Your search keyword '"Yuichiro Kanno"' showing total 6 results

1. Involvement of the CYP1A1 inhibition-mediated activation of aryl hydrocarbon receptor in drug-induced hepatotoxicity

Author

Tomomi Yoda, Tomoaki Tochitani, Toru Usui, Mami Kouchi, Hiroshi Inada, Takuomi Hosaka, Yuichiro Kanno, Izuru Miyawaki, and Kouichi Yoshinari

Subjects

Male, Receptors, Aryl Hydrocarbon, Genes, Reporter, Basic Helix-Loop-Helix Transcription Factors, Cytochrome P-450 CYP1A1, Hepatocytes, Animals, Humans, Chemical and Drug Induced Liver Injury, Toxicology, Rats

Abstract

Hepatotoxicity is one of the most common toxicities observed in non-clinical safety studies of drug candidates, and it is important to understand the hepatotoxicity mechanism to assess the risk of drug-induced liver injury in humans. In this study, we investigated the mechanism of hepatotoxicity caused by 2-[2-Methyl-1-(oxan-4-yl)-1H-benzimidazol-5-yl]-1,3-benzoxazole (DSP-0640), a drug candidate that showed hepatotoxicity characterized by centrilobular hypertrophy and vacuolation of hepatocytes in a 4-week oral repeated-dose toxicity study in male rats. In the liver of rats treated with DSP-0640, the expression of aryl hydrocarbon receptor (AHR) target genes, including Cyp1a1, was upregulated. In in vitro reporter assays, however, DSP-0640 showed only minimal AHR-activating potency. Therefore, we investigated the possibility that DSP-0640 indirectly activated AHR by inhibiting the CYP1 enzyme-dependent clearance of endogenous AHR agonists. In in vitro assays, DSP-0640 showed inhibitory effects on both rat and human CYP1A1 and enhanced rat and human AHR-mediated reporter gene expression induced by 6-formylindolo[3,2-b]carbazole, a well-known endogenous AHR agonist. The possible involvement of CYP1A1 inhibition in AHR activation was also demonstrated with other hepatotoxic compounds tacrine and albendazole. These results suggest that CYP1A1 inhibition-mediated AHR activation is involved in the hepatotoxicity caused by DSP-0640 and that DSP-0640 might induce hepatotoxicity in humans as well. We propose that CYP1A1 inhibition-mediated AHR activation is a novel mechanism for drug-induced hepatotoxicity.

Published

2022

2. Androgen receptor functions as a negative transcriptional regulator of DEPTOR, mTOR inhibitor

Author

Shuai Zhao, Kazuyuki Yanai, Naoya Yamashita, Kiyomitsu Nemoto, Yoshio Inouye, and Yuichiro Kanno

Subjects

Male, Time Factors, Transcription, Genetic, P70-S6 Kinase 1, mTORC1, Toxicology, DEPTOR, mTORC2, Histones, Tosyl Compounds, Cell Line, Tumor, Nitriles, LNCaP, Tumor Cells, Cultured, Humans, Anilides, Cyclin D1, RNA, Messenger, Phosphorylation, PI3K/AKT/mTOR pathway, Cell Proliferation, Chemistry, TOR Serine-Threonine Kinases, RPTOR, Intracellular Signaling Peptides and Proteins, Prostatic Neoplasms, Ribosomal Protein S6 Kinases, 70-kDa, Androgen Antagonists, Dihydrotestosterone, Receptor Cross-Talk, Cell biology, Receptors, Androgen, DEPTOR Gene, Signal Transduction

Abstract

It has been noticed that crosstalk between androgen receptor (AR) and mammalian target of rapamycin (mTOR) signaling pathways plays a crucial role in the proliferation of prostate cancer cells. To clarify this mechanism, we focused on DEPTOR, a naturally occurring inhibitor of mTOR. The treatment of a human AR-positive prostate cancer cell line, LNCaP, with the AR-agonist dihydrotestosterone (DHT) repressed DEPTOR mRNA expression in a time-dependent manner. This repression was abrogated by treatment with the AR-antagonist bicalutamide. Knockdown of DEPTOR mRNA by siRNA resulted in the increased phosphorylation of 70 kDa ribosomal protein S6 kinase 1 (S6K), a substrate of mTORC1, accompanied by the elevated expression of cyclin D1, a positive regulator of cell proliferation. Furthermore, the ChIP assay demonstrated that AR could bind to AR-responsible element-like region within the 4th intron of the DEPTOR gene. The amount of acetylated histone H3 (Lys9, Lys14) was reduced by the DHT treatment in this region. Taken together, these results propose that AR-dependent prostate cancer cell proliferation requires decreased DEPTOR transcription directly controlled by AR.

Published

2015

3. Polycyclic aromatic hydrocarbons induce CYP3A5 gene expression via aryl hydrocarbon receptor in HepG2 cells.

Author

Naoya Yamashita, Yuichiro Kanno, Minami Yoshikawa, Moeno Ozawa, Noriko Sanada, Kiyomitsu Nemoto, and Ryoichi Kizu

Subjects

*ARYL hydrocarbon receptors, *POLYCYCLIC aromatic hydrocarbons, *CELL receptors, *GENE expression, *GENETIC regulation, *DRUG metabolism

Abstract

The aryl hydrocarbon receptor (AhR) regulates expression of genes encoding drug/xenobiotic metabolizing enzymes. Cytochrome P450 (CYP) 3A5 is involved in drug metabolism. However, regulation of CYP3A5 gene expression is not yet well understood. In this study, we aimed to investigate the effect of the ligands of AhR on CYP3A5 gene expression. CYP3A5 mRNA expression was induced by the polycyclic aromatic hydrocarbons (PAHs) such as 3-methylcholanthrene (3MC) and benzo[a]pyrene in HepG2 cells. To determine whether the PAHs induced CYP3A5 gene expression via AhR, we generated AhR knockout (AhR KO) HepG2 cells. CYP3A5 mRNA expression was not induced by 3MC treatment in AhR KO cells. In addition, we generated AhR rescue cells from AhR KO cells and evaluated CYP3A5 mRNA expression. We found that CYP3A5 mRNA expression was induced by 3MC treatment in AhR rescue cells. Taken together, these results demonstrated that CYP3A5 mRNA expression was induced by PAHs via AhR in HepG2 cells. Our findings suggest that ligand-activated AhR affects CYP3A5-mediated drug metabolism. [ABSTRACT FROM AUTHOR]

Published

2021

4. T0901317, a potent LXR agonist, is an inverse agonist of CAR

Author

Nobuaki Tanuma, Ami Takahashi, Yoshio Inouye, and Yuichiro Kanno

Subjects

Agonist, medicine.medical_specialty, medicine.drug_class, Biology, Toxicology, Cell biology, Nuclear receptor coactivator 1, Endocrinology, Nuclear receptor, Internal medicine, Constitutive androstane receptor, medicine, Inverse agonist, Receptor, Liver X receptor, Nuclear receptor co-repressor 1

Abstract

The basal transcriptional activity of unliganded human constitutive androstane receptor (hCAR) was shown to be repressed by the potent liver X receptor (LXR) agonist, TO901317, in a concentration-dependent manner using a reporter assay in cultured cells. TO901317 also repressed the basal transcriptional activity of both mouse and rat CAR. The certified hCAR agonist, CITCO, partially reversed this repressive effect of TO901317 on hCAR basal activity. Unlike hCAR, a three alanine insertion mutant and the splice variant 2 of hCAR require agonists, such as CITCO, to become transcriptionally active and the CITCO-induced reporter activity was repressed by TO901317. As has been previously shown for the typical hCAR inverse agonist, PK11195, TO901317 blocked the interaction of hCAR with steroid receptor co-activator 1 (SRC1). In contrast, the interaction between hCAR and nuclear receptor corepressor 1 (NCoR1) was promoted by PK11195 and TO901317. Furthermore, the hCAR-mediated basal induction of endogenous cytochrome P450 2B6 (CYP2B6) mRNA was adversely affected by co-treatment with TO901317.

Published

2013

5. Androgen receptor functions as a negative transcriptional regulator of DEPTOR, mTOR inhibitor.

Author

Yuichiro Kanno, Shuai Zhao, Naoya Yamashita, Kazuyuki Yanai, Kiyomitsu Nemoto, and Yoshio Inouye

Subjects

*ANDROGEN receptors, *PROSTATE cancer, *CANCER cells, *RAPAMYCIN, *PROTEIN kinases, *CELL cycle

Abstract

It has been noticed that crosstalk between androgen receptor (AR) and mammalian target of rapamycin (mTOR) signaling pathways plays a crucial role in the proliferation of prostate cancer cells. To clarify this mechanism, we focused on DEPTOR, a naturally occurring inhibitor of mTOR. The treatment of a human AR-positive prostate cancer cell line, LNCaP, with the AR-agonist dihydrotestosterone (DHT) repressed DEPTOR mRNA expression in a time-dependent manner. This repression was abrogated by treatment with the AR-antagonist bicalutamide. Knockdown of DEPTOR mRNA by siRNA resulted in the increased phosphorylation of 70 kDa ribosomal protein S6 kinase 1 (S6K), a substrate of mTORC1, accompanied by the elevated expression of cyclin D1, a positive regulator of cell proliferation. Furthermore, the ChIP assay demonstrated that AR could bind to AR-responsible element-like region within the 4th intron of the DEPTOR gene. The amount of acetylated histone H3 (Lys9, Lys14) was reduced by the DHT treatment in this region. Taken together, these results propose that AR-dependent prostate cancer cell proliferation requires decreased DEPTOR transcription directly controlled by AR. [ABSTRACT FROM AUTHOR]

Published

2015

6. T0901317, a potent LXR agonist, is an inverse agonist of CAR.

Author

Yuichiro Kanno, Nobuaki Tanuma, Ami Takahashi, and Yoshio Inouye

Subjects

*ANDROSTANE receptors, *GENETIC transcription, *CELL culture, *NUCLEAR receptors (Biochemistry), *ANIMAL models in research, *CELL communication, *GENETIC repressors, *CYTOCHROME P-450

Abstract

The basal transcriptional activity of unliganded human constitutive androstane receptor (hCAR) was shown to be repressed by the potent liver X receptor (LXR) agonist, T0901317, in a concentration-dependent manner using a reporter assay in cultured cells. T0901317 also repressed the basal transcriptional activity of both mouse and rat CAR. The certified hCAR agonist, CITCO, partially reversed this repressive effect of T0901317 on hCAR basal activity. Unlike hCAR, a three alanine insertion mutant and the splice variant 2 of hCAR require agonists, such as CITCO, to become transcriptionally active and the CITCO-induced reporter activity was repressed by T0901317. As has been previously shown for the typical hCAR inverse agonist, PK11195, T0901317 blocked the interaction of hCAR with steroid receptor co-activator 1 (SRC1). In contrast, the interaction between hCAR and nuclear receptor corepressor 1 (NCoR1) was promoted by PK11195 and T0901317. Furthermore, the hCAR-mediated basal induction of endogenous cytochrome P450 2B6 (CYP2B6) mRNA was adversely affected by co-treatment with T0901317. [ABSTRACT FROM AUTHOR]

Published

2013