Lonidamine and domperidone inhibit expansion of transformed cell areas by modulating motility of surrounding nontransformed cells

Megumi Aoyama; Kosuke Ishikawa; Shuntaro Nemoto; Hiroyuki Hirano; Nobumoto Watanabe; Hiroyuki Osada; Shinya Watanabe; Kentaro Semba

doi:10.1016/j.jbc.2022.102635

Lonidamine and domperidone inhibit expansion of transformed cell areas by modulating motility of surrounding nontransformed cells

Megumi Aoyama^*, Kosuke Ishikawa, Shuntaro Nemoto, Hiroyuki Hirano, Nobumoto Watanabe, Hiroyuki Osada, Shinya Watanabe, Kentaro Semba

^*この研究の対応する著者

先進理工学部

研究成果: Article › 査読

抄録

Cancer cells intrinsically proliferate in an autonomous manner; however, the expansion of cancer cell areas in a tissue is known to be regulated by surrounding nontransformed cells. Whether these nontransformed cells can be targeted to control the spread of cancer cells is not understood. In this study, we established a system to evaluate the cancer-inhibitory activity of surrounding nontransformed cells and screened chemical compounds that could induce this activity. Our findings revealed that lonidamine (LND) and domperidone (DPD) inhibited expansion of oncogenic foci of KRASG12D-expressing transformed cells, whereas they did not inhibit the proliferation of monocultured KRASG12D-expressing cells. Live imaging revealed that LND and DPD suppressed the movement of nontransformed cells away from the attaching cancer cells. Moreover, we determined that LND and DPD promoted stress fiber formation, and the dominant-negative mutant of a small GTPase RhoA relieved the suppression of focus expansion, suggesting that RhoA-mediated stress fiber formation is involved in the inhibition of the movement of nontransformed cells and focus expansion. In conclusion, we suggest that elucidation of the mechanism of action of LND and DPD may lead to the development of a new type of drug that could induce the anticancer activity of surrounding nontransformed cells.

本文言語	English
論文番号	102635
ジャーナル	Journal of Biological Chemistry
巻	298
号	12
DOI	https://doi.org/10.1016/j.jbc.2022.102635
出版ステータス	Published - 2022 12月

ASJC Scopus subject areas

生化学
分子生物学
細胞生物学

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10.1016/j.jbc.2022.102635

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@article{9d45a17973894b2692a7f46f37756809,

title = "Lonidamine and domperidone inhibit expansion of transformed cell areas by modulating motility of surrounding nontransformed cells",

abstract = "Cancer cells intrinsically proliferate in an autonomous manner; however, the expansion of cancer cell areas in a tissue is known to be regulated by surrounding nontransformed cells. Whether these nontransformed cells can be targeted to control the spread of cancer cells is not understood. In this study, we established a system to evaluate the cancer-inhibitory activity of surrounding nontransformed cells and screened chemical compounds that could induce this activity. Our findings revealed that lonidamine (LND) and domperidone (DPD) inhibited expansion of oncogenic foci of KRASG12D-expressing transformed cells, whereas they did not inhibit the proliferation of monocultured KRASG12D-expressing cells. Live imaging revealed that LND and DPD suppressed the movement of nontransformed cells away from the attaching cancer cells. Moreover, we determined that LND and DPD promoted stress fiber formation, and the dominant-negative mutant of a small GTPase RhoA relieved the suppression of focus expansion, suggesting that RhoA-mediated stress fiber formation is involved in the inhibition of the movement of nontransformed cells and focus expansion. In conclusion, we suggest that elucidation of the mechanism of action of LND and DPD may lead to the development of a new type of drug that could induce the anticancer activity of surrounding nontransformed cells.",

keywords = "anticancer drugs, cell motility, domperidone, drug screening, epithelial cells, lonidamine, oncogene, proliferation",

author = "Megumi Aoyama and Kosuke Ishikawa and Shuntaro Nemoto and Hiroyuki Hirano and Nobumoto Watanabe and Hiroyuki Osada and Shinya Watanabe and Kentaro Semba",

note = "Funding Information: This research was supported by AMED under Grant Number JP21lm0203004 (K. S. and N. W.), Japan Society for the Promotion of Science KAKENHI Grant Number 21J14495 , Grant-in-Aid for JSPS Fellows (M. A.) and Grant Number 21K19418 , Grant-in-Aid for Challenging Research (Exploratory) (K. S.. and N W.) and in part by translational research program from Fukushima Prefecture (K. I., S. W., ,and K. S.). Funding Information: We would like to thank Enago ( www.enago.jp ) for the English language review. We appreciate to Dr Fujimoto (Japan Biological informatics Consortium (JBiC), Tokyo, Japan) and laboratory members for valuable discussion. We also thank Screening Committee of Anticancer Drugs supported by Grant-in-Aid for Scientific Research on Innovative Areas, Scientific Support Programs for Cancer Research, from The Ministry of Education, Culture, Sports, Science and Technology, Japan ( http://scads.jfcr.or.jp/kit/kit.html ) for giving us SCADS Inhibitor Kit. Funding Information: We would like to thank Enago (www.enago.jp) for the English language review. We appreciate to Dr Fujimoto (Japan Biological informatics Consortium (JBiC), Tokyo, Japan) and laboratory members for valuable discussion. We also thank Screening Committee of Anticancer Drugs supported by Grant-in-Aid for Scientific Research on Innovative Areas, Scientific Support Programs for Cancer Research, from The Ministry of Education, Culture, Sports, Science and Technology, Japan (http://scads.jfcr.or.jp/kit/kit.html) for giving us SCADS Inhibitor Kit. M. A. and K. S. conceptualization; M. A. K. I. S. N. and K. S. methodology; M. A. software; M. A. validation; M. A. formal analysis; M. A. and S. N. investigation; H. H. N. W. H. O. and S. W. resources; M. A. data curation; M. A. K. I. and K. S. writing–original draft; M. A. N. W. H. O. and K. S. writing–review & editing; M. A. visualization; K. S. supervision; K. S. project administration; M. A. N. W. S. W. and K. S. funding acquisition. This research was supported by AMED under Grant Number JP21lm0203004 (K. S. and N. W.), Japan Society for the Promotion of Science KAKENHI Grant Number 21J14495, Grant-in-Aid for JSPS Fellows (M. A.) and Grant Number 21K19418, Grant-in-Aid for Challenging Research (Exploratory) (K. S. and N W.) and in part by translational research program from Fukushima Prefecture (K. I. S. W. and K. S.). Publisher Copyright: {\textcopyright} 2022 The Authors",

year = "2022",

month = dec,

doi = "10.1016/j.jbc.2022.102635",

language = "English",

volume = "298",

journal = "Journal of Biological Chemistry",

issn = "0021-9258",

publisher = "American Society for Biochemistry and Molecular Biology Inc.",

number = "12",

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TY - JOUR

T1 - Lonidamine and domperidone inhibit expansion of transformed cell areas by modulating motility of surrounding nontransformed cells

AU - Aoyama, Megumi

AU - Ishikawa, Kosuke

AU - Nemoto, Shuntaro

AU - Hirano, Hiroyuki

AU - Watanabe, Nobumoto

AU - Osada, Hiroyuki

AU - Watanabe, Shinya

AU - Semba, Kentaro

N1 - Funding Information: This research was supported by AMED under Grant Number JP21lm0203004 (K. S. and N. W.), Japan Society for the Promotion of Science KAKENHI Grant Number 21J14495 , Grant-in-Aid for JSPS Fellows (M. A.) and Grant Number 21K19418 , Grant-in-Aid for Challenging Research (Exploratory) (K. S.. and N W.) and in part by translational research program from Fukushima Prefecture (K. I., S. W., ,and K. S.). Funding Information: We would like to thank Enago ( www.enago.jp ) for the English language review. We appreciate to Dr Fujimoto (Japan Biological informatics Consortium (JBiC), Tokyo, Japan) and laboratory members for valuable discussion. We also thank Screening Committee of Anticancer Drugs supported by Grant-in-Aid for Scientific Research on Innovative Areas, Scientific Support Programs for Cancer Research, from The Ministry of Education, Culture, Sports, Science and Technology, Japan ( http://scads.jfcr.or.jp/kit/kit.html ) for giving us SCADS Inhibitor Kit. Funding Information: We would like to thank Enago (www.enago.jp) for the English language review. We appreciate to Dr Fujimoto (Japan Biological informatics Consortium (JBiC), Tokyo, Japan) and laboratory members for valuable discussion. We also thank Screening Committee of Anticancer Drugs supported by Grant-in-Aid for Scientific Research on Innovative Areas, Scientific Support Programs for Cancer Research, from The Ministry of Education, Culture, Sports, Science and Technology, Japan (http://scads.jfcr.or.jp/kit/kit.html) for giving us SCADS Inhibitor Kit. M. A. and K. S. conceptualization; M. A. K. I. S. N. and K. S. methodology; M. A. software; M. A. validation; M. A. formal analysis; M. A. and S. N. investigation; H. H. N. W. H. O. and S. W. resources; M. A. data curation; M. A. K. I. and K. S. writing–original draft; M. A. N. W. H. O. and K. S. writing–review & editing; M. A. visualization; K. S. supervision; K. S. project administration; M. A. N. W. S. W. and K. S. funding acquisition. This research was supported by AMED under Grant Number JP21lm0203004 (K. S. and N. W.), Japan Society for the Promotion of Science KAKENHI Grant Number 21J14495, Grant-in-Aid for JSPS Fellows (M. A.) and Grant Number 21K19418, Grant-in-Aid for Challenging Research (Exploratory) (K. S. and N W.) and in part by translational research program from Fukushima Prefecture (K. I. S. W. and K. S.). Publisher Copyright: © 2022 The Authors

PY - 2022/12

Y1 - 2022/12

N2 - Cancer cells intrinsically proliferate in an autonomous manner; however, the expansion of cancer cell areas in a tissue is known to be regulated by surrounding nontransformed cells. Whether these nontransformed cells can be targeted to control the spread of cancer cells is not understood. In this study, we established a system to evaluate the cancer-inhibitory activity of surrounding nontransformed cells and screened chemical compounds that could induce this activity. Our findings revealed that lonidamine (LND) and domperidone (DPD) inhibited expansion of oncogenic foci of KRASG12D-expressing transformed cells, whereas they did not inhibit the proliferation of monocultured KRASG12D-expressing cells. Live imaging revealed that LND and DPD suppressed the movement of nontransformed cells away from the attaching cancer cells. Moreover, we determined that LND and DPD promoted stress fiber formation, and the dominant-negative mutant of a small GTPase RhoA relieved the suppression of focus expansion, suggesting that RhoA-mediated stress fiber formation is involved in the inhibition of the movement of nontransformed cells and focus expansion. In conclusion, we suggest that elucidation of the mechanism of action of LND and DPD may lead to the development of a new type of drug that could induce the anticancer activity of surrounding nontransformed cells.

AB - Cancer cells intrinsically proliferate in an autonomous manner; however, the expansion of cancer cell areas in a tissue is known to be regulated by surrounding nontransformed cells. Whether these nontransformed cells can be targeted to control the spread of cancer cells is not understood. In this study, we established a system to evaluate the cancer-inhibitory activity of surrounding nontransformed cells and screened chemical compounds that could induce this activity. Our findings revealed that lonidamine (LND) and domperidone (DPD) inhibited expansion of oncogenic foci of KRASG12D-expressing transformed cells, whereas they did not inhibit the proliferation of monocultured KRASG12D-expressing cells. Live imaging revealed that LND and DPD suppressed the movement of nontransformed cells away from the attaching cancer cells. Moreover, we determined that LND and DPD promoted stress fiber formation, and the dominant-negative mutant of a small GTPase RhoA relieved the suppression of focus expansion, suggesting that RhoA-mediated stress fiber formation is involved in the inhibition of the movement of nontransformed cells and focus expansion. In conclusion, we suggest that elucidation of the mechanism of action of LND and DPD may lead to the development of a new type of drug that could induce the anticancer activity of surrounding nontransformed cells.

KW - anticancer drugs

KW - cell motility

KW - domperidone

KW - drug screening

KW - epithelial cells

KW - lonidamine

KW - oncogene

KW - proliferation

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