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皮质酮和孕酮对雄性大鼠应激时 HPA 轴和神经免疫反应的调节作用不同。

Corticosterone and progesterone differentially regulate HPA axis and neuroimmune responses to stress in male rats.

机构信息

Behavioral Neuroscience Program, Department of Psychology, State University of New York at Binghamton, Binghamton, NY, USA.

出版信息

Stress. 2020 Jul;23(4):368-385. doi: 10.1080/10253890.2019.1678025. Epub 2019 Oct 26.

Abstract

In response to stressor exposure, expression of the inflammatory cytokine interleukin-1β (IL-1) is increased within the paraventricular nucleus of the hypothalamus (PVN). Surgical removal of the adrenal glands (ADX) potentiated stress-induced IL-1 expression, suggesting a role for adrenal-derived hormones in constraining stress-evoked increases in IL-1. While corticosterone (CORT) is a primary factor inhibiting IL-1 expression, progesterone (PROG) is also released by the adrenal glands in male rats in response to stress and also has potent anti-inflammatory properties. This series of studies first established doses of CORT and PROG that adequately recapitulate the normal stress-induced rise, and then tested for individual and combined roles of CORT and PROG in mitigating stress-induced expression of inflammatory genes. We found that CORT injection alone attenuated ADX-induced increases in IL-1 expression and normalized the HPA axis response to stress. In general, PROG replacement had little effect on changes in HPA axis responsivity or stress-induced inflammatory measures. When CORT and PROG were co-administered, a small effect on expression of the decoy receptor, IL-1R2 was observed, suggestive of an anti-inflammatory response. Overall, these results suggest that although CORT is likely to be the primary stress-related hormone responsible for constraining cytokine expression evoked by stress, CORT and PROG may exert certain combined actions that temper stress-induced neuroinflammation.LAY SUMMARYExposure to stress promoted expression of inflammation-related genes in the PVN and BNST. This inflammation was mainly suppressed by the adrenal hormone corticosterone, whereas progesterone had a smaller role in mitigating post-stress inflammation.

摘要

面对应激源的刺激,下丘脑室旁核(PVN)内的促炎细胞因子白细胞介素-1β(IL-1)的表达增加。对肾上腺(ADX)进行手术切除增强了应激诱导的 IL-1 表达,这表明肾上腺源性激素在限制应激诱导的 IL-1 增加方面发挥作用。虽然皮质酮(CORT)是抑制 IL-1 表达的主要因素,但孕激素(PROG)也是雄性大鼠在应激时由肾上腺分泌的,也具有很强的抗炎作用。这一系列研究首先确定了 CORT 和 PROG 的剂量,这些剂量足以重现正常应激诱导的升高,然后测试了 CORT 和 PROG 在减轻应激诱导的炎症基因表达方面的单独和共同作用。我们发现,单独注射 CORT 即可减弱 ADX 诱导的 IL-1 表达增加,并使 HPA 轴对应激的反应正常化。一般来说,PROG 替代对 HPA 轴反应性或应激诱导的炎症指标的变化影响不大。当 CORT 和 PROG 同时给药时,观察到诱饵受体 IL-1R2 的表达略有变化,表明存在抗炎反应。总体而言,这些结果表明,尽管 CORT 可能是主要的应激相关激素,负责限制应激引起的细胞因子表达,但 CORT 和 PROG 可能发挥某些协同作用,调节应激诱导的神经炎症。

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