Gut microbiome and CAR-T therapy

被引:0
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作者
Muhammad Bilal Abid
Nirav N. Shah
Theresa C. Maatman
Parameswaran N. Hari
机构
[1] Medical College of Wisconsin (MCW),Division of Infectious Diseases
[2] Hub for Collaborative Medicine,Division of Hematology/Oncology
[3] Medical College of Wisconsin (MCW),Division of Internal Medicine
[4] Medical College of Wisconsin (MCW),undefined
关键词
Immunotherapy; Immuno-oncology; CAR T-cells; TRUCKs; Gut microbiome; Dysbiosis; CRISPR/cas9;
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摘要
Considerable progress has been made in cancer therapeutics recently with targeted strategies that are efficacious and less toxic. Immunotherapy and chimeric antigen receptor (CAR) T-cells are increasingly being evaluated in a variety of tumors in the relapsed/refractory as well as frontline disease settings, predominantly in hematologic malignancies (HM). Despite impressive outcomes in select patients, there remains significant heterogeneity in clinical response to CAR T-cells. The gut microbiome has emerged as one of the key host factors that could potentially be modulated to enhance responses to immunotherapy. Several recent human studies receiving immunotherapy showed a significantly superior response and survival in patients with the more diverse gut microbiome. Currently, it is unknown if gut microbiota modulates anti-tumor responses to CAR T-cells. Based on molecular and immunological understanding, we hypothesize that strategically manipulating gut microbiota may enhance responses to CAR T-cells. In this review, we further discuss resistance mechanisms to CAR T-cells in HM, potential approaches to overcome resistance by harnessing gut microbiota and other related novel strategies.
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