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Peripheral accumulation of newly produced T and B lymphocytes in natalizumab-treated multiple sclerosis patients
Authors:Cinzia Zanotti  Marco Chiarini  Federico Serana  Alessandra Sottini  Emirena Garrafa  Fabio Torri  Luigi Caimi  Sarah Rasia  Ruggero Capra  Luisa Imberti
Affiliation:Biotechnology Laboratory, Diagnostics Department, Spedali Civili di Brescia, P.le Spedali Civili 1, 25123 Brescia, Italy. Electronic address: zanotti.cinzia@gmail.com.
Abstract:The anti-α4 monoclonal antibody natalizumab inhibits lymphocyte extravasation into the central nervous system and increases peripheral T and B lymphocytes in multiple sclerosis patients. To investigate whether the lymphocyte accumulation was due to a higher lymphocyte production, an altered homeostasis, or a differential transmigration of lymphocyte subsets through endothelia, T-cell receptor excision circles and kappa-deleting recombination excision circles were quantified before and after treatment, T-cell receptor repertoire was analyzed by spectratyping, and T- and B-lymphocyte subset migration was studied using transwell coated with vascular and lymphatic endothelial cells. We found that the number of newly produced T and B lymphocytes is increased because of a high release and of a low propensity of naïve subsets to migrate across endothelial cells. In some patients this resulted in an enlargement of T-cell heterogeneity. Because new lymphocyte production ensures the integrity of immune surveillance, its quantification could be used to monitor natalizumab therapy safety.
Keywords:MS, multiple sclerosis   VLA-4, very late antigen-4   VCAM-1, vascular cell adhesion molecule 1   BBB, blood–brain barrier   CNS, central nervous system   BM, bone marrow   TCR, T-cell receptor   TRECs, T-cell receptor excision circles   KRECs, kappa-deleting recombination excision circles   BECs, blood endothelial cells   LECs, lymphatic endothelial cells   HDs, healthy donors   PBMCs, peripheral blood mononuclear cells   TCRAC, TCR constant alpha chain   mAbs, monoclonal antibodies   TCRBV, TCR variable beta   TEMRA, CD45RA+ T effector memory   PML, progressive multifocal leukoencephalopathy.
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