Early Embryonic Lethality Caused by Targeted Disruption of the 3-hydroxy-3-methylglutaryl-CoA Reductase Gene

Overview

Journal J Biol Chem

Specialty Biochemistry

Date 2003 Aug 16

PMID 12920113

Citations 48

Authors

Ken Ohashi

Jun-Ichi Osuga

Ryuichi Tozawa

Tetsuya Kitamine

Hiroaki Yagyu

Motohiro Sekiya

Sachiko Tomita

Hiroaki Okazaki

Yoshiaki Tamura

Naoya Yahagi

Yoko Iizuka

Kenji Harada

Takanari Gotoda

Hitoshi Shimano

Nobuhiro Yamada

Shun Ishibashi

Affiliations

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Abstract

The endoplasmic reticulum (ER) enzyme 3-hydroxy-3-methylglutaryl coenzyme A (HMG-CoA) reductase, which converts HMG-CoA to mevalonate, catalyzes the ratelimiting step in cholesterol biosynthesis. Because this mevalonate pathway also produces several non-sterol isoprenoid compounds, the level of HMG-CoA reductase activity may coordinate many cellular processes and functions. We used gene targeting to knock out the mouse HMG-CoA reductase gene. The heterozygous mutant mice (Hmgcr+/-) appeared normal in their development and gross anatomy and were fertile. Although HMG-CoA reductase activities were reduced in Hmgcr+/- embryonic fibroblasts, the enzyme activities and cholesterol biosynthesis remained unaffected in the liver from Hmgcr+/- mice, suggesting that the haploid amount of Hmgcr gene is not rate-limiting in the hepatic cholesterol homeostasis. Consistently, plasma lipoprotein profiles were similar between Hmgcr+/- and Hmgcr+/+ mice. In contrast, the embryos homozygous for the Hmgcr mutant allele were recovered at the blastocyst stage, but not at E8.5, indicating that HMG-CoA reductase is crucial for early development of the mouse embryos. The lethal phenotype was not completely rescued by supplementing the dams with mevalonate. Although it has been postulated that a second, peroxisome-specific HMG-CoA reductase could substitute for the ER reductase in vitro, we speculate that the putative peroxisomal reductase gene, if existed, does not fully compensate for the lack of the ER enzyme at least in embryogenesis.

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