小的热休克蛋白hsp27增加了乳腺癌细胞的侵袭性,但降低了活动性。

Invasion & metastasis Pub Date : 1997-01-01
P Lemieux, S Oesterreich, J A Lawrence, P S Steeg, S G Hilsenbeck, J M Harvey, S A Fuqua
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引用次数: 0

摘要

小热休克蛋白hsp27在临床乳腺肿瘤中高水平表达;然而,其在该病中的生物学作用仍不清楚。几个实验室最近表明,hsp27的表达与肿瘤的侵袭性行为有关。我们假设hsp27可能影响肿瘤转移过程,因为这是肿瘤“侵袭性”的一部分。因此,我们分别用正(MDA-MB-231)和反义(MDA-MB-435) hsp27构建物稳定转染乳腺癌细胞系,并检测了与转移过程相关的各个细胞方面。我们发现,与低表达的细胞相比,hsp27过表达的克隆失去了它们的突出形态,但表现出更高的膜褶皱。hsp27过表达也导致细胞活力下降,但侵袭性、黏附性和生长均显著增加。相反,反义抑制hsp27表达导致细胞运动性增加,但体外侵袭性降低。通过注射hsp27转染细胞的小鼠体内检测肺转移的数量,证实了hsp27水平与转移的直接相关性。因此,我们得出结论,hsp27过表达可能影响人乳腺癌细胞的侵袭和转移潜能。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
The small heat shock protein hsp27 increases invasiveness but decreases motility of breast cancer cells.

The small heat shock protein hsp27 is often expressed at high levels in clinical breast tumors; however, its biological role in this disease still remains unclear. Several laboratories have recently shown that hsp27 expression is associated with aggressive tumor behavior. We hypothesized that hsp27 may influence the metastatic tumor process since this is part of tumor 'aggressiveness'. Therefore, we stably transfected breast cancer cell lines with sense (MDA-MB-231) and antisense (MDA-MB-435) hsp27 constructs, respectively, and examined various cellular aspects associated with the metastatic process. We found that hsp27-overexpressing clones lost their protrusive morphology, but exhibited higher membrane ruffling as compared to low expressing cells. hsp27 overexpression also resulted in decreased cell motility, but invasiveness, adhesion, and growth in Matrigel were all significantly increased. Conversely, antisense suppression of hsp27 expression resulted in increased cell motility, but decreased in vitro invasiveness. The direct correlation of hsp27 levels with metastasis was confirmed by an in vivo assay measuring the number of lung metastases in mice injected with hsp27-transfected cells. Thus, we conclude that hsp27 overexpression may influence the invasive and metastatic potential of human breast cancer cells.

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