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Literature DB >> 20724468

Characterization of HACD1 K64Q mutant found in arrhythmogenic right ventricular dysplasia patients.

Hiroyuki Konishi¹, Ayaka Okuda, Yusuke Ohno, Akio Kihara.

Abstract

Arrhythmogenic right ventricular dysplasia (ARVD) is an autosomal dominant heart disease. A K64Q mutation was found in ARVD-affected individuals in the HACD1 gene, which encodes an enzyme involved in very long-chain fatty acid (VLCFA) elongation, although any relationship between mutation and pathology remained unclear. Here, we demonstrate that HACD1 (K64Q) exhibits normal enzyme activity, intracellular localization and interaction with other VLCFA enzymes, with no dominant negative effect on VLCFA elongation. Thus, it appears unlikely that this mutation is ARVD-causative. Moreover, through these analyses we found that HACD1 interacts with KAR and TER, the reductase enzymes involved in the second and fourth VLCFA elongation cycle, respectively. This finding indicates that the enzymes responsible for the VLCFA elongation cycle form an elongase complex.

Entities: Chemical Disease Gene Species

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Year: 2010 PMID： 20724468 DOI： 10.1093/jb/mvq092

Source DB: PubMed Journal: J Biochem ISSN： 0021-924X Impact factor: 3.387

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8. Identification of Key Pathways and Genes in Obesity Using Bioinformatics Analysis and Molecular Docking Studies.

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8 in total

Characterization of HACD1 K64Q mutant found in arrhythmogenic right ventricular dysplasia patients.

1. Protein tyrosine phosphatase-like A regulates myoblast proliferation and differentiation through MyoG and the cell cycling signaling pathway.

2. Hetero-oligomeric interactions of an ELOVL4 mutant protein: implications in the molecular mechanism of Stargardt-3 macular dystrophy.

3. Deciphering mutant ELOVL4 activity in autosomal-dominant Stargardt macular dystrophy.

4. Endoplasmic reticulum microenvironment and conserved histidines govern ELOVL4 fatty acid elongase activity.

Review 5. Novel Cellular Functions of Very Long Chain-Fatty Acids: Insight From ELOVL4 Mutations.

6. Congenital myopathy is caused by mutation of HACD1.

7. Two modes of regulation of the fatty acid elongase ELOVL6 by the 3-ketoacyl-CoA reductase KAR in the fatty acid elongation cycle.

8. Identification of Key Pathways and Genes in Obesity Using Bioinformatics Analysis and Molecular Docking Studies.