Invited Review: Chronic Inflammatory Demyelinating Polyneuropathy: How Pathophysiology Can Guide Treatment
Abstract
Chronic inflammatory demyelinating polyneuropathy (CIDP) is an autoimmune demyelinating neuropathy that is most commonly characterized clinically by progressive proximal and distal weakness affecting the upper and lower extremities, sensory loss, and reduced or absent reflexes. These symptoms evolve over the time course of 8 weeks or more. While the majority of CIDP demonstrates this clinical phenotype, there are CIDP variants as well. The milieu of the underlying pathophysiology and immunologic factors involved is complex and involves components of both the innate and adaptive immune systems. As more is understood about the underlying pathophysiology, novel targets and patterns have emerged guiding further classification and management. This is most notable in the discovery of antibodies targeting paranodal and nodal regions related to anti-neurofascin-155 and anti-contactin-1 antibody-mediated
disease resulting in a reclassification as demyelinating nodo-paranodopathies. Triggering antigens and correlative antibodies for CIDP are otherwise undiscovered. While first-line therapies for CIDP currently are broad and non-targeted, a shift in approach has been to develop specific targeted treatments guided by what is understood about the underlying pathophysiology. Some of these targets include specific types of B-cell depletion, complement inhibition, immunoglobulin G (IgG) reduction via inhibition of the neonatal Fc receptor (FcRn) recycling of IgGs, treatments related to T-cell dysfunction, and macrophage inhibition.
Objectives:The objectives of this activity are to: 1) Understand the roles of cell-mediated and humoral-mediated immunity in the pathogenesis of CIDP, in order to facilitate rational decision-making regarding therapies; 2) Understand the underlying pathogenetic mechanisms by which first line therapies (immunoglobulins, corticosteroids, and plasma exchange) may be effective in treating CIDP; 3) Understand how targeted therapies can be used to expand the treatment options for CIDP, and the mechanisms by which they do so.
This paper underwent review by the Muscle & Nerve editor, but did not undergo additional, external peer review.
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DISCLOSURES
Dr. Zach Simmons (editor) has no conflicts of interest. Relevant financial relationships of the article’s authors have been disclosed and managed through the journal’s editorial review process.
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Karissa L. Gable; Yingkai Li