A novel variant of human Grb7 is associated with invasive esophageal carcinoma.

Tanaka, Shinji; Mori, Masaki; Akiyoshi, Tsuyoshi; Tanaka, Yoïchi; Mafune, Ken Ichi; Wands, Jack R.; Sugimachi, Keizō

doi:10.1172/jci2921

Cited by 84 publications

(99 citation statements)

References 17 publications

(24 reference statements)

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“…17 Conversely, expression of an antisense GRB7 RNA lowers endogenous grb7 protein levels and suppresses the in vitro invasive phenotype of these cells. 18 It is noteworthy to stress that we found GRB7 and ERBB2 coamplified and coexpressed in invasive adenocarcinoma and high grade intraepithelial neoplasia in Barrett's esophagus. Interestingly, other types of cancer show gene amplification without overexpression (e.g., gastric cancer 12 ) or mRNA overexpression without gene amplification (e.g., esophageal squamous cell carcinoma 18 ).…”

Section: Fish Analysismentioning

confidence: 57%

“…18 It is noteworthy to stress that we found GRB7 and ERBB2 coamplified and coexpressed in invasive adenocarcinoma and high grade intraepithelial neoplasia in Barrett's esophagus. Interestingly, other types of cancer show gene amplification without overexpression (e.g., gastric cancer 12 ) or mRNA overexpression without gene amplification (e.g., esophageal squamous cell carcinoma 18 ). Although an increase of DNA copy numbers and mRNA expression are well correlated, other mechanisms than gene amplification may induce mRNA overexpression such as gene mutation, modifications resulting in a prolonged half live of mRNA level or moderately increase elevated expression caused by polysomy of chromosome 17 as reported previously.…”

Section: Fish Analysismentioning

confidence: 57%

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Coamplification and coexpression of GRB7 and ERBB2 is found in high grade intraepithelial neoplasia and in invasive Barrett's carcinoma

Walch

Specht

Braselmann³

et al. 2004

Intl Journal of Cancer

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The human growth factor receptor-bound protein 7 gene (GRB7), the founding member of a family of adaptor molecules has been shown to regulate cell migration and has been implicated in tumor progression. GRB7 is localized in close proximity to the ERBB2 gene within an amplicon previously identified in Barrett's adenocarcinoma (BCA). We evaluated gene amplification and mRNA expression of GRB7 and ERBB2 in Barrett's carcinoma and its associated precursor lesions to assess their possible role in Barrett's malignant transformation. Copy number and expression levels were analyzed by Q-PCR (GRB7, ERBB2) and QRT-PCR (GRB7, ERBB2) using TaqMan technology and fluorescence in situ hybridization (ERBB2) in a series of 24 laser-microdissected samples of Barrett's carcinomas and 32 samples of associated premalignant lesions. Parallel analysis of gene copy number changes and expression levels demonstrated that GRB7 and ERBB2 displayed concomitant elevated expression levels and increased copy numbers in 32% of Barrett's carcinomas. There was a correlation between GRB7 and ERBB2 in BCA at the DNA level (r s ‫؍‬ 0.76, p < 0.001) and the mRNA level (r s ‫؍‬ 0.89, p < 0.001). Moreover, coamplification (r s ‫؍‬ 0.97, p < 0.001) and coexpression (r s ‫؍‬ 0.81, p < 0.001) of GRB7 and ERBB2 are shown to be already present in a subset of BCA associated high-grade intraepithelial neoplasia (HGIN), possibly reflecting a role of a concerted expression of GRB7 and ERBB2. No alterations, neither gene amplification nor overexpression were detected in Barrett's carcinoma associated low grade intraepithelial neoplasia (LGIN), intestinal metaplasia (IM) and squamous epithelium, indicating that alterations of GRB7 and ERBB2 are late events in the carcinogenesis of Barrett's esophagus. These findings may be of particular interest because the transition from high grade intraepithelial neoplasia to invasive carcinoma is a crucial step in malignant transformation in Barrett's carcinogenesis and might underline the putative role of GRB7 and ERBB2 in cell migration and tumor invasion.

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Section: Fish Analysismentioning

confidence: 57%

Section: Fish Analysismentioning

confidence: 57%

Coamplification and coexpression of GRB7 and ERBB2 is found in high grade intraepithelial neoplasia and in invasive Barrett's carcinoma

Walch

Specht

Braselmann³

et al. 2004

Intl Journal of Cancer

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“…The importance of Grb7 in tumour progression has been suggested by several studies (Tanaka et al, 1997(Tanaka et al, , 1998(Tanaka et al, , 2000Han and Guan, 1999). Downregulating Grb7 either by anti-sense or siRNA technology has shown to inhibit the invasive (Tanaka et al, Figure 3 Effects of combined treatment with G7-18NATE-P and Doxorubicin on SK-BR-3 breast cancer cells.…”

Section: Discussionmentioning

confidence: 96%

Combination treatment with Grb7 peptide and Doxorubicin or Trastuzumab (Herceptin) results in cooperative cell growth inhibition in breast cancer cells

et al. 2007

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Grb7 has potential importance in the progression of cancer. We have previously identified a novel peptide that binds to the SH2 domain of Grb7 and inhibits its association with several different receptor tyrosine kinases. We have synthesised the Grb7 peptide, G7-18NATE, with two different cell penetrating peptides, Penetratin and Tat. In this study, we have shown that both Penetratin-and Tat-conjugated G7-18NATE peptides are able to inhibit the proliferation of SK-BR-3, ZR-75-30, MDA-MB-361 and MDA-MB-231 breast cancer cells. There was no significant effects on breast cancer MCF-7cells, non-malignant MCF 10A or 3T3 cells. In addition, there was no significant inhibition of proliferation by Penetratin or Tat alone or by their conjugates with arbitrary peptide sequence in any of the cell lines tested. We determined the EC 50 of G7-18NATE-P peptide for SK-BR-3 cell proliferation to be 7.663 Â 10 À6 M. Co-treatment of G7-18NATE-P peptide plus Doxorubicin in SK-BR-3 breast cancer cells resulted in an additional inhibition of proliferation, resulting in 56 and 84% decreases in the Doxorubicin EC 50 value in the presence of 5 Â 10 À6 and 1.0 Â 10 À5 M G7-18NATE-P peptide, respectively. Importantly, the co-treatment with Doxorubicin and the delivery peptide did not change the Doxorubicin EC 50 . Since Grb7 associates with ErbB2, we assessed whether the peptide inhibitor would have a combined effect with a molecule that targets ErbB2, Herceptin. Co-treatment of Herceptin plus 1.0 Â 10 À5 M G7-18NATE-P peptide in SK-BR-3 cells resulted in a 46% decrease in the Herceptin EC 50 value and no decrease following the co-treatment with Herceptin and penetratin alone. This Grb7 peptide has potential to be developed as a therapeutic agent alone, in combination with traditional chemotherapy, or in combination with other targeting molecules.

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“…Grb7 is not a substrate of the insulin receptor tyrosine kinase activity. In contrast, it has been reported that Grb7 is phosphorylated on tyrosine residues when it binds the EGF receptor and erbB2 (Pandey et al, 1996;Stein et al, 1994;Tanaka et al, 1998), but not the PDGF receptor (Yokote et al, 1996). Grb10 and Grb14, members of the same family of adapters, display similar properties: they bind various activated tyrosine kinase receptors, and if they are tyrosine phosphorylated by some of them (Mano et al, 1998) In vitro interaction between Grb7 domains and the insulin receptor.…”

Section: Discussionmentioning

confidence: 99%

“…The ®rst observation was the overexpression of Grb7 together with erbB2 in numerous breast tumors and cell lines (Stein et al, 1994). A variant of Grb7, lacking the C-terminus SH2 domain, is likely to be involved in the cell invasion and metastatic progression of human oesophageal carcinomas (Tanaka et al, 1998). Grb10 and Grb14 are also overexpressed in several breast and prostate cancer cell lines (Daly et al, 1996;Dong et al, 1997).…”

Section: Introductionmentioning

confidence: 99%

Evidence for an interaction between the insulin receptor and Grb7. A role for two of its binding domains, PIR and SH2

et al. 2000

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Grb7 is not a substrate of the insulin receptor tyrosine kinase activity. Grb7 binds the activated tyrosine kinase loop of the insulin receptors. Two domains of Grb7 are implicated in the insulin receptor binding: the SH2 domain and the PIR (phosphotyrosine interacting region). The role of these two domains in the interaction with the insulin receptor was already reported for Grb10 and Grb14, the other members of the Grb7 family of proteins. However, the relative importance of these domains varies, considering the receptor and the Grb protein. These di erences should be a determinant of the speci®city of the receptor tyrosine kinase-Grbs binding, and thus of the implication of Grb7/10/14 in signal transduction.

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A novel variant of human Grb7 is associated with invasive esophageal carcinoma.

Cited by 84 publications

References 17 publications

Coamplification and coexpression of GRB7 and ERBB2 is found in high grade intraepithelial neoplasia and in invasive Barrett's carcinoma

Coamplification and coexpression of GRB7 and ERBB2 is found in high grade intraepithelial neoplasia and in invasive Barrett's carcinoma

Combination treatment with Grb7 peptide and Doxorubicin or Trastuzumab (Herceptin) results in cooperative cell growth inhibition in breast cancer cells

Evidence for an interaction between the insulin receptor and Grb7. A role for two of its binding domains, PIR and SH2

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