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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.

Abstract

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.

摘要

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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