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Distribution of laminin and fibronectin isoforms in oral mucosa and oral squamous cell carcinoma

机译:层粘连蛋白和纤连蛋白同工型在口腔粘膜和口腔鳞状细胞癌中的分布

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摘要

The expression of laminin and fibronectin isoforms varies with cellular maturation and differentiation and these differences may well influence cellular processes such as adhesion and motility. The basement membrane (BM) of fetal oral squamous epithelium contains the laminin chains, α2, α3, α5, β1, β2, β3, γ1 and γ2. The BM of adult normal oral squamous epithelium comprises the laminin chains, α3, α5, β1, β3, γ1 and γ2. A re-expression of the laminin α2 and β2 chains could be shown in adult hyperproliferative, dysplastic and carcinomatous lesions. In dysplasia and oral squamous cell carcinoma (OSCC), multifocal breaks of the BM are present as indicated by laminin chain antibodies. These breaks correlate to malignancy grade in their extent. Moreover, in the invasion front the α3 and γ2 chain of laminin-5 can immunohistochemically be found outside the BM within the cytoplasm of budding carcinoma cells and in the adjacent stroma. The correlation between the morphological pattern of invasive tumour clusters and a laminin-5 immunostaining in the adjacent stroma may suggest, first, that a laminin-5 deposition outside the BM is an immunohistochemical marker for invasion and second, that OSCC invasion is guided by the laminin-5 matrix. Expression of oncofetal fibronectins (IIICS de novo glycosylated fibronectin and ED-B fibronectin) could be demonstrated throughout the stromal compartment. However, the ED-B fibronectin synthesizing cells (RNA/RNA in situ hybridization) are confined to small stroma areas and to single stroma and inflammatory cells in the invasion front. A correlation of the number of ED-B fibronectin synthesizing cells to malignancy grade could not be seen. ED-B fibronectin mRNA-positive cells seem to be concentrated in areas of fibrous stroma recruitment with a linear alignment of stromal fibro-/myofibroblasts (desmoplasia). Double staining experiments (ED-B fibronectin in situ hybridization and α-smooth muscle actin immunohistochemistry) indicated that the stroma myofibroblasts are a preferential source of ED-B fibronectin. In conclusion, in OSCC, a fetal extracellular matrix conversion is demonstrable. Tumour cells (laminin α2 and β2 chain) and recruited stromal myofibroblasts (oncofetal ED-B fibronectin) contribute to the fetal extracellular matrix milieu. © 1999 Cancer Research Campaign
机译:层粘连蛋白和纤连蛋白同工型的表达随细胞成熟和分化而变化,这些差异可能很好地影响细胞过程,如粘附和运动。胎儿口腔鳞状上皮的基底膜(BM)包含层粘连蛋白链α2,α3,α5,β1,β2,β3,γ1和γ2。成人正常口腔鳞状上皮的BM由层粘连蛋白链α3,α5,β1,β3,γ1和γ2组成。层粘连蛋白α2和β2链的重新表达可在成人过度增殖,发育异常和癌性病变中显示。在不典型增生和口腔鳞状细胞癌(OSCC)中,如层粘连蛋白链抗体所示,存在BM的多灶性断裂。这些断裂与恶性程度相关。此外,在浸润前层中,层粘连蛋白5的α3和γ2链可以通过免疫组织化学方法发现在芽胞状癌细胞的细胞质内和邻近基质中的BM外部。浸润性肿瘤簇的形态学模式与相邻基质中的层粘连蛋白5免疫染色之间的相关性可能表明,首先,BM层外的层粘连蛋白5沉积是浸润的免疫组织化学标记,其次,OSCC浸润是由肿瘤的层粘连蛋白5基质。可以在整个基质区室中证明胎粪纤连蛋白(IIICS de novo糖基化纤连蛋白和ED-B纤连蛋白)的表达。但是,ED-B纤连蛋白合成细胞(RNA / RNA原位杂交)仅限于较小的基质区域以及侵袭前沿的单个基质和炎性细胞。没有看到ED-B纤连蛋白合成细胞的数量与恶性程度的相关性。 ED-B纤连蛋白mRNA阳性细胞似乎集中在纤维基质募集区域,并与间质成纤维/成肌纤维细胞线性排列(异型增生)。双重染色实验(ED-B纤连蛋白原位杂交和α-平滑肌肌动蛋白免疫组织化学)表明,基质成纤维细胞是ED-B纤连蛋白的优先来源。总之,在OSCC中,可以证明胎儿细胞外基质的转化。肿瘤细胞(lamininα2和β2链)和募集的基质成肌纤维细胞(胎粪ED-B纤连蛋白)有助于胎儿细胞外基质环境。 ©1999癌症研究运动

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