Defects in the biogenesis of lamin A from its farnesylated precursor, prelamin A, lead to the accumulation of prelamin A at the nuclear envelope, cause misshapen nuclei, and result in progeroid syndromes. A deficiency in ZMPSTE24, a protease involved in prelamin A processing, leads to prelamin A accumulation, an absence of mature lamin A, misshapen nuclei, and a lethal perinatal progeroid syndrome: restrictive dermopathy (RD). HutchinsonGilford progeria syndrome (HGPS) is caused by a mutant prelamin A that cannot be processed to lamin A. The hallmark cellular abnormality in RD and HGPS is misshapen nuclei. We hypothesized that the farnesylation of prelamin A is important for its targeting to the nuclear envelope in RD and HGPS and that blocking farnesylation would ameliorate the nuclear shape abnormalities. Indeed, when RD fibroblasts were treated with a farnesyltransferase inhibitor (FTI), prelamin A was partially mislocalized away from the nuclear envelope, and the frequency of nuclear shape abnormalities was reduced (P < 0.0001). A FTI also mislocalized prelamin A and improved nuclear shape in Zmpste24-deficient mouse embryonic fibroblasts (P < 0.0001) and improved nuclear shape in human HGPS fibroblasts (P < 0.0001). Most remarkably, a FTI significantly improved nuclear shape in two fibroblast cell lines from atypical progeria patients with lamin A missense mutations in the absence of prelamin A accumulation (P ؍ 0.0003 and P < 0.0001). These findings establish a paradigm for ameliorating the most obvious cellular pathology in lamin-related progeroid syndromes and suggest a potential strategy for treating these diseases.aging ͉ Hutchinson-Gilford progeria syndrome ͉ lamin ͉ restrictive dermopathy ͉ ZMPSTE24 T wo progerioid disorders in humans, restrictive dermopathy (RD) and Hutchinson-Gilford progeria syndrome (HGPS), are caused by defective biogenesis of lamin A from prelamin A, a farnesylated precursor protein (1-3). RD is a lethal perinatal progeroid disorder characterized by retarded growth, tight and rigid skin, alopecia, micrognathia, and other bone abnormalities. RD is caused by a deficiency in ZMPSTE24 (1, 2), a protease required for the endoproteolytic processing of prelamin A to mature lamin A (4, 5). HGPS is characterized by retarded growth, partial lipodystrophy, osteoporosis, osteolytic lesions, thin skin, micrognathia, and premature atherosclerosis (3). HGPS is caused by a mutant form of prelamin A (commonly called progerin) that cannot be processed to mature lamin A (3). Lamin A is a key protein within the nuclear lamina, an intermediate filament meshwork lining the inner nuclear membrane that provides structural support for the nucleus (6).Some progeroid syndromes are caused by missense mutations in LMNA (the gene for prelamin A and lamin C) (7,8). For example, E578V and R644C mutations cause progeroid disorders and are associated with nuclear shape abnormalities (8). In these cases, the structural abnormality in lamin A is apparently sufficient to impair nuclear envelope integrity and cau...
