Prevalence of antibodies to Ro-52 in a serologically defined population of patients with systemic sclerosis

doi:10.1186/1740-2557-6-2

Journal of Autoimmune Diseases

Volume 6

Viewing options:

Abstract
Full text
PDF (223KB)

Associated material:

Related literature:

Articles citing this article
on Google Scholar
on PubMed Central
Other articles by authors
on Google Scholar

Parker JC
Burlingame RW
Bunn CC

on PubMed

Parker JC
Burlingame RW
Bunn CC
Related articles/pages
on Google

on Google Scholar

on PubMed

Tools:

Post to:

Research

Prevalence of antibodies to Ro-52 in a serologically defined population of patients with systemic sclerosis

Jennifer C Parker¹, Rufus W Burlingame² and Christopher C Bunn¹

¹Department of Clinical Immunology, Royal Free Hospital, London, NW3 2QG, UK

²INOVA Diagnostics Inc., San Diego, California, 92131-1638, USA

Journal of Autoimmune Diseases 2009, 6:2doi:10.1186/1740-2557-6-2


Published:	6 March 2009

Abstract

Background

Antibodies against Ro-52 have been described in patients with a broad spectrum of autoimmune disease, most commonly in association with anti-Ro-60 in systemic lupus erythematosus and Sjogrens syndrome. However, in inflammatory myositis anti-Ro-52 is frequently present without anti-Ro-60 and is closely linked to the presence of aminoacyl-tRNA synthetase (aats) antibodies. To date there have been no comprehensive reports on the frequency of anti-Ro-52 in systemic sclerosis (SSc), a disease characterised by hallmark autoantibodies that occur in non-overlapping subsets. Clinically, each antibody-defined group has a distinct pattern of organ involvement, some featuring myositis.

Objectives

To determine the frequency of anti-Ro-52 in serologically defined groups of SSc patients and to investigate a possible link with myositis-associated autoantibodies.

Methods

Serum samples from 1010 patients with SSc and 55 and 32 patients with anti-aats and anti-Ku respectively were tested for the presence of anti-Ro-52 using a commercial ELISA.

Results

The prevalence of anti-Ro-52 was 15–38% in nine of the eleven sub-groups. There were no significant differences in mean anti-Ro-52 levels in these groups with the exception of that defined by the presence of anti-U1-RNP. In the remaining groups defined by anti-Ro-60 and anti-aats, anti-Ro-52 was present in 92% and 100% respectively. In sera from non-SSc patients with anti-aats, anti-Ro-52 was detected in 64%.

Conclusion

Anti-Ro-52 is present throughout the SSc population. It is neither more prevalent in the myositis-associated antibody groups nor does it segregate with any other major SSc-specific autoantibodies. The co-existence of anti-Ro-52 with both anti-Ro-60 and anti-aats is confirmed.