The relationship between the mechanical properties of cells and their molecular architecture has been the focus of extensive research for decades. The cytoskeleton, an internal polymer network, in particular determines a cell's mechanical strength and morphology. This cytoskeleton evolves during the normal differentiation of cells, is involved in many cellular functions, and is characteristically altered in many diseases, including cancer. Here we examine this hypothesized link between function and elasticity, enabling the distinction between different cells, by using a microfluidic optical stretcher, a two-beam laser trap optimized to serially deform single suspended cells by optically induced surface forces. In contrast to previous cell elasticity measurement techniques, statistically relevant numbers of single cells can be measured in rapid succession through microfluidic delivery, without any modification or contact. We find that optical deformability is sensitive enough to monitor the subtle changes during the progression of mouse fibroblasts and human breast epithelial cells from normal to cancerous and even metastatic state. The surprisingly low numbers of cells required for this distinction reflect the tight regulation of the cytoskeleton by the cell. This suggests using optical deformability as an inherent cell marker for basic cell biological investigation and diagnosis of disease.
Optical deformability as an inherent cell marker for testing malignant transformation and metastatic competence.
光学形变性作为细胞固有的标志物,可用于检测恶性转化和转移能力
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作者:Guck Jochen, Schinkinger Stefan, Lincoln Bryan, Wottawah Falk, Ebert Susanne, Romeyke Maren, Lenz Dominik, Erickson Harold M, Ananthakrishnan Revathi, Mitchell Daniel, Käs Josef, Ulvick Sydney, Bilby Curt
| 期刊: | Biophysical Journal | 影响因子: | 3.100 |
| 时间: | 2005 | 起止号: | 2005 May;88(5):3689-98 |
| doi: | 10.1529/biophysj.104.045476 | 研究方向: | 细胞生物学 |
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