A Bispecific Molecule Targeting CD40 and Tumor Antigen Mesothelin Enhances Tumor-Specific Immunity

被引:38
作者
Ye, Shiming [1 ]
Cohen, Diane [1 ]
Belmar, Nicole A. [1 ]
Choi, Donghee [1 ]
Tan, Siu Sze [1 ]
Sho, Mien [1 ]
Akamatsu, Yoshiko [1 ]
Kim, Han [1 ]
Iyer, Ramesh [2 ]
Cabel, Jean [2 ]
Lake, Marc [2 ]
Song, Danying [2 ]
Harlan, John [2 ]
Zhang, Catherine [1 ]
Fang, Yuni [1 ]
Wahl, Alan F. [1 ,3 ]
Culp, Patricia [1 ,4 ]
Hollenbaugh, Diane [1 ,5 ]
Chao, Debra T. [1 ]
机构
[1] AbbVie Biotherapeut Inc, 1500 Seaport Blvd, Redwood City, CA 94063 USA
[2] AbbVie Inc, N Chicago, IL USA
[3] Ambrx, San Diego, CA USA
[4] Maverick Therapeut Inc, Brisbane, CA USA
[5] Good Therapeut Inc, Seattle, WA USA
关键词
PRESENTING CELLS; DENDRITIC CELLS; B-CELLS; ANTIBODY; ACTIVATION; THERAPY; INDUCTION; TOLERANCE; RESPONSES; EFFICACY;
D O I
10.1158/2326-6066.CIR-18-0805
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Agonistic CD40 monoclonal antibodies (mAb) have demonstrated some clinical activity, but with dose-limiting toxicity. To reduce systemic toxicity, we developed a bispecific molecule that was maximally active in the presence of a tumor antigen and had limited activity in the absence of the tumor antigen. LB-1 is a bispecific molecule containing single-chain Fv domains targeting mouse CD40 and the tumor antigen mesothelin. LB-1 exhibited enhanced activity upon binding to cell-surface mesothelin but was less potent in the absence of mesothelin binding. In a mouse model implanted with syngeneic 4T1 tumors expressing cell-surface mesothelin, LB-1 demonstrated comparable antitumor activity as an agonistic CD40 mAb but did not cause elevation of serum cytokines and liver enzymes, as was observed in anti-CD40- treated mice. The results from our study of LB-1 were used to develop a human cross-reactive bispecific molecule (ABBV-428) that targeted human CD40 and mesothelin. ABBV-428 demonstrated enhanced activation of antigen-presenting cells and T cells upon binding to cell-surface mesothelin, and inhibition of cultured or implanted PC3 tumor cell growth after immune activation. Although expression of cell-surface mesothelin is necessary, the bispecific molecules induced immune-mediated antitumor activity against both mesothelin(+) and mesothelin(-) tumor cells. ABBV-428 represents a class of bispecific molecules with conditional activity dependent on the binding of a tumor-specific antigen, and such activity could potentially maximize antitumor potency while limiting systemic toxicity in clinical studies.
引用
收藏
页码:1864 / 1875
页数:12
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