@article{pmid30712876,
title = {Commensal Microbiota Promote Lung Cancer Development via γδ T Cells},
author = {Chengcheng Jin and Georgia K Lagoudas and Chen Zhao and Susan Bullman and Arjun Bhutkar and Bo Hu and Samuel Ameh and Demi Sandel and Xu Sue Liang and Sarah Mazzilli and Mark T Whary and Matthew Meyerson and Ronald Germain and Paul C Blainey and James G Fox and Tyler Jacks},
doi = {10.1016/j.cell.2018.12.040},
issn = {1097-4172},
year  = {2019},
date = {2019-02-01},
journal = {Cell},
volume = {176},
number = {5},
pages = {998--1013.e16},
abstract = {Lung cancer is closely associated with chronic inflammation, but the causes of inflammation and the specific immune mediators have not been fully elucidated. The lung is a mucosal tissue colonized by a diverse bacterial community, and pulmonary infections commonly present in lung cancer patients are linked to clinical outcomes. Here, we provide evidence that local microbiota provoke inflammation associated with lung adenocarcinoma by activating lung-resident γδ T cells. Germ-free or antibiotic-treated mice were significantly protected from lung cancer development induced by Kras mutation and p53 loss. Mechanistically, commensal bacteria stimulated Myd88-dependent IL-1β and IL-23 production from myeloid cells, inducing proliferation and activation of Vγ6Vδ1 γδ T cells that produced IL-17 and other effector molecules to promote inflammation and tumor cell proliferation. Our findings clearly link local microbiota-immune crosstalk to lung tumor development and thereby define key cellular and molecular mediators that may serve as effective targets in lung cancer intervention.},
keywords = {},
pubstate = {published},
tppubtype = {article}
}

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G","Jacks, T."],"bibdata":{"bibtype":"article","type":"article","title":"Commensal Microbiota Promote Lung Cancer Development via γδ T Cells","author":[{"firstnames":["Chengcheng"],"propositions":[],"lastnames":["Jin"],"suffixes":[]},{"firstnames":["Georgia","K"],"propositions":[],"lastnames":["Lagoudas"],"suffixes":[]},{"firstnames":["Chen"],"propositions":[],"lastnames":["Zhao"],"suffixes":[]},{"firstnames":["Susan"],"propositions":[],"lastnames":["Bullman"],"suffixes":[]},{"firstnames":["Arjun"],"propositions":[],"lastnames":["Bhutkar"],"suffixes":[]},{"firstnames":["Bo"],"propositions":[],"lastnames":["Hu"],"suffixes":[]},{"firstnames":["Samuel"],"propositions":[],"lastnames":["Ameh"],"suffixes":[]},{"firstnames":["Demi"],"propositions":[],"lastnames":["Sandel"],"suffixes":[]},{"firstnames":["Xu","Sue"],"propositions":[],"lastnames":["Liang"],"suffixes":[]},{"firstnames":["Sarah"],"propositions":[],"lastnames":["Mazzilli"],"suffixes":[]},{"firstnames":["Mark","T"],"propositions":[],"lastnames":["Whary"],"suffixes":[]},{"firstnames":["Matthew"],"propositions":[],"lastnames":["Meyerson"],"suffixes":[]},{"firstnames":["Ronald"],"propositions":[],"lastnames":["Germain"],"suffixes":[]},{"firstnames":["Paul","C"],"propositions":[],"lastnames":["Blainey"],"suffixes":[]},{"firstnames":["James","G"],"propositions":[],"lastnames":["Fox"],"suffixes":[]},{"firstnames":["Tyler"],"propositions":[],"lastnames":["Jacks"],"suffixes":[]}],"doi":"10.1016/j.cell.2018.12.040","issn":"1097-4172","year":"2019","date":"2019-02-01","journal":"Cell","volume":"176","number":"5","pages":"998–1013.e16","abstract":"Lung cancer is closely associated with chronic inflammation, but the causes of inflammation and the specific immune mediators have not been fully elucidated. The lung is a mucosal tissue colonized by a diverse bacterial community, and pulmonary infections commonly present in lung cancer patients are linked to clinical outcomes. Here, we provide evidence that local microbiota provoke inflammation associated with lung adenocarcinoma by activating lung-resident γδ T cells. Germ-free or antibiotic-treated mice were significantly protected from lung cancer development induced by Kras mutation and p53 loss. Mechanistically, commensal bacteria stimulated Myd88-dependent IL-1β and IL-23 production from myeloid cells, inducing proliferation and activation of Vγ6Vδ1 γδ T cells that produced IL-17 and other effector molecules to promote inflammation and tumor cell proliferation. Our findings clearly link local microbiota-immune crosstalk to lung tumor development and thereby define key cellular and molecular mediators that may serve as effective targets in lung cancer intervention.","keywords":"","pubstate":"published","tppubtype":"article","bibtex":"@article{pmid30712876,\ntitle = {Commensal Microbiota Promote Lung Cancer Development via γδ T Cells},\nauthor = {Chengcheng Jin and Georgia K Lagoudas and Chen Zhao and Susan Bullman and Arjun Bhutkar and Bo Hu and Samuel Ameh and Demi Sandel and Xu Sue Liang and Sarah Mazzilli and Mark T Whary and Matthew Meyerson and Ronald Germain and Paul C Blainey and James G Fox and Tyler Jacks},\ndoi = {10.1016/j.cell.2018.12.040},\nissn = {1097-4172},\nyear = {2019},\ndate = {2019-02-01},\njournal = {Cell},\nvolume = {176},\nnumber = {5},\npages = {998--1013.e16},\nabstract = {Lung cancer is closely associated with chronic inflammation, but the causes of inflammation and the specific immune mediators have not been fully elucidated. The lung is a mucosal tissue colonized by a diverse bacterial community, and pulmonary infections commonly present in lung cancer patients are linked to clinical outcomes. Here, we provide evidence that local microbiota provoke inflammation associated with lung adenocarcinoma by activating lung-resident γδ T cells. Germ-free or antibiotic-treated mice were significantly protected from lung cancer development induced by Kras mutation and p53 loss. Mechanistically, commensal bacteria stimulated Myd88-dependent IL-1β and IL-23 production from myeloid cells, inducing proliferation and activation of Vγ6Vδ1 γδ T cells that produced IL-17 and other effector molecules to promote inflammation and tumor cell proliferation. 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G","Jacks, T."],"key":"pmid30712876","id":"pmid30712876","bibbaseid":"jin-lagoudas-zhao-bullman-bhutkar-hu-ameh-sandel-etal-commensalmicrobiotapromotelungcancerdevelopmentviatcells-2019","role":"author","urls":{},"metadata":{"authorlinks":{}}},"bibtype":"article","biburl":"https://bibbase.org/network/files/KRpSceBtgDX8h56tc","dataSources":["BR3FBurNqPdq5b7Jh","5GAofPTZnXeNstHQf","y8tT6mzHEZ8Q9E8Kd","Q5xvqKLoz8uikDzpD","hu7RM8PAjD5uaaYoh","KWQN3nHEDpQ2tZAun"],"keywords":[],"search_terms":["commensal","microbiota","promote","lung","cancer","development","via","cells","jin","lagoudas","zhao","bullman","bhutkar","hu","ameh","sandel","liang","mazzilli","whary","meyerson","germain","blainey","fox","jacks"],"title":"Commensal Microbiota Promote Lung Cancer Development via γδ T Cells","year":2019}