人血浆中促肾上腺皮质激素释放因子及其结合蛋白。

P. Lowry
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引用次数: 48

摘要

CRF是不寻常的,因为它是由胎盘合成并释放到人体循环中,在妊娠晚期达到下丘脑门静脉系统在压力下正常预期的水平。这种上升在妊娠高血压和早产中更为明显。矛盾的是,ACTH和皮质醇都没有相应的升高。这种缺乏生物反应和肽在体外人(而不是大鼠)血浆中的稳定性引发了对人crf结合血浆蛋白的研究。该CRF-BP被证明具有40 kDa左右的分子质量,并已被纯化到均匀性。它在纳摩尔范围内具有亲和力常数,当与适量的CRF混合时,在体外完全抑制肽的acth释放活性。随着CRF-BP cDNA的克隆,为放射免疫测定的发展提供了足够的纯材料。虽然孕妇的CRF-BP水平在妊娠中期是正常的,但在第35周开始下降,到足月时大约达到正常值的50%。这样做的净效果将是自由的、具有潜在生物活性的CRF的加速增加。
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Corticotropin-releasing factor and its binding protein in human plasma.
CRF is unusual in that it is synthesized and released from the placenta into the circulation in humans, reaching levels in the third trimester that would normally be expected in the hypothalamic portal system during stress. This rise is even more pronounced in pregnancy-induced hypertension and preterm labour. Paradoxically, there is no associated rise of either ACTH or cortisol. This lack of biological response and the stability of the peptide in human (but not rat) plasma in vitro initiated a search for the human CRF-binding plasma protein. This CRF-BP proved to have a molecular mass in the region of 40 kDa, and has been purified to homogeneity. It has an affinity constant in the nanomolar range and when mixed with appropriate amounts of CRF completely inhibits the ACTH-releasing activity of the peptide in vitro. With the cloning of the cDNA for CRF-BP, sufficient pure material has become available for the development of a radioimmunoassay. Although CRF-BP levels in pregnant women are normal in the second trimester, they begin to fall by week 35, reaching approximately 50% of normal values by term. The net effect of this would be an accelerated increase in free, potentially biologically active CRF.
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