Analysis of the TGF β functional pathway in epithelial ovarian carcinoma

Francis-Thickpenny, K M; Richardson, D M; Ee, Cliffton; Love, Donald R.; Winship, Ingrid; Baguley, Bruce C.; Chenevix-Trench, Georgia; Shelling, Andrew N.

doi:10.1054/bjoc.2001.1950

Cited by 28 publications

(14 citation statements)

References 25 publications

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“…43 Somatic mutations of TbR-II are noticeable in hereditary nonpolyposis colorectal cancer, although these mutations are less frequent in most carcinomas without microsatellite instability. 14,15 Taken together, it seems likely that mutation of exon 3, 5, and 7 of TbR-II is a minor mechanism for TGF-b-resistance in ICC cells.…”

Section: Tgf-b1mentioning

confidence: 99%

“…Somatic mutations of TbR-II were firstly reported in some carcinoma cells, especially hereditary nonpolyposis colorectal cancer, 12,13 though the frequency was found to be relatively low in other carcinomas. 14,15 Other mechanisms of escaping tumor growth inhibition by TGF-b1 such as somatic mutation of Smads, transcriptional downregulation of TGF-b receptors, and overexpression of smad7, are also reported. [16][17][18][19] TGF-b1 is known to inhibit the proliferation of non-neoplastic epithelium at the G1/S phase via several cell cycle-related molecules such as cyclins (cyclins D, cyclin E), cdks (cdk2, cdk4, cdk6), and cdk inhibitors (p15, p21, p27).…”

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confidence: 99%

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Intrahepatic cholangiocarcinoma escapes from growth inhibitory effect of transforming growth factor-β1 by overexpression of cyclin D1

Zen

Harada

Sasaki

et al. 2005

Laboratory Investigation

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Transforming growth factor-b1 (TGF-b1) is involved in tumor progression by promoting angiogenesis or suppressing the immune system; yet TGF-b1 also has a growth-inhibitory effect on epithelial cells including carcinoma cells. Several mechanisms of impaired TGF-b1 responsiveness of carcinoma cells have been reported. In this study, we examined how TGF-b1 participates in the development and progression of intrahepatic cholangiocarcinoma (ICC) associated with hepatolithiasis, and how ICC cells escape from growth inhibitory effect of TGF-b1. A total of 40 cases of hepatolithiasis were studied, including 16 cases of ICC, and in vitro studies were conducted with cultured murine non-neoplastic biliary epithelial cells (MBEC) and three ICC cell lines. Immunohistochemically, TGF-b1 was expressed in mononuclear cells and mesenchymal cells around the stone-containing bile ducts and invasive ICC, and also in biliary epithelial cells (hyperplastic and precursor lesions, and ICC). TGF-b type II receptor (TbR-II) was constantly expressed on biliary epithelial cells irrespective of biliary lesions. In cell culture studies, TGF-b1 significantly inhibited proliferation of MBEC via downregulation of cyclin D1, cdk4, and cdk6, while TGF-b1 did not influence the proliferation of ICC cells. After suppression of cyclin D1 expression in one ICC cell line using cyclin D1 small interfering RNA, TGF-b1 significantly inhibited the proliferation of ICC cells. In conclusion, high levels of TGF-b1 around ICC or its precursors may be involved in development and progression of ICC in hepatolithiasis. ICC cells could escape the growth inhibitory effect of TGF-b1 by overexpression of cyclin D1.

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Section: Tgf-b1mentioning

confidence: 99%

mentioning

confidence: 99%

Intrahepatic cholangiocarcinoma escapes from growth inhibitory effect of transforming growth factor-β1 by overexpression of cyclin D1

Zen

Harada

Sasaki

et al. 2005

Laboratory Investigation

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“…Although abnormalities in the expression or function of TGFß1 and its receptors, or molecules in the downstream signaling cascade, have been reported in several studies of ovarian cancer, some authors have reported significant abnormalities, while others have found minor changes and controversy exists (30)(31)(32)(33)(34). In addition, very few studies of ovarian cancer have assessed the associations between TGFß1 expression and the prognosis or sensitivity to anticancer drugs.…”

Section: Discussionmentioning

confidence: 99%

Expression of TGFß1 and its receptors is associated with biological features of ovarian cancer and sensitivity to paclitaxel/carboplatin

et al. 2011

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Abstract. It has been suggested that expression of TGFß1 and its receptors [TGFß receptor type I (TßRI) and TGFß receptor type II (TßRII)] may play a key role in the proliferation and progression of epithelial ovarian cancer. We investigated the biological significance of TGFß1 and its receptors, as well as their association with the tumor response to paclitaxel (PTX) and carboplatin (CBDCA). We studied 24 patients with ovarian cancer, primary peritoneal cancer, or fallopian tube cancer who had undergone surgery and chemotherapy with PTX and CBDCA. Tissues from the primary tumor were examined and the expression of TGFß1, TßRI, and TßRII mRNA was assessed by the RNase protection assay. It was found that TGFß1 mRNA expression was significantly lower in the tumors of patients who had optimal surgery than in the tumors of patients with suboptimal surgery. TGFß1 mRNA expression was also significantly lower in tumors with high sensitivity to PTX and CBDCA than in those with low sensitivity. TßRI mRNA expression was not associated with any clinicopathological factors. Expression of TßRII mRNA was significantly higher in clear cell adenocarcinoma and mucinous adenocarcinoma, while it was lower in serous adenocarcinoma and endometrioid adenocarcinoma. Moreover, it tended to be higher in early-stage tumors compared with advanced tumors. Among TGFß1, TßRI, and TßRII, expression of TGFß1 mRNA was most strongly associated with progression-free survival. When the prognosis of the patients with advanced cancer was compared on the basis of TGFß1 mRNA expression, those whose tumors showed low expression tended to have a better prognosis than those whose tumors showed high expression. It is suggested that TGFß1 mRNA expression is an indicator of tumor sensitivity to standard therapy with PTX and CBDCA, that it can identify biologically aggressive and highly malignant tumors and that it can predict the prognosis of patients with ovarian cancer.

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“…Specifically, a frameshift mutation has been identified in Exon 5 of TGFRI in 31% of ovarian tumors (Wang et al, 2000b), in exons 2, 3, 4, and 6 of TGFRI (catalytic domain of the kinase) in 33% primary ovarian cancers (Chen et al, 2001), and deletions in exon 1 of TGFRI in <30% of ovarian tumors (Antony et al, 2010). Likewise, missense mutations have been identified in TGFRII (Francis-Thickpenny et al, 2001) and deletions in exon 3 of TGFRII in ovarian tumors (Antony et al, 2010).…”

Section: Tgfreceptor Expression In Ovarian Cancermentioning

confidence: 99%