Literature DB >> 33740033

Stochastic combinations of actin regulatory proteins are sufficient to drive filopodia formation.

Ulrich Dobramysl1,2, Iris Katharina Jarsch1,2, Yoshiko Inoue1,2, Hanae Shimo1,2, Benjamin Richier1,2, Jonathan R Gadsby1,2, Julia Mason1,2, Alicja Szałapak1,2, Pantelis Savvas Ioannou1,2, Guilherme Pereira Correia1, Astrid Walrant1,2, Richard Butler1, Edouard Hannezo1,3, Benjamin D Simons1,4, Jennifer L Gallop1,2.   

Abstract

Assemblies of actin and its regulators underlie the dynamic morphology of all eukaryotic cells. To understand how actin regulatory proteins work together to generate actin-rich structures such as filopodia, we analyzed the localization of diverse actin regulators within filopodia in Drosophila embryos and in a complementary in vitro system of filopodia-like structures (FLSs). We found that the composition of the regulatory protein complex where actin is incorporated (the filopodial tip complex) is remarkably heterogeneous both in vivo and in vitro. Our data reveal that different pairs of proteins correlate with each other and with actin bundle length, suggesting the presence of functional subcomplexes. This is consistent with a theoretical framework where three or more redundant subcomplexes join the tip complex stochastically, with any two being sufficient to drive filopodia formation. We provide an explanation for the observed heterogeneity and suggest that a mechanism based on multiple components allows stereotypical filopodial dynamics to arise from diverse upstream signaling pathways.
© 2021 Dobramysl et al.

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Year:  2021        PMID: 33740033      PMCID: PMC7980258          DOI: 10.1083/jcb.202003052

Source DB:  PubMed          Journal:  J Cell Biol        ISSN: 0021-9525            Impact factor:   8.077


  61 in total

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