1987
DOI: 10.1083/jcb.105.4.1873
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Identification of multiple cell adhesion receptors for collagen and fibronectin in human fibrosarcoma cells possessing unique alpha and common beta subunits.

Abstract: Abstract. Using monoclonal antibody technology and affinity chromatography we have identified four distinct classes of cell surface receptors for native collagen on a cultured human fibrosarcoma cell line, HT-1080. Two classes of monoclonal antibodies prepared against HT-1080 cells inhibited adhesion to extracellular matrix components. Class I antibodies inhibited cell adhesion to collagen, fibronectin, and iaminin. These antibodies immunoprecipitated two noncovalently linked proteins (subunits) with molecular… Show more

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Cited by 688 publications
(456 citation statements)
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“…Figure 5A and B demonstrate clearly that pancreatic cancer cell adhesion and migration on type I collagen is mediated exclusively by the a 2 b 1 integrin, and that neither the a 1 , a 3 , a 5 , or a 6 integrin subunits, nor the a v b 3 or a v b 5 integrins appear to be involved in the adhesive interactions between AsPC-1, BxPC-3, CFPAC, or FG pancreatic cancer cells and type I collagen. Immunoprecipitation studies shown in Figure 4 and previous studies by us and other laboratories (Cheresh and Spiro, 1987;Wayner and Carter, 1987;Sonnenberg et al, 1988;Wayner et al, 1988Wayner et al, , 1993Grzesiak et al, 1992Grzesiak et al, , 2005aFabbri et al, 1996) demonstrate that the monoclonal antibodies used for the type I collagen inhibition studies are functional.…”
Section: Type I Collagen Promotes Maximal Haptokinetic Cell Migrationsupporting
confidence: 58%
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“…Figure 5A and B demonstrate clearly that pancreatic cancer cell adhesion and migration on type I collagen is mediated exclusively by the a 2 b 1 integrin, and that neither the a 1 , a 3 , a 5 , or a 6 integrin subunits, nor the a v b 3 or a v b 5 integrins appear to be involved in the adhesive interactions between AsPC-1, BxPC-3, CFPAC, or FG pancreatic cancer cells and type I collagen. Immunoprecipitation studies shown in Figure 4 and previous studies by us and other laboratories (Cheresh and Spiro, 1987;Wayner and Carter, 1987;Sonnenberg et al, 1988;Wayner et al, 1988Wayner et al, , 1993Grzesiak et al, 1992Grzesiak et al, , 2005aFabbri et al, 1996) demonstrate that the monoclonal antibodies used for the type I collagen inhibition studies are functional.…”
Section: Type I Collagen Promotes Maximal Haptokinetic Cell Migrationsupporting
confidence: 58%
“…The function-blocking monoclonal antibodies directed against particular integrin subunits and integrins used in these studies have been described (Cheresh and Spiro, 1987;Wayner and Carter, 1987;Sonnenberg et al, 1988;Wayner et al, 1988Wayner et al, , 1993Fabbri et al, 1996), and include FB12 (a 1 ), P1E6 (a 2 ), P1B5 (a 3 ), P1D6 (a 5 ), GoH3 (a 6 ), P5D2 (b 1 ), LM609 (a v b 3 ), P1F6 (a v b 5 ), and ASC-3 (b 4 ) (Chemicon International, Temecula, CA, USA). For immunoprecipitation (IP) experiments, we used the monoclonal antibodies described above along with rabbit polyclonal antisera against the a 5 integrin subunit, which has also been described previously (Ruoslahti and Pierschbacher, 1987).…”
Section: Antibodiesmentioning
confidence: 99%
“…No increases in surface expression of the collagen-binding heparan sulfate proteoglycan, CD44/ECMR-111, were detected by immunoprecipitation or immunofluorescence ( Figure 3D and data not shown) (Wayner and Carter, 1987). Finally, because FA-K562 adhesion to FN is trypsin insensitive and RGD inhibitable, syndecan is unlikely to be the receptor mediating FA-K562 adhesion to FN (Saunders and Bernfield, 1988).…”
Section: Selection Of Fa-k562mentioning
confidence: 97%
“…Additional FN-specific sequences or conformation were also required, as FA-K562 did not adhere to plastic coated with thrombin; GRGDS peptide; or the RGD-containing proteins laminin, collagen, or fibrinogen (Figure 1 F and data not shown). Although transforming growth factor-beta (TGF-beta) has been detected in some FN preparations (Fava and McClure, 1987) and could be responsible for morphologic changes, no bioactive TGF-beta was found in the FN preparation used in this study (personal communication, Dr. A. Purchio (Wayner and Carter, 1987;Wayner et al, 1989). Cells with similar phenotypes and FNR expression levels have been independently generated three times.…”
Section: Selection Of Fa-k562mentioning
confidence: 99%
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