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中脑皮质多巴胺对压力的遗传易感性决定了在抑郁症小鼠模型中中脑伏隔核多巴胺受抑制的倾向以及行为“绝望”的倾向。

Genetic susceptibility of mesocortical dopamine to stress determines liability to inhibition of mesoaccumbens dopamine and to behavioral 'despair' in a mouse model of depression.

作者信息

Ventura R, Cabib S, Puglisi-Allegra S

机构信息

Dipartimento di Psicologia, University La Sapienza, via dei Marsi 78, 00185, Rome, Italy.

出版信息

Neuroscience. 2002;115(4):999-1007. doi: 10.1016/s0306-4522(02)00581-x.

Abstract

Clinical and preclinical research suggests a major role of mesocortical dopamine (DA) in psychopathology through regulation of subcortical, especially mesoaccumbens, DA functioning. In these experiments we demonstrate that the high vulnerability to stress-induced 'despair' and mesoaccumbens DA inhibition, exhibited by mice of the inbred strain C57BL/6 (C57) in a common animal model of depression, depends on their being highly susceptible to stress-induced mesocortical DA activation. Thus, C57 mice but not mice of the DBA/2 strain showed an extremely high level of immobility on their first experience with the forced swimming test (FST) as well as immediate and strong activation of mesocortical DA metabolism and inhibition of mesoaccumbens DA metabolism and release. In addition, the behavioral and the mesoaccumbens DA responses to FST in C57 mice were reduced and reversed, respectively, by bilateral mesocortical DA depletion. Finally, chronic treatment with the antidepressant clomipramine reduced immobility and eliminated both mesocortical DA activation and mesoaccumbens DA inhibition in response to FST. These results suggest that a genetically determined susceptibility to stress by the mesocortical DA system may favor the development of pathological behavioral responses through inhibition of subcortical DA transmission.

摘要

临床和临床前研究表明,中脑皮质多巴胺(DA)通过调节皮质下尤其是中脑伏隔核的DA功能,在精神病理学中起主要作用。在这些实验中,我们证明,在常见的抑郁症动物模型中,近交系C57BL/6(C57)小鼠表现出的对压力诱导的“绝望”和中脑伏隔核DA抑制的高度易感性,取决于它们对压力诱导的中脑皮质DA激活的高度敏感性。因此,C57小鼠而非DBA/2品系的小鼠在首次进行强迫游泳试验(FST)时表现出极高水平的不动,同时中脑皮质DA代谢立即强烈激活,中脑伏隔核DA代谢和释放受到抑制。此外,双侧中脑皮质DA耗竭分别降低和逆转了C57小鼠对FST的行为和中脑伏隔核DA反应。最后,用抗抑郁药氯米帕明进行慢性治疗可减少不动,并消除对FST的中脑皮质DA激活和中脑伏隔核DA抑制。这些结果表明,中脑皮质DA系统对压力的遗传易感性可能通过抑制皮质下DA传递而促进病理行为反应的发展。

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