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Profilin I is essential for cell survival and cell division in early mouse development

Authors :
Maya Arai
David J. Kwiatkowski
Walter Witke
Arlene H. Sharpe
James D. Sutherland
Publication Year :
2001
Publisher :
The National Academy of Sciences, 2001.

Abstract

Profilins are thought to play a central role in the regulation of de novo actin assembly by preventing spontaneous actin polymerization through the binding of actin monomers, and the adding of monomeric actin to the barbed actin-filament ends. Other cellular functions of profilin in membrane trafficking and lipid based signaling are also likely. Binding of profilins to signaling molecules such as Arp2/3 complex, Mena, VASP, N - WASP, dynamin I, and others, further implicates profilin and actin as regulators of diverse motile activities. In mouse, two profilins are expressed from two distinct genes. Profilin I is expressed at high levels in all tissues and throughout development, whereas profilin II is expressed in neuronal cells. To examine the function of profilin I in vivo , we generated a null profilin I ( pfn1 ko ) allele in mice. Homozygous pfn1 ko/ko mice are not viable. Pfn1 ko/ko embryos died as early as the two-cell stage, and no pfn1 ko/ko blastocysts were detectable. Adult pfn1 ko/wt mice show a 50% reduction in profilin I expression with no apparent impairment of cell function. However, pfn1 ko/wt embryos have reduced survival during embryogenesis compared with wild type. Although weakly expressed in early embryos, profilin II cannot compensate for lack of profilin I. Our results indicate that mouse profilin I is an essential protein that has dosage-dependent effects on cell division and survival during embryogenesis.

Details

Language :
English
Database :
OpenAIRE
Accession number :
edsair.doi.dedup.....45619f71b3fa02dc3a3636d4691c81a4