| Literature DB >> 29654274 |
Leonhard Busch1, Dimitrios Mougiakakos1, Maike Büttner-Herold2, Miriam J Müller3, Dietrich A Volmer3, Christian Bach1, Mario Fabri4, Jörg T Bittenbring5, Frank Neumann5, Rainer Boxhammer6, Jens Nolting7, Savita Bisht7, Martin Böttcher1, Simon Jitschin1, Markus H Hoffmann8, Heidi Balzer1, Fabian Beier9, Deniz Gezer9, Diana Dudziak10, Kolja Gelse11, Friedrich F Hennig11, Christian P Pallasch12, Bernd Spriewald1, Andreas Mackensen1, Heiko Bruns13.
Abstract
Macrophages are key mediators of the therapeutic effects exerted by monoclonal antibodies, such as the anti-CD38 antibody MOR202, currently introduced in multiple myeloma (MM) therapy. Therefore, it is important to understand how antibody-mediated effector functions of myeloma-associated macrophages (MAMs) are regulated. Here, we focused on the effects of vitamin D, a known regulator of macrophage effector functions. Consequently, it was the aim of this study to assess whether modulation of the vitamin D pathway alters the tumoricidal activity of MAMs. Here, we demonstrate that MAMs display a defective vitamin D pathway with reduced expression level of CYP27B1 and limited tumoricidal activity which can be restored by the IMiD lenalidomide in vitro. Furthermore, our data indicate that the vitamin D pathway of MAMs from MM patients does recover during an IMiD-containing therapy shown by an improved MOR202-mediated cytotoxic activity of these MAMs against primary MM cells ex vivo. Here, the ex vivo cytotoxic activity could be further enhanced by vitamin D supplementation. These data suggest that vitamin D holds a key role for the effector functions of MAMs and that vitamin D supplementation in IMiD combination trials could further increase the therapeutic efficacy of anti-CD38 antibodies such as MOR202, which remains to be investigated in clinical studies.Entities:
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Year: 2018 PMID: 29654274 DOI: 10.1038/s41375-018-0114-0
Source DB: PubMed Journal: Leukemia ISSN: 0887-6924 Impact factor: 11.528