Department of Clinical Neurophysiology, Hospital Universitario Cruces, Barakaldo, Bizkaia, Spain.
Osatek Alta Tecnología Sanitaria S.A., Galdakao, Bizkaia, Spain.
Neuromuscul Disord. 2014 Jan;24(1):56-62. doi: 10.1016/j.nmd.2013.09.005. Epub 2013 Sep 13.
Hereditary neuropathy with liability to pressure palsies (HNPP) is a disorder mainly caused by a 1.5-Mb deletion at 17p11.2-12 (and in some rare cases by point mutations) and clinically associated with recurrent painless palsies. Here, we performed electrophysiological (motor, sensory and terminal latency index), MRI and genetic studies in a family referred for ulnar neuropathy with pain. Surprisingly, we found typical neurophysiological features of HNPP (prolongation of distal motor latencies and diffuse SNCV slowing with significant slowing of motor nerve conduction velocities). Besides, the proband presented conduction block in left ulnar, left median and both peroneal nerves. MRI findings were consistent with an underlying neuropathy. Molecular studies identified a novel frameshift mutation in PMP22 confirming the diagnosis of HNPP. Our data suggest that neurophysiological studies are essential to characterize underdiagnosed HNPP patients referred for peripheral neuropathy. Our experience shows that MRI could be a complementary tool for the diagnosis of these patients.
遗传性压力易发性神经病(HNPP)主要由 17p11.2-12 处 1.5Mb 缺失(在一些罕见情况下由点突变引起)引起,并与复发性无痛性神经病相关。在这里,我们对一个因疼痛性尺神经病就诊的家族进行了电生理学(运动、感觉和末端潜伏期指数)、MRI 和遗传学研究。令人惊讶的是,我们发现了 HNPP 的典型神经生理学特征(远端运动潜伏期延长和弥散性 SNCV 减慢,运动神经传导速度显著减慢)。此外,先证者还表现出左侧尺神经、左侧正中神经和双侧腓总神经的传导阻滞。MRI 结果与神经病变一致。分子研究发现 PMP22 中的一个新的移码突变,证实了 HNPP 的诊断。我们的数据表明,神经生理学研究对于明确诊断为周围神经病的 HNPP 患者至关重要。我们的经验表明,MRI 可能是这些患者诊断的一种补充工具。
