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J Neurol Neurosurg Psychiatry 1999;66:791-793 doi:10.1136/jnnp.66.6.791
  • Short report

Cerebrospinal fluid concentrations of soluble CD27 in HTLV-I associated myelopathy and multiple sclerosis

  1. Rogier Q Hintzen,
  2. Donald Paty,
  3. Joel Oger
  1. Multiple Sclerosis Clinic and Department of Medicine, Faculty of Medicine, Vancouver Hospital, and Health Sciences Center and University of British Columbia Vancouver, British Columbia, Canada
  1. Dr J Oger, Department of Medicine, Vancouver Health Sciences Centre and University of British Columbia, S159–2211 Wesbrook Mall, Vancouver, BC V6T 2B5, Canada. Telephone 001 604 822 7696; fax 001 604 822 0758; email oger{at}interchange.ubc.ca
  • Received 3 August 1998
  • Revised 9 November 1998
  • Accepted 18 November 1998

Abstract

OBJECTIVES Stimulation of T lymphocytes via the T cell receptor strongly enhances CD27 membrane expression and induces the release of a soluble 32 kDa form of CD27 (sCD27). CD27 is a member of the TNF receptor family, a group of molecules that have important roles in lymphocyte differentiation and survival. Raised concentrations of sCD27 have been reported in various immunopathological conditions and there is evidence that this molecule can serve as a marker of T cell activation in vivo. Concentrations of sCD27 in CSF were compared between patients with T cell mediated neurological disease and non-inflammatory controls. Also, the relation of CSF-sCD27 concentrations with clinical disease activity was investigated in patients with multiple sclerosis.

METHODS Four groups were studied: (1) eight patients with HTLV-1 associated myelopathy/ tropical spastic paraparisis (HAM)/TSP), (2) eight HTLV-I carriers, (3) 41 patients with multiple sclerosis, and (4) 43 patients with other neurological disease (OND). Concentrations of CSF-sCD27 were determined by enzyme linked immunosorbent assay (ELISA).

RESULTS Quantification of CSF-sCD27 differentiates patients with HAM/TSP from HTLV-I carriers (p<0.01) and from patients with OND (p<0.001). Moreover, the multiple sclerosis patient group was different from the OND group (p<0.0001). In patients with multiple sclerosis, CSF-sCD27 concentrations were higher in 24 patients with clinically active disease than in 17 with clinically stable disease. In addition, most of the patients with multiple sclerosis with high sCD27 concentrations showed an increase in EDSS, whereas none of the patients with low sCD27 had an EDSS increase.

CONCLUSIONS As a reliable marker of immunological disease activity in inflammatory white matter disease is still not available, it is proposed that quantification of CSF-sCD27 concentrations is a good candidate. Also, it may serve as a tool to stratify neurological diseases in inflammatory and non-inflammatory states.

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