Genetic susceptibility to temporomandibular joint involvement in juvenile idiopathic arthritis

IF 3.1 3区医学 Q1 DENTISTRY, ORAL SURGERY & MEDICINE Journal of oral rehabilitation Pub Date : 2024-08-27 DOI:10.1111/joor.13834

P. Niibo, T. Nikopensius, T. Jagomägi, Ü. Voog, T. Haller, N. Tõnisson, A. Metspalu, M. Saag, C. Pruunsild

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Abstract

Background

Juvenile idiopathic arthritis (JIA) is the most common chronic rheumatic condition of childhood. Temporomandibular joint (TMJ) is among the most commonly affected joints in JIA patients. When JIA involves the TMJ, it may affect condylar growth in the joint; therefore, JIA patients are at risk of unfavourable long-term outcomes from associated joint damage. If undetected, TMJ involvement can lead to various functional disabilities such as reduced mandibular mobility and disorders of the mastication muscles. Limitations in sagittal and vertical mandibular growth can result in micrognathia and anterior open bite with aesthetic and functional restrictions.

Objective

Genetic factors may play a role in determining which individuals are more prone to develop TMJ disorders or in predicting the severity of the disease process. Therefore, we applied a GWAS approach to identify loci associated with TMJ involvement in a sample of Estonian patients with JIA. Our aim was to address the potential role of genetic susceptibility factors in TMJ-JIA, a condition not previously studied in this context.

Methods

The case group consisted of 55 JIA patients with TMJ involvement and 208 patients without TMJ involvement comprised the control group. The entire cohort was genotyped using the Illumina HumanOmniExpress BeadChip arrays. Imputation was performed using a nationwide reference panel obtained of 2240 individuals whose data were obtained from the Estonian Biobank.

Results

We identified six loci as being associated with the risk of TMJ-JIA in Estonian JIA patients. The strongest associations were identified at CD6 rs3019551 (P = 3.80 × 10⁻⁶), SLC26A8/MAPK14 rs9470191 (P = 6.15 × 10⁻⁶), NLRP3 rs2056795 (P = 8.91 × 10⁻⁶) and MAP2K4 rs7225328 (P = 1.64 × 10⁻⁵).

Conclusion

This study provides first insights into the risk-associated loci between JIA and its manifestation in the TMJ. The reported loci are involved in molecular pathways of immunological relevance and likely represent genomic regions that render the TMJ susceptible to involvement by JIA in Estonian patients.

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幼年特发性关节炎颞下颌关节受累的遗传易感性。

背景：幼年特发性关节炎（JIA）是儿童时期最常见的慢性风湿病。颞下颌关节（TMJ）是 JIA 患者最常受影响的关节之一。当 JIA 累及颞下颌关节时，可能会影响关节内的髁突生长；因此，JIA 患者有可能因相关的关节损伤而导致不利的长期后果。如果未被发现，颞下颌关节受累可导致各种功能障碍，如下颌骨活动度降低和咀嚼肌功能紊乱。下颌骨矢状和垂直生长受限可导致小颌畸形和前方开放性咬合，造成美观和功能上的限制：遗传因素可能在决定哪些人更容易患颞下颌关节疾病或预测疾病过程的严重程度方面发挥作用。因此，我们采用基因组学分析方法，在爱沙尼亚 JIA 患者样本中找出与颞下颌关节受累相关的基因位点。我们的目的是研究遗传易感因素在颞下颌关节-JIA 中的潜在作用，这种情况以前从未研究过：病例组包括 55 名颞下颌关节受累的 JIA 患者，对照组包括 208 名无颞下颌关节受累的患者。使用 Illumina HumanOmniExpress BeadChip 芯片对整个群体进行了基因分型。利用从爱沙尼亚生物库中获得数据的 2240 人组成的全国性参考面板进行了推算：结果：我们确定了六个位点与爱沙尼亚 JIA 患者颞下颌关节-JIA 的风险有关。其中，CD6 rs3019551（P = 3.80 × 10-6）、SLC26A8/MAPK14 rs9470191（P = 6.15 × 10-6）、NLRP3 rs2056795（P = 8.91 × 10-6）和 MAP2K4 rs7225328（P = 1.64 × 10-5）的相关性最强：本研究首次揭示了 JIA 与颞下颌关节表现之间的风险相关位点。所报告的基因位点涉及与免疫学相关的分子通路，很可能代表了使爱沙尼亚患者的颞下颌关节易受 JIA 影响的基因组区域。

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来源期刊

Journal of oral rehabilitation 医学-牙科与口腔外科

CiteScore

5.60

自引率

10.30%

发文量

116

审稿时长

4-8 weeks

期刊介绍： Journal of Oral Rehabilitation aims to be the most prestigious journal of dental research within all aspects of oral rehabilitation and applied oral physiology. It covers all diagnostic and clinical management aspects necessary to re-establish a subjective and objective harmonious oral function. Oral rehabilitation may become necessary as a result of developmental or acquired disturbances in the orofacial region, orofacial traumas, or a variety of dental and oral diseases (primarily dental caries and periodontal diseases) and orofacial pain conditions. As such, oral rehabilitation in the twenty-first century is a matter of skilful diagnosis and minimal, appropriate intervention, the nature of which is intimately linked to a profound knowledge of oral physiology, oral biology, and dental and oral pathology. The scientific content of the journal therefore strives to reflect the best of evidence-based clinical dentistry. Modern clinical management should be based on solid scientific evidence gathered about diagnostic procedures and the properties and efficacy of the chosen intervention (e.g. material science, biological, toxicological, pharmacological or psychological aspects). The content of the journal also reflects documentation of the possible side-effects of rehabilitation, and includes prognostic perspectives of the treatment modalities chosen.