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I型遗传性运动和感觉神经病中膈神经与肺功能的评估

Evaluation of phrenic nerve and pulmonary function in hereditary motor and sensory neuropathy, type I.

作者信息

Carter G T, Kilmer D D, Bonekat H W, Lieberman J S, Fowler W M

机构信息

Department of Physical Medicine and Rehabilitation, University of California, Davis.

出版信息

Muscle Nerve. 1992 Apr;15(4):459-62. doi: 10.1002/mus.880150407.

Abstract

Phrenic nerve and diaphragmatic dysfunction has been assumed to be the cause of respiratory failure in hereditary motor and sensory neuropathy, type 1 (HMSN I). In order to determine the relationship between phrenic nerve and pulmonary function in this disease, 25 patients underwent a 4-step evaluation process consisting of: (1) bilateral phrenic nerve conduction study; (2) median, peroneal, and tibial motor conduction studies; (3) measurement of forced vital capacity (FVC) and maximal inspiratory and expiratory pressures (MIP, MEP); and (4) pulmonary-focused history and physical. Phrenic nerve motor latency was abnormally prolonged in 22 of the 23 (96%) subjects when a response was obtained. All had slowed velocity or absent peripheral motor conduction responses. Vital capacity was abnormally reduced in 6 of the 25 (24%) subjects. Eight (32%) had an abnormally reduced MIP, while 19 (76%) had an abnormally reduced MEP. Only 2 (8%) subjects had clinical evidence of pulmonary dysfunction. None of the dependent variables (FVC, MIP, MEP, peripheral nerve conduction, or clinical examination) correlated with phrenic nerve latencies. Although phrenic nerve latencies are markedly prolonged in HMSN I, these values are not useful in predicting respiratory dysfunction.

摘要

膈神经和膈肌功能障碍被认为是遗传性运动和感觉神经病1型(HMSN I)呼吸衰竭的病因。为了确定该疾病中膈神经与肺功能之间的关系,25例患者接受了一个由四步组成的评估过程,包括:(1)双侧膈神经传导研究;(2)正中神经、腓总神经和胫神经运动传导研究;(3)用力肺活量(FVC)以及最大吸气和呼气压力(MIP、MEP)的测量;(4)以肺部为重点的病史和体格检查。在23例获得反应的受试者中,有22例(96%)膈神经运动潜伏期异常延长。所有人均存在速度减慢或外周运动传导反应缺失的情况。25例受试者中有6例(24%)肺活量异常降低。8例(32%)最大吸气压力异常降低,而19例(76%)最大呼气压力异常降低。只有2例(8%)受试者有肺功能障碍的临床证据。没有一个因变量(FVC、MIP、MEP、外周神经传导或临床检查)与膈神经潜伏期相关。虽然在HMSN I中膈神经潜伏期明显延长,但这些数值对预测呼吸功能障碍并无帮助。

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