Fehr Christoph, Shirley Renee L, Belknap John K, Crabbe John C, Buck Kari J
Portland Alcohol Research Center and Department of Behavioral Neuroscience, Oregon Health and Science University, Portland, Oregon 97201, USA.
J Neurosci. 2002 May 1;22(9):3730-8. doi: 10.1523/JNEUROSCI.22-09-03730.2002.
Risk for onset of alcoholism is related to genetic differences in acute alcohol withdrawal liability. We previously mapped a locus responsible for 26% of the genetic variance in acute alcohol withdrawal convulsion liability to a >35 centimorgan (cM) interval of murine chromosome 4. Here, we narrow the position of this locus to a <1 cM interval (approximately 1.8 megabase, containing 15 genes and/or predicted genes) using a combination of novel, interval-specific congenic strains and recombinant progeny testing. We report the development of a small-donor-segment congenic strain, which confirms capture of a gene affecting alcohol withdrawal within the <1 cM interval. We also confirm a pentobarbital withdrawal locus within this interval, suggesting that the same gene may influence predisposition to physiological dependence on alcohol and a barbiturate. This congenic strain will be invaluable for determining whether this interval also harbors a gene(s) underlying other quantitative trait loci mapped to chromosome 4, including loci affecting voluntary alcohol consumption, alcohol-induced ataxia, physical dependence after chronic alcohol exposure, and seizure response to pentylenetetrazol or an audiogenic stimulus. To date, Mpdz, which encodes the multiple PSD95/DLG/ZO-1 (PDZ) domain protein (MPDZ), is the only gene within the interval shown to have allelic variants that differ in coding sequence and/or expression. Sequence analysis of 15 standard inbred mouse strains identifies six Mpdz haplotypes that predict three MPDZ protein variants. These analyses, and evidence using interval-specific congenic lines, show that alcohol withdrawal severity is genetically correlated with MPDZ status, indicating that MPDZ variants may influence alcohol withdrawal liability.
酒精中毒发病风险与急性酒精戒断易感性的基因差异有关。我们之前将一个导致急性酒精戒断惊厥易感性26%遗传变异的基因座定位到小鼠4号染色体上大于35厘摩(cM)的区间。在此,我们通过结合新型的、区间特异性近交系和重组后代测试,将该基因座的位置缩小至小于1 cM的区间(约1.8兆碱基,包含15个基因和/或预测基因)。我们报告了一种小供体片段近交系的培育情况,这证实了在小于1 cM的区间内捕获到了一个影响酒精戒断的基因。我们还证实了该区间内存在一个戊巴比妥戒断基因座,这表明同一个基因可能影响对酒精和巴比妥类药物生理依赖的易感性。这种近交系对于确定该区间是否还包含其他定位到4号染色体上的数量性状基因座的一个或多个基因将非常宝贵,这些基因座包括影响自愿饮酒量、酒精诱导的共济失调、慢性酒精暴露后的身体依赖性以及对戊四氮或听源性刺激的癫痫反应的基因座。迄今为止,编码多PDZ结构域蛋白(MPDZ)的Mpdz是该区间内唯一显示在编码序列和/或表达上存在等位基因变体的基因。对15个标准近交小鼠品系的序列分析确定了6种Mpdz单倍型,可预测3种MPDZ蛋白变体。这些分析以及使用区间特异性近交系的证据表明,酒精戒断严重程度与MPDZ状态存在遗传相关性,这表明MPDZ变体可能影响酒精戒断易感性。