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Article: Endothelial CD146 is required for in vitro tumor-induced angiogenesis: The role of a disulfide bond in signaling and dimerization

TitleEndothelial CD146 is required for in vitro tumor-induced angiogenesis: The role of a disulfide bond in signaling and dimerization
Authors
KeywordsDimerization
CD146
Tumor angiogenesis
NFκB
Disulfide bond
Issue Date2009
Citation
International Journal of Biochemistry and Cell Biology, 2009, v. 41, n. 11, p. 2163-2172 How to Cite?
AbstractTumor angiogenesis, induced by tumor-secreted pro-angiogenic factors, is an essential process for cancer development and metastasis. CD146 is identified as an endothelial cell adhesion molecule and implicated in blood vessel formation, however, its exact role in angiogenesis, particularly tumor angiogenesis, and its potential function of mediating downstream signaling are still unclear. In present study, we evidenced that silencing endogenous endothelial CD146 by RNAi significantly impaired hepatocarcinoma cell secretions-promoted tubular morphogenesis and -enhanced motility of endothelial cells. Biochemical studies revealed that CD146 was required for the activation of p38/IKK/NFκB signaling cascade and up-regulation of NFκB downstream pro-angiogenic genes, notably IL-8, ICAM-1 and MMP9, in response to tumor secretions. Interestingly, specific anti-CD146 mAb AA98, which bound a conformational epitope depending on C452-C499 disulfide bond, could abrogate NFκB activation and tumor angiogenesis, whereas another anti-CD146 mAb AA1 recognizing a linear epitope containing aa50-54 did not have such effects. Further structure-function analysis identified that C452-C499 disulfide bond within the fifth extracellular Ig domain was indispensible for CD146-mediated signaling and tube formation. Moreover, dimerization of CD146, which was enhanced by tumor secretions and suppressed by AA98 but not AA1, also relied on C452 and C499. Together, this study for the first time uncovered the pro-angiogenic role of CD146 and also pinpointed the key structural basis responsible for its signaling function and dimerization. These findings also suggested that CD146 might serve as not just a cell adhesion molecule but also a membrane signal receptor in tumor-induced angiogenesis. © 2009 Elsevier Ltd. All rights reserved.
Persistent Identifierhttp://hdl.handle.net/10722/265567
ISSN
2023 Impact Factor: 3.4
2023 SCImago Journal Rankings: 1.079
ISI Accession Number ID

 

DC FieldValueLanguage
dc.contributor.authorZheng, Chaogu-
dc.contributor.authorQiu, Yijun-
dc.contributor.authorZeng, Qiqun-
dc.contributor.authorZhang, Ying-
dc.contributor.authorLu, Di-
dc.contributor.authorYang, Dongling-
dc.contributor.authorFeng, Jing-
dc.contributor.authorYan, Xiyun-
dc.date.accessioned2018-12-03T01:21:03Z-
dc.date.available2018-12-03T01:21:03Z-
dc.date.issued2009-
dc.identifier.citationInternational Journal of Biochemistry and Cell Biology, 2009, v. 41, n. 11, p. 2163-2172-
dc.identifier.issn1357-2725-
dc.identifier.urihttp://hdl.handle.net/10722/265567-
dc.description.abstractTumor angiogenesis, induced by tumor-secreted pro-angiogenic factors, is an essential process for cancer development and metastasis. CD146 is identified as an endothelial cell adhesion molecule and implicated in blood vessel formation, however, its exact role in angiogenesis, particularly tumor angiogenesis, and its potential function of mediating downstream signaling are still unclear. In present study, we evidenced that silencing endogenous endothelial CD146 by RNAi significantly impaired hepatocarcinoma cell secretions-promoted tubular morphogenesis and -enhanced motility of endothelial cells. Biochemical studies revealed that CD146 was required for the activation of p38/IKK/NFκB signaling cascade and up-regulation of NFκB downstream pro-angiogenic genes, notably IL-8, ICAM-1 and MMP9, in response to tumor secretions. Interestingly, specific anti-CD146 mAb AA98, which bound a conformational epitope depending on C452-C499 disulfide bond, could abrogate NFκB activation and tumor angiogenesis, whereas another anti-CD146 mAb AA1 recognizing a linear epitope containing aa50-54 did not have such effects. Further structure-function analysis identified that C452-C499 disulfide bond within the fifth extracellular Ig domain was indispensible for CD146-mediated signaling and tube formation. Moreover, dimerization of CD146, which was enhanced by tumor secretions and suppressed by AA98 but not AA1, also relied on C452 and C499. Together, this study for the first time uncovered the pro-angiogenic role of CD146 and also pinpointed the key structural basis responsible for its signaling function and dimerization. These findings also suggested that CD146 might serve as not just a cell adhesion molecule but also a membrane signal receptor in tumor-induced angiogenesis. © 2009 Elsevier Ltd. All rights reserved.-
dc.languageeng-
dc.relation.ispartofInternational Journal of Biochemistry and Cell Biology-
dc.subjectDimerization-
dc.subjectCD146-
dc.subjectTumor angiogenesis-
dc.subjectNFκB-
dc.subjectDisulfide bond-
dc.titleEndothelial CD146 is required for in vitro tumor-induced angiogenesis: The role of a disulfide bond in signaling and dimerization-
dc.typeArticle-
dc.description.naturelink_to_subscribed_fulltext-
dc.identifier.doi10.1016/j.biocel.2009.03.014-
dc.identifier.pmid19782948-
dc.identifier.scopuseid_2-s2.0-70349299880-
dc.identifier.volume41-
dc.identifier.issue11-
dc.identifier.spage2163-
dc.identifier.epage2172-
dc.identifier.isiWOS:000271124700012-
dc.identifier.issnl1357-2725-

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