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细胞内热休克蛋白72反应的性别二态性。

Sexual dimorphism of the intracellular heat shock protein 72 response.

作者信息

Nickerson M, Kennedy S L, Johnson J D, Fleshner M

机构信息

Dept. of IPHY, CB 354, Boulder, CO 80309, USA.

出版信息

J Appl Physiol (1985). 2006 Aug;101(2):566-75. doi: 10.1152/japplphysiol.00259.2006. Epub 2006 May 11.

DOI:10.1152/japplphysiol.00259.2006
PMID:16690792
Abstract

The majority of previous work examining stress responses has been done in males. Recently, it has become clear that the impact of stressor exposure is modulated by sex. One stress response that may be affected by sex is the induction of intracellular heat shock protein (HSP) 72, which is a stress- responsive molecular chaperone that refolds denatured proteins and promotes cellular survival. The following study compared HSP72 in males and females and also examined whether the estrous cycle altered HSP72 induction in females. We hypothesized that females compared with males would have a constrained HSP72 response after an acute stressor and that the stress-induced HSP72 response in females would fluctuate with the estrous cycle. Male and female F344 rats were either left in their home cage or exposed to acute tail-shock stress (8-10/group). Immediately following stressor, trunk blood was collected and tissues were flash frozen. Vaginal smear and estrogen enzyme immunoassay were used to categorize the phase of estrous. Results show that female rats had a greater corticosterone response than males, that both males and females exhibit a stress-induced release of progesterone, and that males and females had equal levels of stress-induced circulating norepinephrine. Sexual dimorphism of the HSP72 (ELISA) response existed in pituitary gland, mesenteric lymph nodes, and liver such that female rats had an attenuated HSP72 response compared with males after stress. The adrenal glands, spleen, and heart did not exhibit sexual dimorphism of the HSP72 response. The estrous cycle did not have a significant effect on basal or stress-induced HSP72 in females.

摘要

先前大多数研究应激反应的工作都是在雄性动物身上进行的。最近,应激源暴露的影响受性别调节这一点已变得清晰。一种可能受性别影响的应激反应是细胞内热休克蛋白(HSP)72的诱导,它是一种应激反应性分子伴侣,可使变性蛋白质重新折叠并促进细胞存活。以下研究比较了雄性和雌性动物体内的HSP72,并研究了发情周期是否会改变雌性动物体内HSP72的诱导情况。我们假设,与雄性相比,雌性在急性应激源作用后HSP72反应会受到限制,并且雌性动物应激诱导的HSP72反应会随发情周期波动。将雄性和雌性F344大鼠置于其饲养笼中或暴露于急性尾部电击应激(每组8 - 10只)。应激源作用后立即采集躯干血液并将组织速冻。使用阴道涂片和雌激素酶免疫测定法对发情阶段进行分类。结果显示,雌性大鼠的皮质酮反应比雄性大鼠更强,雄性和雌性大鼠均表现出应激诱导的孕酮释放,并且雄性和雌性大鼠应激诱导的循环去甲肾上腺素水平相等。垂体、肠系膜淋巴结和肝脏中存在HSP72(酶联免疫吸附测定)反应的性别差异,即应激后雌性大鼠的HSP72反应比雄性大鼠减弱。肾上腺、脾脏和心脏未表现出HSP72反应的性别差异。发情周期对雌性大鼠基础或应激诱导的HSP72没有显著影响。

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