| Literature DB >> 34258584 |
Erin W Meermeier1, Seth J Welsh1, Meaghen E Sharik1, Megan T Du1, Victoria M Garbitt1, Daniel L Riggs1, Chang-Xin Shi1, Caleb K Stein1, Marco Bergsagel1, Bryant Chau2, Matthew L Wheeler3, Natalie Bezman3, Feng Wang2, Pavel Strop2, P Leif Bergsagel1, Marta Chesi4.
Abstract
BCMA-CD3-targeting bispecific antibodies (BsAb) are a recently developed immunotherapy class which shows potent tumor killing activity in multiple myeloma (MM). Here, we investigated a murine BCMA-CD3-targeting BsAb in the immunocompetent Vk*MYC and its IMiD-sensitive derivative Vk*MYChCRBN models of MM. The BCMA-CD3 BsAb was safe and efficacious in a subset of mice, but failed in those with high-tumor burden, consistent with clinical reports of BsAb in leukemia. The combination of BCMA-CD3 BsAb with pomalidomide expanded lytic T cells and improved activity even in IMiD resistant high-tumor burden cases. Yet, survival was only marginally extended due to acute toxicity and T cell exhaustion, which impaired T cell persistence. In contrast, the combination with cyclophosphamide was safe and allowed for a tempered pro-inflammatory response associated with long-lasting complete remission. Concurrent cytotoxic therapy with BsAb actually improved T cell persistence and function, offering a promising approach to patients with a large tumor burden.Entities:
Mesh:
Substances:
Year: 2021 PMID: 34258584 PMCID: PMC8266040 DOI: 10.1158/2643-3230.BCD-21-0038
Source DB: PubMed Journal: Blood Cancer Discov ISSN: 2643-3230