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多巴胺转运体的基因改变对雄性和雌性黑质纹状体转运体系统的影响存在差异。

Genetic alteration in the dopamine transporter differentially affects male and female nigrostriatal transporter systems.

作者信息

Ji Jing, Bourque Mélanie, Di Paolo Thérèse, Dluzen Dean E

机构信息

Department of Anatomy, Northeastern Ohio Universities College of Medicine, Rootstown, OH 44272, USA.

出版信息

Biochem Pharmacol. 2009 Dec 1;78(11):1401-11. doi: 10.1016/j.bcp.2009.07.004. Epub 2009 Jul 15.

DOI:10.1016/j.bcp.2009.07.004
PMID:19615345
Abstract

Female mice with a heterozygous mutation of their dopamine transporter (+/- DAT) showed relatively robust reductions in striatal DAT specific binding (38-50%), while +/- DAT males showed modest reductions (24-32%). Significant decreases in substantia nigra DAT specific binding (42%) and mRNA (24%) were obtained in +/- DAT females, but not +/- DAT males (19% and 5%, respectively). The effects of this DAT perturbation upon vesicular monoamine transporter-2 (VMAT-2) function revealed significantly greater reserpine-evoked DA output from +/+ and +/- DAT female as compared to male mice and the DA output profile differed markedly between +/+ and +/- DAT females, but not males. No changes in VMAT-2 protein or mRNA levels were present among these conditions. On the basis of these data, we propose: (1) a genetic mutation of the DAT does not exert equivalent effects upon the DAT in female and male mice, with females being more affected; (2) an alteration in the DAT may also affect VMAT-2 function; (3) this interaction between DAT and VMAT-2 function is more prevalent in female mice; and (4) the +/- DAT mutation affects VMAT-2 function through an indirect mechanism, that does not involve an alteration in VMAT-2 protein or mRNA. Such DAT/VMAT-2 interactions can be of significance to the gender differences observed in drug addiction and Parkinson's disease.

摘要

多巴胺转运体杂合突变(+/- DAT)的雌性小鼠纹状体DAT特异性结合相对显著降低(38 - 50%),而+/- DAT雄性小鼠的降低幅度较小(24 - 32%)。+/- DAT雌性小鼠黑质DAT特异性结合(42%)和mRNA(24%)显著降低,但+/- DAT雄性小鼠未出现显著降低(分别为19%和5%)。这种DAT扰动对囊泡单胺转运体2(VMAT - 2)功能的影响显示,与雄性小鼠相比,+/+和+/- DAT雌性小鼠中利血平诱发的多巴胺输出显著增加,并且+/+和+/- DAT雌性小鼠之间的多巴胺输出谱有明显差异,但雄性小鼠中没有。在这些情况下,VMAT - 2蛋白或mRNA水平没有变化。基于这些数据,我们提出:(1)DAT的基因突变对雌性和雄性小鼠DAT的影响并不相同,雌性受影响更大;(2)DAT的改变可能也会影响VMAT - 2功能;(3)DAT与VMAT - 2功能之间的这种相互作用在雌性小鼠中更普遍;(4)+/- DAT突变通过一种间接机制影响VMAT - 2功能,该机制不涉及VMAT - 2蛋白或mRNA的改变。这种DAT/VMAT - 2相互作用可能与药物成瘾和帕金森病中观察到的性别差异有关。

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