Publication: Functional genomics reveals an off-target dependency of drug synergy in gastric cancer therapy
| dc.contributor.coauthor | Honeywell, Megan E. | |
| dc.contributor.coauthor | Lee, Michael J. | |
| dc.contributor.coauthor | Hemann, Michael T. | |
| dc.contributor.department | School of Medicine | |
| dc.contributor.department | Graduate School of Health Sciences | |
| dc.contributor.facultymember | Yes | |
| dc.contributor.kuauthor | Leylek, Özen | |
| dc.contributor.kuauthor | Özcan, Gülnihal | |
| dc.contributor.schoolcollegeinstitute | GRADUATE SCHOOL OF HEALTH SCIENCES | |
| dc.contributor.schoolcollegeinstitute | SCHOOL OF MEDICINE | |
| dc.date.accessioned | 2025-01-19T10:32:54Z | |
| dc.date.issued | 2023 | |
| dc.description.abstract | The rational combination of anticancer agents is critical to improving patient outcomes in cancer. Nonetheless, most combination regimens in the clinic result from empirical methodologies disregarding insight into the mechanism of action and missing the opportunity to improve therapy outcomes incrementally. Deciphering the genetic dependencies and vulnerabilities responsible for synergistic interactions is crucial for rationally developing effective anticancer drug combinations. Hence, we screened pairwise pharmacological interactions between molecular-targeted agents and conventional chemotherapeutics and examined the genome-scale genetic dependencies in gastric adenocarcinoma cell models. Since this type of cancer is mainly chemoresistant and incurable, clinical situations demand effective combination strategies. Our pairwise combination screen revealed SN38/erlotinib as the drug pair with the most robust synergism. Genome-wide CRISPR screening and a shRNA-based signature assay indicated that the genetic dependency/vulnerability signature of SN38/erlotinib is the same as SN38 alone. Additional investigation revealed that the enhanced cell death with improved death kinetics caused by the SN38/erlotinib combination is surprisingly due to erlotinib's off-target effect that inhibits ABCG2 but not its on-target effect on EGFR. Our results confirm that a genetic dependency signature different from the single-drug application may not be necessary for the synergistic interaction of molecular-targeted agents with conventional chemotherapeutics in gastric adenocarcinoma. The findings also demonstrated the efficacy of functional genomics approaches in unveiling biologically validated mechanisms of pharmacological interactions. | eng |
| dc.description.fulltext | No | |
| dc.description.harvestedfrom | Manual | |
| dc.description.indexedby | PubMed | |
| dc.description.openaccess | N/A | |
| dc.description.peerreviewstatus | N/A | |
| dc.description.publisherscope | International | |
| dc.description.readpublish | N/A | |
| dc.description.sponsoredbyTubitakEu | TÜBİTAK | |
| dc.description.sponsorship | The authors gratefully acknowledge Hakan S. Orer and Mehmet Gonen from Koç University for their valuable insights as advisors in the project with grant number 117Z460-TUBITAK and the use of the services and facilities of the Koç University Research Center for Translational Medicine (KUTTAM), funded by the Presidency of Turkey, Head of Strategy and Budget. We also gratefully acknowledge Peter M. Bruno for his helpful comments on the RNAi-based signature assay, Tugba Bagci Onder for supportive insights, and Alisan Kayabolen, Tolga Sever, and James Ham for helpful discussions. We thank all members of Lee and Hemann Labs for their valuable feedback. O.L. gratefully acknowledges the support of Ph.D. Dissertation Research Grant sponsored by the U.S. Department of State and the Turkish Fulbright Commission. The contents presented in the manuscript are solely the responsibility of the authors and do not necessarily represent the official views of the Fulbright Program, the U.S. Department of State, and the Turkish Fulbright Commission. | eng |
| dc.description.studentonlypublication | No | |
| dc.description.studentpublication | Yes | |
| dc.description.version | N/A | |
| dc.identifier.doi | 10.1101/2023.10.07.561351 | |
| dc.identifier.embargo | N/A | |
| dc.identifier.grantno | 117Z460 | |
| dc.identifier.pubmed | 37873383 | |
| dc.identifier.quartile | N/A | |
| dc.identifier.uri | https://doi.org/10.1101/2023.10.07.561351 | |
| dc.identifier.uri | https://hdl.handle.net/20.500.14288/26500 | |
| dc.keywords | Functional genomics | |
| dc.keywords | Combination therapy | |
| dc.keywords | Synergism | |
| dc.keywords | Gastric adenocarcinoma | |
| dc.keywords | Genetic dependency | |
| dc.language.iso | eng | |
| dc.publisher | Cold Spring Harbor Laboratory | |
| dc.relation.affiliation | Koç University | |
| dc.relation.collection | Koç University Institutional Repository | |
| dc.relation.ispartof | bioRxiv | |
| dc.relation.openaccess | N/A | |
| dc.rights | N/A | |
| dc.subject | Functional genomics | |
| dc.subject | Combination therapy | |
| dc.subject | Drug synergism | |
| dc.subject | Gastric adenocarcinoma | |
| dc.subject | Genetic dependency | |
| dc.subject | CRISPR screening | |
| dc.subject | Erlotinib | |
| dc.title | Functional genomics reveals an off-target dependency of drug synergy in gastric cancer therapy | |
| dc.type | Other | |
| dspace.entity.type | Publication | |
| local.contributor.kuauthor | Leylek, Özen | |
| local.contributor.kuauthor | Özcan, Gülnihal | |
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