2012
DOI: 10.1136/gutjnl-2011-301061
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microRNA-145 in Barrett's oesophagus: regulating BMP4 signalling via GATA6

Abstract: These results imply that miRNA-145 indirectly targets BMP4 via GATA6 and is potentially involved in the development of BE.

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Cited by 47 publications
(52 citation statements)
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“…Several of the miRNAs identified as highly expressed in BE are linked to the intestinal phenotype, and are expressed in the mouse small intestine [40]. Logically, this similarity between BE and intestinal phenotype makes sense, and recently, investigators have begun to assess the role of specific miRNAs (such as miR-145) in the development of BE [41]. Some of the miRNAs that increase in BE then decrease in some EACs as the cancer phenotype develops.…”
Section: Discussionmentioning
confidence: 99%
“…Several of the miRNAs identified as highly expressed in BE are linked to the intestinal phenotype, and are expressed in the mouse small intestine [40]. Logically, this similarity between BE and intestinal phenotype makes sense, and recently, investigators have begun to assess the role of specific miRNAs (such as miR-145) in the development of BE [41]. Some of the miRNAs that increase in BE then decrease in some EACs as the cancer phenotype develops.…”
Section: Discussionmentioning
confidence: 99%
“…In particular, miR-143, miR-145 and miR-215 are considered tumor suppressors, downregulated in EAC probably due to additional molecular alterations that occur during carcinogenesis, such as loss of p53 homozygosity with consequent alteration of the functionality and ability that p53 exerts on the regulation of these three miRNAs [23, 3436]. In addition, the analysis of miR-145, most upregulated in BE compared to CLO, is consistent with its role in the differentiation towards the intestinal metaplasia via the feedback circuit with BMP-4, which is reported to be overexpressed in BE [37]. In the present study, miR-145 is also up-regulated in the CLO, although to a lesser extent.…”
Section: Discussionmentioning
confidence: 84%
“…Similarly, GATA6 expression is also increased in BE lesions compared to normal esophageal epithelium [57] and the overexpression of GATA6, together with FGFR2IIb, has been found to increase the anchorage-independent growth of the BE cell line CP-A [58] . Conflicting results show that upregulated miR-145 in BE lesions downregulates GATA6 and inhibits proliferation in nonneoplastic esophageal Het-1A cells [59] . Interestingly, it is thought that the binding of FOXA and GATA factors, which are pioneer transcription factors, opens up and reshapes closed (hetero)chromatin [60] .…”
Section: Cdx-2 As a Potential Key Regulator During Be Developmentmentioning
confidence: 91%