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Expression of secreted Wnt antagonists in gastrointestinal tissues: potential role in stem cell homeostasis.

机译:分泌型Wnt拮抗剂在胃肠道组织中的表达:在干细胞稳态中的潜在作用。

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BACKGROUND: Wnt signalling dysregulation has been implicated in cancer, including colon and gastric cancer. Initiation of Wnt signalling is modulated by soluble Wnt antagonists (sWAs), including soluble frizzled related proteins, dickkopf (Dkk) proteins, and Wnt inhibitory factor-1 (Wif1).AIMS: To evaluate the role of sWAs in upper (gastric) and lower (colon) gastrointestinal tract tumorigenesis.METHODS: Dkk1-3, Wif1, and FrzB expression was evaluated by in situ RNA hybridisation on normal and malignant human gastric and colon tissues. Expression was graded semiquantitatively.RESULTS: Wif1, Dkk1, and Dkk2 were not expressed in normal gastric tissue. Dkk3 was expressed in some samples, with stronger expression in deep gastric glands. FrzB was expressed in several normal gastric samples, but not in matched tumour specimens. In contrast, Dkk1 and FrzB were not expressed in normal colon. Wif1 was expressed in most colon samples, with stronger expression at crypt bases. Dkk3 and Dkk2 expression was also concentrated at crypt bases. There were no differences between sWA expression in malignant colon and matched normal tissue.CONCLUSIONS: sWA expression differed between upper and lower gastrointestinal tract. The loss of FrzB in gastric cancer suggests that it acts as a tumour suppressor. The graded expression of Dkk3 in gastric tissue, and Dkk2, Dkk3, and Wif1 in colon tissue, with increased expression in the deep gastric glands/colonic crypt bases, where gastrointestinal stem cells reside, suggests that sWAs may be crucial Wnt signalling regulators in these tissues, and may contribute to stem cell pool maintenance. sWAs are important components of the gastrointestinal proliferative regulatory network.
机译:背景:Wnt信号调节异常与癌症有关,包括结肠癌和胃癌。 Wnt信号的启动受可溶性Wnt拮抗剂(sWAs)调节,包括可溶性卷曲相关蛋白,Dickkopf(Dkk)蛋白和Wnt抑制因子-1(Wif1)。目的:评估sWAs在上层(胃)和胃中的作用。方法:Dkk1-3,Wif1和FrzB表达通过在正常和恶性人胃和结肠组织上的原位RNA杂交进行评估。结果:Wif1,Dkk1和Dkk2在正常胃组织中不表达。 Dkk3在某些样品中表达,在胃深腺中表达更强。 FrzB在几个正常的胃样本中表达,但在匹配的肿瘤样本中不表达。相反,Dkk1和FrzB在正常结肠中不表达。 Wif1在大多数结肠样本中表达,在隐窝碱基处表达更强。 Dkk3和Dkk2表达也集中在隐窝碱基处。结论:在上消化道和下消化道之间,sWA的表达均存在差异。胃癌中FrzB的丢失表明它起着抑癌作用。胃组织中Dkk3和结肠组织中Dkk2,Dkk3和Wif1的分级表达,在胃肠干细胞所在的深胃腺/结肠隐窝基底中的表达增加,表明sWAs可能是这些中重要的Wnt信号调节剂组织,并可能有助于维持干细胞池。 sWAs是胃肠道增殖调节网络的重要组成部分。

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