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Expression and cellular localization of TSC-22 in normal salivary glands and salivary gland tumors: implications for tumor cell differentiation.

机译:TSC-22在正常唾液腺和涎腺肿瘤中的表达和细胞定位:对肿瘤细胞分化的影响。

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摘要

TGF-beta-stimulated clone-22 (TSC-22) was reported to be a differentiation-inducing factor which negatively regulates the growth of salivary gland cancer cells. In the present study, we examined the expression of TSC-22 in salivary gland tumors by immunohistochemistry. In pleomorphic adenoma (PA), most of the sparse myoepithelial-like tumor cells, which are considered as the differentiated cells because they produce extracellular matrix, expressed TSC-22. However, only a limited number of cases of the solid myoepithelial-like tumor cells in PA, which are considered as the growing cells, expressed TSC-22. In adenoid cystic carcinoma (ACC), inner ductal cells in the tubular structure, strongly expressed TSC-22, though the outer myoepithelial-like tumor cells did not express TSC-22. In the cribriform structure, myoepithelial-like tumor cells did not express TSC-22. However, a small ductal structure in the micro-cyst wall strongly expressed TSC-22. Sparse type myoepithelial-like tumor cells in ACC also expressed TSC-22. In mucoepidermoid carcinoma, epidermoid tumor cells and mucous-producing tumor cells in mucoepidermoid carcinoma frequently expressed TSC-22. Thus, the expression of TSC-22 was frequently observed in the cells with differentiated-phenotypes, although rarely in the cells with growing potentials. These results suggest that TSC-22 may play an important role in maintaining the differentiated phenotype in salivary gland tumors.
机译:据报道,TGF-β刺激的克隆22(TSC-22)是分化诱导因子,它负调控唾液腺癌细胞的生长。在本研究中,我们通过免疫组织化学检查了TSC-22在涎腺肿瘤中的表达。在多形性腺瘤(PA)中,大多数稀疏的肌上皮样肿瘤细胞(由于它们产生细胞外基质而被视为分化细胞)表达TSC-22。然而,在PA中仅有限数量的被认为是正在生长的细胞的实体肌上皮样肿瘤细胞表达TSC-22。在腺样囊性癌(ACC)中,尽管肌上皮样外肿瘤细胞不表达TSC-22,但管状结构的内部导管细胞强烈表达TSC-22。在筛状结构中,肌上皮样肿瘤细胞不表达TSC-22。然而,微囊壁中的小导管结构强烈表达了TSC-22。 ACC中的稀疏型肌上皮样肿瘤细胞也表达TSC-22。在粘液表皮样癌中,粘液表皮样癌中的表皮样肿瘤细胞和产生粘液的肿瘤细胞经常表达TSC-22。因此,在分化表型的细胞中经常观察到TSC-22的表达,尽管在具有增长潜力的细胞中很少见。这些结果表明TSC-22可能在维持唾液腺肿瘤的分化表型中起重要作用。

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