A Human IPSC-derived Hepatocyte Screen Identifies Compounds That Inhibit Production of Apolipoprotein B

Overview

Journal Commun Biol

Specialty Biology

Date 2023 Apr 24

PMID 37095219

Authors

Jui-Tung Liu

Caren Doueiry

Yu-Lin Jiang

Josef Blaszkiewicz

Mary Paige Lamprecht

James A Heslop

Yuri K Peterson

Juliana Debrito Carten

Paula Traktman

Yang Yuan

Salman R Khetani

Waleed O Twal

Stephen A Duncan

Affiliations

Soon will be listed here.

Abstract

Familial hypercholesterolemia (FH) patients suffer from excessively high levels of Low Density Lipoprotein Cholesterol (LDL-C), which can cause severe cardiovascular disease. Statins, bile acid sequestrants, PCSK9 inhibitors, and cholesterol absorption inhibitors are all inefficient at treating FH patients with homozygous LDLR gene mutations (hoFH). Drugs approved for hoFH treatment control lipoprotein production by regulating steady-state Apolipoprotein B (apoB) levels. Unfortunately, these drugs have side effects including accumulation of liver triglycerides, hepatic steatosis, and elevated liver enzyme levels. To identify safer compounds, we used an iPSC-derived hepatocyte platform to screen a structurally representative set of 10,000 small molecules from a proprietary library of 130,000 compounds. The screen revealed molecules that could reduce the secretion of apoB from cultured hepatocytes and from humanized livers in mice. These small molecules are highly effective, do not cause abnormal lipid accumulation, and share a chemical structure that is distinct from any known cholesterol lowering drug.

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