流体剪切应力暴露后癌细胞力学特性的改变:一项微管抽吸研究。

Venkat Keshav Chivukula, Benjamin L Krog, Jones T Nauseef, Michael D Henry, Sarah C Vigmostad
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引用次数: 48

摘要

超过90%的癌症死亡不是由于原发肿瘤的发展,而是由于癌细胞通过循环系统循环到远端部位后出现的转移性肿瘤。虽然已知转移是一个低效的过程,但血流动力学参数如流体剪切应力(FSS)对转移的活力和疗效的影响尚不清楚。最近的研究表明,某些癌细胞可能能够在体外存活,甚至可能适应FSS。目前的研究旨在表征FSS对体外悬浮癌细胞力学性能的影响。本研究采用非转化前列腺上皮细胞(PrEC LH)和转化前列腺癌细胞(PC-3)。杨氏模量采用微移管抽吸法测定。我们检测了悬浮但未暴露于FSS(未剪切)和暴露于高(6,400 dyn/cm2)和低(510 dyn/cm2) FSS后立即检测的细胞。PrEC LH细胞比未暴露于FSS的PC-3细胞硬约140%。FSS暴露后,PC-3细胞暴露于高FSS后杨氏模量增加了~77%,暴露于低FSS后杨氏模量增加了~47%。暴露于fss后,PrEC LH细胞的杨氏模量没有明显变化。我们的研究结果表明,癌细胞适应FSS,杨氏模量增加是适应性反应之一,这种适应仅针对PC-3细胞,而在PrEC LH细胞中未见。此外,这种适应似乎是根据癌细胞经历的FSS的大小而分级的。这是第一个研究FSS对悬浮癌细胞力学特性影响的研究,并可能为一些选定的癌细胞在循环中存活并最终导致远端转移的机制提供重要的见解。我们的研究结果表明,对癌细胞的生物力学分析可以在未来帮助识别和诊断癌症。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Alterations in cancer cell mechanical properties after fluid shear stress exposure: a micropipette aspiration study.

Alterations in cancer cell mechanical properties after fluid shear stress exposure: a micropipette aspiration study.

Alterations in cancer cell mechanical properties after fluid shear stress exposure: a micropipette aspiration study.

Alterations in cancer cell mechanical properties after fluid shear stress exposure: a micropipette aspiration study.

Over 90% of cancer deaths result not from primary tumor development, but from metastatic tumors that arise after cancer cells circulate to distal sites via the circulatory system. While it is known that metastasis is an inefficient process, the effect of hemodynamic parameters such as fluid shear stress (FSS) on the viability and efficacy of metastasis is not well understood. Recent work has shown that select cancer cells may be able to survive and possibly even adapt to FSS in vitro. The current research seeks to characterize the effect of FSS on the mechanical properties of suspended cancer cells in vitro. Nontransformed prostate epithelial cells (PrEC LH) and transformed prostate cancer cells (PC-3) were used in this study. The Young's modulus was determined using micropipette aspiration. We examined cells in suspension but not exposed to FSS (unsheared) and immediately after exposure to high (6,400 dyn/cm2) and low (510 dyn/cm2) FSS. The PrEC LH cells were ~140% stiffer than the PC-3 cells not exposed to FSS. Post-FSS exposure, there was an increase of ~77% in Young's modulus after exposure to high FSS and a ~47% increase in Young's modulus after exposure to low FSS for the PC-3 cells. There was no significant change in the Young's modulus of PrEC LH cells post-FSS exposure. Our findings indicate that cancer cells adapt to FSS, with an increased Young's modulus being one of the adaptive responses, and that this adaptation is specific only to PC-3 cells and is not seen in PrEC LH cells. Moreover, this adaptation appears to be graded in response to the magnitude of FSS experienced by the cancer cells. This is the first study investigating the effect of FSS on the mechanical properties of cancer cells in suspension, and may provide significant insights into the mechanism by which some select cancer cells may survive in the circulation, ultimately leading to metastasis at distal sites. Our findings suggest that biomechanical analysis of cancer cells could aid in identifying and diagnosing cancer in the future.

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