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首页> 外文期刊>Biology of Reproduction: Offical Journal of the Society for the Study of Reproduction >Developmental changes in expression of genes involved in regulation of apoptosis in the bovine preimplantation embryo.
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Developmental changes in expression of genes involved in regulation of apoptosis in the bovine preimplantation embryo.

机译:牛胚胎植入前胚胎中调控细胞凋亡的基因表达的发育变化。

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The early bovine preimplantation embryo is resistant to proapoptotic signals until around the 8- to 16-cell stage. We hypothesized that 2-cell embryos have higher amounts of antiapoptotic proteins and lower amounts of proapoptotic proteins when compared to embryos >/=16 cells. Steady-state concentrations of mRNA for the antiapoptotic genes BCL2 and HSPA1A were higher for MII oocytes, 2-cell embryos, and 2-cell embryos treated with alpha-amanitin as compared to >/=16-cell embryos. Steady-state concentrations of mRNA for the proapoptotic gene BAD increased in embryos >/=16 cells. There was no significant effect of stage of development on steady-state mRNA concentrations of BCL2L1, DFFA, or BAX. Using immunohistochemistry, it was found that BCL2 was present in greater relative concentrations for 2-cell embryos than for embryos >/=16 cells. These results were confirmed by Western blotting. Relative amounts of immunoreactive BAX detected by immunofluorescence were lower for 2-cell embryos than for embryos >/=16 cells. Using Western blotting, a high molecular weight (46 kDa) form of BAX was highest in >/=16-cell embryos, intermediate in 2-cell embryos, and lowest in MII oocytes. There were no effects of stage of development on relative amounts of immunoreactive BCL2L1, HSPA1A, or BAD, as determined by immunofluorescence. Treatment of embryos with alpha-amanitin from Day 0 to Day 5 or Day 4 to Day 5 after insemination reduced activation of group II caspases and terminal deoxynucleotidyl transferase dUTP nick end labeling after treatment with the proapoptotic signal C(2) ceramide at Day 5 after fertilization. Thus, transcription of BAX or other proteins is required for acquisition of the capacity for apoptosis. Results support the idea that changes in amounts of BCL2 family members are important for the inhibition of apoptosis in the 2-cell embryo and in the establishment of the capacity for apoptosis later in development.
机译:早期的牛植入前胚胎对细胞凋亡信号具有抗性,直到大约8至16个细胞阶段。我们假设与> / = 16细胞的胚胎相比,2细胞胚胎具有更高的抗凋亡蛋白和更低的促凋亡蛋白。 MII卵母细胞,2-细胞胚胎和用α-amanitin处理的2-细胞胚胎的抗凋亡基因BCL2和HSPA1A的mRNA的稳态浓度高于> / = 16-细胞胚胎。促凋亡基因BAD的mRNA稳态浓度在> / = 16细胞的胚胎中增加。发育阶段对BCL2L1,DFFA或BAX的稳态mRNA浓度没有显着影响。使用免疫组织化学,发现BCL2在2细胞胚胎中的相对浓度高于> / = 16细胞胚胎。通过蛋白质印迹证实了这些结果。通过免疫荧光检测到的2细胞胚胎的免疫反应性BAX的相对数量低于> / = 16细胞的胚胎。使用蛋白质印迹法,BAX的高分子量(46 kDa)形式在> / = 16-细胞胚胎中最高,在2细胞胚胎中居中,在MII卵母细胞中最低。通过免疫荧光测定,发育阶段对免疫反应性BCL2L1,HSPA1A或BAD的相对量没有影响。授精后第0天至第5天或第4天至第5天用α-amanitin处理胚胎后,在第5天后用促凋亡信号C(2)神经酰胺处理后,降低了II组半胱天冬酶的激活和末端脱氧核苷酸转移酶dUTP缺口末端标记受精。因此,需要BAX或其他蛋白质的转录以获得凋亡的能力。结果支持这样的想法,即BCL2家族成员数量的变化对于抑制2细胞胚胎中的凋亡和建立后期发育中的凋亡能力很重要。

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