Intrathecal antibody production against Chlamydia pneumoniae in multiple sclerosis is part of a polyspecific immune response

doi:10.1093/brain/124.7.1325

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Brain, Vol. 124, No. 7, 1325-1335, July 2001
© 2001 Oxford University Press

Intrathecal antibody production against Chlamydia pneumoniae in multiple sclerosis is part of a polyspecific immune response

Tobias Derfuss¹^,*, Robert Gürkov¹^,*, Florian Then Bergh², Norbert Goebels², Matthias Hartmann⁵, Corinna Barz³, Bettina Wilske³, Ingo Autenrieth³, Manfred Wick⁴, Reinhard Hohlfeld¹^,2 and Edgar Meinl¹^,2

¹ Department of Neuroimmunology, Max-Planck-Institute of Neurobiology, Martinsried, ² Institute for Clinical Neuroimmunology and Department of Neurology and ³ Institute for Clinical Chemistry, Ludwig-Maximilians University, ⁴ Max-v-Pettenkofer-Institute, Munich and ⁵ Institute for Medical Microbiology, FSU Jena, Germany

Correspondence to: Dr Edgar Meinl, Department of Neuroimmunology, Max-Planck-Institute of Neurobiology, Am Klopferspitz 18a, D-82152 Martinsried, Germany E-mail: meinl{at}neuro.mpg.de

Chronic intrathecal immunoglobulin (Ig) production is a hallmarkof multiple sclerosis characterized by the presence of oligoclonalIgGs and, in addition, polyspecific recognition of differentpathogens such as measles, rubella and herpes zoster virus.While the antigen specificity of the oligoclonal IgGs in multiplesclerosis is largely unknown, the oligoclonal IgGs arising duringCNS infectious diseases are reactive against the specific pathogen.Recently, a link between Chlamydia pneumoniae and multiple sclerosishas been claimed. To test the possible role of C. pneumoniaein multiple sclerosis, we analysed (i) whether there is intrathecalIgG production against C. pneumoniae in multiple sclerosis and(ii) if the oligoclonal IgGs in the CSF of multiple sclerosispatients recognize C. pneumoniae. By studying paired serum–CSFsamples from 120 subjects (definite multiple sclerosis, 46;probable multiple sclerosis, 12; other inflammatory neurologicaldiseases, 35; other neurological diseases, 27) by enzyme-linkedimmunosorbent assay, we found that 24% of all patients withdefinite multiple sclerosis, but only 5% of patients with otherinflammatory or non-inflammatory diseases, produced IgGs specificfor C. pneumoniae intrathecally (definite multiple sclerosisversus other inflammatory neurological diseases: P = 0.027).The presence of intrathecal IgGs to C. pneumoniae was independentof the duration of disease and relatively stable over time.The major CSF oligoclonal IgG bands from multiple sclerosispatients with an intrathecal Ig production to C. pneumoniaedid not react towards purified elementary bodies and reticulatebodies of C. pneumoniae on affinity-mediated immunoblot followingisoelectric focusing (IEF-western blots). In contrast, the IgGsin the CSF of control patients with neuroborreliosis stronglyreacted with their specific pathogen, Borrelia burgdorferi,by IEF-western blot analysis. Concomitant analysis of the CSFof 23 patients with a nested polymerase chain reaction for C.pneumoniae was negative in all cases. Together, our findingsstrongly suggest that the immune response to C. pneumoniae ispart of a polyspecific intrathecal Ig production, as is commonlyobserved with other pathogens. This argues against a specificrole for C. pneumoniae in multiple sclerosis.

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