严重急性呼吸综合征(SARS)中的神经肌肉障碍

来源 :世界核心医学期刊文摘(神经病学分册) | 被引量 : 0次 | 上传用户:CT1978
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Objective: To delineate and clarify neuromuscular disorders in patients with p robable severe acute respiratory syndrome (SARS). Design: Case series with follo w up ranging from 3 weeks to 2 months. Setting: National Taiwan University Hosp ital, Taipei. Patients: We investigated 4 patients with SARS who had concomitant neuromuscular problems. A diagnosis of SARS was based on the demonstration of s erum coronavirus antibodies. Clinical presentations, laboratory results, electro physiologic findings, and follow up conditions were determined. Results: Patien ts developed neuromuscular problems approximately 3 weeks after the onset of SAR S. Two women experienced motor predominant peripheral nerve disorders. A man de veloped myopathy and a third woman experienced neuropathy and myopathy. Cerebros pinal fluid obtained from 2 patients with neuropathy disclosed normal protein co ntent and the absence of pleocytosis and SARS coronavirus antibodies. Both patie nts with myopathy had elevated serum creatine kinase levels. A rapid clinical an d electrophysiologic improvement was evident during follow up examinations, wit h a good prognosis. Conclusions: The neuromuscular problems in patients with SAR S are considered to be critical illness polyneuropathy or myopathy, possibly co existent. Further pathological and microbiological studies are necessary to dete rmine the relationship between SARS coronavirus and neuromuscular problems. Objective: To delineate and clarify neuromuscular disorders in patients with p robable severe acute respiratory syndrome (SARS). Design: Case series with follo w up ranging from 3 weeks to 2 months. Settings: National Taiwan University Hosp ital, Taipei. Patients: We investigated 4 patients with SARS who had concomitant neuromuscular problems. A diagnosis of SARS was based on the demonstration of erum coronavirus antibodies. Clinical findings, laboratory results, electro physiologic findings, and follow up conditions were determined. Results: Patien ts developed neuromuscular problems approximately 3 weeks after the onset of SAR S. Two women experienced motor predominant peripheral nerve disorders. A man de veloped myopathy and a third woman experienced neuropathy and myopathy. Cerebros pinal fluid obtained from 2 patients with neuropathy discloses normal protein co ntent and absence of pleocytosis and SARS coronavirus antibodies. Both patie nts with myopathy had elevated ser A rapid clinical an d electrophysiologic improvement was evident during follow up examinations, wit ha good prognosis. Conclusions: The neuromuscular problems in patients with SAR S are considered to be critical illness polyneuropathy or myopathy, possibly co existent. Further pathological and microbiological studies are necessary to dete rmine the relationship between SARS coronavirus and neuromuscular problems.
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