| Literature DB >> 22816666 |
Mareen Matz1, Martin Lehnert, Christine Lorkowski, Katharina Fabritius, Nadine Unterwalder, Salim Doueiri, Ulrike A Weber, Mir-Farzin Mashreghi, Hans-H Neumayer, Klemens Budde.
Abstract
Humoral rejection processes may lead to allograft injury and subsequent dysfunction. Today, only one B-cell-specific agent is in clinical use and the effects of standard and new immunosuppressant substances on B-cell activation and function are not fully clarified. The impact of sotrastaurin, mycophenolic acid and everolimus on human B-lymphocyte function was assessed by analysing proliferation, apoptosis, CD80/CD86 expression and immunoglobulin and IL-10 production in primary stimulated B cells. In addition, B-cell co-cultures with pre-activated T cells were performed to evaluate the effect of the different immunosuppressive agents on T-cell-dependent immunoglobulin production. Sotrastaurin did not inhibit B-cell proliferation, CD80/CD86 expression, and IgG production and had only minor effects on IgM levels at the highest concentration administered. In contrast, mycophenolic acid and everolimus had strong effects on all B-cell functions in a dose-dependent manner. All immunosuppressive agents caused decreased immunoglobulin levels in T-cell-dependent B-cell cultures. The data provided here suggest that mycophenolic acid and everolimus, but not sotrastaurin, are potent inhibitors of human B-lymphocyte function and activation.Entities:
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Year: 2012 PMID: 22816666 DOI: 10.1111/j.1432-2277.2012.01537.x
Source DB: PubMed Journal: Transpl Int ISSN: 0934-0874 Impact factor: 3.782