Multi-Niche Human Bone Marrow On-A-Chip for Studying the Interactions of Adoptive CAR-T Cell Therapies with Multiple Myeloma

Author:

Ghoshal DeltaORCID,Petersen Ingrid,Ringquist Rachel,Kramer Liana,Bhatia Eshant,Hu Thomas,Richard Ariane,Park Reda,Corbin Jenna,Agarwal Savi,Thomas Abel,Ramirez Sebastian,Tharayil Jacob,Downey Emma,Ketchum Frank,Ochal Abigail,Sonthi Neha,Lonial Sagar,Kochenderfer James N.,Tran Reginald,Zhu Mandy,Lam Wilbur A.,Coskun Ahmet F.,Roy Krishnendu

Abstract

ABSTRACTMultiple myeloma (MM), a cancer of bone marrow plasma cells, is the second-most common hematological malignancy. However, despite immunotherapies like chimeric antigen receptor (CAR)-T cells, relapse is nearly universal. The bone marrow (BM) microenvironment influences how MM cells survive, proliferate, and resist treatment. Yet, it is unclear which BM niches give rise to MM pathophysiology. Here, we present a 3D microvascularized culture system, which models the endosteal and perivascular bone marrow niches, allowing us to study MM-stroma interactions in the BM niche and model responses to therapeutic CAR-T cells. We demonstrated the prolonged survival of cell line-based and patient-derived multiple myeloma cells within ourin vitrosystem and successfully flowed in donor-matched CAR-T cells. We then measured T cell survival, differentiation, and cytotoxicity against MM cells using a variety of analysis techniques. Our MM-on-a-chip system could elucidate the role of the BM microenvironment in MM survival and therapeutic evasion and inform the rational design of next-generation therapeutics.TEASERA multiple myeloma model can study why the disease is still challenging to treat despite options that work well in other cancers.

Publisher

Cold Spring Harbor Laboratory

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