LMNA公司
拉明
生物
NAD+激酶
早熟
早衰
染色质
细胞生物学
线粒体
线粒体DNA
DNA修复
DNA损伤
遗传学
分子生物学
基因
生物化学
DNA
酶
作者
Scott Maynard,Arnaldur Hall,Panagiotis Galanos,Salvatore Rizza,Tatsuro Yamamoto,Helena Hagner Gram,Sebastian Howen Nesgaard Munk,Muhammad Shoaib,Claus Storgaard Sørensen,Vilhelm A. Bohr,Mads Lerdrup,Apolinar Maya‐Mendoza,Jiří Bártek
摘要
Abstract Mutations in the lamin A/C gene (LMNA) cause laminopathies such as the premature aging Hutchinson Gilford progeria syndrome (HGPS) and altered lamin A/C levels are found in diverse malignancies. The underlying lamin-associated mechanisms remain poorly understood. Here we report that lamin A/C-null mouse embryo fibroblasts (Lmna−/− MEFs) and human progerin-expressing HGPS fibroblasts both display reduced NAD+ levels, unstable mitochondrial DNA and attenuated bioenergetics. This mitochondrial dysfunction is associated with reduced chromatin recruitment (Lmna−/− MEFs) or low levels (HGPS) of PGC1α, the key transcription factor for mitochondrial homeostasis. Lmna−/− MEFs showed reduced expression of the NAD+-biosynthesis enzyme NAMPT and attenuated activity of the NAD+-dependent deacetylase SIRT1. We find high PARylation in lamin A/C-aberrant cells, further decreasing the NAD+ pool and consistent with impaired DNA base excision repair in both cell models, a condition that fuels DNA damage-induced PARylation under oxidative stress. Further, ATAC-sequencing revealed a substantially altered chromatin landscape in Lmna−/− MEFs, including aberrantly reduced accessibility at the Nampt gene promoter. Thus, we identified a new role of lamin A/C as a key modulator of mitochondrial function through impairments of PGC1α and the NAMPT-NAD+ pathway, with broader implications for the aging process.
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