ENPP1和ESR1基因分型与颅面部不对称的亚分类及颞下颌关节紊乱症的严重程度相关。
ENPP1 and ESR1 genotypes associated with subclassifications of craniofacial asymmetry and severity of temporomandibular disorders.
作者信息
Chung Kay, Richards Tabitha, Nicot Romain, Vieira Alexandre R, Cruz Christiane V, Raoul Gwénaël, Ferri Joel, Sciote James J
机构信息
Department of Orthodontics, Temple University, Philadelphia, Pa.
Department of Oral and Maxillofacial Surgery, Roger Salengro Hospital, Université Lille Nord de France, Lille, France.
出版信息
Am J Orthod Dentofacial Orthop. 2017 Nov;152(5):631-645. doi: 10.1016/j.ajodo.2017.03.024.
INTRODUCTION
We investigated whether ACTN3, ENPP1, ESR1, PITX1, and PITX2 genes which contribute to sagittal and vertical malocclusions also contribute to facial asymmetries and temporomandibular disorders (TMD) before and after orthodontic and orthognathic surgery treatment.
METHODS
One hundred seventy-four patients with a dentofacial deformity were diagnosed as symmetric or subdivided into 4 asymmetric groups according to posteroanterior cephalometric measurements. TMD examination diagnosis and jaw pain and function (JPF) questionnaires assessed the presence and severity of TMD.
RESULTS
Fifty-two percent of the patients were symmetric, and 48% were asymmetric. The asymmetry classification demonstrated significant cephalometric differences between the symmetric and asymmetric groups, and across the 4 asymmetric subtypes: group 1, mandibular body asymmetry; group 2, ramus asymmetry; group 3, atypical asymmetry; and group 4, C-shaped asymmetry. ENPP1 SNP-rs6569759 was associated with group 1 (P = 0.004), and rs858339 was associated with group 3 (P = 0.002). ESR1 SNP-rs164321 was associated with group 4 (P = 0.019). These results were confirmed by principal component analysis that showed 3 principal components explaining almost 80% of the variations in the studied groups. Principal components 1 and 2 were associated with ESR1 SNP-rs3020318 (P <0.05). Diagnoses of disc displacement with reduction, masticatory muscle myalgia, and arthralgia were highly prevalent in the asymmetry groups, and all had strong statistical associations with ENPP1 rs858339. The average JPF scores for asymmetric subjects before surgery (JPF, 7) were significantly higher than for symmetric subjects (JPF, 2). Patients in group 3 had the highest preoperative JPF scores, and groups 2 and 3 were most likely to be cured of TMD 1 year after treatment.
CONCLUSIONS
Posteroanterior cephalometrics can classify asymmetry into distinct groups and identify the probability of TMD and genotype associations. Orthodontic and orthognathic treatments of facial asymmetry are effective at eliminating TMD in most patients.
引言
我们研究了有助于矢状和垂直错牙合畸形的ACTN3、ENPP1、ESR1、PITX1和PITX2基因在正畸和正颌外科治疗前后是否也与面部不对称和颞下颌关节紊乱病(TMD)有关。
方法
174例牙颌面畸形患者根据头影测量结果被诊断为对称或分为4个不对称组。TMD检查诊断以及颌面部疼痛和功能(JPF)问卷评估了TMD的存在和严重程度。
结果
52%的患者为对称型,48%为不对称型。不对称分类显示对称组与不对称组之间以及4种不对称亚型之间存在显著的头影测量差异:第1组,下颌体不对称;第2组,下颌升支不对称;第3组,非典型不对称;第4组,C形不对称。ENPP1基因单核苷酸多态性(SNP)-rs6569759与第1组相关(P = 0.004),rs858339与第3组相关(P = 0.002)。ESR1 SNP-rs164321与第4组相关(P = 0.019)。主成分分析证实了这些结果,该分析显示3个主成分解释了研究组中近80%的变异。主成分1和2与ESR1 SNP-rs3020318相关(P <0.05)。可复性盘移位、咀嚼肌肌痛和关节痛在不对称组中高度流行,并且所有这些都与ENPP1 rs858339有很强的统计学关联。不对称受试者术前的平均JPF评分(JPF,7)显著高于对称受试者(JPF,2)。第3组患者术前JPF评分最高,但第2组和第3组在治疗1年后最有可能治愈TMD。
结论
头影测量可以将不对称分为不同的组,并确定TMD与基因型关联的可能性。面部不对称的正畸和正颌治疗对大多数患者消除TMD有效。
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