文章基本信息

标题：Thematic Review Series: Lipid Posttranslational Modifications. Prelamin A, Zmpste24, misshapen cell nuclei, and progeria--new evidence suggesting that protein farnesylation could be important for disease pathogenesis
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作者：Young, Stephen G. ; Fong, Loren G. ; Michaelis, Susan 等
期刊名称：JLR Papers In Press
印刷版ISSN：0022-2275
电子版ISSN：1539-7262
出版年度：2005
卷号：46
期号：12
页码：2531-2558
DOI：10.1194/jlr.R500011-JLR200
出版社：American Society for Biochemistry and Molecular Biology
摘要：Prelamin A undergoes multistep processing to yield lamin A,a structural protein of the nuclear lamina. Prelamin A terminateswith a CAAX motif, which triggers farnesylation of a C-terminalcysteine (the C of the CAAX motif), endoproteolytic releaseof the last three amino acids (the AAX), and methylation ofthe newly exposed farnesylcysteine residue. In addition, prelaminA is cleaved a second time, releasing 15 more residues fromthe C terminus (including the farnesylcysteine methyl ester),generating mature lamin A. This second cleavage step is carriedout by an endoplasmic reticulum membrane protease, ZMPSTE24.Interest in the posttranslational processing of prelamin A hasincreased with the recognition that certain progeroid syndromescan be caused by mutations that lead to an accumulation of farnesyl-prelaminA. Recently, we showed that a key cellular phenotype of theseprogeroid disorders, misshapen cell nuclei, can be amelioratedby inhibitors of protein farnesylation, suggesting a potentialstrategy for treating these diseases. In this article, we review the posttranslational processingof prelamin A, describe several mouse models for progeroid syndromes,explain the mutations underlying several human progeroid syndromes,and summarize recent data showing that misshapen nuclei canbe ameliorated by treating cells with protein farnesyltransferaseinhibitors. Supplementary key words protein prenylation • laminopathy • aging • Ste24 • a-factor • lamin A/C