Reducing Chemotherapy-Induced DNA Damage via nAChR-Mediated Redox Reprograming—A New Mechanism for SCLC Chemoresistance Boosted by Nicotine

Yuzhi Wang; Tengfei Bian; Lina Song; Yunhan Jiang; Zhiguang Huo; Ramzi G. Salloum; Graham W. Warren; Frederic J. Kaye; Naomi Fujioka; Lingtao Jin; Chengguo Xing

doi:10.3390/cancers14092272

Reducing Chemotherapy-Induced DNA Damage via nAChR-Mediated Redox Reprograming—A New Mechanism for SCLC Chemoresistance Boosted by Nicotine

Yuzhi Wang, Tengfei Bian, Lina Song, Yunhan Jiang, Zhiguang Huo, Ramzi G. Salloum, Graham W. Warren, Frederic J. Kaye, Naomi Fujioka, Lingtao Jin, Chengguo Xing

Medicine - Hematology, Oncology, Transplant

Research output: Contribution to journal › Article › peer-review

3 Scopus citations

Abstract

Up to 60% of patients with small cell lung cancer (SCLC) continue to smoke, which is associated with worse clinical outcomes. Platinum-based chemotherapies, in combination with topoisomerase inhibitors, are first-line therapies for SCLC, with rapid chemoresistance as a major barrier. We provided evidence in this study that nicotine and its major metabolite, cotinine, at physiologically relevant concentrations, reduced the efficacy of platinum-based chemotherapies and facilitated chemoresistance in SCLC cells. Mechanistically, nicotine or cotinine reduced chemotherapy-induced DNA damage by modulating cellular redox processes, with nAChRs as the upstream targets. Surprisingly, cisplatin treatment alone also increased the levels of nAChRs in SCLC cells, which served as a self-defense mechanism against platinum-based therapies. These discoveries were confirmed in long-term in vitro and in vivo studies. Collectively, our results depicted a novel and clinically important mechanism of chemoresistance in SCLC treatment: nicotine exposure significantly compromises the efficacy of platinum-based chemotherapies in SCLC treatment by reducing therapy-induced DNA damage and accelerating chemoresistance acquisition. The results also emphasized the urgent need for tobacco cessation and the control of NRT use for SCLC management.

Original language	English (US)
Article number	2272
Journal	Cancers
Volume	14
Issue number	9
DOIs	https://doi.org/10.3390/cancers14092272
State	Published - May 1 2022

Bibliographical note

Funding Information:
Funding: This research was funded by grants from the National Institute of Health (R01CA193286) and LCRF awarded to C.X., College of Pharmacy Frank Duckworth Endowment to C.X. Additionally: NIH/NCI R37 award CA249305 to L.J., DoD LCRP Career Development Award W81XWH2010309 to L.J.

Publisher Copyright:
© 2022 by the authors. Licensee MDPI, Basel, Switzerland.

Keywords

DNA damage
SCLC
chemoresistance
cotinine
nicotine
platinum-based therapy

PubMed: MeSH publication types

Journal Article

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title = "Reducing Chemotherapy-Induced DNA Damage via nAChR-Mediated Redox Reprograming—A New Mechanism for SCLC Chemoresistance Boosted by Nicotine",

abstract = "Up to 60% of patients with small cell lung cancer (SCLC) continue to smoke, which is associated with worse clinical outcomes. Platinum-based chemotherapies, in combination with topoisomerase inhibitors, are first-line therapies for SCLC, with rapid chemoresistance as a major barrier. We provided evidence in this study that nicotine and its major metabolite, cotinine, at physiologically relevant concentrations, reduced the efficacy of platinum-based chemotherapies and facilitated chemoresistance in SCLC cells. Mechanistically, nicotine or cotinine reduced chemotherapy-induced DNA damage by modulating cellular redox processes, with nAChRs as the upstream targets. Surprisingly, cisplatin treatment alone also increased the levels of nAChRs in SCLC cells, which served as a self-defense mechanism against platinum-based therapies. These discoveries were confirmed in long-term in vitro and in vivo studies. Collectively, our results depicted a novel and clinically important mechanism of chemoresistance in SCLC treatment: nicotine exposure significantly compromises the efficacy of platinum-based chemotherapies in SCLC treatment by reducing therapy-induced DNA damage and accelerating chemoresistance acquisition. The results also emphasized the urgent need for tobacco cessation and the control of NRT use for SCLC management.",

keywords = "DNA damage, SCLC, chemoresistance, cotinine, nicotine, platinum-based therapy",

author = "Yuzhi Wang and Tengfei Bian and Lina Song and Yunhan Jiang and Zhiguang Huo and Salloum, {Ramzi G.} and Warren, {Graham W.} and Kaye, {Frederic J.} and Naomi Fujioka and Lingtao Jin and Chengguo Xing",

note = "Funding Information: Funding: This research was funded by grants from the National Institute of Health (R01CA193286) and LCRF awarded to C.X., College of Pharmacy Frank Duckworth Endowment to C.X. Additionally: NIH/NCI R37 award CA249305 to L.J., DoD LCRP Career Development Award W81XWH2010309 to L.J. Publisher Copyright: {\textcopyright} 2022 by the authors. Licensee MDPI, Basel, Switzerland.",

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AU - Wang, Yuzhi

AU - Bian, Tengfei

AU - Song, Lina

AU - Jiang, Yunhan

AU - Huo, Zhiguang

AU - Salloum, Ramzi G.

AU - Warren, Graham W.

AU - Kaye, Frederic J.

AU - Fujioka, Naomi

AU - Jin, Lingtao

AU - Xing, Chengguo

N1 - Funding Information: Funding: This research was funded by grants from the National Institute of Health (R01CA193286) and LCRF awarded to C.X., College of Pharmacy Frank Duckworth Endowment to C.X. Additionally: NIH/NCI R37 award CA249305 to L.J., DoD LCRP Career Development Award W81XWH2010309 to L.J. Publisher Copyright: © 2022 by the authors. Licensee MDPI, Basel, Switzerland.

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N2 - Up to 60% of patients with small cell lung cancer (SCLC) continue to smoke, which is associated with worse clinical outcomes. Platinum-based chemotherapies, in combination with topoisomerase inhibitors, are first-line therapies for SCLC, with rapid chemoresistance as a major barrier. We provided evidence in this study that nicotine and its major metabolite, cotinine, at physiologically relevant concentrations, reduced the efficacy of platinum-based chemotherapies and facilitated chemoresistance in SCLC cells. Mechanistically, nicotine or cotinine reduced chemotherapy-induced DNA damage by modulating cellular redox processes, with nAChRs as the upstream targets. Surprisingly, cisplatin treatment alone also increased the levels of nAChRs in SCLC cells, which served as a self-defense mechanism against platinum-based therapies. These discoveries were confirmed in long-term in vitro and in vivo studies. Collectively, our results depicted a novel and clinically important mechanism of chemoresistance in SCLC treatment: nicotine exposure significantly compromises the efficacy of platinum-based chemotherapies in SCLC treatment by reducing therapy-induced DNA damage and accelerating chemoresistance acquisition. The results also emphasized the urgent need for tobacco cessation and the control of NRT use for SCLC management.

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Reducing Chemotherapy-Induced DNA Damage via nAChR-Mediated Redox Reprograming—A New Mechanism for SCLC Chemoresistance Boosted by Nicotine

Abstract

Bibliographical note

Keywords

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UN SDGs

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