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Joint involvement in Noonan syndrome. A retrospective paediatric descriptive study

医学 努南综合征 色素沉着绒毛结节性滑膜炎 回顾性队列研究 关节过度活动 关节痛 滑膜炎 关节炎 内科学 外科 儿科 物理疗法
作者
Aurore Le Quellec,Thomas Édouard,Séverine Audebert‐Bellanger,Antoine Pouzet,Karine Bourdet,Cindy Colson,Charlotte Oriot,Sylvaine Poignant,Alain Saraux,Valérie Devauchelle‐Pensec,Aurore Le Quellec
出处
期刊:Joint Bone Spine [Elsevier BV]
卷期号:89 (1): 105270-105270 被引量:4
标识
DOI:10.1016/j.jbspin.2021.105270
摘要

Noonan syndrome is a rare genetic disorder characterized mainly by congenital heart disease, occasional intellectual disability, and varied orthopaedic, rheumatological and haematologic anomalies. Despite potentially serious functional consequences, joint involvement has been rarely studied in the literature. Our objective was to perform a retrospective study evaluating the prevalence and characteristics of joint involvement in Noonan syndrome.We recorded articular symptoms, including their type and frequency, in patients with Noonan syndrome followed up in French hospitals. Patients were included if the diagnosis was confirmed before the age of 20 based on the van der Burgt criteria or genetic analysis. Data are presented as frequencies or medians (ranges), and patient groups were compared using chi-square or Fisher tests.Seventy-one patients were included from 4 centres. The average age was 12.5 years (range: 2-36). Musculoskeletal pain was found in 18 patients (25%) and joint stiffness in 10 (14%) located in the wrists, elbows, ankles, knees and hips, which was usually bilateral. Only one destructive form was described (multiple villonodular synovitis and a giant cell lesion of the jaw). There were no cases of systemic lupus erythaematosus (SLE) or other autoimmune arthritis. Raynaud's phenomenon was observed in 3 patients. Only 50% of joint complaints led to additional exploration. SOS1 mutations (P<0.05) and treatment with growth hormone (GH) (P<0.05) were the only factors significantly related to musculoskeletal pain. Patients treated with GH did not have more SOS1 mutations. Patients experiencing pain were not more likely to experience stiffness, joint hypermobility, or coagulation abnormalities.Joint manifestations were frequent in Noonan syndrome, predominant in large joints, and rarely explored. Multiple villonodular synovitis is characteristic but rare. Auto-immune disorders were not described in this cohort. A more multidisciplinary approach could be recommended for the early detection of possibly disabling rheumatologic manifestations.
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