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том 14 издание 1 номер публикации 92

FL118, a novel camptothecin derivative, is insensitive to ABCG2 expression and shows improved efficacy in comparison with irinotecan in colon and lung cancer models with ABCG2-induced resistance

David Westover 1
Xiang Ling 1, 2
Hong Lam 1
Jacob Welch 1
Chunyang Jin 3
Céline Gongora 4
Maguy Del Rio 4
Mansukh Wani 3
Fengzhi Li 1
Тип публикацииJournal Article
Дата публикации2015-04-28
scimago Q1
wos Q1
БС1
SJR9.263
CiteScore47.4
Impact factor33.9
ISSN14764598
Cancer Research
Oncology
Molecular Medicine
Краткое описание
Irinotecan is a camptothecin analogue currently used in clinical practice to treat advanced colorectal cancer. However, acquired resistance mediated by the drug efflux pump ABCG2 is a recognized problem. We reported on a novel camptothecin analogue, FL118, which shows anticancer activity superior to irinotecan. In this study, we sought to investigate the potency of FL118 versus irinotecan or its active metabolite, SN-38, in both in vitro and in vivo models of human cancer with high ABCG2 activity. We also sought to assess the potency and ABCG2 affinity of several FL118 analogues with B-ring substitutions. Colon and lung cancer cells with and without ABCG2 overexpression were treated with FL118 in the presence and absence of Ko143, an ABCG2-selective inhibitor, or alternatively by genetically modulating ABCG2 expression. Using two distinct in vivo human tumor animal models, we further assessed whether FL118 could extend time to progression in comparison with irinotecan. Lastly, we investigated a series of FL118 analogues with B-ring substitutions for ABCG2 sensitivity. Both pharmacological inhibition and genetic modulation of ABCG2 demonstrated that, in contrast to SN-38, FL118 was able to bypass ABCG2-mediated drug resistance. FL118 also extended time to progression in both in vivo models by more than 50% compared with irinotecan. Lastly, we observed that FL118 analogues with polar substitutions had higher affinity for ABCG2, suggesting that the nonpolar nature of FL118 plays a role in bypassing ABCG2-mediated resistance. Our results suggest that in contrast to SN-38 and topotecan, FL118 is a poor substrate for ABCG2 and can effectively overcome ABCG2-mediated drug resistance. Our findings expand the uniqueness of FL118 and support continued development of FL118 as an attractive therapeutic option for patients with drug-refractory cancers resulting from high expression of ABCG2.
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Westover D. et al. FL118, a novel camptothecin derivative, is insensitive to ABCG2 expression and shows improved efficacy in comparison with irinotecan in colon and lung cancer models with ABCG2-induced resistance // Molecular Cancer. 2015. Vol. 14. No. 1. 92
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Westover D., Ling X., Lam H., Welch J., Jin C., Gongora C., Del Rio M., Wani M., Li F. FL118, a novel camptothecin derivative, is insensitive to ABCG2 expression and shows improved efficacy in comparison with irinotecan in colon and lung cancer models with ABCG2-induced resistance // Molecular Cancer. 2015. Vol. 14. No. 1. 92
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TY - JOUR
DO - 10.1186/s12943-015-0362-9
UR - https://doi.org/10.1186/s12943-015-0362-9
TI - FL118, a novel camptothecin derivative, is insensitive to ABCG2 expression and shows improved efficacy in comparison with irinotecan in colon and lung cancer models with ABCG2-induced resistance
T2 - Molecular Cancer
AU - Westover, David
AU - Ling, Xiang
AU - Lam, Hong
AU - Welch, Jacob
AU - Jin, Chunyang
AU - Gongora, Céline
AU - Del Rio, Maguy
AU - Wani, Mansukh
AU - Li, Fengzhi
PY - 2015
DA - 2015/04/28
PB - Springer Nature
IS - 1
VL - 14
PMID - 25928015
SN - 1476-4598
ER -
BibTex
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BibTex (до 50 авторов) Скопировать
@article{2015_Westover,
author = {David Westover and Xiang Ling and Hong Lam and Jacob Welch and Chunyang Jin and Céline Gongora and Maguy Del Rio and Mansukh Wani and Fengzhi Li},
title = {FL118, a novel camptothecin derivative, is insensitive to ABCG2 expression and shows improved efficacy in comparison with irinotecan in colon and lung cancer models with ABCG2-induced resistance},
journal = {Molecular Cancer},
year = {2015},
volume = {14},
publisher = {Springer Nature},
month = {apr},
url = {https://doi.org/10.1186/s12943-015-0362-9},
number = {1},
pages = {92},
doi = {10.1186/s12943-015-0362-9}
}