Goland R S, Stark R I, Wardlaw S L
Department of Medicine, Columbia University College of Physicians and Surgeons, New York, New York 10032.
J Clin Endocrinol Metab. 1990 Apr;70(4):925-9. doi: 10.1210/jcem-70-4-925.
CRH is secreted by the placenta into human maternal and fetal plasma during gestation. In the present study plasma CRH was measured in the plasma of five pregnant baboons and their fetuses to ascertain whether the baboon is a suitable model for study of placental CRH. Studies were performed in chronically catheterized animals that exhibited no behavioral or endocrinological signs of stress; maternal animals moved freely about the cage. Mean maternal plasma CRH was 620 +/- 110 pmol/L (2970 pg/mL) at 146 +/- 11 days gestation, and mean fetal plasma CRH was 133 +/- 29 pmol/L (640 pg/mL) at delivery in four animals. Plasma CRH was undetectable (less than 8.5 pmol/L; less than 41 pg/mL) in nonpregnant animals and in animals 8 h after delivery. Maternal and fetal plasma CRH levels in the chronically catheterized baboon were very similar to human maternal and umbilical cord CRH levels at comparable gestational ages. In addition, the majority of maternal plasma CRH eluted in the same position as synthetic human CRH by gel filtration. CRH stimulation tests were performed in the chronically catheterized maternal baboon to investigate whether pituitary-adrenal function during pregnancy is similar to that observed after chronic CRH infusion; blunted ACTH and cortisol responses to acute injections of CRH are observed after chronic CRH infusion. The administration of 0.5 micrograms/kg ovine CRH (oCRH) failed to result in an ACTH or cortisol rise in four pregnant baboons. Baseline ACTH levels were 5.2 +/- 0.4 pmol/L (23.5 pg/mL), and baseline cortisol levels were 800 +/- 55 nmol/L (29.1 micrograms/dL); neither rose after CRH administration. In contrast, 0.5 micrograms/kg oCRH did result in significant ACTH and cortisol elevations in five nonpregnant baboons [ACTH: baseline, 5.9 +/- 1.4; peak, 16 +/- 4.8 pmol/L (P less than 0.05); cortisol: baseline, 430 +/- 55 nmol/L; peak, 960 +/- 200 nmol/L (P less than 0.05)]. In contrast, the administration of a larger dose of oCRH (5.0 micrograms/kg) led to stimulation of ACTH release in five pregnant baboons (baseline, 6.6 +/- 1.3 pmol/L; peak, 34.1 +/- 6.4; P less than 0.001). After this dose cortisol levels also rose in the pregnant animals (baseline = 1040 +/- 30 nmol/L; peak, 1620 +/- 130); however, this response was blunted compared to that in the nonpregnant animals (P less than 0.05). CRH (5.0 micrograms/kg) significantly stimulated both ACTH and cortisol in the nonpregnant animals.(ABSTRACT TRUNCATED AT 400 WORDS)
促肾上腺皮质激素释放激素(CRH)在妊娠期间由胎盘分泌至人类母体和胎儿血浆中。在本研究中,检测了5只怀孕狒狒及其胎儿血浆中的CRH,以确定狒狒是否是研究胎盘CRH的合适模型。研究在长期插管的动物中进行,这些动物未表现出行为或内分泌应激迹象;母体动物可在笼内自由活动。妊娠146±11天时,母体血浆CRH平均为620±110 pmol/L(2970 pg/mL),4只动物分娩时胎儿血浆CRH平均为133±29 pmol/L(640 pg/mL)。非怀孕动物及分娩后8小时的动物血浆中未检测到CRH(低于8.5 pmol/L;低于41 pg/mL)。长期插管狒狒的母体和胎儿血浆CRH水平与人类在相应孕周时的母体和脐带CRH水平非常相似。此外,通过凝胶过滤,大多数母体血浆CRH与合成人CRH在相同位置洗脱。对长期插管的母体狒狒进行了CRH刺激试验,以研究孕期垂体-肾上腺功能是否与慢性输注CRH后观察到的相似;慢性输注CRH后,观察到促肾上腺皮质激素(ACTH)和皮质醇对急性注射CRH的反应减弱。给4只怀孕狒狒注射0.5微克/千克的绵羊CRH(oCRH)未能导致ACTH或皮质醇升高。基线ACTH水平为5.2±0.4 pmol/L(23.5 pg/mL),基线皮质醇水平为800±55 nmol/L(29.1微克/分升);注射CRH后两者均未升高。相比之下,0.5微克/千克的oCRH确实使5只非怀孕狒狒的ACTH和皮质醇显著升高[ACTH:基线,5.9±1.4;峰值,16±4.8 pmol/L(P<0.05);皮质醇:基线,430±55 nmol/L;峰值,960±200 nmol/L(P<0.05)]。相反,给予较大剂量的oCRH(5.0微克/千克)导致5只怀孕狒狒的ACTH释放受到刺激(基线,6.6±1.3 pmol/L;峰值,34.
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