Extended DNA threading through a dual-engine motor module of the activating signal co-integrator 1 complex

Author:

Jia JunqiaoORCID,Hilal TarekORCID,Bohnsack Katherine E.ORCID,Chernev Aleksandar,Tsao Ning,Bethmann Juliane,Arumugam ArunaORCID,Parmely Lane,Holton Nicole,Loll BernhardORCID,Mosammaparast NimaORCID,Bohnsack Markus T.,Urlaub HenningORCID,Wahl Markus C.ORCID

Abstract

AbstractActivating signal co-integrator 1 complex (ASCC) subunit 3 (ASCC3) supports diverse genome maintenance and gene expression processes, and contains tandem Ski2-like NTPase/helicase cassettes crucial for these functions. Presently, the molecular mechanisms underlying ASCC3 helicase activity and regulation remain unresolved. We present cryogenic electron microscopy, DNA-protein cross-linking/mass spectrometry as well as in vitro and cellular functional analyses of the ASCC3-TRIP4 sub-module of ASCC. Unlike the related spliceosomal SNRNP200 RNA helicase, ASCC3 can thread substrates through both helicase cassettes. TRIP4 docks on ASCC3 via a zinc finger domain and stimulates the helicase by positioning an ASC-1 homology domain next to the C-terminal helicase cassette of ASCC3, likely supporting substrate engagement and assisting the DNA exit. TRIP4 binds ASCC3 mutually exclusively with the DNA/RNA dealkylase, ALKBH3, directing ASCC3 for specific processes. Our findings define ASCC3-TRIP4 as a tunable motor module of ASCC that encompasses two cooperating NTPase/helicase units functionally expanded by TRIP4.

Funder

Deutsche Forschungsgemeinschaft

American Cancer Society

U.S. Department of Health & Human Services | National Institutes of Health

Berlin University Alliance, project number 501_BIS-CryoFac

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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