The clinical spectrum of neuralgic amyotrophy in 246 cases

doi:10.1093/brain/awh722

Brain Advance Access originally published online on December 21, 2005
Brain 2006 129(2):438-450; doi:10.1093/brain/awh722

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The clinical spectrum of neuralgic amyotrophy in 246 cases

Nens van Alfen¹^,2 and Baziel G. M. van Engelen¹

¹ Department of Neurology, Neuromuscular Centre Nijmegen and ² Clinical Neurophysiology, Radboud University Nijmegen Medical Centre, Nijmegen, The Netherlands

Correspondence to: Nens van Alfen, MD, Neuromuscular Centre Nijmegen, Department of Clinical Neurophysiology, 920 Radboud University Nijmegen Medical Centre, PO Box 9101, 6500 HB, Nijmegen, The Netherlands E-mail: n.vanalfen{at}neuro.umcn.nl

We investigated the symptoms, course and prognosis of neuralgicamyotrophy (NA) in a large group of patients with idiopathicneuralgic amyotrophy (INA, n = 199) and hereditary neuralgicamyotrophy (HNA, n = 47) to gain more insight into the broadclinical spectrum of the disorder. Several findings from earliersmaller-scale studies were tested, and for the first time thepotential differences between the hereditary and idiopathicphenotypes and between males and females were explored. Generally,the course of the pain manifests itself in three consecutivephases with an initial severe, continuous pain lasting for $~$ 4weeks on average. Sensory involvement was quite common and foundin 78.4% of patients but was clinically less impairing thanthe initial pain and subsequent paresis. As a typically patchydisorder NA can affect almost any nerve in the brachial plexus,although damage in the upper and middle trunk distribution withinvolvement of the long thoracic and/or suprascapular nerveoccurred most frequently (71.1%). We found no correlation betweenthe distribution of motor and sensory symptoms. In INA recurrentattacks were found in 26.1% of the patients during an average6 year follow-up. HNA patients had an earlier onset (28.4 versus41.3 years), more attacks (mean 3.5 versus 1.5) and more frequentinvolvement of nerves outside the brachial plexus (55.8 versus17.3%) than INA patients, and a more severe maximum paresis,with a subsequent poorer functional outcome. In males the initialpain tended to last longer than it did in females (45 versus23 days). In females the middle or lower parts of the brachialplexus were involved more frequently (23.1 versus 10.5% in males),and their functional outcome was worse. Overall recovery wasless favourable than usually assumed, with persisting pain andparesis in approximately two-thirds of the patients who werefollowed for 3 years or more.

Key Words: brachial plexus neuropathy; corticosteroid treatment; neuralgic amyotrophy; Parsonage–Turner syndrome

Abbreviations: HNA = hereditary neuralgic amyotrophy; HNPP = hereditary neuropathy with liability to pressure palsies; INA = idiopathic neuralgic amyotrophy; NRS = Numerical Rating Scale

Received August 29, 2005. Revised October 21, 2005. Accepted November 12, 2005.

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