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生活是痛苦的:纤维肌痛作为多种责任分布的枢纽。

Life is pain: Fibromyalgia as a nexus of multiple liability distributions.

机构信息

The Charles Bronfman Institute for Personalized Medicine, Icahn School of Medicine at Mount Sinai, New York, New York, USA.

Division of Genetic Medicine, Department of Medicine, Vanderbilt University Medical Center, Nashville, Tennessee, USA.

出版信息

Am J Med Genet B Neuropsychiatr Genet. 2023 Oct-Dec;192(7-8):171-182. doi: 10.1002/ajmg.b.32949. Epub 2023 Jun 19.

Abstract

Fibromyalgia is a complex disease of unclear etiology that is complicated by difficulties in diagnosis, treatment, and clinical heterogeneity. To clarify this etiology, healthcare-based data are leveraged to assess the influences on fibromyalgia in several domains. Prevalence is less than 1% of females in our population register data, and about 1/10th that in males. Fibromyalgia often presents with co-occurring conditions including back pain, rheumatoid arthritis, and anxiety. More comorbidities are identified with hospital-associated biobank data, falling into three broad categories of pain-related, autoimmune, and psychiatric disorders. Selecting representative phenotypes with published genome-wide association results for polygenic scoring, we confirm genetic predispositions to psychiatric, pain sensitivity, and autoimmune conditions show associations with fibromyalgia, although these may differ by ancestry group. We conduct a genome-wide association analysis of fibromyalgia in biobank samples, which did not result in any genome-wide significant loci; further studies with increased sample size are necessary to identify specific genetic effects on fibromyalgia. Overall, fibromyalgia appears to have strong clinical and likely genetic links to several disease categories, and could usefully be understood as a composite manifestation of these etiological sources.

摘要

纤维肌痛是一种病因不明的复杂疾病,其诊断、治疗和临床异质性存在困难。为了阐明这种病因,我们利用基于医疗保健的数据来评估几个领域对纤维肌痛的影响。在我们的人口登记数据中,女性的患病率不到 1%,男性的患病率约为十分之一。纤维肌痛常伴有并存病症,包括背痛、类风湿关节炎和焦虑症。在与医院相关的生物库数据中,发现更多的合并症,分为与疼痛相关、自身免疫和精神障碍三大类。通过对具有多基因评分发表的全基因组关联研究结果的代表性表型进行选择,我们证实了与精神障碍、疼痛敏感性和自身免疫性疾病相关的遗传易感性与纤维肌痛有关,尽管这些易感性可能因种族群体而异。我们对生物库样本中的纤维肌痛进行了全基因组关联分析,但没有发现任何全基因组显著的基因座;需要进一步增加样本量的研究来确定纤维肌痛的具体遗传效应。总的来说,纤维肌痛似乎与几个疾病类别具有很强的临床和可能的遗传联系,并且可以将其理解为这些病因来源的综合表现。

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