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微管、细胞极性和黏附在电场介导的3T3成纤维细胞运动中的作用。

Roles of microtubules, cell polarity and adhesion in electric-field-mediated motility of 3T3 fibroblasts.

作者信息

Finkelstein Erik, Chang Winston, Chao P-H Grace, Gruber Dorota, Minden Audrey, Hung Clark T, Bulinski J Chloë

机构信息

Department of Biological Sciences, Columbia University, New York, NY 10027, USA.

出版信息

J Cell Sci. 2004 Mar 15;117(Pt 8):1533-45. doi: 10.1242/jcs.00986.

Abstract

Direct-current electric fields mediate motility (galvanotaxis) of many cell types. In 3T3 fibroblasts, electric fields increased the proportion, speed and cathodal directionality of motile cells. Analogous to fibroblasts' spontaneous migration, we initially hypothesized that reorientation of microtubule components modulates galvanotaxis. However, cells with intact microtubules did not reorient them in the field and cells without microtubules still migrated, albeit slowly, thus disproving the hypothesis. We next proposed that, in monolayers wounded and placed in an electric field, reorientation of microtubule organizing centers and stable, detyrosinated microtubules towards the wound edge is necessary and/or sufficient for migration. This hypothesis was negated because field exposure mediated migration of unoriented, cathode-facing cells and curtailed migration of oriented, anode-facing cells. This led us to propose that ablating microtubule detyrosination would not affect galvanotaxis. Surprisingly, preventing microtubule detyrosination increased motility speed, suggesting that detyrosination inhibits galvanotaxis. Microtubules might enhance adhesion/de-adhesion remodeling during galvanotaxis; thus, electric fields might more effectively mediate motility of cells poorly or dynamically attached to substrata. Consistent with this hypothesis, incompletely spread cells migrated more rapidly than fully spread cells. Also, overexpression of PAK4, a Cdc42-activated kinase that decreases adhesion, enhanced galvanotaxis speed, whereas its lack decreased speed. Thus, electric fields mediate fibroblast migration via participation of microtubules and adhesive components, but their participation differs from that during spontaneous motility.

摘要

直流电场介导多种细胞类型的运动(趋电性)。在3T3成纤维细胞中,电场增加了运动细胞的比例、速度和向阴极的方向性。类似于成纤维细胞的自发迁移,我们最初假设微管成分的重新定向调节趋电性。然而,微管完整的细胞在电场中并未重新定向,而没有微管的细胞仍能迁移,尽管速度缓慢,从而推翻了这一假设。接下来我们提出,在单层细胞受伤并置于电场中时,微管组织中心和稳定的、去酪氨酸化的微管向伤口边缘的重新定向对于迁移是必要的和/或充分的。这一假设也被否定了,因为电场暴露介导了未定向的、面向阴极的细胞的迁移,并减少了定向的、面向阳极的细胞的迁移。这使我们提出,消除微管去酪氨酸化不会影响趋电性。令人惊讶的是,阻止微管去酪氨酸化会提高运动速度,这表明去酪氨酸化抑制趋电性。微管可能在趋电性过程中增强黏附/去黏附重塑;因此,电场可能更有效地介导与基质黏附不良或动态黏附的细胞的运动。与此假设一致,未完全铺展的细胞比完全铺展的细胞迁移得更快。此外,PAK4(一种Cdc42激活的激酶,可降低黏附力)的过表达提高了趋电速度,而其缺失则降低了速度。因此,电场通过微管和黏附成分的参与介导成纤维细胞迁移,但其参与方式与自发运动过程不同。

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