Please use this identifier to cite or link to this item: http://hdl.handle.net/1942/36543
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dc.contributor.authorWILSON, David-
dc.contributor.authorDuncton, Matthew A. J.-
dc.contributor.authorChang, Caleb-
dc.contributor.authorLee Luo, Christie-
dc.contributor.authorGeorgiadis, Taxiarchis M.-
dc.contributor.authorPellicena, Patricia-
dc.contributor.authorDeacon, Ashley M.-
dc.contributor.authorGao, Yang-
dc.contributor.authorDas, Debanu-
dc.date.accessioned2022-01-20T07:52:57Z-
dc.date.available2022-01-20T07:52:57Z-
dc.date.issued2021-
dc.date.submitted2022-01-17T05:55:40Z-
dc.identifier.citationFrontiers in Oncology, 11 (Art N° 778925)-
dc.identifier.urihttp://hdl.handle.net/1942/36543-
dc.description.abstractPolymerase eta (or Pol eta or POLH) is a specialized DNA polymerase that is able to bypass certain blocking lesions, such as those generated by ultraviolet radiation (UVR) or cisplatin, and is deployed to replication foci for translesion synthesis as part of the DNA damage response (DDR). Inherited defects in the gene encoding POLH (a.k.a., XPV) are associated with the rare, sun-sensitive, cancer-prone disorder, xeroderma pigmentosum, owing to the enzyme's ability to accurately bypass UVR-induced thymine dimers. In standard-of-care cancer therapies involving platinum-based clinical agents, e.g., cisplatin or oxaliplatin, POLH can bypass platinum-DNA adducts, negating benefits of the treatment and enabling drug resistance. POLH inhibition can sensitize cells to platinum-based chemotherapies, and the polymerase has also been implicated in resistance to nucleoside analogs, such as gemcitabine. POLH overexpression has been linked to the development of chemoresistance in several cancers, including lung, ovarian, and bladder. Co-inhibition of POLH and the ATR serine/threonine kinase, another DDR protein, causes synthetic lethality in a range of cancers, reinforcing that POLH is an emerging target for the development of novel oncology therapeutics. Using a fragment-based drug discovery approach in combination with an optimized crystallization screen, we have solved the first X-ray crystal structures of small novel drug-like compounds, i.e., fragments, bound to POLH, as starting points for the design of POLH inhibitors. The intrinsic molecular resolution afforded by the method can be quickly exploited in fragment growth and elaboration as well as analog scoping and scaffold hopping using medicinal and computational chemistry to advance hits to lead. An initial small round of medicinal chemistry has resulted in inhibitors with a range of functional activity in an in vitro biochemical assay, leading to the rapid identification of an inhibitor to advance to subsequent rounds of chemistry to generate a lead compound. Importantly, our chemical matter is different from the traditional nucleoside analog-based approaches for targeting DNA polymerases.-
dc.description.sponsorshipResearch included in this publication was supported by the National Center For Advancing Translational Sciences of the NIH under Award Number R43 TR001736, and the National Institute of General Medical Sciences of the NIH under Award Number R44 GM132796, to Accelero Biostructures Inc.; National Cancer Institute of the NIH under Award Number R43 CA254552 to XPose Therapeutics, Inc.; and Cancer Prevention & Research Institute of Texas (CPRIT) Award RR190046 and Welch Foundation Grant Number C-2033- 20200401 to YG. CC was supported by a fellowship from the Houston Area Molecular Biophysics Program (NIH Grant No. T32 GM008280, Program Director Dr. Theodore Wensel). Synchrotron X-ray diffraction data collection and data processing was performed by Accelero Biostructures, Inc., California. Synchrotron data was collected at Stanford Synchrotron Radiation Lightsource (SSRL), SLAC National Accelerator Laboratory, Menlo Park, California. Use of the Stanford Synchrotron Radiation Lightsource (SSRL), SLAC National Accelerator Laboratory, is supported by the U.S. Department of Energy, Office of Science, Office of Basic Energy Sciences under Contract No. DE-AC02-76SF00515. The SSRL Structural Molecular Biology Program is supported by the DOE Office of Biological and Environmental Research, and by the National Institutes of Health, National Institute of General Medical Sciences (P41 GM103393). The contents of this publication are solely the responsibility of the authors and do not necessarily represent the official views of NIGMS or NIH.-
dc.language.isoen-
dc.publisherFRONTIERS MEDIA SA-
dc.rights2021 Wilson, Duncton, Chang, Lee Luo, Georgiadis, Pellicena, Deacon, Gao and Das. This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.-
dc.subject.otherfragment-based drug discovery (FBDD)-
dc.subject.otherstructure-based drug discovery (SBDD)-
dc.subject.otherX-ray crystallography-
dc.subject.othercancer therapeutics-
dc.subject.otherDNA damage response (DDR)-
dc.subject.otherpolymerases-
dc.subject.otherPol eta-
dc.subject.otherPOLH-
dc.titleEarly Drug Discovery and Development of Novel Cancer Therapeutics Targeting DNA Polymerase Eta (POLH)-
dc.typeJournal Contribution-
dc.identifier.volume11-
local.format.pages8-
local.bibliographicCitation.jcatA1-
dc.description.notesDas, D (corresponding author), XPose Therapeutics Inc, San Carlos, CA USA.-
dc.description.notesinfo@xposetx.com-
local.publisher.placeAVENUE DU TRIBUNAL FEDERAL 34, LAUSANNE, CH-1015, SWITZERLAND-
local.type.refereedRefereed-
local.type.specifiedArticle-
local.bibliographicCitation.artnr778925-
dc.identifier.doi10.3389/fonc.2021.778925-
dc.identifier.pmid34900730-
dc.identifier.isiWOS:000738779600001-
local.provider.typewosris-
local.description.affiliation[Wilson, David M.; Georgiadis, Taxiarchis M.; Pellicena, Patricia; Deacon, Ashley M.; Das, Debanu] XPose Therapeutics Inc, San Carlos, CA USA.-
local.description.affiliation[Wilson, David M.] Hasselt Univ, Biomed Res Inst, Diepenbeek, Belgium.-
local.description.affiliation[Chang, Caleb; Lee Luo, Christie; Gao, Yang] Rice Univ, Dept BioSci, Houston, TX USA.-
local.uhasselt.internationalyes-
item.fullcitationWILSON, David; Duncton, Matthew A. J.; Chang, Caleb; Lee Luo, Christie; Georgiadis, Taxiarchis M.; Pellicena, Patricia; Deacon, Ashley M.; Gao, Yang & Das, Debanu (2021) Early Drug Discovery and Development of Novel Cancer Therapeutics Targeting DNA Polymerase Eta (POLH). In: Frontiers in Oncology, 11 (Art N° 778925).-
item.validationecoom 2023-
item.accessRightsOpen Access-
item.fulltextWith Fulltext-
item.contributorWILSON, David-
item.contributorDuncton, Matthew A. J.-
item.contributorChang, Caleb-
item.contributorLee Luo, Christie-
item.contributorGeorgiadis, Taxiarchis M.-
item.contributorPellicena, Patricia-
item.contributorDeacon, Ashley M.-
item.contributorGao, Yang-
item.contributorDas, Debanu-
crisitem.journal.issn2234-943X-
crisitem.journal.eissn2234-943X-
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