| Literature DB >> 25024386 |
Ann L White1, Lang Dou1, H T Claude Chan1, Vikki L Field1, C Ian Mockridge1, Kane Moss1, Emily L Williams1, Steven G Booth1, Ruth R French1, Elizabeth A Potter1, Cherié Butts2, Aymen Al-Shamkhani1, Mark S Cragg1, J Sjef Verbeek3, Peter W M Johnson4, Martin J Glennie1, Stephen A Beers5.
Abstract
Immunomodulatory mAbs, led by the anti-CTLA4 mAb ipilimumab, are an exciting new class of drugs capable of promoting anticancer immunity and providing durable control of some tumors. Close analysis of a number of agents has revealed a critical yet variable role for Fcγ receptors in their efficacy. In this article, we reveal that agonistic anti-CD40 mAbs have an absolute requirement for cross-linking by inhibitory FcγRIIB when used systemically to treat established BCL1 syngeneic lymphoma, and therapy is lost when using a mouse IgG2a mAb not cross-linked by FcγRIIB. Furthermore, in FcγRIIB-deficient mice the lymphoma itself can provide FcγRIIB to cross-link anti-CD40 on neighboring cells, and only when this is blocked does therapy fail. The dependence on FcγRIIB for immunostimulatory activity was not absolute, however, because when anti-CD40 mAbs were administered systemically with the TLR3 agonist polyinosinic:polycytidylic acid or were given subcutaneously, activatory FcγR could also provide cross-linking. Using this mechanistic insight, we designed multimeric forms of anti-CD40 mAb with intrinsic FcγR-independent activity that were highly effective in the treatment of lymphoma-bearing mice. In conclusion, FcγR-independent anti-CD40 activation is a viable strategy in vivo. These findings have important translational implications, as humans, unlike mice, do not have IgG that binds strongly to FcγRIIB; therefore FcγR-independent derivatives represent an attractive therapeutic option.Entities:
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Year: 2014 PMID: 25024386 DOI: 10.4049/jimmunol.1303204
Source DB: PubMed Journal: J Immunol ISSN: 0022-1767 Impact factor: 5.422