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Schizophrenia thalamus imaging: Low benzamide binding to dopamine D2 receptors suggests fewer D2Short receptors and fewer presynaptic terminals

机译:精神分裂症丘脑成像:低苯甲酰胺与多巴胺D2受体的结合表明D2短受体少,突触前末端少

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The dopamine D2 receptor continues to be the major target for the treatment of schizophrenia and is one of many genes genetically associated with this disease. Recent data show that fewer short forms of the D2 receptor protein are synthesized if there is a genetic variant in the D2 receptor (with a T in rs 1076560 in intron 6). At the same time, at least six publications report that the binding of radioactive benzamides is reduced in the schizophrenia thalamus. A review of the benzamide pharmacology of the short and long forms of the D2 receptor shows that benzamides have a 2.4-fold higher affinity for the D2Short receptor relative to the D2Long form. Hence, the reduced amount of benzamide binding to the D2 receptors in the schizophrenia thalamus suggests that there is a reduced amount of D2Short receptors in this diseased region, and may possibly also mean fewer presynaptic terminals because that is where D2Short receptors mostly reside. If so, fewer presynaptic dopamine terminals in various brain regions may be the basis of the known behavioural dopamine supersensitivity in schizophrenia.
机译:多巴胺D2受体继续是治疗精神分裂症的主要靶标,并且是与该疾病遗传相关的许多基因之一。最新数据显示,如果D2受体中存在遗传变异(内含子6中的rs 1076560中带有T),则合成的D2受体蛋白的短形式就会更少。同时,至少有六个出版物报道在精神分裂症丘脑中放射性苯甲酰胺的结合减少。对D2受体短和长形式的苯甲酰胺药理学的综述表明,相对于D2Long形式,苯甲酰胺对D2Short受体的亲和力高2.4倍。因此,减少与精神分裂症丘脑中D2受体结合的苯甲酰胺的数量表明该患病区域中D2Short受体的数量减少,并且可能还意味着较少的突触前末端,因为那是D2Short受体最常居住的地方。如果是这样,则在各个脑区域中较少的突触前多巴胺末端可能是精神分裂症中已知的行为多巴胺超敏性的基础。

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