Literature DB >> 7624366

A splice variant of alpha 6 integrin is associated with malignant conversion in mouse skin tumorigenesis.

T Tennenbaum1, A J Belanger, A B Glick, R Tamura, V Quaranta, S H Yuspa.   

Abstract

The epithelial-specific integrin alpha 6 beta 4 is suprabasally expressed in benign skin tumors (papillomas) and is diffusely expressed in carcinomas associated with an increase in the proliferating compartment. Analysis of RNA samples by reverse transcriptase-PCR and DNA sequencing revealed that chemically or oncogenically induced papillomas (n = 8) expressed a single transcript of the alpha 6 subunit, identified as the alpha 6 A splice variant. In contrast, carcinomas (n = 13) expressed both alpha 6A and an alternatively spliced form, alpha 6B. Primary keratinocytes and a number of keratinocyte cell lines that vary in biological potential from normal skin, to benign papillomas, to well-differentiated slowly growing carcinomas exclusively expressed alpha 6A. However, I7, an oncogene-induced cell line that produces highly invasive carcinomas, expressed both alpha 6A and alpha 6B transcript and protein. The expression of alpha 6B in I7 cells was associated with increased attachment to a laminin matrix compared to cell lines exclusively expressing alpha 6A. Furthermore, introduction of an alpha 6B expression vector into a papilloma cell line expressing alpha 6A increased laminin attachment. When a papilloma cell line was converted to an invasive carcinoma by introduction of the v-fos oncogene, the malignant cells expressed both alpha 6A and alpha 6B, while the parent cell line and cells transduced with v-jun or c-myc, which retained the papilloma phenotype, expressed only alpha 6A. Comparative analysis of alpha 6B expression in cell lines and their derived tumors indicate that alpha 6B transcripts are more abundant in tumors than cell lines, and alpha 6B is expressed to a greater extent in poorly differentiated tumors. These results establish a link between malignant conversion and invasion of squamous tumor cells and the regulation of transcript processing of the alpha 6 beta 4 integrin.

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Year:  1995        PMID: 7624366      PMCID: PMC41467          DOI: 10.1073/pnas.92.15.7041

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  37 in total

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  10 in total

1.  Expression of a2, a5 and a6 subunits of integrin in de-differentiated NIH3T3 cells by cell-free extract of embryonic stem cells.

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Journal:  Mol Biol Rep       Date:  2012-07       Impact factor: 2.316

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Authors:  C Yan Cheng; Pearl Py Lie; Ka-Wai Mok; Yan-Ho Cheng; Elissa Wp Wong; Jayakanthan Mannu; Premendu P Mathur; Helen H N Yan; Dolores D Mruk
Journal:  Spermatogenesis       Date:  2011-07-01

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Authors:  Hira Lal Goel; Tatiana Gritsko; Bryan Pursell; Cheng Chang; Leonard D Shultz; Dale L Greiner; Jens Henrik Norum; Rune Toftgard; Leslie M Shaw; Arthur M Mercurio
Journal:  Cell Rep       Date:  2014-04-24       Impact factor: 9.423

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Authors:  Rotem Karni; Elisa de Stanchina; Scott W Lowe; Rahul Sinha; David Mu; Adrian R Krainer
Journal:  Nat Struct Mol Biol       Date:  2007-02-18       Impact factor: 15.369

7.  Mammalian Sulf1 RNA alternative splicing and its significance to tumour growth regulation.

Authors:  Rai B S Gill; Amy Day; Amy Barstow; Gul Zaman; Chantal Chenu; Gurtej K Dhoot
Journal:  Tumour Biol       Date:  2012-06-15

8.  Multipotent luminal mammary cancer stem cells model tumor heterogeneity.

Authors:  Lei Bao; Robert D Cardiff; Paul Steinbach; Karen S Messer; Lesley G Ellies
Journal:  Breast Cancer Res       Date:  2015-10-14       Impact factor: 6.466

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Authors:  Kai Zhang; Hang-Mao Lee; Gong-Hong Wei; Aki Manninen
Journal:  Oncotarget       Date:  2016-12-20

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Journal:  J Cell Biol       Date:  1998-10-05       Impact factor: 10.539

  10 in total

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