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恒河猴中一种μ-阿片受体单核苷酸多态性:与应激反应和攻击行为的关联。

A mu-opioid receptor single nucleotide polymorphism in rhesus monkey: association with stress response and aggression.

作者信息

Miller G M, Bendor J, Tiefenbacher S, Yang H, Novak M A, Madras B K

机构信息

Division of Neurochemistry, New England Primate Research Center, Harvard Medical School, One Pine Hill Drive, Southborough, MA 01772-9102, USA.

出版信息

Mol Psychiatry. 2004 Jan;9(1):99-108. doi: 10.1038/sj.mp.4001378.

Abstract

Variations in the human mu-opioid receptor gene have driven exploration of their biochemical, physiological and pathological relevance. We investigated the existence of variations in the nonhuman primate mu-opioid receptor gene to determine whether nonhuman primates can model genotype/phenotype associations of relevance to humans. Similar to the A118G single nucleotide polymorphism (SNP) in the human mu-opioid receptor gene, a SNP discovered in the rhesus monkey mu-opioid receptor gene (C77G) alters an amino acid in the N-terminal arm of the receptor (arginine for proline at position 26). Two mu-opioid receptor coding regions isolated from a single heterozygous (C77/G77) rhesus monkey brain were expressed in HEK-293 cells and characterized in radioreceptor assays. Paralleling the findings of increased affinity of beta-endorphin by the A118G allele in the human, the rhesus monkey mu-opioid receptor protein derived from the G77-containing clone demonstrated a 3.5-fold greater affinity for beta-endorphin than the receptor derived from the C77-containing clone. An assay developed to assess the incidence of the C77G SNP in a behaviorally and physiologically characterized cohort of rhesus monkeys (n=32) indicated that 44% were homozygous for C77-containing alleles, 50% were heterozygous and 6% were homozygous for G77-containing alleles. The presence of G77-containing alleles was associated with significantly lower basal and ACTH-stimulated plasma cortisol levels (P<0.03-0.05 and P<0.02, respectively) and a significantly higher aggressive threat score (P<0.05) in vivo. In a cohort of 20 monkeys, a trend towards an inverse correlation between aggressive threat and plasma cortisol levels was observed. The findings suggest that mu-opioid receptor haplotypes in monkeys can contribute to individual variability in stress response and related aggression. The data support the use of nonhuman primates to investigate mu-opioid receptor genotype/phenotype relations of relevance to humans.

摘要

人类μ-阿片受体基因的变异推动了对其生化、生理和病理相关性的探索。我们研究了非人类灵长类动物μ-阿片受体基因变异的存在情况,以确定非人类灵长类动物是否可以模拟与人类相关的基因型/表型关联。与人类μ-阿片受体基因中的A118G单核苷酸多态性(SNP)类似,在恒河猴μ-阿片受体基因中发现的一个SNP(C77G)改变了受体N端臂中的一个氨基酸(第26位脯氨酸变为精氨酸)。从一只杂合(C77/G77)恒河猴大脑中分离出的两个μ-阿片受体编码区在HEK-293细胞中表达,并在放射受体测定中进行了表征。与人类中A118G等位基因增加β-内啡肽亲和力的研究结果相似,来自含G77克隆的恒河猴μ-阿片受体蛋白对β-内啡肽的亲和力比来自含C77克隆的受体高3.5倍。一项用于评估行为和生理特征明确的恒河猴群体(n = 32)中C77G SNP发生率的检测表明,44%为含C77等位基因的纯合子,50%为杂合子,6%为含G77等位基因的纯合子。含G77等位基因的存在与体内基础和促肾上腺皮质激素刺激的血浆皮质醇水平显著降低(分别为P < 0.03 - 0.05和P < 0.02)以及显著更高的攻击性威胁评分(P < 0.05)相关。在一组20只猴子中,观察到攻击性威胁与血浆皮质醇水平之间呈负相关的趋势。这些发现表明,猴子中的μ-阿片受体单倍型可导致应激反应和相关攻击行为的个体差异。这些数据支持使用非人类灵长类动物来研究与人类相关的μ-阿片受体基因型/表型关系。

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