βIII Spectrin Binds to the Arp1 Subunit of Dynactin

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Abstract

Cytoplasmic dynein is an intracellular motor responsible for endoplasmic reticulum-to-Golgi vesicle trafficking and retrograde axonal transport. The accessory protein dynactin has been proposed to mediate the association of dynein with vesicular cargo. Dynactin contains a 37-nm filament made up of the actin-related protein, Arp1, which may interact with a vesicle-associated spectrin network. Here, we demonstrate that Arp1 binds directly to the Golgi-associated βIII spectrin isoform. We identify two Arp1-binding sites in βIII spectrin, one of which overlaps with the actin-binding site conserved among spectrins. Although conventional actin binds weakly to βIII spectrin, Arp1 binds robustly in the presence of excess F-actin. Dynein, dynactin, and βIII spectrin co-purify on vesicles isolated from rat brain, and βIII spectrin co-immunoprecipitates with dynactin from rat brain cytosol. In interphase cells, βIII spectrin and dynactin both localize to cytoplasmic vesicles, co-localizing most significantly in the perinuclear region of the cell. In dividing cells, βIII spectrin and dynactin co-localize to the developing cleavage furrow and mitotic spindle, a novel localization for βIII spectrin. We hypothesize that the interaction between βIII spectrin and Arp1 recruits dynein and dynactin to intracellular membranes and provides a direct link between the microtubule motor complex and its membrane-bounded cargo.

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Holleran, E. A., Ligon, L. A., Tokito, M., Stankewich, M. C., Morrow, J. S., & Holzbaur, E. L. F. (2001). βIII Spectrin Binds to the Arp1 Subunit of Dynactin. Journal of Biological Chemistry, 276(39), 36598–36605. https://doi.org/10.1074/jbc.M104838200

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