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A NOVEL WAY TO CHARACTERIZE THE NON-SPECIFIC SURFACE ADHESION OF CANCER CELLS AND UNDERSTAND CANCER METASTASIS

机译:一种表征癌细胞的非特异性表面粘附的新方法,理解癌症转移

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Cancer deaths are mostly caused by the metastasis of the malignant cells, not by the primary tumor itself. During metastasis, cancer cells detach from the primary tumor, spread to different tissues via blood circulation or lymph system, and reattach to invade new tissues and organs. In this project, we hypothesize that cancer cells manage their invasion by changing their surface adhesivity. To study the cell surface adhesivity, a novel and versatile microelectromechanical systems (MEMS) force sensor is developed to quantify the strength of adhesion between living cancer cells and a probe. The Silicon sensors consist of a probe and 2 flexible cantilever beams, while the probe is used to contact the cancer cell and the flexible beams are used to measure the cell force response in the range from nN to uN. The spring constant of the sensor is 14 nN/ μm. Our results demonstrate that the aggressive HCT-8 cells (from human colon adenocarcinoma) show high nonspecific adhesivity when they aggregate into cell islands, and low surface non-specific adhesivity after they disassociate from the cell islands. The surface adhesivity of less aggressive Caco- 2 cells (from human colon carcinoma) and normal MA104 cell (from monkey kidney) are found to be lower than that of before-disassociation HCT-8 cells. Furthermore, the adhesion force response of cancer cells is found to show 2-slope force behavior, which is different from previous results of focaladhesion detachment experiments. The 2-stage force bearing model is proposed to interpret the underlying mechanism.
机译:癌症死亡主要由恶性细胞转移引起的,而不是由原发性肿瘤本身引起的。在转移期间,癌细胞从原发性肿瘤分离,通过血液循环或淋巴系统扩散到不同的组织,并重新侵入新的组织和器官。在该项目中,我们假设癌细胞通过改变其表面粘附性来管理其侵袭。为了研究细胞表面粘附性,开发了一种新颖和通用的微机电系统(MEMS)力传感器以量化生物癌细胞和探针之间的粘附强度。硅传感器由探头和2个柔性悬臂梁组成,而探针用于接触癌细胞,并且柔性梁用于测量从NN到UN的范围内的细胞力响应。传感器的弹簧常数为14 nn /μm。我们的结果表明,当它们聚集到细胞岛后,侵袭性HCT-8细胞(来自人结肠腺癌)显示出高的非特异性粘合性,以及在离细胞岛中分离的低表面非特异性粘合性。发现不太侵蚀性CaCo-2细胞(来自人结肠癌)和正常MA104细胞(来自猴子肾脏)的表面粘附性低于脱离前的HCT-8细胞的细胞。此外,发现癌细胞的粘附力响应显示出2斜率的力行为,其与先前的聚焦粘附脱离实验结果不同。提出了2级力轴承模型来解释潜在机制。

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