Your search keyword '"Takeru, Nose"' showing total 6 results

1. Bisphenol AF: Halogen bonding effect is a major driving force for the dual ERα-agonist and ERβ-antagonist activities

Author

Xiaohui Liu, Kohei Torikai, Takeru Nose, Miki Shimohigashi, Keitaro Suyama, Junichi Shiki, and Yasuyuki Shimohigashi

Subjects

Agonist, endocrine system, Stereochemistry, Bisphenol, medicine.drug_class, medicine.medical_treatment, Clinical Biochemistry, Pharmaceutical Science, Estrogen receptor, 01 natural sciences, Biochemistry, Bisphenol AF, Steroid, chemistry.chemical_compound, Structure-Activity Relationship, Phenols, Drug Discovery, medicine, Structure–activity relationship, Estrogen Receptor beta, Humans, Benzhydryl Compounds, Molecular Biology, Dose-Response Relationship, Drug, Molecular Structure, 010405 organic chemistry, Chemistry, Organic Chemistry, Antagonist, Estrogen Receptor alpha, Estrogens, Ligand (biochemistry), 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, Molecular Medicine, Estrogen Receptor Antagonists, hormones, hormone substitutes, and hormone antagonists, HeLa Cells

Abstract

17β-Estradiol (E2) is a natural steroid ligand for the structurally and physiologically independent estrogen receptors (ERs) ERα and ERβ. We recently observed that CF3-containing bisphenol AF (BPAF) works as an agonist for ERα but as an antagonist for ERβ. Similar results were also observed for the CCl3-containing bisphenol designated as HPTE. Both BPAF and HPTE are comprised of a tri-halogenated methyl group in the central alkyl moiety of their bisphenol structures, which strongly suggests that halogens contribute directly to the agonist/antagonist dual biological functions. We conducted this study to investigate the structure-activity relationships by assessing together newly synthesized CF3- and CBr3-containing bisphenol E analogs (BPE-X). We first tested bisphenols for their receptor binding ability and then for their transcriptional activities. Halogen-containing bisphenols were found to be fully active for ERα, but almost completely inactive for ERβ. When we examined these bisphenols for their inhibitory activities for E2 in ERβ, we observed that they worked as distinct antagonists. The ascending order of agonist/antagonist dual biological functions was BPE-F

Published

2019

2. Spare interactions of highly potent [Arg(14),Lys(15)]nociceptin for cooperative induction of ORL1 receptor activation

Author

Hirokazu Nishimura, Jinglan Li, Ayami Matsushima, Kazushi Okada, Kaname Isozaki, Tommaso Costa, Takeru Nose, and Yasuyuki Shimohigashi

Subjects

Agonist, Arginine, Stereochemistry, medicine.drug_class, Clinical Biochemistry, Molecular Sequence Data, Pharmaceutical Science, Biochemistry, Binding, Competitive, Nociceptin Receptor, Drug Discovery, Tachykinin receptor 1, medicine, Amino Acid Sequence, Binding site, Receptor, Molecular Biology, Peptide sequence, Chemistry, Lysine, Organic Chemistry, Biological activity, Nociceptin receptor, Kinetics, Opioid Peptides, Receptors, Opioid, Mutagenesis, Site-Directed, Molecular Medicine

Abstract

[Arg(14),Lys(15)]Nociceptin is a very potent for ORL1 receptor, showing a few times stronger binding activity and much more enhanced biological activity than endogenous nociceptin. This synergistic outcome has been suggested to be due to the interaction with the receptor aromatic and/or acidic amino acid residues crucial to receptor activation. In order to identify such receptor residues in the second ORL1 extracellular loop, we prepared a series of recombinant mutant receptors. The mutant receptor Gln205Ala was found to be as active as wild-type ORL1 for both nociceptin and [Arg(14),Lys(15)]nociceptin. In contrast, Asp206Ala and Tyr207Ala exhibited considerably reduced activity for [Arg(14),Lys(15)]nociceptin, exhibiting no synergistic activity enhancement. These results suggest that Asp206 and Tyr207 are directly involved in the interaction with nociceptin-[Arg(14),Lys(15)]. Trp208Ala was found to bind strongly both nociceptin and [Arg(14),Lys(15)]nociceptin, although it elicited no biological activity. All these results indicate that the consecutive amino acid residues Asp206, Tyr207, and Trp208 are critical to the activation of the ORL1 receptor, but not to nociceptin-binding.

Published

2009

3. Discriminatory synergistic effect of Trp-substitutions in superagonist [(Arg/Lys)(14), (Arg/Lys)(15)]nociceptin on ORL1 receptor binding and activation

Author

Jinglan Li, Tommaso Costa, Yasuyuki Shimohigashi, Hirokazu Nishimura, Takeru Nose, Kazushi Okada, Kaname Isozaki, and Ayami Matsushima

Subjects

Agonist, Stereochemistry, medicine.drug_class, Clinical Biochemistry, Molecular Sequence Data, GTPgammaS, Pharmaceutical Science, Peptide, Arginine, Biochemistry, Nociceptin Receptor, chemistry.chemical_compound, Drug Discovery, Peptide synthesis, Pi, medicine, Animals, Amino Acid Sequence, Receptor, Molecular Biology, chemistry.chemical_classification, Lysine, Organic Chemistry, Tryptophan, Biological activity, Rats, Nociceptin receptor, chemistry, Opioid Peptides, Receptors, Opioid, Molecular Medicine, Protein Binding

Abstract

ORL1 is an endogenous G protein-coupled receptor for neuropeptide nociceptin. [(R/K)(14), (R/K)(15)]nociceptin is a superagonist that strongly activates the ORL1 receptor. We have previously found that substituting with Trp can reproduce the potentiation induced by Arg or Lys at position 14. In the present study, in order to ensure the effect of Trp-substitution on the activities of [(R/K)(14), (R/K)(15)]nociceptin, we synthesized [W(14), (R/K)(15)]nociceptin and [(R/K)(14), W(15)]nociceptin. [W(14), (R/K)(15)]nociceptin was found to exhibit threefold higher binding activity and 10-fold greater potency in a functional [(35)S]GTPgammaS functional assay as compared to wild-type nociceptin. However, when only Trp was placed in position 15, the resulting analogues, [(R/K)(14), W(15)]nociceptin, showed only a moderate enhancement of binding and biological activity (2-3 fold in both). These results indicate that the placement of Trp at position 14, unlike at position 15, enhances in a synergistic fashion the interaction of nociceptin with the ORL1 receptor. The results indicate that specific interactions feasible for Arg/Lys and Trp in common must be there for aromatic residues in ORL1, thus forming a cation/pi interaction or pi/pi hydrophobic interaction. The necessity for a favorable electrostatic interaction appears strict in position 15.

Published

2009

4. Synergistic effect of basic residues at positions 14-15 of nociceptin on binding affinity and receptor activation

Author

Ayami Matsushima, Kaname Isozaki, Yasuyuki Shimohigashi, Tommaso Costa, Kazushi Okada, Takeru Nose, and Jinglan Li

Subjects

Stereochemistry, Clinical Biochemistry, Molecular Sequence Data, Pharmaceutical Science, Peptide, Biochemistry, Nociceptin Receptor, chemistry.chemical_compound, Structure-Activity Relationship, Drug Discovery, Chlorocebus aethiops, Peptide synthesis, Animals, Amino Acid Sequence, Receptor, Molecular Biology, G protein-coupled receptor, chemistry.chemical_classification, Dipeptide, Organic Chemistry, Biological activity, Amino acid, Rats, Nociceptin receptor, chemistry, Opioid Peptides, COS Cells, Receptors, Opioid, Molecular Medicine, Protein Binding

Abstract

Nociceptin is an endogenous ligand that activates a G protein-coupled receptor ORL1 and contains two indispensable Arg-Lys (RK) dipeptide units at positions 8–9 and 12–13. By replacing an additional RK unit at positions 6–7, 10–11, 14–15, or 16–17, of the peptide we have identified the analog, [RK14–15]nociceptin as a superagonist. In fact, this peptide exhibits 3-fold higher binding affinity and 17-fold greater potency in a functional GTPγS-binding assay compared to wild-type nociceptin. Here, we have further investigated the role of basic residues in position 14–15. The replacement of three other possible basic dipeptides, KR, RR, and KK, into nociceptin at positions 14–15 resulted in similar enhancements of binding affinity (3–5-fold) and biological potency (10–12-fold in the GTPγS assay). However, when only a single basic residue (Arg or Lys) was replaced in either position 14 or 15, all the resulting analogs showed moderate enhancements of binding and biological activity (2–4-fold in both). These results indicate that the addition of basic charges in positions 14 and 15 enhance in a synergistic fashion the interaction of nociceptin with the receptor and only the simultaneous presence of two adjacent basic residues yields an optimal effect. This suggests that specific electrostatic interactions between both amino acids present in 14–15 and corresponding residues in the receptor are responsible for the enhancement of nociceptin activity.

Published

2008

5. Designed modification of partial agonist of ORL1 nociceptin receptor for conversion into highly potent antagonist

Author

Ayami Matsushima, Takeru Nose, Yasuyuki Shimohigashi, Jinglan Li, Kazushi Okada, Kaname Isozaki, and Tommaso Costa

Subjects

Agonist, medicine.drug_class, Stereochemistry, Narcotic Antagonists, Clinical Biochemistry, Pharmaceutical Science, Biochemistry, Partial agonist, Nociceptin Receptor, Mice, Structure-Activity Relationship, Drug Discovery, Chlorocebus aethiops, medicine, Inverse agonist, Animals, Humans, Molecular Biology, Chromatography, High Pressure Liquid, Molecular Structure, Chemistry, Organic Chemistry, Antagonist, Ligand (biochemistry), GTP-Binding Protein alpha Subunits, Nociceptin receptor, Competitive antagonist, Drug Design, COS Cells, Receptors, Opioid, Molecular Medicine, Peptides, Endogenous agonist

Abstract

Nociceptin is an endogenous agonist ligand of the ORL1 (opioid receptor-like 1) receptor, and its antagonist is a potential target of therapeutics for analgesic and antineuropathy drugs. Ac-RYYRIK-NH 2 is a hexapeptide isolated from the peptide library as an antagonist that inhibits the nociceptin activities mediated through ORL1. However, the structural elements required for this antagonist activity are still indeterminate. In the present study, we evaluated the importance of the acetyl-methyl group in receptor binding and activation, examining the peptides acyl-RYYRIK-NH 2 , where acyl (R-CO) possesses a series of alkyl groups, R = C n H 2 n +1 ( n = 0–5). The isovaleryl derivative with the C 4 H 9 (=(CH 3 ) 2 CHCH 2 –) group was found to reveal a high receptor-binding affinity and a strong antagonist nature. This peptide achieved a primary goal of eliminating the agonist activity of Ac-RYYRIK-NH 2 and producing pure antagonist activity.

Published

2007

6. Differential receptor binding characteristics of consecutive phenylalanines in micro-opioid specific peptide ligand endomorphin-2

Author

Yoshiro Chuman, Takeru Nose, Daiki Shigehiro, Kaname Isozaki, Naoto Shirasu, Tsugumi Fujita, Michiaki Kawano, Takeshi Honda, and Yasuyuki Shimohigashi

Subjects

Threonine, Stereochemistry, Phenylalanine, Clinical Biochemistry, Molecular Sequence Data, Receptors, Opioid, mu, Pharmaceutical Science, Ligands, Biochemistry, chemistry.chemical_compound, Drug Discovery, Peptide synthesis, Animals, Amino Acid Sequence, Opioid peptide, Receptor, Molecular Biology, Peptide sequence, chemistry.chemical_classification, Organic Chemistry, Ligand (biochemistry), Amino acid, Rats, chemistry, Amino Acid Substitution, Molecular Medicine, NK1 receptor antagonist, μ-opioid receptor, Oligopeptides

Abstract

Endogenous opioid peptides consist of a conserved amino acid residue of Phe(3) and Phe(4), although their binding modes for opioid receptors have not been elucidated in detail. Endomorphin-2, which is highly selective and specific for the mu opioid receptor, possesses two Phe residues at the consecutive positions 3 and 4. In order to clarify the role of Phe(3) and Phe(4) in binding to the mu receptor, we synthesized a series of analogs in which Phe(3) and Phe(4) were replaced by various amino acids. It was found that the aromaticity of the Phe-beta-phenyl groups of Phe(3) and Phe(4) is a principal determinant of how strongly it binds to the receptor, although better molecular hydrophobicity reinforces the activity. The receptor binding subsites of Phe(3) and Phe(4) of endomorphin-2 were found to exhibit different structural requirements. The results suggest that [Trp(3)]endomorphin-2 (native endomorphin-1) and endomorphin-2 bind to different receptor subclasses.

Published

2007