Cancer cells undergoing epigenetic transition show short-term resistance and are transformed into cells with medium-term resistance by drug treatment

Shiv Poojan; Seung Hyun Bae; Jae Woong Min; Eun Young Lee; Yura Song; Hee Yeon Kim; Hye Won Sim; Eun Kyung Kang; Young Ho Kim; Hae Ock Lee; Yourae Hong; Woong Yang Park; Hyonchol Jang; Kyeong Man Hong

doi:10.1038/s12276-020-0464-3

Cancer cells undergoing epigenetic transition show short-term resistance and are transformed into cells with medium-term resistance by drug treatment

Shiv Poojan, Seung Hyun Bae, Jae Woong Min, Eun Young Lee, Yura Song, Hee Yeon Kim, Hye Won Sim, Eun Kyung Kang, Young Ho Kim, Hae Ock Lee, Yourae Hong, Woong Yang Park, Hyonchol Jang, Kyeong Man Hong

Department of Microbiology

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

12 Scopus citations

Abstract

To elucidate the epigenetic mechanisms of drug resistance, epigenetically reprogrammed H460 cancer cells (R-H460) were established by the transient introduction of reprogramming factors. Then, the R-H460 cells were induced to differentiate by the withdrawal of stem cell media for various durations, which resulted in differentiated R-H460 cells (dR-H460). Notably, dR-H460 cells differentiated for 13 days (13dR-H460 cells) formed a significantly greater number of colonies showing drug resistance to both cisplatin and paclitaxel, whereas the dR-H460 cells differentiated for 40 days (40dR-H460 cells) lost drug resistance; this suggests that 13dR-cancer cells present short-term resistance (less than a month). Similarly, increased drug resistance to both cisplatin and paclitaxel was observed in another R-cancer cell model prepared from N87 cells. The resistant phenotype of the cisplatin-resistant (CR) colonies obtained through cisplatin treatment was maintained for 2–3 months after drug treatment, suggesting that drug treatment transforms cells with short-term resistance into cells with medium-term resistance. In single-cell analyses, heterogeneity was not found to increase in 13dR-H460 cells, suggesting that cancer cells with short-term resistance, rather than heterogeneous cells, may confer epigenetically driven drug resistance in our reprogrammed cancer model. The epigenetically driven short-term and medium-term drug resistance mechanisms could provide new cancer-fighting strategies involving the control of cancer cells during epigenetic transition.

Original language	English
Pages (from-to)	1102-1115
Number of pages	14
Journal	Experimental and Molecular Medicine
Volume	52
Issue number	7
DOIs	https://doi.org/10.1038/s12276-020-0464-3
State	Published - 1 Jul 2020

Bibliographical note

Funding Information:
The bioinformatics analysis was supported by Dr. Jong-Kwang Kim at the Research Core Center of the National Cancer Center (NCC), Korea. Cell authentication was performed by Dr. Jeong-Ah Hwang at the Research Core Center of the NCC, Korea. This study was funded by grants from the National Cancer Center, Korea (1910150 to K.-M.H., and 2010272 to H.J.), and the National Research Foundation of Korea (NRF-2015R1A2A2A04007432 to K.-M.H.).

Publisher Copyright:
© 2020, The Author(s).

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Poojan, S., Bae, S. H., Min, J. W., Lee, E. Y., Song, Y., Kim, H. Y., Sim, H. W., Kang, E. K., Kim, Y. H., Lee, H. O., Hong, Y., Park, W. Y., Jang, H., & Hong, K. M. (2020). Cancer cells undergoing epigenetic transition show short-term resistance and are transformed into cells with medium-term resistance by drug treatment. Experimental and Molecular Medicine, 52(7), 1102-1115. https://doi.org/10.1038/s12276-020-0464-3

@article{457d349e79924601b29aa78145ae885b,

title = "Cancer cells undergoing epigenetic transition show short-term resistance and are transformed into cells with medium-term resistance by drug treatment",

abstract = "To elucidate the epigenetic mechanisms of drug resistance, epigenetically reprogrammed H460 cancer cells (R-H460) were established by the transient introduction of reprogramming factors. Then, the R-H460 cells were induced to differentiate by the withdrawal of stem cell media for various durations, which resulted in differentiated R-H460 cells (dR-H460). Notably, dR-H460 cells differentiated for 13 days (13dR-H460 cells) formed a significantly greater number of colonies showing drug resistance to both cisplatin and paclitaxel, whereas the dR-H460 cells differentiated for 40 days (40dR-H460 cells) lost drug resistance; this suggests that 13dR-cancer cells present short-term resistance (less than a month). Similarly, increased drug resistance to both cisplatin and paclitaxel was observed in another R-cancer cell model prepared from N87 cells. The resistant phenotype of the cisplatin-resistant (CR) colonies obtained through cisplatin treatment was maintained for 2–3 months after drug treatment, suggesting that drug treatment transforms cells with short-term resistance into cells with medium-term resistance. In single-cell analyses, heterogeneity was not found to increase in 13dR-H460 cells, suggesting that cancer cells with short-term resistance, rather than heterogeneous cells, may confer epigenetically driven drug resistance in our reprogrammed cancer model. The epigenetically driven short-term and medium-term drug resistance mechanisms could provide new cancer-fighting strategies involving the control of cancer cells during epigenetic transition.",

author = "Shiv Poojan and Bae, \{Seung Hyun\} and Min, \{Jae Woong\} and Lee, \{Eun Young\} and Yura Song and Kim, \{Hee Yeon\} and Sim, \{Hye Won\} and Kang, \{Eun Kyung\} and Kim, \{Young Ho\} and Lee, \{Hae Ock\} and Yourae Hong and Park, \{Woong Yang\} and Hyonchol Jang and Hong, \{Kyeong Man\}",

note = "Funding Information: The bioinformatics analysis was supported by Dr. Jong-Kwang Kim at the Research Core Center of the National Cancer Center (NCC), Korea. Cell authentication was performed by Dr. Jeong-Ah Hwang at the Research Core Center of the NCC, Korea. This study was funded by grants from the National Cancer Center, Korea (1910150 to K.-M.H., and 2010272 to H.J.), and the National Research Foundation of Korea (NRF-2015R1A2A2A04007432 to K.-M.H.). Publisher Copyright: {\textcopyright} 2020, The Author(s).",

year = "2020",

month = jul,

day = "1",

doi = "10.1038/s12276-020-0464-3",

language = "English",

volume = "52",

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Poojan, S, Bae, SH, Min, JW, Lee, EY, Song, Y, Kim, HY, Sim, HW, Kang, EK, Kim, YH, Lee, HO, Hong, Y, Park, WY, Jang, H & Hong, KM 2020, 'Cancer cells undergoing epigenetic transition show short-term resistance and are transformed into cells with medium-term resistance by drug treatment', Experimental and Molecular Medicine, vol. 52, no. 7, pp. 1102-1115. https://doi.org/10.1038/s12276-020-0464-3

TY - JOUR

T1 - Cancer cells undergoing epigenetic transition show short-term resistance and are transformed into cells with medium-term resistance by drug treatment

AU - Poojan, Shiv

AU - Bae, Seung Hyun

AU - Min, Jae Woong

AU - Lee, Eun Young

AU - Song, Yura

AU - Kim, Hee Yeon

AU - Sim, Hye Won

AU - Kang, Eun Kyung

AU - Kim, Young Ho

AU - Lee, Hae Ock

AU - Hong, Yourae

AU - Park, Woong Yang

AU - Jang, Hyonchol

AU - Hong, Kyeong Man

N1 - Funding Information: The bioinformatics analysis was supported by Dr. Jong-Kwang Kim at the Research Core Center of the National Cancer Center (NCC), Korea. Cell authentication was performed by Dr. Jeong-Ah Hwang at the Research Core Center of the NCC, Korea. This study was funded by grants from the National Cancer Center, Korea (1910150 to K.-M.H., and 2010272 to H.J.), and the National Research Foundation of Korea (NRF-2015R1A2A2A04007432 to K.-M.H.). Publisher Copyright: © 2020, The Author(s).

PY - 2020/7/1

Y1 - 2020/7/1

N2 - To elucidate the epigenetic mechanisms of drug resistance, epigenetically reprogrammed H460 cancer cells (R-H460) were established by the transient introduction of reprogramming factors. Then, the R-H460 cells were induced to differentiate by the withdrawal of stem cell media for various durations, which resulted in differentiated R-H460 cells (dR-H460). Notably, dR-H460 cells differentiated for 13 days (13dR-H460 cells) formed a significantly greater number of colonies showing drug resistance to both cisplatin and paclitaxel, whereas the dR-H460 cells differentiated for 40 days (40dR-H460 cells) lost drug resistance; this suggests that 13dR-cancer cells present short-term resistance (less than a month). Similarly, increased drug resistance to both cisplatin and paclitaxel was observed in another R-cancer cell model prepared from N87 cells. The resistant phenotype of the cisplatin-resistant (CR) colonies obtained through cisplatin treatment was maintained for 2–3 months after drug treatment, suggesting that drug treatment transforms cells with short-term resistance into cells with medium-term resistance. In single-cell analyses, heterogeneity was not found to increase in 13dR-H460 cells, suggesting that cancer cells with short-term resistance, rather than heterogeneous cells, may confer epigenetically driven drug resistance in our reprogrammed cancer model. The epigenetically driven short-term and medium-term drug resistance mechanisms could provide new cancer-fighting strategies involving the control of cancer cells during epigenetic transition.

AB - To elucidate the epigenetic mechanisms of drug resistance, epigenetically reprogrammed H460 cancer cells (R-H460) were established by the transient introduction of reprogramming factors. Then, the R-H460 cells were induced to differentiate by the withdrawal of stem cell media for various durations, which resulted in differentiated R-H460 cells (dR-H460). Notably, dR-H460 cells differentiated for 13 days (13dR-H460 cells) formed a significantly greater number of colonies showing drug resistance to both cisplatin and paclitaxel, whereas the dR-H460 cells differentiated for 40 days (40dR-H460 cells) lost drug resistance; this suggests that 13dR-cancer cells present short-term resistance (less than a month). Similarly, increased drug resistance to both cisplatin and paclitaxel was observed in another R-cancer cell model prepared from N87 cells. The resistant phenotype of the cisplatin-resistant (CR) colonies obtained through cisplatin treatment was maintained for 2–3 months after drug treatment, suggesting that drug treatment transforms cells with short-term resistance into cells with medium-term resistance. In single-cell analyses, heterogeneity was not found to increase in 13dR-H460 cells, suggesting that cancer cells with short-term resistance, rather than heterogeneous cells, may confer epigenetically driven drug resistance in our reprogrammed cancer model. The epigenetically driven short-term and medium-term drug resistance mechanisms could provide new cancer-fighting strategies involving the control of cancer cells during epigenetic transition.

UR - https://www.scopus.com/pages/publications/85087755559

U2 - 10.1038/s12276-020-0464-3

DO - 10.1038/s12276-020-0464-3

M3 - Article

C2 - 32661348

AN - SCOPUS:85087755559

SN - 1226-3613

VL - 52

SP - 1102

EP - 1115

JO - Experimental and Molecular Medicine

JF - Experimental and Molecular Medicine

IS - 7

ER -

Cancer cells undergoing epigenetic transition show short-term resistance and are transformed into cells with medium-term resistance by drug treatment

Abstract

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