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首页> 外文期刊>Psychoneuroendocrinology: An International Journal >Biomarker discovery for disease status and symptom severity in children with autism
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Biomarker discovery for disease status and symptom severity in children with autism

机译:生物标志物发现自闭症儿童的疾病状态和症状严重程度

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Autism spectrum disorder (ASD) is characterized by social impairments and repetitive behaviors, and affects 1 in 68 US children. Despite ASD's societal impact, its disease mechanisms remain poorly understood. Recent preclinical ASD biomarker discovery research has implicated the neuropeptides oxytocin (OXT) and arginine vasopressin (AVP), and their receptors, OXTR and A VPRIA, in animal models. Efforts to translate these findings to individuals with ASD have typically involved evaluating single neuropeptide measures as biomarkers of ASD and/or behavioral functioning. Given that ASD is a heterogeneous disorder, and unidimensional ASD biomarker studies have been challenging to reproduce, here we employed a multidimensional neuropeptide biomarker analysis to more powerfully interrogate disease status and symptom severity in a well characterized child cohort comprised of ASD patients and neurotypical controls. These blood-based neuropeptide measures, considered as a whole, correctly predicted disease status for 57 out of 68 (i.e., 84%) participants. Further analysis revealed that a composite measure of OXTR and AVPR1A gene expression was the key driver of group classification, and that children with ASD had lower neuropeptide receptor mRNA levels compared to controls. Lower neuropeptide receptor mRNA levels also predicted greater symptom severity for core ASD features (i.e., social impairments and stereotyped behaviors), but were unrelated to intellectual impairment, an associated feature of ASD.& para;& para;Findings from this research highlight the value of assessing multiple related biological measures, and their relative contributions, in the same study, and suggest that low blood neuropeptide receptor availability may be a promising biomarker of disease presence and symptom severity in ASD.
机译:自闭症谱系障碍(ASD)的特点是社会障碍和重复行为,并影响68个美国儿童中的1。尽管ASD的社会影响,但其疾病机制仍然明白很差。近期临床前ASD生物标志物发现研究涉及动物模型中的神经肽催产素(OXT)和精氨酸加压素(AVP),及其受体,OXTR和VPRIA。将这些发现转化为具有ASD的个体的努力通常涉及评估单一神经肽措施作为ASD和/或行为功能的生物标志物。考虑到ASD是一种异质疾病,并且单款ASD生物标志物研究一直挑战繁殖,在这里,在这里,我们使用了一种多维神经肽生物标志物分析,以在由ASD患者和神经典型对照组成的良好表征的儿童群体中更有力地询问疾病状态和症状严重程度。这些基于血液的神经肽措施,被视为整体,正确预测的疾病状态为57分中的57例(即84%)参与者。进一步的分析表明,oxTr和AVPR1A基因表达的复合措施是组分类的关键驱动器,与对照相比,具有亚本子的儿童具有较低的神经肽受体mRNA水平。降低神经肽受体mRNA水平还预测了核心ASD特征(即社会障碍和陈规定型行为)的更大症状严重程度,但与智力损害无关,是ASD的相关特征。&段;&段;&Para;从本研究中发现了价值评估多种相关的生物学措施及其相对贡献,在同一研究中,表明低血神经肽受体可用性可能是ASD中疾病存在和症状严重程度的有前途的生物标志物。

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