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

Westover, David; Ling, Xiang; Lam, Hong; Welch, Jacob; Jin, Chunyang; Gongora, Céline; Rio, Maguy Del; Wani, Mansukh C.; Li, Fengzhi

doi:10.1186/s12943-015-0362-9

Cited by 52 publications

(36 citation statements)

References 38 publications

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“…Third, irinotecan, SN-38 and topotecan are the substrates of efflux pump proteins ABCG2/BCRP [83][84][85][86][87] and Pgp/MDR1 [88][89][90][91][92]. In contrast, FL118 is not a substrate for them, and can bypass their resistance [78,93].…”

Section: Fl118mentioning

confidence: 99%

Cancer therapeutics using survivin BIRC5 as a target: what can we do after over two decades of study?

Aljahdali

Ling

2019

J Exp Clin Cancer Res

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187

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Survivin (also named BIRC5) is a well-known cancer therapeutic target. Since its discovery more than two decades ago, the use of survivin as a target for cancer therapeutics has remained a central goal of survivin studies in the cancer field. Many studies have provided intriguing insight into survivin's functional role in cancers, thus providing promise for survivin as a cancer therapeutic target. Despite this, moving survivin-targeting agents into and through the clinic remains a challenge. In order to address this challenge, we may need to rethink current strategies in order to develop a new mindset for targeting survivin. In this Review, we will first summarize the current survivin mechanistic studies, and then review the status of survivin cancer therapeutics, which is classified into five categories: (i) survivin-partner protein interaction inhibitors, (ii) survivin homodimerization inhibitors, (iii) survivin gene transcription inhibitors, (iv) survivin mRNA inhibitors and (v) survivin immunotherapy. We will then provide our opinions on cancer therapeutics using survivin as a target, with the goal of stimulating discussion that might facilitate translational research for discovering improved strategies and/or more effective anticancer agents that target survivin for cancer therapy.

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Section: Fl118mentioning

confidence: 99%

Cancer therapeutics using survivin BIRC5 as a target: what can we do after over two decades of study?

Aljahdali

Ling

2019

J Exp Clin Cancer Res

Self Cite

187

171

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“…FL118, a novel camptothecin analogue, was first discovered in high-throughput screening for survivin inhibitors in a previous study by the current authors (16). FL118 was found to display potent anticancer activity against several different types of cancer both in vitro and in vivo (17)(18)(19)(20). Moreover, its antitumor activity was superior to that of several camptothecin analogues, such as irinotecan and topotecan, that have been approved by the FDA for cancer treatment (21,22).…”

Section: Discussionmentioning

confidence: 99%

“…Moreover, its antitumor activity was superior to that of several camptothecin analogues, such as irinotecan and topotecan, that have been approved by the FDA for cancer treatment (21,22). FL118 is rapidly cleared from circulation and it effectively accumulates in tumors with a long half-life of elimination, suggesting its potential for use in cancer therapy (18,20). However, the effects of FL118 on breast cancer invasion and metastasis have not been reported.…”

Section: Discussionmentioning

confidence: 99%

FL118, a novel camptothecin analogue, suppressed migration and invasion of human breast cancer cells by inhibiting epithelial-mesenchymal transition <i>via</i> the Wnt/β-catenin signaling pathway

Yang

Jiang

et al. 2018

BST

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“…Irinotecan is also used as a first-line therapy for metastatic colon cancer in combination with other antitumor agents. Unfortunately, resistance to irinotecan has been observed in the clinic (30). Thus, it is clear resistance to chemotherapeutic agents for colon cancers is a great challenge in clinical use.…”

Section: Discussionmentioning

confidence: 99%

Gap junction composed of connexin43 modulates 5-fluorouracil, oxaliplatin and irinotecan resistance on colorectal cancers

Zou

Chen

et al. 2016

Molecular Medicine Reports

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Chemotherapy is one of the most commonly used therapeutic strategies for metastatic colon cancer. However, the development of resistance to chemotherapeutic agents limits their application in clinical use. The underlying mechanisms of this resistance development require further elucidation. The current study investigated the effects of connexin43 (Cx43) gap junctions on 5‑fluorouracil (5‑FU), oxaliplatin and irinotecan in colon cancer cells. Three different methods were used to manipulate Cx43 gap junction function: i) Cell culture at different densities; ii) pretreatment with a Cx43 specific inhibitor or enhancer; and iii) Cx43 gene knock‑down. Results indicated that the cell toxicity of 5‑FU, oxaliplatin and irinotecan was cell density‑dependent, which was mediated by gap junctions. Downregulation of Cx43 gap junction functioning attenuated 5‑FU, oxaliplatin and irinotecan toxicity in colon cancer cells, which was increased in cells treated with a Cx43 gap junction function enhancer. Thus, the results of the present study suggest that resistance to 5‑FU, oxaliplatin and irinotecan in colon cancer cells was relative to Cx43 expression loss as cancer developed, which may indicate a novel basis for therapeutic strategy development to combat drug resistance in numerous cell types, in addition to colon cancer cells.

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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

Cited by 52 publications

References 38 publications

Cancer therapeutics using survivin BIRC5 as a target: what can we do after over two decades of study?

Cancer therapeutics using survivin BIRC5 as a target: what can we do after over two decades of study?

FL118, a novel camptothecin analogue, suppressed migration and invasion of human breast cancer cells by inhibiting epithelial-mesenchymal transition <i>via</i> the Wnt/β-catenin signaling pathway

Gap junction composed of connexin43 modulates 5-fluorouracil, oxaliplatin and irinotecan resistance on colorectal cancers

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