4.4 Article

The Charged Linker Modulates the Conformations and Molecular Interactions of Hsp90

Journal

CHEMBIOCHEM
Volume 22, Issue 6, Pages 1084-1092

Publisher

WILEY-V C H VERLAG GMBH
DOI: 10.1002/cbic.202000699

Keywords

charged linkers; client interactions; dynamics; Hsp90; NMR spectroscopy

Funding

  1. German Research Foundation (DFG) [SFB 1035, 201302640]

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The molecular chaperone Hsp90 supports the functional activity of specific substrate proteins by undergoing ATP-driven conformational rearrangements. The long charged linker connecting the NTD and MD domains plays a crucial role in client binding. Characterization of the conformation and dynamics of the linker and NTD-MD domain interactions reveals important insights into the regulatory role of the charged linker.
The molecular chaperone Hsp90 supports the functional activity of specific substrate proteins (clients). For client processing, the Hsp90 dimer undergoes a series of ATP-driven conformational rearrangements. Flexible linkers connecting the three domains of Hsp90 are crucial to enable dynamic arrangements. The long charged linker connecting the N-terminal (NTD) and middle (MD) domains exhibits additional functions in vitro and in vivo. The structural basis for these functions remains unclear. Here, we characterize the conformation and dynamics of the linker and NTD-MD domain interactions by NMR spectroscopy. Our results reveal two regions in the linker that are dynamic and exhibit secondary structure conformation. We show that these regions mediate transient interactions with strand beta 8 of the NTD. As a consequence, this strand detaches and exposes a hydrophobic surface patch, which enables binding to the p53 client. We propose that the charged linker plays an important regulatory role by coupling the Hsp90 NTD-MD arrangement with the accessibility of a client binding site on the NTD.

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