AI Article Synopsis
- Emerin and LEM2 are crucial inner nuclear membrane proteins that, when absent, lead to abnormalities, particularly in the context of muscular dystrophy in humans.
- The study used C. elegans to investigate the effects of losing these proteins, finding that while single-null and hypomorphic animals remained viable, double-null animals faced significant developmental arrest and defects during cell division.
- The findings suggest that mutations in the human LEM2 gene may contribute to more severe muscular disorders beyond EDMD, especially given the observed reductions in lifespan and smooth muscle function in the absence of LEM-2.
Article Abstract
Emerin and LEM2 are ubiquitous inner nuclear membrane proteins conserved from humans to Caenorhabditis elegans. Loss of human emerin causes Emery-Dreifuss muscular dystrophy (EDMD). To test the roles of emerin and LEM2 in somatic cells, we used null alleles of both genes to generate C. elegans animals that were either hypomorphic (LEM-2-null and heterozygous for Ce-emerin) or null for both proteins. Single-null and hypomorphic animals were viable and fertile. Double-null animals used the maternal pool of Ce-emerin to develop to the larval L2 stage, then arrested. Nondividing somatic cell nuclei appeared normal, whereas dividing cells had abnormal nuclear envelope and chromatin organization and severe defects in postembryonic cell divisions, including the mesodermal lineage. Life span was unaffected by loss of Ce-emerin alone but was significantly reduced in LEM-2-null animals, and double-null animals had an even shorter life span. In addition to striated muscle defects, double-null animals and LEM-2-null animals showed unexpected defects in smooth muscle activity. These findings implicate human LEM2 mutations as a potential cause of EDMD and further suggest human LEM2 mutations might cause distinct disorders of greater severity, since C. elegans lacking only LEM-2 had significantly reduced life span and smooth muscle activity.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3279384 | PMC |
| http://dx.doi.org/10.1091/mbc.E11-06-0505 | DOI Listing |
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