rs11171733 - RPS26 - ERBB3

Magnitude 2.2 · 3 studies on file

Reported associations

  • A multi-ancestry genetic study of pain intensity in 598,339 veterans. - Nature medicine (2024) · Toikumo S, Vickers-Smith R, Jinwala Z, Xu H, Saini D, Hartwell EE, Pavicic M, Sullivan KA, Xu K, Jacobson DA, Gelernter J, Rentsch CT, Stahl E, Cheatle M, Zhou H, Waxman SG, Justice AC, Kember RL, Kranzler HR · PubMed 38429522

    Chronic pain is a common problem, with more than one-fifth of adult Americans reporting pain daily or on most days. It adversely affects the quality of life and imposes substantial personal and economic costs. Efforts to treat chronic pain using opioids had a central role in precipitating the opioid crisis. Despite an estimated heritability of 25-50%, the genetic architecture of chronic pain is not well-characterized, in part because studies have largely been limited to samples of European ancestry. To help address this knowledge gap, we conducted a cross-ancestry meta-analysis of pain intensity in 598,339 participants in the Million Veteran Program, which identified 126 independent genetic loci, 69 of which are new. Pain intensity was genetically correlated with other pain phenotypes, lev

  • Cross-trait analyses identify shared genetics between migraine, headache, and glycemic traits, and a causal relationship with fasting proinsulin - Unknown journal (n.d.) · Unknown authors · PubMed 36808568

    ABSTRACT: The co-occurrence of migraine and glycemic traits has long been reported in observational epidemiological studies, but it has remained unknown how they are linked genetically. We used large-scale GWAS summary statistics on migraine, headache, and nine glycemic traits in European populations to perform cross-trait analyses to estimate genetic correlation, identify shared genomic regions, loci, genes, and pathways, and test for causal relationships. Out of the nine glycemic traits, significant genetic correlation was observed for fasting insulin (FI) and glycated haemoglobin (HbA1c) with both migraine and headache, while 2-h glucose was genetically correlated only with migraine. Among 1703 linkage disequilibrium (LD) independent regions of the genome, we found pleiotropic regions b

  • Genetic association and Mendelian randomization for hypothyroidism highlight immune molecular mechanisms - Unknown journal (n.d.) · Unknown authors · PubMed 36093044

    ABSTRACT: Summary We carried out a genome-wide association analysis including 51,194 cases of hypothyroidism and 443,383 controls. In total, 139 risk loci were associated to hypothyroidism with genes involved in lymphocyte function. Candidate genes associated with hypothyroidism were identified by using molecular quantitative trait loci, colocalization, and enhancer-promoter chromatin looping. Mendelian randomization (MR) identified 42 blood expressed genes and circulating proteins as candidate causal molecules in hypothyroidism. Drug-gene interaction analysis provided evidence that immune checkpoint and tyrosine kinase inhibitors used in cancer therapy increase the risk of hypothyroidism. Hence, integrative mapping and MR support that expression of genes and proteins enriched in lymphocyt


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Lifestyle context

Concrete actions anchored to the cited research. We do not prescribe, we describe.

Lifestyle

  • Identify and manage migraine triggers Moderate

    Associated with migraine risk; trigger avoidance is evidence-based migraine management

    Maintain headache diary; track patterns with sleep, stress, caffeine, and food intake

Screening

  • Fasting glucose and insulin levels Moderate

    Associated with elevated fasting insulin and metabolic dysfunction

    Annual fasting glucose and insulin testing; more frequent if elevated

  • Thyroid function (TSH) Moderate

    Strong association with hypothyroidism risk

    Baseline TSH screening; repeat testing every 1-2 years or per clinical judgment