Affiliation:
1. Department and Laboratory of Neurology, National Reference Center for ‘Rare Peripheral Neuropathies’ University Hospital of Limoges (CHU Limoges) Limoges France
2. Department of Neurology (Nerve‐Muscle Unit), ‘Grand Sud‐Ouest’ National Reference Center for Neuromuscular Disorders, ALS Center University Hospital of Bordeaux (CHU Bordeaux) Bordeaux France
Abstract
AbstractAutoimmune neuropathies are a heterogeneous group of rare and disabling diseases in which the immune system is thought to target antigens in the peripheral nervous system: they usually respond to immune therapies. Guillain–Barré syndrome is divided into several subtypes including “acute inflammatory demyelinating polyradiculoneuropathy,” “acute motor axonal neuropathy,” “acute motor sensory neuropathy,” and other variants. Chronic forms such as chronic inflammatory demyelinating polyneuropathy (CIDP) and other subtypes and polyneuropathy associated with IgM monoclonal gammopathy; autoimmune nodopathies also belong to this group of auto‐immune neuropathies. It has been shown that immunoglobulin G from the serum of about 30% of CIDP patients immunolabels nodes of Ranvier or paranodes of myelinated axons. Whatever the cause of myelin damage of the peripheral nervous system, the initial attack on myelin by a dysimmune process may begin either at the internodal area or in the paranodal and nodal regions. The term “nodoparanodopathy” was first applied to some “axonal Guillain–Barré syndrome” subtypes, then extended to cases classified as CIDP bearing IgG4 antibodies against paranodal axoglial proteins. In these cases, paranodal dissection develops in the absence of macrophage‐induced demyelination. In contrast, the mechanisms of demyelination of other dysimmune neuropathies induced by macrophages are unexplained, as no antibodies have been identified in such cases. The main objective of this presentation is to show that the pathology illustrates, confirms, and may explain such mechanisms.
Subject
Neurology (clinical),Pathology and Forensic Medicine,General Neuroscience
Cited by
3 articles.
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