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首页> 外文期刊>Rheumatology international. >Lower extremity lipedema, upper extremity lipodystrophy and severe calcinosis complicating juvenile dermatomyositis.
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Lower extremity lipedema, upper extremity lipodystrophy and severe calcinosis complicating juvenile dermatomyositis.

机译:下肢脂肪性水肿,上肢脂肪营养不良和严重的钙化病并发青少年皮肌炎。

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摘要

Juvenile dermatomyositis (JDM) is a rare but complex and potentially life-threatening autoimmune disease of childhood. Significant proportions of patients have residual weakness, muscle atrophy, joint contractures, and calcinosis. Recently, new clinical findings, such as lipodystrophy accompanied with increased fat deposition in certain areas, have been reported. So far, it is not known whether the redistribution of body fat may be the type of lipedema of lower extremity. We describe a 39-year-old woman who was diagnosed with JDM at the age of 7. Later she developed symmetrical lipodystrophy of upper extremities and symmetrical lipedema of lower extremities (making 2 and 58.3 % of total body fat mass, respectively), with multiple calcified nodules in the subcutaneous tissues. These nodules gradually increased in size despite therapy. Capillaroscopy findings showed scleroderma-like abnormalities. ANA and anti-U1RNP antibodies were positive. Similar cases with simultaneous occurrence of the lipedema of lower extremities, lipodystrophy of upper extremities, and severe calcinosis complicating JDM have not been published so far. We showed that the calcinosis and lipodystrophy were associated with short duration of active disease. Also, we display case that raises the question whether it is possible overlapping autoimmune diseases revealed during follow-up.
机译:青少年皮肌炎(JDM)是一种罕见但复杂且可能威胁生命的儿童自身免疫性疾病。很大比例的患者有残余无力,肌肉萎缩,关节挛缩和钙化。最近,已经报道了新的临床发现,例如脂肪营养不良症伴随某些区域脂肪沉积增加。到目前为止,还不知道体内脂肪的重新分布是否可能是下肢脂肪性水肿的类型。我们描述了一名39岁的女性,该女性在7岁时被诊断为JDM。后来她出现了上肢对称性脂肪营养不良和下肢对称性脂肪浮肿(分别占人体总脂肪量的2%和58.3%),皮下组织中有多个钙化结节。尽管进行了治疗,但这些结节的大小逐渐增加。毛细血管镜检查结果显示硬皮样异常。 ANA和抗U1RNP抗体均为阳性。到目前为止,尚未发表类似的病例,这些病例同时发生下肢血脂,上肢脂肪营养不良和严重的钙化病并发JDM。我们表明,煅烧和脂肪营养不良与活动性疾病的持续时间短有关。此外,我们展示了一个案例,提出了一个问题,即是否有可能在随访期间发现自身免疫疾病重叠。

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