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首页> 外文期刊>Biology of Reproduction: Offical Journal of the Society for the Study of Reproduction >Select nutrients in the ovine uterine lumen. VI. Expression of FK506-binding protein 12-rapamycin complex-associated protein 1 (FRAP1) and regulators and effectors of mTORC1 and mTORC2 complexes in ovine uteri and conceptuses.
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Select nutrients in the ovine uterine lumen. VI. Expression of FK506-binding protein 12-rapamycin complex-associated protein 1 (FRAP1) and regulators and effectors of mTORC1 and mTORC2 complexes in ovine uteri and conceptuses.

机译:在绵羊子宫腔中选择营养物质。 VI。 FK506结合蛋白12-雷帕霉素复合物相关蛋白1(FRAP1)和mTORC1和mTORC2复合物的调节剂和效应子在绵羊子宫和子宫中的表达。

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摘要

FRAP1 (FK506-binding protein 12-rapamycin complex-associated protein 1), a component of the nutrient-sensing cell signaling pathway, is critical for cell growth and metabolism. The present study determined expression of FRAP1 and associated members of the mTORC1 and mTORC2 cell signaling pathways in uteri of cyclic and pregnant ewes and conceptuses, as well as effects of pregnancy, progesterone (P4), and interferon tau (IFNT) on their expression. The mRNAs for FRAP1, LST8, MAPKAP1, RAPTOR, RICTOR, TSC1, TSC2, RHEB, and EIF4EBP1 were localized to luminal, superficial glandular, and glandular epithelia and stromal cells of uteri from cyclic and pregnant ewes, as well as trophectoderm and endoderm of conceptuses between Days 13 and 18 of pregnancy. The abundance of FRAP1, RAPTOR, RICTOR, TSC1, and TSC2 mRNAs in endometria was unaffected by pregnancy status or by day of the estrous cycle or pregnancy; however, levels of LST8, MAPKAP1, RHEB, and EIF4EBP1 mRNA increased in endometria during early pregnancy. In ovariectomized ewes, P4 and IFNT stimulated expression of RHEB and EIF4EBP1 in uterine endometria. Total endometrial FRAP1 protein and phosphorylated FRAP1 protein levels were affected by pregnancy status and by day after onset of estrus, and phosphorylated FRAP1 protein was detected in nuclei of uterine epithelia and conceptuses. In endometria of pregnant ewes, increases in abundance of mRNAs for RICTOR, RHEB, and EIF4EBP1, as well as RHEB protein, correlated with rapid conceptus growth and development during the peri-implantation period. These results suggest that the FRAP1 cell signaling pathway mediates interactions between the maternal uterus and peri-implantation conceptuses and that P4 and IFNT affect this pathway by regulating expression of RHEB and EIF4EBP1.
机译:FRAP1(FK506结合蛋白12-雷帕霉素复合物相关蛋白1)是营养敏感细胞信号通路的组成部分,对细胞生长和代谢至关重要。本研究确定了FRAP1以及周期和妊娠母羊和受孕子宫中mTORC1和mTORC2细胞信号通路相关成员的表达,以及妊娠,孕酮(P4)和干扰素tau(IFNT)对其表达的影响。 FRAP1,LST8,MAPKAP1,RAPTOR,RICTOR,TSC1,TSC2,RHEB和EIF4EBP1的mRNA定位于环状和妊娠母羊的子宫腔,浅腺和腺上皮和间质细胞以及滋养层和内胚层怀孕第13至18天之间的孕期。子宫内膜中FRAP1,RAPTOR,RICTOR,TSC1和TSC2 mRNA的丰度不受妊娠状况或发情周期或妊娠天的影响。然而,在怀孕早期子宫内膜中的LST8,MAPKAP1,RHEB和EIF4EBP1 mRNA的水平升高。在去卵巢母羊中,P4和IFNτ刺激子宫内膜中RHEB和EIF4EBP1的表达。子宫内膜总FRAP1蛋白和磷酸化FRAP1蛋白水平受妊娠状态和发情发作后一天的影响,并且在子宫上皮细胞核和子宫内膜中检测到磷酸化FRAP1蛋白。在怀孕母羊的子宫内膜中,RICTOR,RHEB和EIF4EBP1以及RHEB蛋白的mRNA丰度增加,与围着床期快速概念生长和发育有关。这些结果表明,FRAP1细胞信号传导途径介导了母体子宫与着床前后概念之间的相互作用,而P4和IFNT通过调节RHEB和EIF4EBP1的表达影响了该途径。

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