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通过重组基底膜体外侵袭筛选出的人前列腺癌细胞高侵袭性和转移性变体中α3β1和α6β4整合素表达的特异性改变。

Specific alterations in the expression of alpha 3 beta 1 and alpha 6 beta 4 integrins in highly invasive and metastatic variants of human prostate carcinoma cells selected by in vitro invasion through reconstituted basement membrane.

作者信息

Dedhar S, Saulnier R, Nagle R, Overall C M

机构信息

Division of Cancer Research, Sunnybrook Health Science Centre, Toronto, Canada.

出版信息

Clin Exp Metastasis. 1993 Sep;11(5):391-400. doi: 10.1007/BF00132982.

Abstract

Highly invasive cell subpopulations from a human prostate carcinoma cell line, PC-3, were selected for by allowing the parental PC-3 cells to invade through reconstituted basement membrane, Matrigel. These cells were collected, cultured and then selected further by repeated invasion through the in vitro invasion chamber. The invasive subpopulations (I-PC3 (2) and (3)) were found to be approximately 15-fold more invasive in vitro than the parental cells, had a distinct rounded morphology in culture, and proliferated more rapidly than the parental cells. When injected either subcutaneously or intraperitoneally into immunocompromised SCID mice, the I-PC3 cells were found to form tumors at the primary sites and to be highly invasive and metastatic. In contrast, the parental PC-3 cells formed tumors at the site of inoculation in these mice but failed to invade or metastasize. The I-PC3 cells attached equally as well as PC-3 cells to fibronectin, laminin, collagen type IV and vitronectin, but unlike the parental PC-3 cells these invasive variants failed to spread on any of these substrates. On Matrigel, the PC-3 cells became highly organized, whereas the I-PC3 cells remained rounded, clumped together and penetrated into the Matrigel. Biochemical analysis of the expression of adhesion proteins and integrins demonstrated that whereas the parental cells synthesized and secreted substantial amounts of fibronectin, the I-PC3 cell variants did not secrete any fibronectin. Although both PC-3 and I-PC3 cells expressed equivalent levels of cell surface alpha v beta 3, alpha 2 beta 1 and alpha 5 beta 1 integrins, the expression of the alpha 3 beta 1 integrin, which is expressed at very high levels on the parental PC-3 cells, was drastically reduced on the invasive I-PC3 cells. This decrease in expression of alpha 3 occurred also at the level of mRNA expression. Finally, whereas the PC-3 cells express alpha 6 beta 1, in the invasive I-PC3 cells the alpha 6 subunit was associated mostly with the beta 4 subunit. Since the alpha 6 beta 4 integrin is analogous to the A9 tumor antigen which is associated with aggressive human squamous cell carcinomas, the apparent overexpression of alpha 6 beta 4 may also participate in the aggressive behavior of these variant prostate carcinoma cells. Alterations in the expression of the alpha 3 beta 1 and alpha 6 beta 4 integrins may thus allow these cells to become more invasive, and lead to an increased propensity for metastasis.

摘要

通过让亲代PC-3细胞穿过重组基底膜基质胶进行侵袭,从人前列腺癌细胞系PC-3中筛选出高侵袭性细胞亚群。收集这些细胞并进行培养,然后通过体外侵袭小室的反复侵袭进一步筛选。发现侵袭性亚群(I-PC3(2)和(3))在体外的侵袭性比亲代细胞高约15倍,在培养中具有明显的圆形形态,并且比亲代细胞增殖更快。当皮下或腹腔注射到免疫缺陷的SCID小鼠体内时,发现I-PC3细胞在原发部位形成肿瘤,并且具有高度侵袭性和转移性。相比之下,亲代PC-3细胞在这些小鼠的接种部位形成肿瘤,但未能侵袭或转移。I-PC3细胞与PC-3细胞同等程度地附着于纤连蛋白、层粘连蛋白、IV型胶原和玻连蛋白,但与亲代PC-3细胞不同的是,这些侵袭性变体在任何这些底物上都未能铺展。在基质胶上,PC-3细胞变得高度有序,而I-PC3细胞保持圆形,聚集在一起并侵入基质胶。对黏附蛋白和整合素表达的生化分析表明,亲代细胞合成并分泌大量纤连蛋白,而I-PC3细胞变体不分泌任何纤连蛋白。尽管PC-3和I-PC3细胞表达同等水平的细胞表面αvβ3、α2β1和α5β1整合素,但在亲代PC-3细胞上高表达的α3β1整合素在侵袭性I-PC3细胞上的表达急剧降低。α3表达的这种降低在mRNA表达水平也有发生。最后,PC-3细胞表达α6β1,而在侵袭性I-PC3细胞中,α6亚基主要与β4亚基结合。由于α6β4整合素类似于与侵袭性人类鳞状细胞癌相关的A9肿瘤抗原,α6β4的明显过表达也可能参与这些变异前列腺癌细胞的侵袭行为。因此,α3β1和α6β4整合素表达的改变可能使这些细胞更具侵袭性,并导致转移倾向增加。

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