C-CAM (cell-CAM 105) is an adhesive cell surface glycoprotein with homophilic binding properties
(1990) In Journal of Cell Science 96(1). p.17-25- Abstract
- C-CAM (Cell-CAM 105) is a cell surface glycoprotein that is involved in cell-cell adhesion of rat hepatocytes in vitro. To elucidate the adhesion mechanism the binding properties of purified C-CAM were investigated. Using proteins immobilized on nitrocellulose it was found that radiolabeled C-CAM bound to C-CAM but not to a variety of other proteins. Partitioning in Triton X-114 showed that C-CAM has hydrophobic properties. In accordance with this, C-CAM was effectively incorporated into phosphatidylcholine liposomes by dialysis from octylglucoside-containing solutions. The C-CAM-containing liposomes bound specifically to isolated hepatocytes. This binding was blocked by Fab fragments of anti-C-CAM antibodies. Furthermore, preincubation of... (More)
- C-CAM (Cell-CAM 105) is a cell surface glycoprotein that is involved in cell-cell adhesion of rat hepatocytes in vitro. To elucidate the adhesion mechanism the binding properties of purified C-CAM were investigated. Using proteins immobilized on nitrocellulose it was found that radiolabeled C-CAM bound to C-CAM but not to a variety of other proteins. Partitioning in Triton X-114 showed that C-CAM has hydrophobic properties. In accordance with this, C-CAM was effectively incorporated into phosphatidylcholine liposomes by dialysis from octylglucoside-containing solutions. The C-CAM-containing liposomes bound specifically to isolated hepatocytes. This binding was blocked by Fab fragments of anti-C-CAM antibodies. Furthermore, preincubation of hepatocytes with anti-C-CAM antibodies followed by washing of the cells blocked binding of C-CAM-containing liposomes. At increasing C-CAM contents in the reconstituted liposomes a marked self-aggregation of the liposomes occurred. This aggregation was blocked by Fab fragments of anti-C-CAM antibodies and by alkaline pH. After neutralization a rapid reaggregation occurred. Neither C-CAM binding to C-CAM immobilized on nitrocellulose nor C-CAM-liposome aggregation required calcium ions. Liposomes reconstituted with C-CAM-depleted membrane glycoproteins did not self-aggregate or bind to hepatocytes. Thus, it is concluded that C-CAM can bind specifically to C-CAM in a homophilic binding reaction that does not require calcium. Accordingly, C-CAM has the potential of directly mediating cell-cell adhesion via C-CAM-C-CAM binding between adjacent cells. (Less)
Please use this url to cite or link to this publication:
https://lup.lub.lu.se/record/1105492
- author
- Tingström, Anders LU ; Blikstad, Ingrid ; Aurivillius, Magnus LU and Obrink, Björn
- organization
- publishing date
- 1990
- type
- Contribution to journal
- publication status
- published
- subject
- keywords
- glycoprotein, adhesion, C-CAM
- in
- Journal of Cell Science
- volume
- 96
- issue
- 1
- pages
- 17 - 25
- publisher
- The Company of Biologists Ltd
- external identifiers
-
- pmid:2373740
- scopus:0025275169
- ISSN
- 0021-9533
- language
- English
- LU publication?
- yes
- id
- 79350f9a-521c-4ef2-9951-3c1b9f93f54b (old id 1105492)
- alternative location
- http://jcs.biologists.org/cgi/reprint/96/1/17
- date added to LUP
- 2016-04-01 11:59:59
- date last changed
- 2021-01-03 10:04:08
@article{79350f9a-521c-4ef2-9951-3c1b9f93f54b,
abstract = {{C-CAM (Cell-CAM 105) is a cell surface glycoprotein that is involved in cell-cell adhesion of rat hepatocytes in vitro. To elucidate the adhesion mechanism the binding properties of purified C-CAM were investigated. Using proteins immobilized on nitrocellulose it was found that radiolabeled C-CAM bound to C-CAM but not to a variety of other proteins. Partitioning in Triton X-114 showed that C-CAM has hydrophobic properties. In accordance with this, C-CAM was effectively incorporated into phosphatidylcholine liposomes by dialysis from octylglucoside-containing solutions. The C-CAM-containing liposomes bound specifically to isolated hepatocytes. This binding was blocked by Fab fragments of anti-C-CAM antibodies. Furthermore, preincubation of hepatocytes with anti-C-CAM antibodies followed by washing of the cells blocked binding of C-CAM-containing liposomes. At increasing C-CAM contents in the reconstituted liposomes a marked self-aggregation of the liposomes occurred. This aggregation was blocked by Fab fragments of anti-C-CAM antibodies and by alkaline pH. After neutralization a rapid reaggregation occurred. Neither C-CAM binding to C-CAM immobilized on nitrocellulose nor C-CAM-liposome aggregation required calcium ions. Liposomes reconstituted with C-CAM-depleted membrane glycoproteins did not self-aggregate or bind to hepatocytes. Thus, it is concluded that C-CAM can bind specifically to C-CAM in a homophilic binding reaction that does not require calcium. Accordingly, C-CAM has the potential of directly mediating cell-cell adhesion via C-CAM-C-CAM binding between adjacent cells.}},
author = {{Tingström, Anders and Blikstad, Ingrid and Aurivillius, Magnus and Obrink, Björn}},
issn = {{0021-9533}},
keywords = {{glycoprotein; adhesion; C-CAM}},
language = {{eng}},
number = {{1}},
pages = {{17--25}},
publisher = {{The Company of Biologists Ltd}},
series = {{Journal of Cell Science}},
title = {{C-CAM (cell-CAM 105) is an adhesive cell surface glycoprotein with homophilic binding properties}},
url = {{http://jcs.biologists.org/cgi/reprint/96/1/17}},
volume = {{96}},
year = {{1990}},
}