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Nurturing the genome: A-type lamins preserve genomic stability
Ignacio González-Suárez, Susana Gonzalo
Nucleus · 2010 · ▲ 44 citations
Abstract
A-type lamins provide a scaffold for tethering chromatin and protein complexes regulating nuclear structure and function. Interest in lamins increased after mutations in the LMNA gene were found to be associated with a variety of human disorders termed laminopathies. These include muscular dystrophy, cardiomyopathy, lipodystrophy, peripheral neuropathy and premature aging syndromes such as progeria. In addition, altered expression of A-type lamins is emerging as a contributing factor to tumorigenesis. How different alterations in a gene that is ubiquitously expressed can cause such an array of systemic as well as tissue specific diseases remains an enigma. Several lines of evidence indicate that mutant forms of A-type lamins impact on genome function and integrity. A current model suggests that genomic instability plays a major part in the pathophysiology of some lamin-related diseases. However, this model remains to be fully investigated. Here we discuss recent studies revealing novel functions for A-type lamins in the maintenance of telomeres and in the DNA damage response (DDR) pathway. These findings have shed some light onto the putative molecular mechanisms by which alterations in A-type lamins induce genomic instability and contribute to disease.
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- 10.4161/nucl.1.2.10797
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- 2026-06-02 MST
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APA
González-Suárez, I., & Gonzalo, S. (2010). Nurturing the genome: A-type lamins preserve genomic stability. <em>Nucleus</em>. https://doi.org/10.4161/nucl.1.2.10797
Vancouver
González-Suárez I, Gonzalo S. Nurturing the genome: A-type lamins preserve genomic stability. Nucleus. 2010. doi:10.4161/nucl.1.2.10797.
BibTeX
@unpublished{ignacio2010Nurtur,
title = {Nurturing the genome: A-type lamins preserve genomic stability},
author = {Ignacio González-Suárez and Susana Gonzalo},
journal = {Nucleus},
year = {2010},
doi = {10.4161/nucl.1.2.10797},
}
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