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Conserved hydrophobic residues in the CARP/β-sheet domain of cyclase-associated protein are involved in actin monomer regulation.

Cytoskeleton (Hoboken). 2017 Sep;74(9):343-355. doi:10.1002/cm.21385. Epub 2017 Jul 21
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摘要


Cyclase-associated protein (CAP) is a multidomain protein that promotes actin filament dynamics. The C-terminal region of CAP contains a CAP and X-linked retinitis pigmentosa 2 protein domain (or a β-sheet domain), which binds to actin monomer and is essential for enhancing exchange of actin-bound nucleotides. However, how the domain binds to actin is not clearly understood. Here, we report that conserved hydrophobic residues in the Cduanyu37 domain play important roles in the function of CAP to regulate actin dynamics. Single mutations of three conserved surface-exposed hydrophobic residues in the Cduanyu37 domain of CAS-2, a Caenorhabditis elegans CAP, significantly reduce its binding to actin monomers and suppress its nucleotide exchange activity on actin. As a result, these mutants are weaker than wild-type to compete with ADF/cofilin to promote recycling of actin monomers for polymerization. A double mutation (V367A/I373A) eliminates these actin-regulatory functions of CAS-2. These hydrophobic residues and previously identified functional residues are scattered on a concave β-sheet of the Cduanyu37 domain, suggesting that a wide area of the β-sheet is involved in binding to actin. These observations suggest that the Cduanyu37 domain of CAP binds to actin in a distinct manner from other known actin-binding proteins.

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