Comparative immune responses to candidate arthritogenic bacteria do not confirm a dominant role for Klebsiella pneumonia in the pathogenesis of familial ankylosing spondylitis

doi:10.1093/rheumatology/keg482

Rheumatology Advance Access published online on August 29, 2003
Rheumatology, doi:10.1093/rheumatology/keg482
Rheumatology © British Society for Rheumatology 2003; all rights reserved

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Original Papers

Comparative immune responses to candidate arthritogenic bacteria do not confirm a dominant role for Klebsiella pneumonia in the pathogenesis of familial ankylosing spondylitis

M. A. Stone ¹, U. Payne ², C. Schentag ², P. Rahman ³, C. Pacheco-Tena ², and R. D. Inman ¹^*

¹ Toronto Western Research Institute, University Health Network, University of Toronto, Toronto, Ontario, Canada; Department of Medicine, University of Toronto, Toronto, Ontario, Canada
² Toronto Western Research Institute, University Health Network, University of Toronto, Toronto, Ontario, Canada
³ Department of Medicine, Memorial University, St John's, Newfoundland, Canada

^* Corresponding author. E-mail: robert.inman{at}uhn.on.ca.

Received 20 March 2003 ; accepted 3 July 2003

Abstract

Objective. Using humoral immune responses, Klebsiella pneumoniaehas been implicated as a candidate microbial trigger in ankylosingspondylitis (AS) by several investigators but refuted by others.The objective of this case-control study was to compare thecellular (T-cell proliferation) and humoral (IgG and IgA, byELISA) immune responses of affected individuals in multiplexAS families with those of unaffected family members and normalhealthy controls in order to find out whether affected individualsexhibit a predominant immune response to K. pneumoniae.

Methods.Twenty-five families with two or more individuals affected withAS and 34 normal healthy controls matched with the affectedfamily members for age, sex and ethnicity were enrolled in thestudy. All affected (n = 57) and unaffected (n = 37) familymembers had a detailed clinical evaluation. Peripheral bloodwas drawn to determine T-lymphocyte proliferation and the IgGand IgA (by ELISA analysis) immune responses to K. pneumoniae,Salmonella typhimurium, Yersinia enterocolitica and Chlamydiatrachomatis. Immune responses to each of the four candidateorganisms were compared in affected and unaffected individuals.Each individual was classified by the predominant antigenicimmune response that they showed when comparison was made amongthe same concentrations of the four candidate microbial antigens.This stratification was then used (i) to compare immune responsesin affected and unaffected family members and (ii) to compareclinical characteristics of affected family members.

Results.There was no difference in mean stimulation indices or antibodyresponses between affected and unaffected family members foreach of the candidate organisms. In terms of predominant cellularimmune responses to these organisms, there was no differencebetween affected and unaffected family members with respectto K. pneumoniae, C. trachomatis or Y. enterocolitica. However,a higher percentage of affected family members (25.9%) exhibiteda predominant response to S. typhimurium compared with unaffectedfamily members (5.9%, P < 0.02). In assessing antibody titres,K. pneumoniae was the predominant amongst these four organisms,but there was no difference between affected family members,unaffected family members and normal healthy controls. Therewas no relationship between immune responses and clinical characteristics.

Conclusion.Our analysis of affected and unaffected family members in familialAS demonstrated no significant differences with respect to cellularor humoral immune responses to K. pneumoniae and three controlmicrobes. In addition, K. pneumoniae did not exhibit a predominantimmune response in affected individuals. Thus we find no supportiveevidence to implicate a causal role for K. pneumoniae in familialAS.

Key words: Ankylosing spondylitis, Klebsiella pneumoniae, HLA-B27, Immune responses.
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