AI Article Synopsis

  • Centrosomes play a crucial role in microtubule dynamics, and removing them leads to decreased microtubule mass and changes in behavior from dynamic instability to treadmilling.
  • In cadherin-expressing cells, the presence of cadherin can reverse these effects, allowing for dense microtubule arrays even without centrosomes.
  • Among the cadherin-associated proteins, only membrane-targeted alpha-catenin was effective in significantly enhancing microtubule length and density in cells lacking centrosomes, indicating its unique regulatory role in microtubule dynamics independent of centrosomes.

Article Abstract

Centrosomes control microtubule dynamics in many cell types, and their removal from the cytoplasm leads to a shift from dynamic instability to treadmilling behavior and to a dramatic decrease of microtubule mass (Rodionov et al., 1999; PNAS 96:115). In cadherin-expressing cells, these effects can be reversed:non-centrosomal cytoplasts that form cadherin-mediated adherens junctions display dense arrays of microtubules (Chausovsky et al., 2000; Nature Cell Biol 2:797). In adherens junctions, cadherin's cytoplasmic domain binds p120 catenin and beta-catenin, which in turn binds alpha-catenin. To elucidate the roles of the cadherin-associated proteins in regulating microtubule dynamics, we prepared GFP-tagged, plasma membrane targeted or untargeted p120 catenin, alpha-catenin and beta-catenin and tested their ability to rescue the loss of microtubule mass caused by centrosomal removal in the poorly adhesive cell line CHO-K1. Only membrane targeting of alpha-catenin led to a significant increase in microtubule length and density in centrosome-free cytoplasts. Expression of non-membrane-targeted alpha-catenin produced only a slight effect, while both membrane-targeted and non-targeted p120 and beta-catenin were ineffective in this assay. Together, these findings suggest that alpha-catenin is able to regulate microtubule dynamics in a centrosome-independent manner.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2668206PMC
http://dx.doi.org/10.4161/cc.6362DOI Listing

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