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Merck
CN
  • Preconditioning the uterine unfolded protein response maintains non-apoptotic Caspase 3-dependent quiescence during pregnancy.

Preconditioning the uterine unfolded protein response maintains non-apoptotic Caspase 3-dependent quiescence during pregnancy.

Cell death & disease (2018-09-19)
Judith Ingles, Arren Simpson, Chandrashekara Kyathanahalli, Prashanth Anamthathmakula, Sonia Hassan, Pancharatnam Jeyasuria, Jennifer C Condon
摘要

The prevention of apoptotic caspase 3 activation through biological preconditioning, mediated through the modulation of the unfolded protein response has been demonstrated to ameliorate multiple pathophysiologies. The maintenance of non-apoptotic caspase 3 activity by the unfolded protein response within the pregnant uterus has previously been proven to be critical in inhibiting uterine myocyte contractility during pregnancy. Here we report that the pregnant uterus utilizes an unfolded protein response-preconditioning paradigm to conserve myometrial caspase 3 in a non-apoptotic state in order to effectively inhibit uterine contractility thereby preventing the onset of preterm labor. In the absence of appropriate endogenous preconditioning during pregnancy, uterine caspase 3 is transformed from a non-apoptotic to an apoptotic phenotype. Apoptotic caspase 3 activation results in the precocious triggering of local uterine inflammatory signaling and prostaglandin production, consequently resulting in an increased incidence of preterm birth. These findings represent a paradigm shift in our understanding of how preconditioning promotes the maintenance of uterine non-apoptotic caspase 3 action during pregnancy preventing the onset of premature uterine contraction and therefore defining the timing of the onset of labor.

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Sigma-Aldrich
毒胡萝卜素, ≥98% (HPLC), solid film
Roche
原位细胞死亡检测试剂盒,AP, sufficient for ≤50 tests, kit of 1 (3 components), suitable for detection
Sigma-Aldrich
衣霉素,来自链霉菌Streptomyces lysosuperficus