期刊
APOPTOSIS
卷 26, 期 1-2, 页码 71-82出版社
SPRINGER
DOI: 10.1007/s10495-020-01647-9
关键词
Cyt c; LRG1; Apaf-1; Survival factor; MCF-7 cells
资金
- Minnesota Medical Foundation
- University of Minnesota Graduate School
- National Science Foundation [9871237, NSF-DBI-0215759]
- National Institutes of Health [R01 CA157971]
Intracellular LRG1 protects against apoptosis by raising the threshold of cytoplasmic Cyt c required to induce apoptosis and preventing the onset of the intrinsic pathway. This survival mechanism is likely distinct from its extracellular survival function reported by several research groups.
Leucine-rich alpha-2-glycoprotein-1 (LRG1) has been shown to compete with apoptosis activating factor-1 (Apaf-1) for binding cytochrome c (Cyt c) and could play a role in inhibition of apoptosis. Employing MCF-7 breast cancer cells, we report that intracellular LRG1 does protect against apoptosis. Thus, cells transfected with the lrg1 gene and expressing higher levels of LRG1 were more resistant to hydrogen peroxide-induced apoptosis than parental cells, while cells in which LRG mRNA was knocked down by short hairpin (sh) RNA-induced degradation were more sensitive. The amount of Cyt c co-immunoprecipitated with Apaf-1 from the cytosol of apoptotic cells was inversely related to the level of LRG1 expression. In lrg1-transfected cells partially-glycosylated LRG1 was found in the cytosol and there was an increase in cytosolic Cyt c in live lrg1-transfected cells relative to parental cells. However, apoptosis was not spontaneously induced because Cyt c was bound to LRG1 and not to Apaf-1. Cyt c was the only detectable protein co-immunoprecipitated with LRG1. Following hydrogen peroxide treatment degradation of LRG1 allowed for induction of apoptosis. We propose that intracellular LRG1 raises the threshold of cytoplasmic Cyt c required to induce apoptosis and, thus, prevents onset of the intrinsic pathway in cells where Cyt c release from mitochondria does not result from committed apoptotic signaling. This mechanism of survival afforded by LRG1 is likely to be distinct from its extracellular survival function that has been reported by several research groups.
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