A farnesyltransferase inhibitor improves disease phenotypes in mice with a Hutchinson-Gilford progeria syndrome mutation
Shao H. Yang, … , Stephen G. Young, Loren G. Fong
Shao H. Yang, … , Stephen G. Young, Loren G. Fong
Published August 1, 2006
Citation Information: J Clin Invest. 2006;116(8):2115-2121. https://doi.org/10.1172/JCI28968.
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A farnesyltransferase inhibitor improves disease phenotypes in mice with a Hutchinson-Gilford progeria syndrome mutation

Abstract

Hutchinson-Gilford progeria syndrome (HGPS) is caused by the production of a truncated prelamin A, called progerin, which is farnesylated at its carboxyl terminus. Progerin is targeted to the nuclear envelope and causes misshapen nuclei. Protein farnesyltransferase inhibitors (FTI) mislocalize progerin away from the nuclear envelope and reduce the frequency of misshapen nuclei. To determine whether an FTI would ameliorate disease phenotypes in vivo, we created gene-targeted mice with an HGPS mutation (LmnaHG/+) and then examined the effect of an FTI on disease phenotypes. LmnaHG/+ mice exhibited phenotypes similar to those in human HGPS patients, including retarded growth, reduced amounts of adipose tissue, micrognathia, osteoporosis, and osteolytic lesions in bone. Osteolytic lesions in the ribs led to spontaneous bone fractures. Treatment with an FTI increased adipose tissue mass, improved body weight curves, reduced the number of rib fractures, and improved bone mineralization and bone cortical thickness. These studies suggest that FTIs could be useful for treating humans with HGPS.

Authors

Shao H. Yang, Margarita Meta, Xin Qiao, David Frost, Joy Bauch, Catherine Coffinier, Sharmila Majumdar, Martin O. Bergo, Stephen G. Young, Loren G. Fong

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Figure 3

LmnaHG/HG mice are small and have poorly mineralized bone.

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LmnaHG/HG mice are small and have poorly mineralized ...
(A and B) Photographs of 17-day-old Lmna+/+ (A) and LmnaHG/HG (B) mice. The LmnaHG/HG mouse had a spontaneous fracture in the left forelimb (red arrow). (CF) Surface renderings of μCT scans of the skull (performed at exactly the same threshold) for a 17-day-old LmnaHG/HG mouse (D and F) and littermate Lmna+/+ mouse (C and E). (C and D) Top view of skulls. The LmnaHG/HG skull is misshapen, poorly mineralized, and exhibits incomplete fusion of the cranial sutures (red arrow). (E and F) Lateral view of skulls. The LmnaHG/HG skull is misshapen, with a small mandible (upper red arrow) and a short lower incisor (lower red arrow).