双相情感障碍中RIC-3与含β2亚基的烟碱型乙酰胆碱受体缺乏一致性。
Lack of RIC-3 congruence with beta2 subunit-containing nicotinic acetylcholine receptors in bipolar disorder.
作者信息
Severance E G, Yolken R H
机构信息
Stanley Division of Developmental Neurovirology, Department of Pediatrics, Johns Hopkins University School of Medicine, 600 North Wolfe Street, Blalock 1105, Baltimore, MD 21287-4933, USA.
出版信息
Neuroscience. 2007 Aug 24;148(2):454-60. doi: 10.1016/j.neuroscience.2007.06.008. Epub 2007 Jul 19.
Nicotinic acetylcholine receptor (nAChR) dysfunction occurs in individuals with schizophrenia (SZ) and may also affect individuals with bipolar disorder (BP). The molecular mechanisms for these disease-associated cholinergic deficits are not known. In vitro, the protein RIC-3 (resistance to inhibitors of cholinesterase-3) aids the assembly and trafficking of alpha7-nAChRs but has unclear action on the biogenesis of alpha4/beta2-nAChRs. To evaluate RIC-3/nAChR dynamics in diseased and normal human brain tissue, we measured RIC-3, alpha7-, alpha4- and beta2-nAChRs transcript levels in postmortem prefrontal cortex of individuals with SZ (n=31), BP (n=28) and unaffected controls (NC, n=33). Of the 28 individuals with BP, 20 had a history of psychotic symptoms. We compared relative message abundances between diagnostic groups and tested correlations of RIC-3 with each nAChR message subtype. RIC-3 and alpha4 messages were significantly increased in BP compared with NC (RIC-3, P< or =0.002; alpha4, P< or =0.04). RIC-3 message was also upregulated in SZ (P< or =0.04). In BP with psychoses, RIC-3 and alpha4 levels were increased compared with BP without psychoses (both P< or =0.02) and compared with NC (RIC-3, P< or =0.0003; alpha4, P< or =0.004). In correlation regression analyses, RIC-3 expression was very highly correlated to alpha7, alpha4 and beta2 in NC (alpha7, P< or =2.5e-05; alpha4, P< or =2.5e-09; beta2, P< or =0.003) and in SZ (alpha7, P< or =1e-07; alpha4, P< or =7e-07; beta2, P< or =3e-09). RIC-3 also strongly correlated with alpha7 and alpha4 in BP (alpha7, P< or =0.003; alpha4, P< or =3.5e-07). RIC-3 was modestly correlated with beta2 in BP overall (P< or =0.04), but showed no significant correlation in BP with psychoses (P< or =0.31) compared with a significant correlation in BP without psychoses (P< or =0.007). In conclusion, coordinated RIC-3/alpha4 upregulation and discordant RIC-3/beta2 levels suggest that alpha4/beta2 nAChR deficits in BP may occur from dysregulated RIC-3 chaperoning of the beta2 nAChR subunit in a subset of patients affected by psychotic features.
精神分裂症(SZ)患者会出现烟碱型乙酰胆碱受体(nAChR)功能障碍,双相情感障碍(BP)患者可能也会受其影响。这些与疾病相关的胆碱能缺陷的分子机制尚不清楚。在体外,蛋白质RIC - 3(抗胆碱酯酶抑制剂 - 3)有助于α7 - nAChR的组装和运输,但对α4/β2 - nAChR的生物合成作用尚不清楚。为了评估患病和正常人类脑组织中RIC - 3/nAChR的动态变化,我们测量了SZ患者(n = 31)、BP患者(n = 28)和未受影响对照组(NC,n = 33)死后前额叶皮质中RIC - 3、α7 -、α4 - 和β2 - nAChR的转录水平。在28例BP患者中,20例有精神病症状史。我们比较了诊断组之间的相对信使丰度,并测试了RIC - 3与每种nAChR信使亚型的相关性。与NC相比,BP患者中RIC - 3和α4信使显著增加(RIC - 3,P≤0.002;α4,P≤0.04)。SZ患者中RIC - 3信使也上调(P≤0.04)。在有精神病的BP患者中,与无精神病的BP患者相比(P均≤0.02)以及与NC相比(RIC - 3,P≤0.0003;α4,P≤0.004),RIC - 3和α4水平升高。在相关性回归分析中,NC组(α7,P≤2.5×10⁻⁵;α4,P≤2.5×10⁻⁹;β2,P≤0.003)和SZ组(α7,P≤1×10⁻⁷;α4,P≤7×10⁻⁷;β2,P≤3×10⁻⁹)中RIC - 3表达与α7、α4和β2高度相关。BP组中RIC - 3也与α7和α4强烈相关(α7,P≤0.003;α4,P≤3.5×10⁻⁷)。BP组总体上RIC - 3与β2呈适度相关(P≤0.04),但与无精神病的BP患者中显著相关(P≤0.007)相比,有精神病的BP患者中无显著相关性(P≤0.31)。总之,RIC - 3/α4的协同上调和RIC - 3/β2水平的不一致表明,在受精神病特征影响的一部分患者中,BP患者的α4/β2 nAChR缺陷可能是由于β2 nAChR亚基的RIC - 3伴侣功能失调所致。
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