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促肾上腺皮质激素原(POMC)测序与发育迟缓:POMC 基因 3'UTR 区 SNP 的初步证据-可能与生物学风险和自伤行为有关。

Proopiomelanocortin (POMC) sequencing and developmental delay: Preliminary evidence for a SNP in the 3' UTR region of the POMC gene-Possible relevance for biological risk and self-injurious behavior.

机构信息

University of Minnesota.

Mayo Clinic.

出版信息

Dev Psychopathol. 2019 May;31(2):433-438. doi: 10.1017/S0954579418000718. Epub 2018 Jul 16.

Abstract

The proopiomelanocortin (POMC) molecule has been implicated in models of self-injurious behavior (SIB) in neurodevelopmental disorders, but it has never been specifically sequenced in search of base specific polymorphisms. The empirical focus of this preliminary study was to sequence the POMC gene in 11 children (mean age = 41.8 months, range = 12-60 months; 73% male) with clinical concerns regarding global developmental delay, 5 with reported self-injury. Genomic DNA was extracted from blood samples, and the POMC gene was amplified by specific oligonucleotide primers via polymerase chain reaction. The amplified gene products were sequenced by the University of Minnesota Genomic Center, and the results were analyzed using Sequencher software. A single nucleotide polymorphism (SNP), 1130 C>T, was found in the 3' untranslated region (UTR) of two samples (one of whom had SIB). The program TargetScanHuman was used to predict the function of this mutation. Variant c.1130 C<T was predicted to be located in the target site of two microRNAs (miRNAs; hsa-mir-3715 and hsa-mir-1909), and the variant allele T may result in an increased minimum free energy for the two miRNAs. Further work with much larger samples is needed to continue the investigation of POMC's possible function as a risk factor for the development of SIB in children with developmental delay/disability. The findings presented in this study show that the SNP found in the 3' UTR could alter the binding of miRNAs to POMC 3'UTR, thus, increasing POMC expression and affecting several biological systems with high relevance to the biology of self-injury. There was a significant difference in β-endorphin levels between SIB (M = 169.25 pg/mL) and no SIB (M = 273.5 pg/mL, SD = 15.2) cases (p < .01). Intervention implications are tied to prior observations of individual differences among SIB responders and nonresponders to treatment with the opioid antagonist naltrexone. Stratifying individuals with SIB by POMC mutation status may provide a potential tailoring-like variable to guide the selection of who is more (or less) likely to respond to opiate antagonist treatment. Currently, opioid antagonistic treatment for SIB is empiric (trial and error).

摘要

阿黑皮素原(POMC)分子已被牵涉到神经发育障碍的自伤行为(SIB)模型中,但从未针对特定碱基的多态性进行过测序。本初步研究的实证重点是对 11 名有发育迟缓(平均年龄=41.8 个月,范围=12-60 个月;73%为男性)且临床怀疑有广泛性发育迟缓的儿童(5 名有自伤报告)的 POMC 基因进行测序。从血液样本中提取基因组 DNA,并通过聚合酶链反应(PCR)使用特定的寡核苷酸引物扩增 POMC 基因。扩增的基因产物由明尼苏达大学基因组中心测序,并使用 Sequencher 软件分析结果。在两个样本(其中一个有 SIB)的 3'非翻译区(UTR)中发现了一个单核苷酸多态性(SNP),1130 C>T。使用 TargetScanHuman 程序预测该突变的功能。变体 c.1130 C<T 预测位于两个 microRNAs(miRNAs;hsa-mir-3715 和 hsa-mir-1909)的靶位点,并且变异等位基因 T 可能导致两个 miRNA 的最小自由能增加。需要进一步进行更大样本的研究,以继续调查 POMC 作为发育迟缓/残疾儿童 SIB 发生的风险因素的可能作用。本研究中的发现表明,在 3'UTR 中发现的 SNP 可能改变 miRNA 与 POMC 3'UTR 的结合,从而增加 POMC 的表达,并影响与自伤生物学密切相关的多个生物学系统。在 SIB(M=169.25pg/mL)和无 SIB(M=273.5pg/mL,SD=15.2)病例之间,β-内啡肽水平有显著差异(p <.01)。干预意义与纳曲酮这种阿片类拮抗剂治疗 SIB 反应者和非反应者之间个体差异的先前观察结果有关。通过 POMC 突变状态对 SIB 个体进行分层,可能为指导选择更有可能(或不太可能)对阿片拮抗剂治疗有反应的个体提供潜在的量身定制变量。目前,SIB 的阿片拮抗治疗是经验性的(试错)。

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