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  • Club cells form lung adenocarcinomas and maintain the alveoli of adult mice.

Club cells form lung adenocarcinomas and maintain the alveoli of adult mice.

eLife (2019-05-30)
Magda Spella, Ioannis Lilis, Mario Aa Pepe, Yuanyuan Chen, Maria Armaka, Anne-Sophie Lamort, Dimitra E Zazara, Fani Roumelioti, Malamati Vreka, Nikolaos I Kanellakis, Darcy E Wagner, Anastasios D Giannou, Vasileios Armenis, Kristina Am Arendt, Laura V Klotz, Dimitrios Toumpanakis, Vassiliki Karavana, Spyros G Zakynthinos, Ioanna Giopanou, Antonia Marazioti, Vassilis Aidinis, Rocio Sotillo, Georgios T Stathopoulos
摘要

Lung cancer and chronic lung diseases impose major disease burdens worldwide and are caused by inhaled noxious agents including tobacco smoke. The cellular origins of environmental-induced lung tumors and of the dysfunctional airway and alveolar epithelial turnover observed with chronic lung diseases are unknown. To address this, we combined mouse models of genetic labeling and ablation of airway (club) and alveolar cells with exposure to environmental noxious and carcinogenic agents. Club cells are shown to survive KRAS mutations and to form lung tumors after tobacco carcinogen exposure. Increasing numbers of club cells are found in the alveoli with aging and after lung injury, but go undetected since they express alveolar proteins. Ablation of club cells prevents chemical lung tumors and causes alveolar destruction in adult mice. Hence club cells are important in alveolar maintenance and carcinogenesis and may be a therapeutic target against premalignancy and chronic lung disease.

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Sigma-Aldrich
抗乙酰化微管蛋白抗体,小鼠单克隆 小鼠抗, clone 6-11B-1, purified from hybridoma cell culture
Sigma-Aldrich
尿烷, ≥99%
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GenElute 哺乳动物基因组DNA小量制备试剂盒, sufficient for 70 purifications
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抗-Prosurfactant蛋白C(proSP-C)抗体, serum, Chemicon®
Sigma-Aldrich
双苯并咪唑 H 33258, suitable for fluorescence, ≥98.0% (HPLC)