Isoform diversity in the Arp2/3 complex determines actin filament dynamics

被引:0
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作者
Jasmine V. G. Abella
Chiara Galloni
Julien Pernier
David J. Barry
Svend Kjær
Marie-France Carlier
Michael Way
机构
[1] Cellular Signalling and Cytoskeletal Function,
[2] The Francis Crick Institute,undefined
[3] Lincoln’s Inn Fields Laboratory,undefined
[4] Laboratoire d’Enzymologie et Biochimie Structurale,undefined
[5] The Structural Biology Science Technology Platform,undefined
[6] The Francis Crick Institute,undefined
[7] Lincoln’s Inn Fields Laboratory,undefined
来源
Nature Cell Biology | 2016年 / 18卷
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摘要
The Arp2/3 complex consists of seven evolutionarily conserved subunits (Arp2, Arp3 and ARPC1–5) and plays an essential role in generating branched actin filament networks during many different cellular processes. In mammals, however, the ARPC1 and ARPC5 subunits are each encoded by two isoforms that are 67% identical. This raises the possibility that Arp2/3 complexes with different properties may exist. We found that Arp2/3 complexes containing ARPC1B and ARPC5L are significantly better at promoting actin assembly than those with ARPC1A and ARPC5, both in cells and in vitro. Branched actin networks induced by complexes containing ARPC1B or ARPC5L are also disassembled ∼2-fold slower than those formed by their counterparts. This difference reflects the ability of cortactin to stabilize ARPC1B- and ARPC5L- but not ARPC1A- and ARPC5-containing complexes against coronin-mediated disassembly. Our observations demonstrate that the Arp2/3 complex in higher eukaryotes is actually a family of complexes with different properties.
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页码:76 / 86
页数:10
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