DNA repair / helicase / ATPase / TRANSFERASE-INHIBITOR complex
Function / homology
Function and homology information
single-stranded DNA endodeoxyribonuclease activity / double-strand break repair via alternative nonhomologous end joining / HDR through MMEJ (alt-NHEJ) / single-stranded DNA helicase activity / replication fork processing / site of DNA damage / negative regulation of double-strand break repair via homologous recombination / 5'-deoxyribose-5-phosphate lyase activity / error-prone translesion synthesis / somatic hypermutation of immunoglobulin genes ...single-stranded DNA endodeoxyribonuclease activity / double-strand break repair via alternative nonhomologous end joining / HDR through MMEJ (alt-NHEJ) / single-stranded DNA helicase activity / replication fork processing / site of DNA damage / negative regulation of double-strand break repair via homologous recombination / 5'-deoxyribose-5-phosphate lyase activity / error-prone translesion synthesis / somatic hypermutation of immunoglobulin genes / DNA helicase activity / base-excision repair / protein homooligomerization / RNA-directed DNA polymerase / RNA-directed DNA polymerase activity / double-strand break repair / site of double-strand break / DNA helicase / damaged DNA binding / DNA-directed DNA polymerase / DNA-directed DNA polymerase activity / DNA repair / DNA damage response / chromatin binding / Golgi apparatus / magnesium ion binding / ATP hydrolysis activity / nucleoplasm / ATP binding / identical protein binding / cytosol Similarity search - Function
DNA polymerase theta-like, helix-turn-helix domain / : / Helix-turn-helix domain / DNA_pol_Q helicase like region helical domain / DNA polymerase A / DNA polymerase family A / DNA-directed DNA polymerase, family A, conserved site / DNA polymerase family A signature. / DNA-directed DNA polymerase, family A, palm domain / DNA polymerase A domain ...DNA polymerase theta-like, helix-turn-helix domain / : / Helix-turn-helix domain / DNA_pol_Q helicase like region helical domain / DNA polymerase A / DNA polymerase family A / DNA-directed DNA polymerase, family A, conserved site / DNA polymerase family A signature. / DNA-directed DNA polymerase, family A, palm domain / DNA polymerase A domain / DEAD/DEAH box helicase domain / DEAD/DEAH box helicase / Helicase conserved C-terminal domain / helicase superfamily c-terminal domain / Superfamilies 1 and 2 helicase C-terminal domain profile. / Superfamilies 1 and 2 helicase ATP-binding type-1 domain profile. / DEAD-like helicases superfamily / Helicase, C-terminal / Helicase superfamily 1/2, ATP-binding domain / Ribonuclease H superfamily / Ribonuclease H-like superfamily / DNA/RNA polymerase superfamily / P-loop containing nucleoside triphosphate hydrolase Similarity search - Domain/homology
National Institutes of Health/National Institute of General Medical Sciences (NIH/NIGMS)
GM130889
United States
Citation
Journal: Nat Commun / Year: 2024 Title: Structural basis for a Polθ helicase small-molecule inhibitor revealed by cryo-EM. Authors: Fumiaki Ito / Ziyuan Li / Leonid Minakhin / Gurushankar Chandramouly / Mrityunjay Tyagi / Robert Betsch / John J Krais / Bernadette Taberi / Umeshkumar Vekariya / Marissa Calbert / Tomasz ...Authors: Fumiaki Ito / Ziyuan Li / Leonid Minakhin / Gurushankar Chandramouly / Mrityunjay Tyagi / Robert Betsch / John J Krais / Bernadette Taberi / Umeshkumar Vekariya / Marissa Calbert / Tomasz Skorski / Neil Johnson / Xiaojiang S Chen / Richard T Pomerantz / Abstract: DNA polymerase theta (Polθ) is a DNA helicase-polymerase protein that facilitates DNA repair and is synthetic lethal with homology-directed repair (HDR) factors. Thus, Polθ is a promising precision ...DNA polymerase theta (Polθ) is a DNA helicase-polymerase protein that facilitates DNA repair and is synthetic lethal with homology-directed repair (HDR) factors. Thus, Polθ is a promising precision oncology drug-target in HDR-deficient cancers. Here, we characterize the binding and mechanism of action of a Polθ helicase (Polθ-hel) small-molecule inhibitor (AB25583) using cryo-EM. AB25583 exhibits 6 nM IC against Polθ-hel, selectively kills BRCA1/2-deficient cells, and acts synergistically with olaparib in cancer cells harboring pathogenic BRCA1/2 mutations. Cryo-EM uncovers predominantly dimeric Polθ-hel:AB25583 complex structures at 3.0-3.2 Å. The structures reveal a binding-pocket deep inside the helicase central-channel, which underscores the high specificity and potency of AB25583. The cryo-EM structures in conjunction with biochemical data indicate that AB25583 inhibits the ATPase activity of Polθ-hel helicase via an allosteric mechanism. These detailed structural data and insights about AB25583 inhibition pave the way for accelerating drug development targeting Polθ-hel in HDR-deficient cancers.
Name: (4P)-N-{5-[(4-chlorophenyl)methoxy]-1,3,4-thiadiazol-2-yl}-4-(2-methoxyphenyl)pyridine-3-carboxamide type: ligand / ID: 2 / Number of copies: 2 / Formula: WCN
Molecular weight
Theoretical: 452.913 Da
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Experimental details
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Structure determination
Method
cryo EM
Processing
single particle reconstruction
Aggregation state
particle
-
Sample preparation
Concentration
0.8 mg/mL
Buffer
pH: 8
Vitrification
Cryogen name: ETHANE / Chamber humidity: 100 % / Chamber temperature: 277 K / Instrument: FEI VITROBOT MARK IV
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Electron microscopy
Microscope
TFS GLACIOS
Image recording
Film or detector model: FEI FALCON IV (4k x 4k) / Number grids imaged: 1 / Number real images: 4500 / Average exposure time: 8.0 sec. / Average electron dose: 58.0 e/Å2
Electron beam
Acceleration voltage: 200 kV / Electron source: FIELD EMISSION GUN
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Movie
Controller
Yorodumi
Open data
Basic information
Map data
Sample
Keywords
Function and homology information
Homo sapiens (human)
Authors
United States, 1 items 
Citation
Structure visualization
Downloads & links
emd_44765.png
http://ftp.pdbj.org/pub/emdb/structures/EMD-44765
Z (Sec.)
Y (Row.)
X (Col.)
Sample components
Escherichia coli (E. coli)
Processing
Electron microscopy
FIELD EMISSION GUN
