AI Article Synopsis

  • Dynamin is a key GTPase involved in various cellular functions, including endocytosis and cytokinesis, with the social amoebozoan exhibiting five dynamin-like proteins.
  • Cells lacking dymA, dlpA, or dlpB showed issues with cytokinesis, and dlpA and dlpB were found together at cleavage furrows during cell division while dymA localized at the bridge between daughter cells.
  • The study suggests that dlpA and dlpB form hetero-oligomers for effective function in cytokinesis, as their interaction is crucial for stabilizing actin filaments and they operate cooperatively with dymA, while dlpA also plays a role in phagocytosis independently

Article Abstract

Dynamin is a large GTPase responsible for diverse cellular processes, such as endocytosis, division of organelles, and cytokinesis. The social amoebozoan, , has five dynamin-like proteins: dymA, dymB, dlpA, dlpB, and dlpC. DymA, dlpA, or dlpB-deficient cells exhibited defects in cytokinesis. DlpA and dlpB were found to colocalize at cleavage furrows from the early phase, and dymA localized at the intercellular bridge connecting the two daughter cells, indicating that these dynamins contribute to cytokinesis at distinct dividing stages. Total internal reflection fluorescence microscopy revealed that dlpA and dlpB colocalized at individual dots at the furrow cortex. However, dlpA and dlpB did not colocalize with clathrin, suggesting that they are not involved in clathrin-mediated endocytosis. The fact that dlpA did not localize at the furrow in dlpB null cells and vice versa, as well as other several lines of evidence, suggests that hetero-oligomerization of dlpA and dlpB is required for them to bind to the furrow. The hetero-oligomers directly or indirectly associate with actin filaments, stabilizing them in the contractile rings. Interestingly, dlpA, but not dlpB, accumulated at the phagocytic cups independently of dlpB. Our results suggest that the hetero-oligomers of dlpA and dlpB contribute to cytokinesis cooperatively with dymA.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6721605PMC
http://dx.doi.org/10.3390/cells8080781DOI Listing

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