| Literature DB >> 32232483 |
Yu Matsuzawa-Ishimoto1,2, Ashley Hine2,3, Yusuke Shono4, Eugene Rudensky1,5, Amina Lazrak4, Frank Yeung1,5, Jessica A Neil1,2, Xiaomin Yao1,2, Ying-Han Chen1,2, Thomas Heaney1, Samantha L Schuster1, Erin E Zwack2, Jordan E Axelrad3, David Hudesman3, Jennifer J Tsai4, Katherine Nichols4, M Zahidunnabi Dewan6, Michael Cammer7, Allison Beal8, Sandra Hoffman8, Brad Geddes8, John Bertin8, Chen Liu9, Victor J Torres2, P'ng Loke2, Marcel R M van den Brink4,10,11, Ken Cadwell1,2,3.
Abstract
A goal in precision medicine is to use patient-derived material to predict disease course and intervention outcomes. Here, we use mechanistic observations in a preclinical animal model to design an ex vivo platform that recreates genetic susceptibility to T-cell-mediated damage. Intestinal graft-versus-host disease (GVHD) is a life-threatening complication of allogeneic hematopoietic cell transplantation. We found that intestinal GVHD in mice deficient in Atg16L1, an autophagy gene that is polymorphic in humans, is reversed by inhibiting necroptosis. We further show that cocultured allogeneic T cells kill Atg16L1-mutant intestinal organoids from mice, which was associated with an aberrant epithelial interferon signature. Using this information, we demonstrate that pharmacologically inhibiting necroptosis or interferon signaling protects human organoids derived from individuals harboring a common ATG16L1 variant from allogeneic T-cell attack. Our study provides a roadmap for applying findings in animal models to individualized therapy that targets affected tissues.Entities:
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Year: 2020 PMID: 32232483 PMCID: PMC7317146 DOI: 10.1182/blood.2019004116
Source DB: PubMed Journal: Blood ISSN: 0006-4971 Impact factor: 22.113