Developing high-affinity decoy receptors to treat multiple myeloma and diffuse large B cell lymphoma

Author:

Miao Yu Rebecca1ORCID,Thakkar Kaushik1ORCID,Cenik Can2ORCID,Jiang Dadi3ORCID,Mizuno Kazue1ORCID,Jia Chenjun4ORCID,Li Caiyun Grace1ORCID,Zhao Hongjuan5ORCID,Diep Anh1ORCID,Xu Yu1ORCID,Zhang Xin Eric6ORCID,Yang Teddy Tat Chi4ORCID,Liedtke Michaela7ORCID,Abidi Parveen7ORCID,Leung Wing-sze1ORCID,Koong Albert C.3ORCID,Giaccia Amato J.16ORCID

Affiliation:

1. Department of Radiation Oncology, Stanford University, Stanford, CA 1

2. Department of Molecular Biosciences, University of Texas at Austin, Austin, TX 2

3. Department of Radiation Oncology, MD Anderson Cancer Center, Houston, TX 3

4. ChemPartner Shanghai, Shanghai, China 4

5. Department of Urology, Stanford University, Stanford, CA 5

6. Department of Oncology, Oxford Institute for Radiation Oncology, University of Oxford, Oxford, UK 7

7. Department of Medicine (Hematology), Stanford University, Stanford, CA 6

Abstract

Disease relapse and treatment-induced immunotoxicity pose significant clinical challenges for patients with hematological cancers. Here, we reveal distinctive requirements for neutralizing TNF receptor ligands APRIL and BAFF and their receptor activity in MM and DLBCL, impacting protein translation and production in MM cells and modulating the translation efficiency of the ATM interactor (ATMIN/ACSIZ). Therapeutically, we investigated the use of BCMA decoy receptor (sBCMA-Fc) as an inhibitor of APRIL and BAFF. While wild-type sBCMA-Fc effectively blocked APRIL signaling in MM, it lacked activity in DLBCL due to its weak BAFF binding. To expand the therapeutic utility of sBCMA-Fc, we engineered an affinity-enhanced mutant sBCMA-Fc fusion molecule (sBCMA-Fc V3) 4- and 500-fold stronger in binding to APRIL and BAFF, respectively. The mutant sBCMA-Fc V3 clone significantly enhanced antitumor activity against both MM and DLBCL. Importantly, we also demonstrated an adequate toxicity profile and on-target mechanism of action in nonhuman primate studies.

Funder

Silicon Valley Community Foundation

Sydney Frank Foundation

Kimmelman Fund

Medical Research Council

Cancer Prevention and Research Institute of Texas

Welch Foundation

Publisher

Rockefeller University Press

Subject

Immunology,Immunology and Allergy

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