Expression of the β6 integrin subunit in development, neoplasia and tissue repair suggests a role in epithelial remodeling

Johannes M. Breuss(University of California, San Francisco), John Gallo(University of California, San Francisco), Horace M. DeLisser(University of Pennsylvania), Irina Klimanskaya(University of California, San Francisco), Hans G. Folkesson(University of California, San Francisco), Jean‐François Pittet(University of California, San Francisco), Stephen L. Nishimura(University of California, San Francisco), Kenneth Aldape(University of California, San Francisco), Daniel V. Landers(University of California, San Francisco), WM. GUEST CARPENTER(University of the Pacific), Nancy A. Gillett(University of California, San Francisco), Dean Sheppard(University of California, San Francisco), Michael A. Matthay(University of California, San Francisco), Steven Albelda(University of Pennsylvania), Randall H. Kramer(University of California, San Francisco), Robert Pytela(University of California, San Francisco)
Journal of Cell Science
June 1, 1995
Cited by 489

Abstract

The alpha v beta 6 integrin was identified in cultured epithelial cells and functions as a fibronectin receptor. We have now used monoclonal antibodies to determine in vivo expression patterns of the beta 6 subunit in normal and pathological human or primate tissues, and during experimental wound healing or induced lung injury. The results indicate that beta 6 expression is restricted to epithelia and is up-regulated in parallel with morphogenetic events, tumorigenesis, and epithelial repair. During development of the kidney, lung, and skin, we found that beta 6 is expressed by specific types of epithelial cells, whereas it is mostly undetectable in normal adult kidney, lung and skin. In contrast, we detected high-level expression in several types of carcinoma. For example, beta 6 is almost invariably neo-expressed in squamous cell carcinomas derived from the oral mucosa, often focally localized at the infiltrating edges of tumor islands. Expression of beta 6 is also upregulated in migrating keratinocytes at the wound edge during experimental epidermal wound healing. Similarly, beta 6 expression is induced in type II alveolar epithelial cells during lung injury caused by injection of live bacteria. We also observed beta 6 expression in adult lungs and kidneys at focal sites of subclinical inflammation, as well as in a variety of clinical specimens from patients with chronic or acute inflammation of the lungs or kidneys. From these findings and earlier results, we hypothesize that alpha v beta 6 affects cell spreading, migration and growth during reorganization of epithelia in development, tissue repair, and neoplasia.


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