Absence of keratin 8 confers a paradoxical microflora-dependent resistance to apoptosis in the colon

Keratin 8 (K8) is a major intermediate filament protein present in enterocytes and serves an antiapoptotic function in hepatocytes. K8-null mice develop colonic hyperplasia and colitis that are reversed after antibiotic treatment. To investigate the pathways that underlie the mechanism of colonocyte...

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Published in:	Proceedings of the National Academy of Sciences - PNAS Vol. 108; no. 4; pp. 1445 - 1450
Main Authors:	Habtezion, Aida, Toivola, Diana M, Asghar, M. Nadeem, Kronmal, Greg S, Brooks, Jacqueline D, Butcher, Eugene C, Omary, M. Bishr
Format:	Journal Article
Language:	English
Published:	United States National Academy of Sciences 25-01-2011 National Acad Sciences
Subjects:	Animals Anti-Bacterial Agents - pharmacology Antibiotics Antibodies Antibodies - immunology Antibodies - pharmacology Apoptosis Apoptosis - drug effects Apoptosis - genetics Biological Sciences Cell culture Cell Line Cell Proliferation - drug effects Cells, Cultured Colon Colon - drug effects Colon - metabolism Colon - microbiology Crypts Drug Resistance - drug effects Drug Resistance - genetics Epithelial cells Female Focal Adhesion Kinase 1 - metabolism Gene Expression Profiling Genomics Genotype & phenotype Hepatocytes Imipenem - pharmacology Immunoblotting In Situ Nick-End Labeling Inhibitor of Apoptosis Proteins - genetics Inhibitor of Apoptosis Proteins - metabolism Integrin beta4 - genetics Integrin beta4 - immunology Integrin beta4 - metabolism Keratin-8 - genetics Keratin-8 - metabolism Keratin-8 - physiology Keratins Male Mice Mice, Inbred C57BL Mice, Knockout Microorganisms Mutation Phosphorylation Phosphorylation - drug effects Repressor Proteins - genetics Repressor Proteins - metabolism Reverse Transcriptase Polymerase Chain Reaction Rodents Small intestine T cell receptors Vancomycin - pharmacology
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Summary:	Keratin 8 (K8) is a major intermediate filament protein present in enterocytes and serves an antiapoptotic function in hepatocytes. K8-null mice develop colonic hyperplasia and colitis that are reversed after antibiotic treatment. To investigate the pathways that underlie the mechanism of colonocyte hyperplasia and the normalization of the colonic phenotype in response to antibiotics, we performed genome-wide microarray analysis. Functional annotation of genes that are differentially regulated in K8⁻/⁻ and K8⁺/⁺ isolated colon crypts (colonocytes) identified apoptosis as a major altered pathway. Exposure of K8⁻/⁻ colonocytes or colon organ ("organoid") cultures, but not K8⁻/⁻ small intestine organoid cultures, to apoptotic stimuli showed, surprisingly, that they are resistant to apoptosis compared with their wild-type counterparts. This resistance is not related to inflammation per se because T-cell receptor α-null (TCR-α⁻/⁻) and wild-type colon cultures respond similarly upon induction of apoptosis. Following antibiotic treatment, K8⁻/⁻ colonocytes and organ cultures become less resistant to apoptosis and respond similarly to the wild-type colonocytes. Antibiotics also normalize most differentially up-regulated genes, including survivin and β4-integrin. Treatment of K8⁻/⁻ mice with anti-β4-integrin antibody up-regulated survivin, and induced phosphorylation of focal adhesion kinase with decreased activation of caspases. Therefore, unlike the proapoptotic effect of K8 mutation or absence in hepatocytes, lack of K8 confers resistance to colonocyte apoptosis in a microflora-dependent manner.
Bibliography:	ObjectType-Article-1 SourceType-Scholarly Journals-1 ObjectType-Feature-2 content type line 23 1A.H. and D.M.T. contributed equally to this work. Author contributions: M.B.O. designed research; A.H., D.M.T., M.N.A., and M.B.O. performed research; G.S.K., J.D.B., E.C.B., and M.B.O. contributed new reagents/analytic tools; A.H., D.M.T., and M.B.O. analyzed data; and A.H., D.M.T., and M.B.O. wrote the paper. Edited by Sven Pettersson, Karolinska Institutet, Stockholm, Sweden, and accepted by the Editorial Board December 16, 2010 (received for review July 23, 2010)
ISSN:	0027-8424 1091-6490
DOI:	10.1073/pnas.1010833108