Title of article
Natural killer cell phenotype and clinical response to interferon-beta therapy in multiple sclerosis
Author/Authors
Martيnez-Rodrيguez، نويسنده , , J.E. and Lَpez-Botet، نويسنده , , M. and Munteis، نويسنده , , E. and Rio، نويسنده , , J. and Roquer، نويسنده , , J. and Montalban، نويسنده , , X. and Comabella، نويسنده , , M.، نويسنده ,
Issue Information
روزنامه با شماره پیاپی سال 2011
Pages
9
From page
348
To page
356
Abstract
CD56bright NK cells, which may play a role in immunoregulation, are expanded in multiple sclerosis (MS) patients treated with immunomodulatory therapies such as daclizumab and interferon-beta (IFNβ). Yet, whether this NK cell subset is directly involved in the therapeutic effect is unknown. As NK receptor (NKR) expression by subsets of NK cells and CD8+ T lymphocytes is related to MS clinical course, we addressed whether CD56bright NK cells and NKR in IFNβ-treated MS patients differ according to the clinical response. IFNβ was associated to lower LILRB1+ and KIR + NK cells, and higher NKG2A + NK cell proportions, an immunophenotypic pattern mainly found in responders. After IFNβ treatment, a CD56bright NK cell expansion was significantly related to a positive clinical response. Our results reveal that IFNβ may promote in responders changes in the NK cell immunophenotype, corresponding to the profile found at early maturation stages of this lymphocyte lineage.
Keywords
MULTIPLE SCLEROSIS , KIR , CD56 , interferon-beta , LILRB1 , Natural killer receptors
Journal title
Clinical Immunology
Serial Year
2011
Journal title
Clinical Immunology
Record number
1855403
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