Celia Lopez-Herrera scite author profile

Celia Lopez-Herrera

2Publications

66Citation Statements Received

82Citation Statements Given

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Affiliations

Abivax (France), Institut de Génétique Moléculaire de Montpellier, French National Centre for Scientific Research

Publications

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Antagonistic functions of LMNA isoforms in energy expenditure and lifespan

et al. 2014

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Alternative RNA processing of LMNA pre-mRNA produces three main protein isoforms, that is, lamin A, progerin, and lamin C. De novo mutations that favor the expression of progerin over lamin A lead to Hutchinson-Gilford progeria syndrome (HGPS), providing support for the involvement of LMNA processing in pathological aging. Lamin C expression is mutually exclusive with the splicing of lamin A and progerin isoforms and occurs by alternative polyadenylation. Here, we investigate the function of lamin C in aging and metabolism using mice that express only this isoform. Intriguingly, these mice live longer, have decreased energy metabolism, increased weight gain, and reduced respiration. In contrast, progerin-expressing mice show increased energy metabolism and are lipodystrophic. Increased mitochondrial biogenesis is found in adipose tissue from HGPS-like mice, whereas lamin C-only mice have fewer mitochondria. Consistently, transcriptome analyses of adipose tissues from HGPS and lamin C-only mice reveal inversely correlated expression of key regulators of energy expenditure, including Pgc1a and Sfrp5. Our results demonstrate that LMNA encodes functionally distinct isoforms that have opposing effects on energy metabolism and lifespan in mammals.

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Pharmacological modulation of LMNA SRSF1-dependent splicing abrogates diet-induced obesity in mice

et al. 2016

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