Rodolico Carmelo, Bonanno Carmen, Toscano Antonio, Vita Giuseppe
Department of Clinical and Experimental Medicine, University of Messina, Messina, Italy.
Front Neurol. 2020 Jul 23;11:660. doi: 10.3389/fneur.2020.00660. eCollection 2020.
Muscle-specific tyrosine kinase (MuSK) myasthenia gravis (MG) is a rare, frequently more severe, subtype of MG with different pathogenesis, and peculiar clinical features. The prevalence varies among countries and ethnic groups, affecting 5-8% of all MG patients. MuSK-MG usually has an acute onset affecting mainly the facial-bulbar muscles. The symptoms usually progress rapidly, within a few weeks. Early respiratory crises are frequent. The disease may lead to generalized muscle weakness up to muscle atrophy. The main bulbar involvement, the absence of significant thymus alterations, and the association with HLA class II DR14, DR16, and DQ5 alleles have been confirmed. Atypical onset, such as ocular involvement, lack of symptom fluctuations, acetylcholinesterase inhibitors failure, and negative results of electrophysiologic testing, if not specifically performed in the mainly involved muscle groups, makes MuSK-MG diagnosis challenging. In most cases, steroids are effective. Conventional immunosuppressants are not commonly able to replace steroids in maintaining a satisfactory long-term control of symptoms. However, the majority of MuSK-MG patients are refractory to treatment. In these cases, the use of rituximab showed promising results, resulting in sustained symptom control.
肌肉特异性酪氨酸激酶(MuSK)重症肌无力(MG)是MG的一种罕见的、通常更为严重的亚型,其发病机制不同,临床特征独特。患病率在不同国家和种族群体中有所差异,占所有MG患者的5 - 8%。MuSK - MG通常急性起病,主要影响面-延髓肌。症状通常在几周内迅速进展。早期呼吸危机很常见。该疾病可能导致全身肌肉无力直至肌肉萎缩。主要的延髓受累、无明显胸腺改变以及与人类白细胞抗原(HLA)II类DR14、DR16和DQ5等位基因的关联已得到证实。非典型起病,如眼部受累、症状无波动、乙酰胆碱酯酶抑制剂治疗无效以及电生理检查结果阴性(如果未在主要受累肌群中专门进行),使得MuSK - MG的诊断具有挑战性。在大多数情况下,类固醇是有效的。传统免疫抑制剂通常无法在维持症状长期满意控制方面替代类固醇。然而,大多数MuSK - MG患者对治疗难治。在这些情况下,使用利妥昔单抗显示出有前景的结果,可实现症状的持续控制。
