Electrophysiological evaluation of pentamidine and 17-AAG in human stem cell-derived cardiomyocytes for safety assessment

Yumiko Asahi¹, Fumimasa Nomura², Yasuyuki Abe³, Masafumi Doi³, Tomoko Sakakura³, Kiyoshi Takasuna³, Kenji Yasuda⁴

Affiliations

¹ Medicinal Safety Research Laboratories, Daiichi Sankyo Co., Ltd., 1-16-13 Edogawa, Tokyo 134-8630, Japan. Electronic address: okimoto.yumiko.bc@daiichisankyo.co.jp.
² Institute of Biomaterials and Bioengineering, Tokyo Medical and Dental University, 2-3-10 Kanda-Surugadai, Chiyoda, Tokyo 101-0062, Japan.
³ Medicinal Safety Research Laboratories, Daiichi Sankyo Co., Ltd., 1-16-13 Edogawa, Tokyo 134-8630, Japan.
⁴ Institute of Biomaterials and Bioengineering, Tokyo Medical and Dental University, 2-3-10 Kanda-Surugadai, Chiyoda, Tokyo 101-0062, Japan; Organization for University Research Initiatives, Waseda University, 3-14-9 Okubo, Shinjuku, Tokyo 169-0072, Japan; Waseda Bioscience Research Institute in Singapore (WABOIS), Helios, 11 Biopolis Way, 138667, Singapore; Department of Pure and Applied Physics, Graduate School of Advanced Science and Engineering, Waseda University, 3-4-1 Okubo, Shinjuku, Tokyo 169-8555, Japan; Department of Physics, School of Advanced Science and Engineering, Waseda University, 3-4-1 Okubo, Shinjuku, Tokyo 169-8555, Japan.

PMID: 30391349
DOI: 10.1016/j.ejphar.2018.10.046

Electrophysiological evaluation of pentamidine and 17-AAG in human stem cell-derived cardiomyocytes for safety assessment

Yumiko Asahi et al. Eur J Pharmacol. 2019.

. 2019 Jan 5:842:221-230.

doi: 10.1016/j.ejphar.2018.10.046. Epub 2018 Nov 1.

Authors

Yumiko Asahi¹, Fumimasa Nomura², Yasuyuki Abe³, Masafumi Doi³, Tomoko Sakakura³, Kiyoshi Takasuna³, Kenji Yasuda⁴

Affiliations

¹ Medicinal Safety Research Laboratories, Daiichi Sankyo Co., Ltd., 1-16-13 Edogawa, Tokyo 134-8630, Japan. Electronic address: okimoto.yumiko.bc@daiichisankyo.co.jp.
² Institute of Biomaterials and Bioengineering, Tokyo Medical and Dental University, 2-3-10 Kanda-Surugadai, Chiyoda, Tokyo 101-0062, Japan.
³ Medicinal Safety Research Laboratories, Daiichi Sankyo Co., Ltd., 1-16-13 Edogawa, Tokyo 134-8630, Japan.
⁴ Institute of Biomaterials and Bioengineering, Tokyo Medical and Dental University, 2-3-10 Kanda-Surugadai, Chiyoda, Tokyo 101-0062, Japan; Organization for University Research Initiatives, Waseda University, 3-14-9 Okubo, Shinjuku, Tokyo 169-0072, Japan; Waseda Bioscience Research Institute in Singapore (WABOIS), Helios, 11 Biopolis Way, 138667, Singapore; Department of Pure and Applied Physics, Graduate School of Advanced Science and Engineering, Waseda University, 3-4-1 Okubo, Shinjuku, Tokyo 169-8555, Japan; Department of Physics, School of Advanced Science and Engineering, Waseda University, 3-4-1 Okubo, Shinjuku, Tokyo 169-8555, Japan.

PMID: 30391349
DOI: 10.1016/j.ejphar.2018.10.046

Abstract

Human ether-a-go-go-related gene (hERG) trafficking inhibition is known to be one of the mechanisms of indirect hERG inhibition, resulting in QT prolongation and lethal arrhythmia. Pentamidine, an antiprotozoal drug, causes QT prolongation/Torsades de Pointes (TdP) via hERG trafficking inhibition, but 17-AAG, a geldanamycin derivative heat shock protein 90 (Hsp90) inhibitor, has not shown torsadogenic potential clinically, despite Hsp90 inhibitors generally being hypothesized to cause TdP by hERG trafficking inhibition. In the present study, we investigated the underlying mechanisms of both drugs' actions on hERG channels using hERG-overexpressing CHO cells (hERG-CHOs) and human embryonic stem cell-derived cardiomyocytes (hES-CMs). The effects on hERG tail current and protein levels were evaluated using population patch clamp and Western blotting in hERG-CHOs. The effects on field potential duration (FPD) were recorded by a multi-electrode array (MEA) in hES-CMs. Neither drug affected hERG tail current acutely. Chronic treatment with each drug inhibited hERG tail current and decreased the mature form of hERG protein in hERG-CHOs, whereas the immature form of hERG protein was increased by pentamidine but decreased by 17-AAG. In MEA assays using hES-CMs, pentamidine time-dependently prolonged FPD, but 17-AAG shortened it. The FPD prolongation in hES-CMs upon chronic pentamidine exposure is relevant to its clinically reported arrhythmic risk. Cav1.2 or Nav1.5 current were not reduced by chronic application of either drug at a relevant concentration to hERG trafficking inhibition in human embryonic kidney (HEK293) cells. Therefore, the reason why chronic 17-AAG shortened the FPD despite the hERG trafficking inhibition occur is still unknown.

Keywords: 17-AAG; Arrhythmia; Hsp90 inhibitor; Human embryonic stem cell derived-cardiomyocytes (hES-CMs); Multi-electrode array (MEA); hERG trafficking.

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Electrophysiological evaluation of pentamidine and 17-AAG in human stem cell-derived cardiomyocytes for safety assessment

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Electrophysiological evaluation of pentamidine and 17-AAG in human stem cell-derived cardiomyocytes for safety assessment

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Abstract

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