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      KLF4 regulates adult lung tumor-initiating cells and represses K-Ras-mediated lung cancer

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          Abstract

          Lung cancer is the leading cause of cancer-related mortality in both men and women worldwide. To identify novel factors that contribute to lung cancer pathogenesis, we analyzed a lung cancer database from The Cancer Genome Atlas and found that Krüppel-like Factor 4 (KLF4) expression is significantly lower in patients' lung cancer tissue than in normal lung tissue. In addition, we identified seven missense mutations in the KLF4 gene. KLF4 is a transcription factor that regulates cell proliferation and differentiation as well as the self-renewal of stem cells. To understand the role of KLF4 in the lung, we generated a tamoxifen-induced Klf4 knockout mouse model. We found that KLF4 inhibits lung cancer cell growth and that depletion of Klf4 altered the differentiation pattern in the developing lung. To understand how KLF4 functions during lung tumorigenesis, we generated the K-ras LSL-G12D/+ ;Klf4 fl/fl mouse model, and we used adenovirus-expressed Cre to induce K-ras activation and Klf4 depletion in the lung. Although Klf4 deletion alone or K-ras mutation alone can trigger lung tumor formation, Klf4 deletion combined with K-ras mutation significantly enhanced lung tumor formation. We also found that Klf4 deletion in conjunction with K-ras activation caused lung inflammation. To understand the mechanism whereby KLF4 is regulated during lung tumorigenesis, we analyzed KLF4 promoter methylation and the profiles of epigenetic factors. We found that Class I histone deacetylases (HDACs) are overexpressed in lung cancer and that HDAC inhibitors induced expression of KLF4 and inhibited proliferation of lung cancer cells, suggesting that KLF4 is probably repressed by histone acetylation and that HDACs are valuable drug targets for lung cancer treatment.

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          Author and article information

          Journal
          Cell Death Differ
          Cell Death Differ
          Cell Death and Differentiation
          Nature Publishing Group
          1350-9047
          1476-5403
          February 2016
          26 June 2015
          : 23
          : 2
          : 207-215
          Affiliations
          [1 ] Department of Molecular and Cellular Biochemistry, University of Kentucky , Lexington, KY 40506-0509, USA
          [2 ] Markey Cancer Center, University of Kentucky, Lexington, KY 40506-0509, USA
          [3 ] Department of Biostatistics, University of Kentucky , Lexington, KY 40506-0509, USA
          [4 ] Department of Microbiology, Immunology and Molecular Genetics, University of Kentucky , Lexington, KY 40506-0509, USA
          [5 ] Department of Pathology, University of Kentucky, Lexington, KY 40506-0509, USA
          Author notes
          [* ] Markey Cancer Center, Department of Molecular and Cellular Biochemistry, University of Kentucky , 741 S. Limestone, B375 BBSRB, Lexington, KY 40506-0509, USA. Tel: 859 323 4558; Fax: 859 257 6030; E-mail: chunming.liu@ 123456uky.edu
          Article
          PMC4716302 PMC4716302 4716302 cdd201585
          10.1038/cdd.2015.85
          4716302
          26113043
          2549b23d-9745-44b6-9b07-3076163e115f
          Copyright © 2016 Macmillan Publishers Limited
          History
          : 16 February 2015
          : 29 April 2015
          : 22 May 2015
          Categories
          Original Paper

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