作者
Leslie B Gordon, Monica E Kleinman, David T Miller, Donna S Neuberg, Anita Giobbie-Hurder, Marie Gerhard-Herman, Leslie B Smoot, Catherine M Gordon, Robert Cleveland, Brian D Snyder, Brian Fligor, W Robert Bishop, Paul Statkevich, Amy Regen, Andrew Sonis, Susan Riley, Christine Ploski, Annette Correia, Nicolle Quinn, Nicole J Ullrich, Ara Nazarian, Marilyn G Liang, Susanna Y Huh, Armin Schwartzman, Mark W Kieran
发表日期
2012/10/9
期刊
Proceedings of the National Academy of Sciences
卷号
109
期号
41
页码范围
16666-16671
出版商
National Academy of Sciences
简介
Hutchinson–Gilford progeria syndrome (HGPS) is an extremely rare, fatal, segmental premature aging syndrome caused by a mutation in LMNA that produces the farnesylated aberrant lamin A protein, progerin. This multisystem disorder causes failure to thrive and accelerated atherosclerosis leading to early death. Farnesyltransferase inhibitors have ameliorated disease phenotypes in preclinical studies. Twenty-five patients with HGPS received the farnesyltransferase inhibitor lonafarnib for a minimum of 2 y. Primary outcome success was predefined as a 50% increase over pretherapy in estimated annual rate of weight gain, or change from pretherapy weight loss to statistically significant on-study weight gain. Nine patients experienced a ≥50% increase, six experienced a ≥50% decrease, and 10 remained stable with respect to rate of weight gain. Secondary outcomes included decreases in arterial pulse wave …
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LB Gordon, ME Kleinman, DT Miller, DS Neuberg… - Proceedings of the National Academy of Sciences, 2012