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

被引:0
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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
机构
[1] Harvard University,Wyss Institute for Biologically Inspired Engineering
[2] Massachusetts General Hospital,Department of Pathology
[3] Clinical Pharmacology and Safety Sciences,Department of Cancer Immunology and Virology
[4] BioPharmaceuticals R&D,Department of Medicine
[5] AstraZeneca,Department of Chemical Engineering
[6] DMPK,Vascular Biology Program and Department of Surgery
[7] Oncology R&D,Department of Bioengineering and Institute for Bioengineering and Biosciences (iBB), Instituto Superior Técnico
[8] AstraZeneca,Department of Pediatrics
[9] Clinical and Quantitative Pharmacology,Division of Bone Marrow Transplantation and Immune Deficiency
[10] Clinical Pharmacology and Safety Sciences,Department of Pathology
[11] Pharmaceutical Sciences,undefined
[12] R&D,undefined
[13] AstraZeneca,undefined
[14] Dana Farber/Boston Children’s Cancer and Blood Disorders Center,undefined
[15] Dana-Farber Cancer Institute,undefined
[16] Harvard Medical School,undefined
[17] Loughborough University,undefined
[18] Boston Children’s Hospital and Harvard Medical School,undefined
[19] Universidade de Lisboa,undefined
[20] University of Cincinnati College of Medicine,undefined
[21] Cincinnati Children’s Hospital,undefined
[22] Boston Children’s Hospital,undefined
[23] Broad Institute of Harvard and MIT,undefined
[24] Harvard John A. Paulson School of Engineering and Applied Sciences,undefined
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摘要
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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页码:394 / 406
页数:12
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