Selective PPARα Modulator Pemafibrate and Sodium-Glucose Cotransporter 2 Inhibitor Tofogliflozin Combination Treatment Improved Histopathology in Experimental Mice Model of Non-Alcoholic Steatohepatitis

Kentaro Murakami; Yusuke Sasaki; Masato Asahiyama; Wataru Yano; Toshiaki Takizawa; Wakana Kamiya; Yoshihiro Matsumura; Motonobu Anai; Tsuyoshi Osawa; Jean-Charles Fruchart; Jamila Fruchart-Najib; Hiroyuki Aburatani; Juro Sakai; Tatsuhiko Kodama; Toshiya Tanaka

doi:10.3390/cells11040720

Cells (Feb 2022)

Selective PPARα Modulator Pemafibrate and Sodium-Glucose Cotransporter 2 Inhibitor Tofogliflozin Combination Treatment Improved Histopathology in Experimental Mice Model of Non-Alcoholic Steatohepatitis

Kentaro Murakami,
Yusuke Sasaki,
Masato Asahiyama,
Wataru Yano,
Toshiaki Takizawa,
Wakana Kamiya,
Yoshihiro Matsumura,
Motonobu Anai,
Tsuyoshi Osawa,
Jean-Charles Fruchart,
Jamila Fruchart-Najib,
Hiroyuki Aburatani,
Juro Sakai,
Tatsuhiko Kodama,
Toshiya Tanaka

Affiliations

Kentaro Murakami: Department of Nuclear Receptor Medicine, Laboratories for Systems Biology and Medicine (LSBM) at the Research Center for Advanced Science and Technology (RCAST), The University of Tokyo, Tokyo 153-8904, Japan
Yusuke Sasaki: Department of Nuclear Receptor Medicine, Laboratories for Systems Biology and Medicine (LSBM) at the Research Center for Advanced Science and Technology (RCAST), The University of Tokyo, Tokyo 153-8904, Japan
Masato Asahiyama: Pharmaceutical Division, Kowa Company, Ltd., Tokyo 189-0022, Japan
Wataru Yano: Pharmaceutical Division, Kowa Company, Ltd., Tokyo 189-0022, Japan
Toshiaki Takizawa: Pharmaceutical Division, Kowa Company, Ltd., Tokyo 189-0022, Japan
Wakana Kamiya: Department of Nuclear Receptor Medicine, Laboratories for Systems Biology and Medicine (LSBM) at the Research Center for Advanced Science and Technology (RCAST), The University of Tokyo, Tokyo 153-8904, Japan
Yoshihiro Matsumura: Division of Metabolic Medicine, Laboratories for Systems Biology and Medicine (LSBM) at the Research Center for Advanced Science and Technology (RCAST), The University of Tokyo, Tokyo 153-8904, Japan
Motonobu Anai: Department of Nuclear Receptor Medicine, Laboratories for Systems Biology and Medicine (LSBM) at the Research Center for Advanced Science and Technology (RCAST), The University of Tokyo, Tokyo 153-8904, Japan
Tsuyoshi Osawa: Division of Integrative Nutriomics and Oncology, Laboratories for Systems Biology and Medicine (LSBM) at the Research Center for Advanced Science and Technology (RCAST), The University of Tokyo, Tokyo 153-8904, Japan
Jean-Charles Fruchart: R3i Foundation, Picassoplatz 8, 4010 Basel, Switzerland
Jamila Fruchart-Najib: R3i Foundation, Picassoplatz 8, 4010 Basel, Switzerland
Hiroyuki Aburatani: Genome Science Division, Laboratories for Systems Biology and Medicine (LSBM) at the Research Center for Advanced Science and Technology (RCAST), The University of Tokyo, Tokyo 153-8904, Japan
Juro Sakai: Division of Metabolic Medicine, Laboratories for Systems Biology and Medicine (LSBM) at the Research Center for Advanced Science and Technology (RCAST), The University of Tokyo, Tokyo 153-8904, Japan
Tatsuhiko Kodama: Department of Nuclear Receptor Medicine, Laboratories for Systems Biology and Medicine (LSBM) at the Research Center for Advanced Science and Technology (RCAST), The University of Tokyo, Tokyo 153-8904, Japan
Toshiya Tanaka: Department of Nuclear Receptor Medicine, Laboratories for Systems Biology and Medicine (LSBM) at the Research Center for Advanced Science and Technology (RCAST), The University of Tokyo, Tokyo 153-8904, Japan

DOI: https://doi.org/10.3390/cells11040720
Journal volume & issue: Vol. 11, no. 4
p. 720

Abstract

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Ballooning degeneration of hepatocytes is a major distinguishing histological feature of non-alcoholic steatosis (NASH) progression that can lead to cirrhosis and hepatocellular carcinoma (HCC). In this study, we evaluated the effect of the selective PPARα modulator (SPPARMα) pemafibrate (Pema) and sodium-glucose cotransporter 2 (SGLT2) inhibitor tofogliflozin (Tofo) combination treatment on pathological progression in the liver of a mouse model of NASH (STAM) at two time points (onset of NASH progression and HCC survival). At both time points, the Pema and Tofo combination treatment significantly alleviated hyperglycemia and hypertriglyceridemia. The combination treatment significantly reduced ballooning degeneration of hepatocytes. RNA-seq analysis suggested that Pema and Tofo combination treatment resulted in an increase in glyceroneogenesis, triglyceride (TG) uptake, lipolysis and liberated fatty acids re-esterification into TG, lipid droplet (LD) formation, and Cidea/Cidec ratio along with an increased number and reduced size and area of LDs. In addition, combination treatment reduced expression levels of endoplasmic reticulum stress-related genes (Ire1a, Grp78, Xbp1, and Phlda3). Pema and Tofo treatment significantly improved survival rates and reduced the number of tumors in the liver compared to the NASH control group. These results suggest that SPPARMα and SGLT2 inhibitor combination therapy has therapeutic potential to prevent NASH-HCC progression.

Published in Cells

ISSN: 2073-4409 (Online)
Publisher: MDPI AG
Country of publisher: Switzerland
LCC subjects: Science: Biology (General): Cytology
Website: https://www.mdpi.com/journal/cells

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