CD40/anti-CD40 antibody complexes which illustrate agonist and antagonist structural switches

被引:19
|
作者
Argiriadi, Maria A. [1 ]
Benatuil, Lorenzo [2 ]
Dubrovska, Ievgeniia [3 ]
Egan, David A. [3 ]
Gao, Lei [2 ]
Greischar, Amy [3 ]
Hardman, Jennifer [2 ]
Harlan, John [3 ]
Iyer, Ramesh B. [3 ]
Judge, Russell A. [3 ]
Lake, Marc [3 ]
Perron, Denise C. [2 ]
Sadhukhan, Ramkrishna [2 ]
Sielaff, Bernhard [2 ]
Sousa, Silvino [2 ]
Wang, Rui [2 ]
McRae, Bradford L. [2 ]
机构
[1] AbbVie Biores Ctr, 381 Plantat St, Worcester, MA 01605 USA
[2] AbbVie Biores Ctr, 100 Res Dr, Worcester, MA 01605 USA
[3] AbbVie Inc, 1 North Waukegan Rd, N Chicago, IL 60064 USA
关键词
CD40; Crystal structure; Agonist; Antagonist; Antibody; MONOCLONAL-ANTIBODY; DENDRITIC CELL; IN-VITRO; CD40;
D O I
10.1186/s12860-019-0213-4
中图分类号
Q2 [细胞生物学];
学科分类号
071009 ; 090102 ;
摘要
Background CD40 is a 48 kDa type I transmembrane protein that is constitutively expressed on hematopoietic cells such as dendritic cells, macrophages, and B cells. Engagement of CD40 by CD40L expressed on T cells results in the production of proinflammatory cytokines, induces T helper cell function, and promotes macrophage activation. The involvement of CD40 in chronic immune activation has resulted in CD40 being proposed as a therapeutic target for a range of chronic inflammatory diseases. CD40 antagonists are currently being explored for the treatment of autoimmune diseases and several anti-CD40 agonist mAbs have entered clinical development for oncological indications. Results To better understand the mode of action of anti-CD40 mAbs, we have determined the x-ray crystal structures of the ABBV-323 (anti-CD40 antagonist, ravagalimab) Fab alone, ABBV-323 Fab complexed to human CD40 and FAB516 (anti-CD40 agonist) complexed to human CD40. These three crystals structures 1) identify the conformational CD40 epitope for ABBV-323 recognition 2) illustrate conformational changes which occur in the CDRs of ABBV-323 Fab upon CD40 binding and 3) develop a structural hypothesis for an agonist/antagonist switch in the LCDR1 of this proprietary class of CD40 antibodies. Conclusions The structure of ABBV-323 Fab demonstrates a unique method for antagonism by stabilizing the proposed functional antiparallel dimer for CD40 receptor via novel contacts to LCDR1, namely residue position R32 which is further supported by a closely related agonist antibody FAB516 which shows only monomeric recognition and no contacts with LCDR1 due to a mutation to L32 on LCDR1. These data provide a structural basis for the full antagonist activity of ABBV-323.
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页数:13
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