Tumor-targeted nanoparticles improve the therapeutic index of BCL2 and MCL1 dual inhibition

Author:

Bala Tannan Neeta1ORCID,Manzari Mandana T.2ORCID,Herviou Laurie1ORCID,Da Silva Ferreira Mariana1,Hagen Connor3,Kiguchi Hiroto2ORCID,Manova-Todorova Katia4ORCID,Seshan Venkatraman5,de Stanchina Elisa3,Heller Daniel A.2ORCID,Younes Anas16

Affiliation:

1. Department of Medicine,

2. Molecular Pharmacology Program,

3. Antitumor Assessment Core,

4. Molecular Cytogenetics Core,

5. Department of Epidemiology and Biostatistics, and

6. Lymphoma Service, Memorial Sloan Kettering Cancer Center, New York, NY

Abstract

Abstract Cancer and normal cells use multiple antiapoptotic BCL2 proteins to prevent cell death. Therapeutic targeting of multiple BCL2 family proteins enhances tumor killing but is also associated with increased systemic toxicity. Here, we demonstrate that the dual targeting of MCL1 and BCL2 proteins using the small molecules S63845 and venetoclax induces durable remissions in mice that harbor human diffuse large B-cell lymphoma (DLBCL) tumors but is accompanied by hematologic toxicity and weight loss. To mitigate these toxicities, we encapsulated S63845 or venetoclax into nanoparticles that target P-selectin, which is enriched in tumor endothelial cells. In vivo and ex vivo imaging demonstrated preferential targeting of the nanoparticles to lymphoma tumors over vital organs. Mass spectrometry analyses after administration of nanoparticle drugs confirmed tumor enrichment of the drug while reducing plasma levels. Furthermore, nanoparticle encapsulation allowed 3.5- to 6.5-fold reduction in drug dose, induced sustained remissions, and minimized toxicity. Our results support the development of nanoparticles to deliver BH3 mimetic combinations in lymphoma and in general for toxic drugs in cancer therapy.

Publisher

American Society of Hematology

Subject

Cell Biology,Hematology,Immunology,Biochemistry

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