{ "number": 10, "subjects": [ "QD" ], "eprintid": 281, "date": "2002-03-08", "userid": 2, "documents": [ { "language": "en", "placement": 1, "eprintid": 281, "files": [ { "hash_type": "MD5", "mtime": "2012-01-05 04:19:15", "datasetid": "document", "fileid": 4394, "objectid": 1621, "uri": "http:\/\/crdd.osdd.net\/open\/id\/file\/4394", "mime_type": "application\/pdf", "hash": "20a5e1bd1e5b655cba0e52c352191c79", "filesize": 349352, "filename": "agrewala2002.pdf" } ], "content": "published", "rev_number": 2, "uri": "http:\/\/crdd.osdd.net\/open\/id\/document\/1621", "main": "agrewala2002.pdf", "mime_type": "application\/pdf", "docid": 1621, "format": "application\/pdf", "security": "validuser", "pos": 1 } ], "official_url": "http:\/\/www.jbc.org\/content\/277\/10\/7766.long", "issn": "0021-9258", "rev_number": 13, "creators": [ { "name": { "lineage": null, "given": "Susmit", "honourific": null, "family": "Suvas" } }, { "name": { "lineage": null, "given": "Vinod", "honourific": null, "family": "Singh" } }, { "name": { "lineage": null, "given": "Sudhir", "honourific": null, "family": "Sahdev" } }, { "name": { "lineage": null, "given": "H", "honourific": null, "family": "Vohra" } }, { "name": { "lineage": null, "given": "J N", "honourific": null, "family": "Agrewala" } } ], "dir": "disk0\/00\/00\/02\/81", "lastmod": "2015-01-09 10:48:29", "ispublished": "pub", "pagerange": "7766-75", "publisher": "ASBMB", "metadata_visibility": "show", "date_type": "published", "eprint_status": "archive", "status_changed": "2015-01-09 10:48:29", "volume": 277, "datestamp": "2012-01-05 15:16:13", "uri": "http:\/\/crdd.osdd.net\/open\/id\/eprint\/281", "note": "Copyright of this article belongs to ASBMB.", "full_text_status": "restricted", "related_url": [ { "url": "http:\/\/www.jbc.org\/content\/277\/10\/7766.long", "type": "pub" } ], "refereed": "TRUE", "contact_email": "javed@imtech.res.in", "publication": "The Journal of biological chemistry", "abstract": "To date, not much has been known regarding the role of CD80 and CD86 molecules in signaling of B cells. The CD28\/CTLA4 ligands, CD80 (B7-1) and CD86 (B7-2), are expressed on the surface of freshly isolated splenic B cells, and their expression is up-regulated by lipopolysaccharides. In the present study, we have investigated whether signaling via CD80\/CD86 could alter the proliferation and immunoglobulin synthesis of B cells. Splenic B cells were stimulated with lipopolysaccharides in the presence of anti-B7-1 (16-10A1) and anti-B7-2 (GL1) monoclonal antibodies (mAbs). Exciting features observed during the study were that cross-linking of CD86 with GL1 enhanced the proliferation and production of IgG1 and IgG2a isotypes. In contrast, anti-B7-1 (16-10A1) mAb could efficiently block the proliferation and production of IgG1 and IgG2a. Furthermore, GL1 mAb could also induce the secretion of IgG isotypes from B cell lymphomas. Importantly, 16-10A1 could retard the growth of lymphomas and favored the up-regulation of pro-apoptotic molecules caspase-3, caspase-8, Fas, FasL, Bak, and Bax and down-regulation of anti-apoptotic molecule Bcl-x(L). In contrast, GL1 augmented the level of anti-apoptotic molecules Bcl-w and Bcl-x(L) and decreased the levels of pro-apoptotic molecule caspase-8, thereby providing a novel insight into the mechanism whereby triggering through CD80 and CD86 could deliver regulatory signals. Thus, this study is the first demonstration of a distinct signaling event induced by CD80 and CD86 molecules in B cell lymphoma. Finally, the significance of the finding is that CD80 provided negative signal for the proliferation and IgG secretion of normal B cells and B cell lymphomas. In contrast, CD86 encouraged the activity of B cells.", "type": "article", "title": "Distinct role of CD80 and CD86 in the regulation of the activation of B cell and B cell lymphoma." }