Journal
JOURNAL OF MOLECULAR BIOLOGY
Volume 435, Issue 8, Pages -Publisher
ACADEMIC PRESS LTD- ELSEVIER SCIENCE LTD
DOI: 10.1016/j.jmb.2023.168035
Keywords
intrinsically disordered proteins; autoinhibition; PIP2; WASP; prenylation
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Human WASP and N-WASP are homologous proteins that require the binding of multiple regulators, including PIP2 and Cdc42, to relieve autoinhibition. In the absence of Cdc42, both proteins associate with PIP2-containing membranes through their basic region. Cdc42 binding compromises the ability of the basic region in WASP, but not N-WASP, to bind PIP2.
Human WASP and N-WASP are homologous proteins that require the binding of multiple regulators, including the acidic lipid PIP2 and the small GTPase Cdc42, to relieve autoinhibition before they can stim-ulate the initiation of actin polymerization. Autoinhibition involves intramolecular binding of the C-terminal acidic and central motifs to an upstream basic region and GTPase binding domain. Little is known about how a single intrinsically disordered protein, WASP or N-WASP, binds multiple regulators to achieve full activation. Here we used molecular dynamics simulations to characterize the binding of WASP and N -WASP with PIP2 and Cdc42. In the absence of Cdc42, both WASP and N-WASP strongly associate with PIP2-containing membranes, through their basic region and also possibly through a tail portion of the N -terminal WH1 domain. The basic region also participates in Cdc42 binding, especially for WASP; conse-quently Cdc42 binding significantly compromises the ability of the basic region in WASP, but not N-WASP, to bind PIP2. PIP2 binding to the WASP basic region is restored only when Cdc42 is prenylated at the C -terminus and tethered to the membrane. This distinction in the activation of WASP and N-WASP may con-tribute to their different functional roles.(c) 2023 Elsevier Ltd. All rights reserved.
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