On-chip recapitulation of clinical bone marrow toxicities and patient-specific pathophysiology

芯片上重现临床骨髓毒性和患者特异性病理生理学

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作者:David B Chou # ,Viktoras Frismantas # ,Yuka Milton ,Rhiannon David ,Petar Pop-Damkov ,Douglas Ferguson ,Alexander MacDonald ,Özge Vargel Bölükbaşı ,Cailin E Joyce ,Liliana S Moreira Teixeira ,Arianna Rech ,Amanda Jiang ,Elizabeth Calamari ,Sasan Jalili-Firoozinezhad ,Brooke A Furlong ,Lucy R O'Sullivan ,Carlos F Ng ,Youngjae Choe ,Susan Marquez ,Kasiani C Myers ,Olga K Weinberg ,Robert P Hasserjian ,Richard Novak ,Oren Levy ,Rachelle Prantil-Baun ,Carl D Novina ,Akiko Shimamura ,Lorna Ewart ,Donald E Ingber

Abstract

The inaccessibility of living bone marrow (BM) hampers the study of its pathophysiology under myelotoxic stress induced by drugs, radiation or genetic mutations. Here, we show that a vascularized human BM-on-a-chip (BM chip) supports the differentiation and maturation of multiple blood cell lineages over 4 weeks while improving CD34+ cell maintenance, and that it recapitulates aspects of BM injury, including myeloerythroid toxicity after clinically relevant exposures to chemotherapeutic drugs and ionizing radiation, as well as BM recovery after drug-induced myelosuppression. The chip comprises a fluidic channel filled with a fibrin gel in which CD34+ cells and BM-derived stromal cells are co-cultured, a parallel channel lined by human vascular endothelium and perfused with culture medium, and a porous membrane separating the two channels. We also show that BM chips containing cells from patients with the rare genetic disorder Shwachman-Diamond syndrome reproduced key haematopoietic defects and led to the discovery of a neutrophil maturation abnormality. As an in vitro model of haematopoietic dysfunction, the BM chip may serve as a human-specific alternative to animal testing for the study of BM pathophysiology.

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