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单剂量摇头丸给药后黑褐大鼠血清素能轴突损伤及Hsp27、Hsp72和Hsp90分子伴侣的免疫定位:时间、空间和细胞模式

Damage of serotonergic axons and immunolocalization of Hsp27, Hsp72, and Hsp90 molecular chaperones after a single dose of MDMA administration in Dark Agouti rat: temporal, spatial, and cellular patterns.

作者信息

Adori Csaba, Andó Rómeó D, Kovács Gábor G, Bagdy György

机构信息

Laboratory of Neurochemistry and Experimental Medicine, National Institute of Psychiatry and Neurology, Budapest, Hungary.

出版信息

J Comp Neurol. 2006 Jul 10;497(2):251-69. doi: 10.1002/cne.20994.

Abstract

3,4-Methylenedioxymethamphetamine (MDMA, "ecstasy") causes long-term disturbance of the serotonergic system. We examined the temporal, spatial, and cellular distribution of three molecular chaperones, Hsp27, Hsp72, and Hsp90, 3 and 7 days after treatment with 7.5, 15, and 30 mg/kg single intraperitoneal (i.p.) doses of MDMA in Dark Agouti rat brains. Furthermore, we compared the immunostaining patterns of molecular chaperones with serotonergic axonal-vulnerability evaluated by tryptophan-hydroxylase (TryOH) immunoreactivity and with astroglial-activation detected by GFAP-immunostaining. There was a marked reduction in TryOH-immunoreactive axon density after MDMA treatment in all examined areas at both time points. Three days after treatment, a significant dose-dependent increase in Hsp27-immunoreactive protoplasmic astrocytes was found in the cingulate, frontal, occipital, and pyriform cortex, and in the hippocampus CA1. However, there was no increase in astroglial Hsp27-immunoreactivity in the caudate putamen, lateral septal nucleus, or anterior hypothalamus. A significant increase in the GFAP immunostaining density of protoplasmic astrocytes was found only in the hippocampus CA1. In addition, numerous strong Hsp72-immunopositive neurons were found in some brain areas only 3 days after treatment with 30 mg/kg MDMA. Increased Hsp27-immunoreactivity exclusively in the examined cortical areas reveals that Hsp27 is a sensitive marker of astroglial response to the effects of MDMA in these regions of Dark Agouti rat brain and suggests differential responses in astroglial Hsp27-expression between distinct brain areas. The co-occurrence of Hsp27 and GFAP response exclusively in the hippocampus CA1 may suggest the particular vulnerability of this region. The presence of strong Hsp72-immunopositive neurons in certain brain areas may reflect additional effects of MDMA on nonserotonergic neurons.

摘要

3,4-亚甲基二氧甲基苯丙胺(摇头丸,MDMA)会导致5-羟色胺能系统的长期紊乱。我们研究了在暗褐鼠脑内腹腔注射(i.p.)7.5、15和30mg/kg单剂量MDMA后3天和7天,三种分子伴侣Hsp27、Hsp72和Hsp90的时间、空间及细胞分布。此外,我们将分子伴侣的免疫染色模式与通过色氨酸羟化酶(TryOH)免疫反应性评估的5-羟色胺能轴突易损性以及通过GFAP免疫染色检测到的星形胶质细胞激活进行了比较。在两个时间点的所有检查区域,MDMA处理后TryOH免疫反应性轴突密度均显著降低。处理后3天,在扣带回、额叶、枕叶和梨状皮质以及海马CA1区发现Hsp27免疫反应性原浆型星形胶质细胞显著剂量依赖性增加。然而,尾状壳核、外侧隔核或下丘脑前部的星形胶质细胞Hsp27免疫反应性并未增加。仅在海马CA1区发现原浆型星形胶质细胞的GFAP免疫染色密度显著增加。此外,仅在30mg/kg MDMA处理3天后,在一些脑区发现了大量强Hsp72免疫阳性神经元。仅在所检查的皮质区域Hsp27免疫反应性增加表明,Hsp27是暗褐鼠脑这些区域星形胶质细胞对MDMA作用反应的敏感标志物,并提示不同脑区星形胶质细胞Hsp27表达存在差异反应。Hsp27和GFAP反应仅在海马CA1区同时出现可能表明该区域具有特殊易损性。某些脑区存在强Hsp72免疫阳性神经元可能反映了MDMA对非5-羟色胺能神经元的额外作用。

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