrophilic Interactions, Peptide Hydrolases metabolism, Peptides chemical synthesis, Peptides chemistry, Peptides pharmacology, Protease Inhibitors chemistry, Protease Inhibitors pharmacology, Structure-Activity Relationship, Human T-lymphotropic virus 1 enzymology, Peptide Hydrolases chemistry, Protease Inhibitors chemical synthesis

Abstract

The human T cell leukemia/lymphotropic virus type 1 (HTLV-I) is clinically associated with adult T cell leukemia/lymphoma, HTLV-I associated myelopathy/tropical spastic paraparesis, and a number of other chronic inflammatory diseases. To stop the replication of the virus, we developed highly potent tetrapeptidic HTLV-I protease inhibitors. In a recent X-ray crystallography study, several of our inhibitors could not form co-crystal complexes with the protease due to their high hydrophobicity. In the current study, we designed, synthesized and evaluated the HTLV-I protease inhibition potency of compounds with hydrophilic end-capping moieties with the aim of improving pharmaceutic and pharmacokinetic properties., (Copyright © 2011 Elsevier Ltd. All rights reserved.)

Published

2011

9. Maintaining potent HTLV-I protease inhibition without the P3-cap moiety in small tetrapeptidic inhibitors.

Author

Nguyen JT, Kato K, Kumada HO, Hidaka K, Kimura T, and Kiso Y

Subjects

Crystallography, X-Ray, Models, Molecular, Human T-lymphotropic virus 1 enzymology, Oligopeptides pharmacology, Protease Inhibitors pharmacology

Abstract

The human T cell lymphotropic/leukemia virus type 1 (HTLV-I) causes adult T cell lymphoma/leukemia. The virus is also responsible for chronic progressive myelopathy and several inflammatory diseases. To stop the manufacturing of new viral components, in our previous reports, we derived small tetrapeptidic HTLV-I protease inhibitors with an important amide-capping moiety at the P(3) residue. In the current study, we removed the P(3)-cap moiety and, with great difficulty, optimized the P(3) residue for HTLV-I protease inhibition potency. We discovered a very potent and small tetrapeptidic HTLV-I protease inhibitor (KNI-10774a, IC(50)=13 nM)., (Copyright © 2011 Elsevier Ltd. All rights reserved.)

Published

2011

10. Improvement of both plasmepsin inhibitory activity and antimalarial activity by 2-aminoethylamino substitution.

Author

Miura T, Hidaka K, Uemura T, Kashimoto K, Hori Y, Kawasaki Y, Ruben AJ, Freire E, Kimura T, and Kiso Y

Subjects

Antimalarials pharmacology, Aspartic Acid Endopeptidases metabolism, Binding Sites, Computer Simulation, Ethylenediamines chemical synthesis, Ethylenediamines pharmacology, Phenylbutyrates chemistry, Protease Inhibitors pharmacology, Protozoan Proteins metabolism, Structure-Activity Relationship, Thiazoles chemical synthesis, Thiazoles pharmacology, Antimalarials chemistry, Aspartic Acid Endopeptidases antagonists & inhibitors, Ethylenediamines chemistry, Protease Inhibitors chemistry, Protozoan Proteins antagonists & inhibitors, Thiazoles chemistry

Abstract

We attached 2-aminoethylamino groups to allophenylnorstatine-containing plasmepsin (Plm) inhibitors and investigated SAR of the methyl or ethyl substitutions on the amino groups. Unexpectedly, compounds 22 (KNI-10743) and 25 (KNI-10742) exhibited extremely potent Plm II inhibitory activities (K(i)<0.1 nM). Moreover, among our peptidomimetic Plm inhibitors, we identified the compounds with the highest antimalarial activity using a SYBR Green I-based fluorescence assay., (2010 Elsevier Ltd. All rights reserved.)

Published

2010

11. Inhibitory effect of a dimerization-arm-mimetic peptide on EGF receptor activation.

Author

Mizuguchi T, Uchimura H, Kakizawa T, Kimura T, Yokoyama S, Kiso Y, and Saito K

Subjects

Cell Line, Tumor, Drug Design, ErbB Receptors antagonists & inhibitors, Humans, Molecular Mimicry, Peptides, Cyclic chemistry, Peptides, Cyclic pharmacology, Protein Multimerization drug effects, Structure-Activity Relationship, ErbB Receptors chemistry, Peptides, Cyclic chemical synthesis

Abstract

A cyclic decapeptide was chemically synthesized that mimics the loop structure of a beta-hairpin arm of the EGF receptor, which is highly involved in receptor dimerization upon activation by ligand binding. This peptide was revealed to reduce dimer formation of the receptor in a detergent-solubilized extract of epidermoid carcinoma A431 cells and to inhibit receptor autophosphorylation at less than 10 microM in the intact cells.

Published

2009

12. Subchronic (13-week) oral toxicity study of dihomo-gamma-linolenic acid (DGLA) oil in rats.

Author

Kawashima H, Toyoda-Ono Y, Suwa Y, and Kiso Y

Subjects

Animals, Blood Cell Count, Blood Chemical Analysis, Body Weight drug effects, Eating drug effects, Eye Diseases chemically induced, Eye Diseases pathology, Female, Male, Mortierella chemistry, Mutagenicity Tests, Organ Size drug effects, Rats, Rats, Sprague-Dawley, Urinalysis, 8,11,14-Eicosatrienoic Acid toxicity

Abstract

Dihomo-gamma-linolenic acid (DGLA) is one of the essential fatty acids, and has anti-inflammatory and anti-allergic effects. To assess the toxicity of a novel DGLA oil produced by the fungus Mortierella alpina, we examined it in the Ames test and in acute and subchronic oral toxicity tests in rats. In the Ames test, no mutagenicity was found up to 5000 microg/plate. The acute toxicity test revealed no toxicity related to DGLA oil at 10 g/kg. In the subchronic toxicity test, DGLA oil (500, 1000, and 2000 mg/kg) was orally administered. Water and soybean oil (2000 mg/kg) were used for the no-oil control and soybean oil control groups, respectively. There was no death in either sex. Because of administration of large amounts of oil, food consumption was low in the soybean oil control and the three test groups, which appeared to mildly decrease urinary excretion of Na, K, and Cl, as well as total serum protein, albumin, and blood urea nitrogen levels. There were no toxicological changes in body weight, food consumption, ophthalmological examination, urinalysis, hematological examination, blood biochemical examination, necropsy, organ weight, or histopathological examination. These findings show that the no-observed-adverse-effect level of the DGLA oil was 2000 mg/kg.

Published

2009

13. New developments for the design, synthesis and biological evaluation of potent SARS-CoV 3CL(pro) inhibitors.

Author

Regnier T, Sarma D, Hidaka K, Bacha U, Freire E, Hayashi Y, and Kiso Y

Subjects

Amino Acid Sequence, Antiviral Agents chemistry, Antiviral Agents pharmacology, Benzothiazoles chemical synthesis, Benzothiazoles chemistry, Benzothiazoles pharmacology, Chymases antagonists & inhibitors, Chymases metabolism, Computer Simulation, Coronavirus 3C Proteases, Cysteine Endopeptidases metabolism, Drug Design, Ketones chemical synthesis, Ketones chemistry, Peptides chemical synthesis, Peptides chemistry, Peptides pharmacology, Protease Inhibitors chemistry, Protease Inhibitors pharmacology, Pyrrolidinones chemical synthesis, Pyrrolidinones chemistry, Pyrrolidinones pharmacology, Structure-Activity Relationship, Thiazoles chemical synthesis, Thiazoles chemistry, Thiazoles pharmacology, Viral Proteins metabolism, Antiviral Agents chemical synthesis, Protease Inhibitors chemical synthesis, Severe acute respiratory syndrome-related coronavirus, Viral Proteins antagonists & inhibitors

Abstract

A series of trifluoromethyl, benzothiazolyl or thiazolyl ketone-containing peptidic compounds as SARS-CoV 3CL protease inhibitors were developed and their potency was evaluated by in vitro protease inhibitory assays. Three candidates had encouraging results for the development of new anti-SARS compounds.

Published

2009

14. Significance of interactions of BACE1-Arg235 with its ligands and design of BACE1 inhibitors with P2 pyridine scaffold.

Author

Hamada Y, Ohta H, Miyamoto N, Sarma D, Hamada T, Nakanishi T, Yamasaki M, Yamani A, Ishiura S, and Kiso Y

Subjects

Blood-Brain Barrier drug effects, Drug Design, Humans, Inhibitory Concentration 50, Ligands, Models, Chemical, Molecular Conformation, Permeability, Protein Binding, Pyridines chemistry, Amyloid Precursor Protein Secretases antagonists & inhibitors, Amyloid Precursor Protein Secretases chemistry, Arginine chemistry, Aspartic Acid Endopeptidases antagonists & inhibitors, Aspartic Acid Endopeptidases chemistry, Chemistry, Pharmaceutical methods, Pyridines antagonists & inhibitors

Abstract

Recently, we reported potent substrate-based pentapeptidic BACE1 inhibitors possessing a hydroxymethylcarbonyl isostere as a substrate transition-state mimic. Because these inhibitors contained some natural amino acids, we would need to improve their enzymatic stability in vivo and permeability across the blood-brain barrier, so that they become practically useful. Subsequently, non-peptidic and small-sized BACE1 inhibitors possessing a heterocyclic scaffold, 2,6-pyridenedicarboxylic, chelidamic or chelidonic moiety, at the P(2) position were reported. These inhibitors were designed based on the conformer of docked inhibitor in BACE1. In this study, we discuss the role and significance of interactions between Arg235 of BACE1 and its inhibitor in BACE1 inhibitory mechanism. Moreover, we designed more potent small-sized BACE1 inhibitors with a 2,6-pyridinedicarboxylic scaffold at the P(2) position, that were optimized for the interactions with Arg235 of BACE1.

Published

2009

15. Inhibitory effect of carnosine on interleukin-8 production in intestinal epithelial cells through translational regulation.

Author

Son DO, Satsu H, Kiso Y, Totsuka M, and Shimizu M

Subjects

Caco-2 Cells, Humans, Hydrogen Peroxide metabolism, Interleukin-8 biosynthesis, Interleukin-8 genetics, Interleukin-8 metabolism, Intestinal Mucosa cytology, Carnosine physiology, Epithelial Cells metabolism, Gene Expression Regulation physiology, Interleukin-8 antagonists & inhibitors, Intestinal Mucosa metabolism

Abstract

The enhanced intestinal production of pro-inflammatory cytokines leads to inflammation and carcinogenesis, and therefore its down-regulation by nutrients could represent a promising therapeutic approach. We found for the first time that the secretion of interleukin-8 (IL-8) in intestinal epithelial cells stimulated by hydrogen peroxide or TNF-alpha was suppressed in the presence of carnosine (beta-Ala-His), a dietary dipeptide. Interestingly, carnosine had no influence on the stimulus-induced IL-8 mRNA expression, although the intracellular production and secretion of IL-8 were significantly inhibited by carnosine. The inhibitory effect of carnosine on the IL-8 secretion differed from that of other histidine-containing dipeptides like Gly-His, Ala-His, and anserine (beta-Ala-1-methyl-His), which inhibited both the hydrogen peroxide-induced secretion and mRNA expression of IL-8. These observations indicate that carnosine inhibited IL-8 secretion along a unique pathway, in which IL-8 production was suppressed at a post-transcriptional level, for instance, translation. The hypothesis that carnosine inhibited the translation of IL-8 mRNA is supported by the finding that the phosphorylation of eIF4E, an initiation factor, in stimulated Caco-2 cells was inhibited by carnosine. These results suggest that carnosine is a novel type of anti-inflammatory agent that down-regulates the inflammatory response in intestinal epithelial cells by a unique mechanism.

Published

2008

16. Novel non-peptidic and small-sized BACE1 inhibitors.

Author

Hamada Y, Ohta H, Miyamoto N, Yamaguchi R, Yamani A, Hidaka K, Kimura T, Saito K, Hayashi Y, Ishiura S, and Kiso Y

Subjects

Models, Molecular, Molecular Structure, Structure-Activity Relationship, Amyloid Precursor Protein Secretases antagonists & inhibitors, Oligopeptides chemistry, Oligopeptides pharmacology

Abstract

Recently, we reported substrate-based beta-secretase (BACE1) inhibitors with a hydroxymethylcarbonyl (HMC) isostere as a substrate transition-state mimic. These inhibitors showed potent BACE1 inhibitory activities (approximately 1.2 nM IC(50)). In order to improve in vivo enzymatic stability and permeability across the blood-brain barrier, these penta-peptidic inhibitors would need to be further optimized. On the other hand, non-peptidic inhibitors possessing isophthalic residue at the P(2) position were reported from other research groups. We selected isophthalic-type aromatic residues at the P(2) position and an HMC isostere at the P(1) position as lead compounds. On the basis of the design approach focused on the conformer of docked inhibitor in BACE1, we found novel non-peptidic and small-sized BACE1 inhibitors possessing a 2,6-pyridinedicarboxylic, chelidamic or chelidonic residue at the P(2) position.

Published

2008

17. BACE1 inhibitors: optimization by replacing the P1' residue with non-acidic moiety.

Author

Hamada Y, Abdel-Rahman H, Yamani A, Nguyen JT, Stochaj M, Hidaka K, Kimura T, Hayashi Y, Saito K, Ishiura S, and Kiso Y

Subjects

Models, Molecular, Molecular Structure, Structure-Activity Relationship, Amyloid Precursor Protein Secretases antagonists & inhibitors, Oligopeptides chemistry, Oligopeptides pharmacology

Abstract

Recently, we reported potent BACE1 inhibitors KMI-429, -684, and -574 possessing a hydroxymethylcarbonyl isostere as a substrate transition-state mimic. These inhibitors showed potent inhibitory activities in enzymatic and cell assays, especially, KMI-429 was confirmed to significantly inhibit Abeta production in vivo. However, acidic moieties at the P(4) and P(1)' positions of KMI-compounds were thought to be unfavorable for membrane permeability across the blood-brain barrier. Herein, we replaced acidic moieties at the P(4) position with other hydrogen bond acceptor groups, and these inhibitors exhibited improved BACE1 inhibitory activities in cultured cells. In this study, we replaced the acidic moieties at the P(1)' position with non-acidic and low molecular sized moieties.

Published

2008

18. Truncation and non-natural amino acid substitution studies on HTLV-I protease hexapeptidic inhibitors.

Author

Nguyen JT, Zhang M, Kumada HO, Itami A, Nishiyama K, Kimura T, Cheng M, Hayashi Y, and Kiso Y

Subjects

Amino Acid Substitution, Structure-Activity Relationship, Substrate Specificity, Amino Acids chemistry, Amino Acids pharmacology, Human T-lymphotropic virus 1 enzymology, Oligopeptides chemistry, Oligopeptides pharmacology, Protease Inhibitors chemistry, Protease Inhibitors pharmacology

Abstract

The culprit behind adult T-cell leukemia, myelopathy/tropical paraparesis, and a plethora of inflammatory diseases is the human T-cell leukemia virus type 1 (HTLV-I). We recently unveiled a potent hexapeptidic HTLV-I protease inhibitor, KNI-10166, composed mostly of natural amino acid residues. Herein, we report the derivation of potent tetrapeptidic inhibitor KNI-10516, possessing only non-natural amino acid residues.

Published

2008

19. Development of oligoarginine-drug conjugates linked to new peptidic self-cleavable spacers toward effective intestinal absorption.

Author

Hayashi Y, Takayama K, Suehisa Y, Fujita T, Nguyen JT, Futaki S, Yamamoto A, and Kiso Y

Subjects

Arginine pharmacology, Chromatography, High Pressure Liquid, Oligopeptides pharmacology, Arginine chemistry, Intestinal Absorption drug effects, Oligopeptides chemistry

Abstract

We designed and synthesized new peptidic self-cleavable spacers that released a parent drug via succinimide formation and the oligoarginine-based cargo-transporter (OACT) system. The self-cleavable efficacy of these compounds was studied and the conversion time was controlled by an amino acid side-chain structure next to the succinyl moiety on the spacer. These novel self-cleavable spacers are promising for developments of the OACT system as means to potentially enhance intestinal absorption of parent drugs.

Published

2007

20. Synthesis and antiviral property of allophenylnorstatine-based HIV protease inhibitors incorporating D-cysteine derivatives as P2/P3 moieties.

Author

Ami E, Nakahara K, Sato A, Nguyen JT, Hidaka K, Hamada Y, Nakatani S, Kimura T, Hayashi Y, and Kiso Y

Subjects

Amides chemistry, Cell Line, HIV drug effects, HIV Protease Inhibitors chemistry, Humans, Models, Molecular, Phenylbutyrates chemistry, Thiazoles chemistry, Amides chemical synthesis, Amides pharmacology, Cysteine chemistry, HIV Protease Inhibitors chemical synthesis, HIV Protease Inhibitors pharmacology, Phenylbutyrates chemical synthesis, Phenylbutyrates pharmacology, Thiazoles chemical synthesis, Thiazoles pharmacology

Abstract

We designed several HIV protease inhibitors with various d-cysteine derivatives as P(2)/P(3) moieties based on the structure of clinical drug candidate, KNI-764. Herein, we report their synthesis, HIV protease inhibitory activity, HIV IIIB cell inhibitory activity, cellular toxicity, and inhibitory activity against drug-resistant HIV strains. KNI-1931 showed distinct selectivity against HIV proteases and high potency against drug-resistant strains, surpassing those of Ritonavir and Nelfinavir.

Published

2007

21. Chipping at large, potent human T-cell leukemia virus type 1 protease inhibitors to uncover smaller, equipotent inhibitors.

Author

Kimura T, Nguyen JT, Maegawa H, Nishiyama K, Arii Y, Matsui Y, Hayashi Y, and Kiso Y

Subjects

Adult, Dose-Response Relationship, Drug, Humans, Models, Molecular, Molecular Weight, Oligopeptides chemistry, Chronic Disease drug therapy, HIV Protease Inhibitors pharmacology, Leukemia-Lymphoma, Adult T-Cell drug therapy, Oligopeptides pharmacology

Abstract

The human T-cell leukemia virus type 1 (HTLV-I) causes adult T-cell leukemia and several severe chronic diseases. HTLV-I protease (PR) inhibition stops the propagation of the virus. Herein, truncation studies were performed on potent octapeptidic HTLV-I PR inhibitor KNI-10161 to derive small hexapeptide KNI-10127 with some loss in activity. After performing residue-substitution studies on compound KNI-10127, HTLV-I PR inhibitory activity was recovered in inhibitor KNI-10166.

Published

2007

22. Additional interaction of allophenylnorstatine-containing tripeptidomimetics with malarial aspartic protease plasmepsin II.

Author

Hidaka K, Kimura T, Tsuchiya Y, Kamiya M, Ruben AJ, Freire E, Hayashi Y, and Kiso Y

Subjects

Animals, Antimalarials pharmacology, Aspartic Acid Endopeptidases chemistry, Biomimetic Materials pharmacology, Oligopeptides chemical synthesis, Oligopeptides pharmacology, Protease Inhibitors pharmacology, Protein Conformation, Protozoan Proteins, Structure-Activity Relationship, Antimalarials chemistry, Aspartic Acid Endopeptidases antagonists & inhibitors, Biomimetic Materials chemistry, Oligopeptides chemistry, Phenylbutyrates chemistry, Plasmodium falciparum enzymology, Protease Inhibitors chemistry

Abstract

Based on a highly potent allophenylnorstatine-containing inhibitor, KNI-10006, against the plasmepsins of Plasmodium falciparum, we synthesized a series of tripeptide-type compounds with various N-terminal moieties and evaluated their inhibitory activities against plasmepsin II. Certain phenylacetyl derivatives exhibited extremely high affinity with K(i) values of less than 0.1n M suggesting successful hydrophobic interactions.

Published

2007

23. Design and synthesis of BACE1 inhibitors containing a novel norstatine derivative (2R,3R)-3-amino-2-hydroxy-4-(phenylthio)butyric acid.

Author

Ziora Z, Kasai S, Hidaka K, Nagamine A, Kimura T, Hayashi Y, and Kiso Y

Subjects

Chromatography, High Pressure Liquid, Drug Design, Humans, Indicators and Reagents, Molecular Conformation, Spectrometry, Mass, Fast Atom Bombardment, Structure-Activity Relationship, Aminocaproates chemistry, Aminocaproates pharmacology, Amyloid Precursor Protein Secretases antagonists & inhibitors, Aspartic Acid Endopeptidases antagonists & inhibitors, Butyrates chemical synthesis, Butyrates pharmacology, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors pharmacology

Abstract

A novel norstatine derivative, phenylthionorstatine [(2R,3R)-3-amino-2-hydroxy-4-(phenylthio)butyric acid; Ptns], containing a hydroxymethylcarbonyl (HMC) isostere was designed, synthesized, and stereochemically determined. Then, Ptns was introduced into the structure of BACE1 inhibitors at the P(1) position. Finally, Ptns was found as a suitable P(1) moiety for potent BACE1 inhibitor design.

Published

2007

24. Visual determination of nitrite and nitrate in waters by color band formation method.

Author

Kiso Y, Jung YJ, Kuzawa K, Seko Y, Saito Y, Yamada T, and Nagai M

Subjects

Adsorption, Chromatography, High Pressure Liquid, Chromatography, Liquid methods, Color, Nitrates analysis, Nitrites analysis, Water analysis

Abstract

A spot test for aqueous nitrate and nitrite for controlling nitrogen removal performance in small-scale wastewater treatment facilities is proposed. In this method, NO(2)(-) ion in water samples was allowed to react with sulfanilic acid and 1-naphthol to form an anionic azo dye. The resulting colored solution was introduced onto a mini column (similar to a gas detecting tube) packed with PVC particles coated with benzyl cetyl dimethyl ammonium chloride (BCDMA) and biphenyl. The NO(2)(-)-N concentration was determined visually by measuring the color band length (CBL) in the column. The CBL correlates linearly with nitrite concentration in the 4-20 mg-N l(-1) range. The concentration of nitrite+nitrate was determined after reduction to nitrite with zinc. The concentration of NO(3)(-)-N species was calculated by difference. This method was used to visually determine the concentrations of NO(2)(-)-N and (NO(2)(-)+NO(3)(-))-N in domestic wastewater samples with maximum suspended solid (SS) and chemical oxygen demand (COD) concentrations of 114 mg l(-1) and 73.9 mg l(-1), respectively.

Published

2006

25. Development of first photoresponsive prodrug of paclitaxel.

Author

Skwarczynski M, Noguchi M, Hirota S, Sohma Y, Kimura T, Hayashi Y, and Kiso Y

Subjects

Molecular Structure, Paclitaxel chemical synthesis, Photosensitizing Agents chemistry, Prodrugs chemistry, Paclitaxel chemistry, Photosensitizing Agents chemical synthesis, Prodrugs chemical synthesis

Abstract

A prodrug of paclitaxel which has a coumarin derivative conjugated to the amino acid moiety of isotaxel (O-acyl isoform of paclitaxel) has been synthesized. The prodrug was selectively converted to isotaxel by visible light irradiation (430 nm) with the cleavage of coumarin. Finally, paclitaxel was released by subsequent spontaneous O-N intramolecular acyl migration.

Published

2006

26. beta-Secretase inhibitors: modification at the P4 position and improvement of inhibitory activity in cultured cells.

Author

Hamada Y, Igawa N, Ikari H, Ziora Z, Nguyen JT, Yamani A, Hidaka K, Kimura T, Saito K, Hayashi Y, Ebina M, Ishiura S, and Kiso Y

Subjects

Amyloid Precursor Protein Secretases, Aspartic Acid Endopeptidases, Carboxylic Acids chemistry, Cells, Cultured, Chemistry, Pharmaceutical, Drug Design, Esters chemistry, Humans, Models, Chemical, Models, Molecular, Protease Inhibitors chemistry, Tetrazoles chemistry, Endopeptidases chemistry, Protease Inhibitors pharmacology

Abstract

Recently, we reported potent and small-sized beta-secretase (BACE1) inhibitors KMI-570 and KMI-684 in which we replaced carboxylic acid groups at the P(1)(') position of KMI-420 and KMI-429, respectively, with tetrazole derivatives as carboxylic acid bioisosteres. These modifications improved significantly BACE1 inhibitory activity and chemical stability. In this study, the acidic tetrazole ring of the P(4) position of KMI-420 and KMI-570, respectively, was replaced with various hydrogen bond acceptor groups. We found BACE1 inhibitor KMI-574 that exhibited potent inhibitory activity in cultured cells as well as in vitro enzymatic assay.

Published

2006

27. Design and synthesis of potent beta-secretase (BACE1) inhibitors with P1' carboxylic acid bioisosteres.

Author

Kimura T, Hamada Y, Stochaj M, Ikari H, Nagamine A, Abdel-Rahman H, Igawa N, Hidaka K, Nguyen JT, Saito K, Hayashi Y, and Kiso Y

Subjects

Alzheimer Disease drug therapy, Amyloid Precursor Protein Secretases, Crystallography, X-Ray, Drug Evaluation, Preclinical, Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacology, Models, Molecular, Molecular Structure, Oligopeptides chemistry, Oligopeptides pharmacology, Stereoisomerism, Structure-Activity Relationship, Carboxylic Acids chemistry, Drug Design, Endopeptidases drug effects, Enzyme Inhibitors chemical synthesis, Oligopeptides chemical synthesis

Abstract

Recently, we reported potent and small-sized beta-secretase (BACE1) inhibitors KMI-420 and KMI-429 in which we replaced the Glu residue at the P4 position of KMI-260 and KMI-360, respectively, with a 1H-tetrazole-5-carbonyl DAP (L-alpha,beta-diaminopropionic acid) residue. At the P1' position, these compounds contain one or two carboxylic acid groups, which are unfavorable for crossing the blood-brain barrier. Herein, we report BACE1 inhibitors with P1' carboxylic acid bioisosteres in order to develop practical anti-Alzheimer's disease drugs. Among them, tetrazole ring-containing compounds, KMI-570 (IC50=4.8 nM) and KMI-684 (IC50=1.2 nM), exhibited significantly potent BACE1 inhibitory activities.

Published

2006

28. Phosphate removal and recovery with a synthetic hydrotalcite as an adsorbent.

Author

Kuzawa K, Jung YJ, Kiso Y, Yamada T, Nagai M, and Lee TG

Subjects

Adsorption, Surface Properties, Aluminum Hydroxide chemistry, Eutrophication, Magnesium Hydroxide chemistry, Phosphates analysis, Water Pollutants, Chemical analysis, Water Purification methods

Abstract

Phosphate removal is important to control eutrophication and an ion exchange process is one of several treatment processes for this purpose. Hydrotalcite compounds (HTALs) are useful as adsorbents for phosphate removal because of their ion exchange properties. In this study, the adsorption properties of a granular synthetic HTAL for phosphate and the method of regeneration of the granular HTAL were examined. The adsorption isotherm of the granular HTAL was approximated by a modified Langmuir type, and the maximum adsorption capacity was 47.3 mg P g(-1), which corresponded to the content of HTAL in the granular one. Phosphate adsorbed on the HTAL was effectively desorbed with alkaline NaCl solutions and the HTAL was regenerated with 25 w/v% MgCl(2) solution. The regenerated HTAL could be reused repeatedly for the phosphate removal. Phosphate in the exhausted desorption solution was recovered as a precipitate of calcium phosphate by addition of CaCl(2), and the residual exhausted desorption solution could be also reused after supplying NaOH. The results suggest the possibility of an effective system for phosphate removal and recovery, which includes the following processes: adsorption, desorption, recovery of phosphate, and regeneration of the HTAL and the desorption solution.

Published

2006

29. Design and synthesis of highly active Alzheimer's beta-secretase (BACE1) inhibitors, KMI-420 and KMI-429, with enhanced chemical stability.

Author

Kimura T, Shuto D, Hamada Y, Igawa N, Kasai S, Liu P, Hidaka K, Hamada T, Hayashi Y, and Kiso Y

Subjects

Amyloid Precursor Protein Secretases, Drug Stability, Endopeptidases, Models, Molecular, Oligopeptides chemistry, Protease Inhibitors chemistry, Aspartic Acid Endopeptidases antagonists & inhibitors, Oligopeptides chemical synthesis, Oligopeptides pharmacology, Protease Inhibitors chemical synthesis, Protease Inhibitors pharmacology

Abstract

Recently, we reported potent and small-sized BACE1 inhibitors KMI-358 and KMI-370 in which the Glu residue is replaced by a beta-N-oxalyl-DAP (l-alpha,beta-diaminopropionyl) residue at the P(4) position. The beta-N-oxalyl-DAP group is important for enhancing BACE1 inhibitory activity, but these inhibitors isomerized to alpha-N-oxalyl-DAP derivatives in solvents. Hence, we used a tetrazole moiety as a bioisostere of the free carboxylic acid of the oxalyl group. KMI-420 and KMI-429, containing a tetrazole ring, showed improved stability and potent enzyme inhibitory activity.

Published

2005

30. Identification of peptidomimetic HTLV-I protease inhibitors containing hydroxymethylcarbonyl (HMC) isostere as the transition-state mimic.

Author

Maegawa H, Kimura T, Arii Y, Matsui Y, Kasai S, Hayashi Y, and Kiso Y

Subjects

Amino Acid Sequence, Aspartic Acid Endopeptidases genetics, Aspartic Acid Endopeptidases metabolism, Humans, Molecular Sequence Data, Protease Inhibitors pharmacology, Aspartic Acid Endopeptidases antagonists & inhibitors, Protease Inhibitors chemistry

Abstract

Towards the development of chemotherapy for the infection by human T-cell leukemia virus type I (HTLV-I), we have established evaluation systems for HTLV-I protease (PR) inhibitors using both recombinant and chemically synthesized HTLV-I PRs. Newly synthesized substrate-based inhibitors containing hydroxymethylcarbonyl (HMC) isostere showed potent anti-HTLV-I PR activity.

Published

2004

31. KMI-358 and KMI-370, highly potent and small-sized BACE1 inhibitors containing phenylnorstatine.

Author

Kimura T, Shuto D, Kasai S, Liu P, Hidaka K, Hamada T, Hayashi Y, Hattori C, Asai M, Kitazume S, Saido TC, Ishiura S, and Kiso Y

Subjects

Amyloid Precursor Protein Secretases, Aspartic Acid Endopeptidases metabolism, Cell Line, Dose-Response Relationship, Drug, Endopeptidases, Humans, Phenylbutyrates metabolism, Protease Inhibitors metabolism, Aspartic Acid Endopeptidases antagonists & inhibitors, Phenylbutyrates chemistry, Protease Inhibitors chemistry

Abstract

Recently, we reported a novel substrate-based octapeptide BACE1 inhibitor KMI-008 containing hydroxymethylcarbonyl (HMC) isostere as a transition-state mimic. Using KMI-008 as a lead compound, a small-sized and highly potent BACE1 inhibitor KMI-370 (IC(50)=3.4 nM) was designed and synthesized.

Published

2004

32. O-N intramolecular acyl migration strategy in water-soluble prodrugs of taxoids.

Author

Skwarczynski M, Sohma Y, Kimura M, Hayashi Y, Kimura T, and Kiso Y

Subjects

Acylation, Indicators and Reagents, Kinetics, Models, Molecular, Molecular Conformation, Nitrogen, Oxygen, Prodrugs chemical synthesis, Solubility, Stereoisomerism, Water, Prodrugs chemistry, Taxoids chemical synthesis, Taxoids chemistry

Abstract

We synthesized a highly water-soluble canadensol prodrug 6 that formed canadensol 3 by a simple pH-dependent chemical mechanism via the O-N intramolecular acyl migration of the isobutyryl group. This prodrug, a 2'-O-isobutyryl isoform of 3, has no additional functional auxiliaries released during the conversion to 3. This is a significant advantage in toxicology and medical economics, since the potential side effects of reported water-soluble auxiliaries and the use of detergent for solubilization can be avoided. The solubility of 6 was 2.26 mg mL(-1) and only the parent drug 3 was released under physiological conditions (pH=7.4) while, in acidic medium, the release of 3 slowed until migration was completely obstructed at pH=2. In further consideration of this strategy, we elucidated the use of an 'O-N acyl-like' migration reaction of the Boc group in the design of a docetaxel prodrug. Both O-N migration and undesired hydrolysis of the Boc group occurred under physiological conditions, although no oxazolidinone formation was observed, suggesting the limitation of our water-soluble prodrug strategy to docetaxel.

Published

2003

33. KMI-008, a novel beta-secretase inhibitor containing a hydroxymethylcarbonyl isostere as a transition-state mimic: design and synthesis of substrate-based octapeptides.

Author

Shuto D, Kasai S, Kimura T, Liu P, Hidaka K, Hamada T, Shibakawa S, Hayashi Y, Hattori C, Szabo B, Ishiura S, and Kiso Y

Subjects

Amino Acid Sequence, Amyloid Precursor Protein Secretases, Drug Design, Models, Molecular, Oligopeptides chemical synthesis, Protease Inhibitors chemical synthesis, Protein Conformation, Structure-Activity Relationship, Endopeptidases metabolism, Oligopeptides metabolism, Oligopeptides pharmacology, Protease Inhibitors pharmacology

Abstract

A novel class of substrate-based beta-secretase (BACE1) inhibitors containing a hydroxymethylcarbonyl (HMC) isostere was designed and synthesized. Phenylnorstatine [(2R,3S)-3-amino-2-hydroxy-4-phenylbutyric acid; Pns] was an effective transition-state mimic at the P(1) position. Structure-activity relationships (SARs) of the P(3)-P(3)' positions of BACE1 inhibitors were studied.

Published

2003

34. Effect of the acyl groups on O-->N acyl migration in the water-soluble prodrugs of HIV-1 protease inhibitor.

Author

Hamada Y, Matsumoto H, Kimura T, Hayashi Y, and Kiso Y

Subjects

Acylation, Benzoates chemistry, Drug Stability, HIV Protease Inhibitors pharmacology, Half-Life, Humans, Hydrogen-Ion Concentration, Phenoxyacetates chemistry, Phenylacetates chemistry, Prodrugs pharmacology, Solubility, Static Electricity, Structure-Activity Relationship, Water, HIV Protease Inhibitors chemical synthesis, HIV-1, Prodrugs chemical synthesis

Abstract

To improve the low water-solubility of HIV-1 protease inhibitors KNI-272, -279 and -727, we previously reported the water-soluble prodrugs of these inhibitors based on O-->N intramolecular acyl migration reaction. These prodrugs were rapidly converted to the corresponding parent drugs under physiological conditions. To understand the steric and electrostatic effects of O-acyl moiety on the migration rate, we examined several types of prodrug. A remarkably slow migration was observed in the benzoyl-type prodrugs, and Hammett plot of migration rate constants of p-substituted benzoyl-type prodrugs gave a linear free energy relationship.

Published

2003

35. Design and synthesis of pseudo-symmetric HIV protease inhibitors containing a novel hydroxymethylcarbonyl (HMC)-hydrazide isostere.

Author

Hidaka K, Kimura T, Hayashi Y, McDaniel KF, Dekhtyar T, Colletti L, and Kiso Y

Subjects

Drug Design, HIV Protease drug effects, HIV Protease Inhibitors pharmacology, Humans, Inhibitory Concentration 50, Molecular Mimicry, Oligopeptides pharmacology, Structure-Activity Relationship, HIV Protease Inhibitors chemical synthesis, Hydrazines chemistry, Oligopeptides chemical synthesis

Abstract

Pseudo-symmetric HIV-1 protease inhibitors containing a novel HMC-hydrazide isostere as the transition-state mimic were designed and synthesized. Most of the synthetic compounds with varied structures at the P and P' sites around this core unit showed potent inhibitory activity against HIV-1 protease with nanomolar K(i) values.

Published

2003

36. An expedient synthesis of N(alpha)-protected-L-tetrahydrofuranylglycine and its application in the synthesis of novel substrate based inhibitors of HIV-1 protease.

Author

Rajesh S, Ami E, Kotake T, Kimura T, Hayashi Y, and Kiso Y

Subjects

Furans chemistry, Furans pharmacology, Glycine chemistry, Glycine pharmacology, HIV Protease metabolism, HIV Protease Inhibitors pharmacology, Humans, Oligopeptides pharmacology, Structure-Activity Relationship, HIV Protease Inhibitors chemical synthesis, Oligopeptides chemical synthesis

Abstract

Z- and Fmoc-L-tetrahydrofuranylglycines have been obtained from L-vinylglycine through dipolar cycloaddition reaction, and its Fmoc derivative has been applied in the synthesis of modified S9 and S10 substrates of HIV-1 protease. These compounds mostly acted as strong inhibitors, rather than substrates, of the protease, probably due to the favourable interactions of the tetrahydrofuranylglycine moiety at the S(2) site.

Published

2002

37. Design and synthesis of new inhibitors of HIV-1 protease dimerization with conformationally constrained templates.

Author

Song M, Rajesh S, Hayashi Y, and Kiso Y

Subjects

Dimerization, Drug Design, Drug Evaluation, Preclinical, HIV Protease chemistry, HIV Protease metabolism, HIV Protease Inhibitors chemical synthesis, Kinetics, Molecular Conformation, Molecular Mimicry, Structure-Activity Relationship, HIV Protease drug effects, HIV Protease Inhibitors chemistry, HIV Protease Inhibitors pharmacology, Hydrazines chemical synthesis, Hydrazines pharmacology

Abstract

To inhibit the HIV-1 protease dimerization necessary to exhibit enzymatic activity, we synthesized and evaluated a new beta-sheet peptide (compound 1), containing 4-(2-aminoethyl)-6-dibenzofuranpropionic acid as a conformationally restricted linker and a non-peptidic beta-strand mimetic, 2-[3-([2-[(9-fluorenylmethoxy)carbonyl]hydrazino]carbonyl)-4-methoxyanilino]-2-oxoacetic acid (Fmoc-Hao-OH, compound 2). Kinetic analysis showed that compound 1 inhibited the dimerization of HIV-1 protease by a dissociative mechanism with a K(id) value of 5.4 microM at 37 degrees C (pH 5.0). However, compound 2 showed a small shift in the slope of the lines in the Zhang-Poorman plot (K(id)=9.1 microM), suggesting that compound 2 inhibits the dimerization of HIV-1 PR not only through a dissociative mechanism but also through an active-site directed mechanism partly. This is the first study of a non-peptidic inhibitor of HIV-1 protease dimerization.

Published

2001

38. Controlled drug release: new water-soluble prodrugs of an HIV protease inhibitor.

Author

Matsumoto H, Sohma Y, Kimura T, Hayashi Y, and Kiso Y

Subjects

Chromatography, High Pressure Liquid, Drug Design, HIV Protease Inhibitors chemistry, Hydrogen-Ion Concentration, Prodrugs chemistry, Solubility, HIV Protease Inhibitors chemical synthesis, Prodrugs chemical synthesis

Abstract

We designed and synthesized a series of highly water-soluble prodrugs of an HIV protease inhibitor, KNI-727 (1), containing tandem-linked two auxiliary units, a solubilizing moiety and a self-cleavable spacer. Prodrugs with an ionized amino group at the solubilizing moiety exhibited a remarkable increase of water-solubility (>10(4) fold) compared to the parent drug 1. These prodrugs released I not enzymatically, but chemically via an intramolecular cyclization-elimination reaction through an imide formation in physiological conditions. Diversified rates of parent drug release were observed when the chemical structure of both the solubilizing and the spacer moieties were modified. This new approach for water-soluble prodrugs will enable to control chemically the release of parent drug as well as to maintain high water-solubility.

Published

2001

39. 'Double-Drugs'--a new class of prodrug form of an HIV protease inhibitor conjugated with a reverse transcriptase inhibitor by a spontaneously cleavable linker.

Author

Matsumoto H, Hamawaki T, Ota H, Kimura T, Goto T, Sano K, Hayashi Y, and Kiso Y

Subjects

Anti-HIV Agents pharmacology, HIV-1 drug effects, Humans, Microbial Sensitivity Tests, Thiazoles pharmacology, Zidovudine chemistry, Zidovudine pharmacology, Anti-HIV Agents chemistry, HIV Protease Inhibitors chemistry, Prodrugs chemistry, Reverse Transcriptase Inhibitors chemistry, Thiazoles chemistry, Zidovudine analogs & derivatives

Abstract

We designed and synthesized a new series of prodrug-type anti-HIV agents consisting of a peptidomimetic HIV protease inhibitor conjugated with a nucleoside reverse transcriptase inhibitor in an effort to enhance the antiviral activity. For the conjugation, a series of linkers that conjoin the two different classes of inhibitors have been investigated. Conjugates using a succinyl amino acid linker were shown to release the parent components via the spontaneous imide formation at a faster rate compared to conjugates using a glutaryl amino acid linker, as expected from the energetically favorable cyclization to the five-membered ring. Herein, we report a new 'double-drug' 4b (KNI-1039) with a glutarylglycine linker, which exhibited extremely potent anti-HIV activity compared with that of the individual components.

Published

2000

40. Structure-activity relationship studies of chloromethyl ketone derivatives for selective human chymase inhibitors.

Author

Hayashi Y, Iijima K, Katada J, and Kiso Y

Subjects

Chymases, Humans, Ketones chemistry, Magnetic Resonance Spectroscopy, Serine Proteinase Inhibitors chemistry, Spectrometry, Mass, Fast Atom Bombardment, Structure-Activity Relationship, Ketones pharmacology, Serine Endopeptidases drug effects, Serine Proteinase Inhibitors pharmacology

Abstract

Based on the SAR study of a classical chloromethyl ketone derivative, Z-PheCH2Cl 1, a series of compounds were synthesized. Among all the derivatives, compound 21 was found to be a potent human chymase inhibitor with no inhibitory activity against human leukocyte cathepsin G.

Published

2000

41. A new class of anti-HIV agents: synthesis and activity of conjugates of HIV protease inhibitors with a reverse transcriptase inhibitor.

Author

Kimura T, Matsumoto H, Matsuda T, Hamawaki T, Akaji K, and Kiso Y

Subjects

Anti-HIV Agents chemical synthesis, Drug Combinations, Models, Chemical, Zidovudine chemistry, Anti-HIV Agents administration & dosage, HIV Protease Inhibitors chemical synthesis, Reverse Transcriptase Inhibitors chemical synthesis

Abstract

Conjugates of HIV protease inhibitors with a reverse transcriptase inhibitor were synthesized, which expressed excellent antiviral activity compared with that of the individual components. The remarkable antiviral activity of the conjugated compounds may be due to their penetration into the cell and later splitting into two different classes of anti-HIV agents.

Published

1999