1. VLA4-Targeted Nanoparticles Hijack Cell Adhesion–Mediated Drug Resistance to Target Refractory Myeloma Cells and Prolong Survival
- Author
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Xiaoxia Yang, Steven Fletcher, Noriko Yanaba, John S. Allen, Julie Ritchey, Julie O'Neal, Grace Cui, Ravi Vij, Mark A. Fiala, Anne H. Schmieder-Atteberry, Kathleen Simons, Francesca Fontana, Michael J. Scott, John F. DiPersio, Dipanjan Pan, Michael P. Rettig, and Gregory M. Lanza
- Subjects
0301 basic medicine ,Melphalan ,Cancer Research ,medicine.medical_treatment ,Drug resistance ,Integrin alpha4beta1 ,Dexamethasone ,Article ,Mice ,03 medical and health sciences ,0302 clinical medicine ,In vivo ,hemic and lymphatic diseases ,Cell Line, Tumor ,Cell Adhesion ,medicine ,Animals ,Humans ,Multiple myeloma ,Chemotherapy ,business.industry ,Cancer ,Prodrug ,medicine.disease ,Mice, Inbred C57BL ,030104 developmental biology ,Oncology ,Drug Resistance, Neoplasm ,030220 oncology & carcinogenesis ,Cancer research ,Nanoparticles ,Camptothecin ,Topoisomerase I Inhibitors ,Multiple Myeloma ,business ,medicine.drug - Abstract
Purpose: In multiple myeloma, drug-resistant cells underlie relapse or progression following chemotherapy. Cell adhesion–mediated drug resistance (CAM-DR) is an established mechanism used by myeloma cells (MMC) to survive chemotherapy and its markers are upregulated in residual disease. The integrin very late antigen 4 (VLA4; α4β1) is a key mediator of CAM-DR and its expression affects drug sensitivity of MMCs. Rather than trying to inhibit its function, here, we hypothesized that upregulation of VLA4 by resistant MMCs could be exploited for targeted delivery of drugs, which would improve safety and efficacy of treatments. Experimental Design: We synthetized 20 nm VLA4-targeted micellar nanoparticles (V-NP) carrying DiI for tracing or a novel camptothecin prodrug (V-CP). Human or murine MMCs, alone or with stroma, and immunocompetent mice with orthotopic multiple myeloma were used to track delivery of NPs and response to treatments. Results: V-NPs selectively delivered their payload to MMCs in vitro and in vivo, and chemotherapy increased their uptake by surviving MMCs. V-CP, alone or in combination with melphalan, was well tolerated and prolonged survival in myeloma-bearing mice. V-CP also reduced the dose requirement for melphalan, reducing tumor burden in association with suboptimal dosing without increasing overall toxicity. Conclusions: V-CP may be a safe and effective strategy to prevent or treat relapsing or refractory myeloma. V-NP targeting of resistant cells may suggest a new approach to environment-induced resistance in cancer.
- Published
- 2020
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