Progerin elicits disease phenotypes of progeria in mice whether or not it is farnesylated
Shao H. Yang, … , Stephen G. Young, Loren G. Fong
Shao H. Yang, … , Stephen G. Young, Loren G. Fong
Published September 2, 2008
Citation Information: J Clin Invest. 2008;118(10):3291-3300. https://doi.org/10.1172/JCI35876.
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Research Article Genetics

Progerin elicits disease phenotypes of progeria in mice whether or not it is farnesylated

Abstract

Hutchinson-Gilford progeria syndrome (HGPS), a rare disease that results in what appears to be premature aging, is caused by the production of a mutant form of prelamin A known as progerin. Progerin retains a farnesyl lipid anchor at its carboxyl terminus, a modification that is thought to be important in disease pathogenesis. Inhibition of protein farnesylation improves the hallmark nuclear shape abnormalities in HGPS cells and ameliorates disease phenotypes in mice harboring a knockin HGPS mutation (LmnaHG/+). The amelioration of disease, however, is incomplete, leading us to hypothesize that nonfarnesylated progerin also might be capable of eliciting disease. To test this hypothesis, we created knockin mice expressing nonfarnesylated progerin (LmnanHG/+). LmnanHG/+ mice developed the same disease phenotypes observed in LmnaHG/+ mice, although the phenotypes were milder, and mouse embryonic fibroblasts (MEFs) derived from these mice contained fewer misshapen nuclei. The steady-state levels of progerin in LmnanHG/+ MEFs and tissues were lower, suggesting a possible explanation for the milder phenotypes. These data support the concept that inhibition of protein farnesylation in progeria could be therapeutically useful but also suggest that this approach may be limited, as progerin elicits disease phenotypes whether or not it is farnesylated.

Authors

Shao H. Yang, Douglas A. Andres, H. Peter Spielmann, Stephen G. Young, Loren G. Fong

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Figure 4

Reduced bone abnormalities in LmnanHG/+ mice at 6 months of age, as judged by surface renderings of μCT analyses.

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Reduced bone abnormalities in LmnanHG/+ mice at 6 months of age, as judg...
(AF) μCT scans of the thoracic spine illustrating reduced number of rib fractures in LmnanHG/+ mice. Red arrowheads indicate rib fractures and surrounding callus. Red arrows indicate thinning ribs along with a small amount of callus. (A and D) Lmna+/+ mouse; (B and E) LmnaHG/+ mouse; (C and F) LmnanHG/+ mouse. (DF) Lateral view of the thoracic spine illustrating reduced kyphosis of the spine in LmnanHG/+ mouse. Bone density (G) and cortical thickness (H) were improved in the ribs of LmnanHG/+ mice compared with LmnaHG/+ mice (n = 4 mice/genotype; P < 0.0001). Error bars indicate SEM.