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Deletion of growth hormone receptor gene but not visceral fat removal decreases expression of apoptosis-related genes in the kidney - Potential mechanism of lifespan extension

机译:删除生长激素受体基因但不去除内脏脂肪会降低肾脏中凋亡相关基因的表达-延长寿命的潜在机制

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摘要

Mice homozygous for the targeted disruption of the growth hormone (GH) receptor (Ghr) gene (GH receptor knockout; GHRKO; KO) are hypoinsulinemic, highly insulin sensitive, normoglycemic, and long-lived. Visceral fat removal (VFR) is a surgical intervention which improves insulin signaling in normal (N) mice and rats and extends longevity in rats. We have previously demonstrated decreased expression level of certain pro-apoptotic genes in skeletal muscles and suggested that this may contribute to the regulation of longevity in GHRKO mice. Alterations in apoptosis-related genes expression in the kidneys also may potentially lead to lifespan extension. In this context, we decided to examine the renal expression of the following genes: caspase-3, caspase-9, caspase-8, bax, bad, bcl-2, Smac/DIABLO, Apaf-1, p53, and cytochrome c1 (cyc1) in male GHRKO and N mice subjected to VFR or sham surgery, at approximately 6 months of age. The kidneys were collected 2 months after VFR. As a result, caspase-3, caspase-9, and bax expressions were decreased in KO mice as compared to N animals. Expressions of Smac/DIABLO, caspase-8, bcl-2, bad, and p53 did not differ between KOs and N mice. VFR did not change the expression of the examined genes in KO or N mice. In conclusion, endocrine abnormalities in GHRKO mice result in decreased expression of pro-apoptotic genes and VFR did not alter the examined genes expression in N and KO mice. These data are consistent with a model in which alterations of GH signaling and/or insulin sensitivity lead to increased lifespan mediated by decreased renal expression of pro-apoptotic genes.
机译:用于靶向破坏生长激素(GH)受体(Ghr)基因(GH受体敲除; GHRKO; KO)的纯合小鼠具有低胰岛素血症,高度胰岛素敏感性,血糖正常且寿命长。内脏脂肪去除(VFR)是一种外科手术,可改善正常(N)小鼠和大鼠的胰岛素信号传导并延长大鼠的寿命。我们先前已经证明某些促凋亡基因在骨骼肌中的表达水平降低,并暗示这可能有助于调节GHRKO小鼠的寿命。肾脏中与凋亡相关的基因表达的改变也可能导致寿命的延长。在这种情况下,我们决定检查以下基因的肾脏表达:caspase-3,caspase-9,caspase-8,bax,bad,bcl-2,Smac / DIABLO,Apaf-1,p53和细胞色素c1( cyc1)在大约6个月大时接受VFR或假手术的雄性GHRKO和N小鼠中。 VFR后2个月收集肾脏。结果,与N只动物相比,KO小鼠中的caspase-3,caspase-9和bax表达降低。 Smac / DIABLO,caspase-8,bcl-2,bad和p53的表达在KO和N小鼠之间没有差异。 VFR不会改变KO或N小鼠中被检查基因的表达。总之,GHRKO小鼠的内分泌异常会导致促凋亡基因的表达降低,而VFR不会改变N和KO小鼠的检测基因表达。这些数据与其中GH信号转导和/或胰岛素敏感性的改变导致由促凋亡基因的肾脏表达降低介导的寿命延长的模型一致。

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