Polymyalgia rheumatica can be distinguished from late onset rheumatoid arthritis at baseline: results of a 5-yr prospective study

doi:10.1093/rheumatology/ken343

Rheumatology Advance Access originally published online on November 2, 2008
Rheumatology 2009 48(2):123-127; doi:10.1093/rheumatology/ken343

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Polymyalgia rheumatica can be distinguished from late onset rheumatoid arthritis at baseline: results of a 5-yr prospective study

C. T. Pease¹, G. Haugeberg¹^,2, B. Montague³, E. M. A. Hensor¹, B. B. Bhakta¹, W. Thomson⁴, W. E. R. Ollier⁵ and A. W. Morgan¹

¹Section of Musculoskeletal Disease, Leeds Institute of Molecular Medicine, University of Leeds, Leeds, UK, ²Norwegian University of Science and Technology, Trondheim, Norway, ³Transplant and Cellular Immunology, St James's University Hospital, Leeds, ⁴ARC-EU, Stopford Building and ⁵The Centre for Integrated Genomic Medical Research, University of Manchester, Manchester, UK.

Correspondence to: C. T. Pease, Department of Rheumatology, Chapel Allerton Hospital, Chapeltown Road, Leeds LS7 4SA, UK. E-mail: colin.pease{at}leedsth.nhs.uk

Abstract

Objective. To describe the pattern of arthropathy and HLA-DRB1alleles associated with PMR in order to develop a diagnosticalgorithm that could help distinguish PMR and RF-negative (RF–ve) late-onset RA (LO-RA) at presentation.

Methods. This was a prospective study of all patients presentingwith PMR or LO-RA over a 10-yr period to one physician. Demographic,clinical and laboratory data were collected at presentationand during a minimum of 5 yrs of follow-up. The accuracy ofthe initial diagnosis was systematically reviewed.

Results. One hundred and forty-two patients with LO-RA, 147with PMR and 42 with PMR + TA were studied. Peripheral synovitiswas observed in 23% of the PMR patients. In comparison withRF –ve LO-RA, PMR patients were younger (P < 0.001),myalgia more frequent [100 vs 16% (P < 0.001)] and arthritisof PIP, MCP and wrist were less frequent (P < 0.001). Thecombination of wrist + MCP/PIP or wrist + PIP + MCP were highlysuggestive of RF –ve LO-RA (P < 0.001). HLA-DRB1*0101/0102and *0401 were significantly increased in PMR patients comparedwith healthy controls. Plasma viscosity and arthritis in thewrist, in combination with at least one MCP or PIP joint atdisease onset, were predictive of whether a non-erosive RF –vepatient would ultimately be diagnosed as having RF –veLO-RA or PMR (±/arthritis).

Conclusion. Our longitudinal follow-up data were consistentwith RF –ve LO-RA being a separate disease entity to PMRdespite some phenotypic and immunogenetic similarities at diseaseonset. A diagnostic algorithm was derived using baseline clinicalfeatures to predict the final diagnosis of RF –ve, non-erosivepatients.

KEY WORDS: Rheumatoid arthritis, Polymyalgia rheumatica, Temporal arteritis, HLA-DRB1, Prospective study, Outcome

Submitted 23 January 2008; revised version accepted 16 July 2008.
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