A subset of fibromyalgia patients have findings suggestive of chronic inflammatory demyelinating polyneuropathy and appear to respond to IVIg

doi:10.1093/rheumatology/kem345

Rheumatology 2008 47(2):208-211; doi:10.1093/rheumatology/kem345

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A subset of fibromyalgia patients have findings suggestive of chronic inflammatory demyelinating polyneuropathy and appear to respond to IVIg

X. J. Caro, E. F. Winter and A. J. Dumas

Division of Rheumatology, David Geffen School of Medicine at UCLA, Los Angeles, CA, USA.

Correspondence to: X. J. Caro, 18350 Roscoe Blvd., Suite 418, CA 91325-4174, USA. E-mail: xjcaro{at}earthlink.net

Abstract

Objectives. The aetiopathogenesis of the fibromyalgia syndrome(FMS) remains unknown. Recent reports, however, suggest thata subgroup of FMS subjects has an immune-mediated disease. Therefore,our primary objective was to study FMS subjects for evidenceof an immune-mediated demyelinating polyneuropathy. Our secondaryobjective was to determine the effects of treating these FMSsubjects with the immune modulator, intravenous immunoglobulin(IVIg).

Methods. Fifty-eight FMS subjects, 26 rheumatic non-FMS subjectsand 52 non-rheumatic non-FMS subjects were studied. Subjectivemeasures of paraesthesias, weakness, stocking hypaesthesia,pain, fatigue and stiffness were made. Objective measures oftenderness, proximal muscle strength and electrodiagnostic (EDX)evidence of polyneuropathy and demyelination were also made.Eleven other FMS subjects underwent sural nerve biopsy.

Results. Paraesthesias, subjective weakness and stocking hypaesthesiawere more common in FMS than in rheumatic non-FMS (P $≤$ 0.0001).Proximal muscle strength was less in FMS than in rheumatic non-FMS(P $≤$ 0.0001). EDX demonstrated a distal demyelinating polyneuropathy,suggestive of chronic inflammatory demyelinating polyneuropathy(CIDP), in 33% of FMS subjects. No rheumatic non-FMS subjecthad polyneuropathy (P = 0.005), or demyelination (P = 0.05).Fifteen FMS/CIDP subjects were subsequently treated with IVIg(400 mg/kg each day for 5 days). Pain (P = 0.01), tenderness(P = 0.001) and strength (P = 0.04) improved significantly.Fatigue and stiffness trended towards improvement.

Conclusions. A significant subset of FMS subjects have clinicaland EDX findings suggestive of CIDP. IVIg treatment shows promisein treating this subset. These observations have implicationsfor better understanding and treating some FMS patients.

KEY WORDS: Fibromyalgia, IVIg, Chronic inflammatory demyelinating polyneuropathy

Submitted 1 August 2007; revised version accepted 19 November 2007.
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