High-throughput screen identifies disulfiram as a potential therapeutic for triple-negative breast cancer cells: Interaction with IQ motif-containing factors

Robinson, Tyler; Pai, Melody Y.; Liu, Jeff C.; Vizeacoumar, Frederick S.; Sun, Thomas; Egan, Sean E.; Datti, Alessandro; Huang, Jing; Zacksenhaus, Eldad

doi:10.4161/cc.26063

Cited by 44 publications

(27 citation statements)

References 87 publications

(82 reference statements)

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“…Mass spectrometry (MS) is then used to identify the proteins present in each band. This unbiased DARTS approach has been successfully utilized to identify novel protein targets for natural products and other bioactive small molecules; see (10) for a recent example identifying a novel protein target for disulfiram, an FDA-approved drug used to treat chronic alcoholism. Although this gel-based approach is the easiest to implement, more efficient gel-free proteomics approaches are also being used with DARTS to facilitate identification of the protected proteins (5, 11).…”

Section: Introductionmentioning

confidence: 99%

“…While DARTS has been successfully performed in an unbiased fashion as a discovery tool to identify unknown targets of natural products and drugs (see (9, 10, 12, 13) for some examples), it is also powerful as a means to screen or validate binding of compounds to proteins of interest. This targeted approach has been widely used, with recombinant and/or purified proteins using gel staining, endogenous proteins in lysates using western blotting, and epitope-tagged proteins expressed in cells or in vitro and detected with epitope-specific antibodies (9, 10, 14-19).…”

Section: Introductionmentioning

confidence: 99%

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Drug Affinity Responsive Target Stability (DARTS) for Small-Molecule Target Identification

Pai

Lomenick

Hwang

et al. 2014

Methods in Molecular Biology

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232

209

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Drug Affinity Responsive Target Stability (DARTS) is a relatively quick and straightforward approach to identify potential protein targets for small molecules. It relies on the protection against proteolysis conferred on the target protein by interaction with a small molecule. The greatest advantage of this method is being able to use the native small molecule without having to immobilize or modify it (e.g. by incorporation of biotin, fluorescent, radioisotope, or photo-affinity labels). Here we describe in detail the protocol for performing unbiased DARTS with complex protein lysate to identify potential binding targets of small molecules and for using DARTS-Western blotting to test, screen, or validate potential small molecule targets. Although the ideas have mainly been developed from studying molecules in areas of biology that are currently of interest to us and our collaborators, the general principles should be applicable to the analysis of all molecules in nature.

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Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Drug Affinity Responsive Target Stability (DARTS) for Small-Molecule Target Identification

Pai

Lomenick

Hwang

et al. 2014

Methods in Molecular Biology

Self Cite

232

209

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show abstract

“…Studies to evaluate the potency of disulfiram against certain types of cancer (12)(13)(14), Menkes disease (15), and HIV-1 infections are ongoing or have just been completed (16,17). Of additional interest to the medical community are its antinematode (18), antifungal (19), and, importantly, its antibacterial properties (11,(20)(21)(22)(23)(24).…”

mentioning

confidence: 99%

Disulfiram and Copper Ions Kill Mycobacterium tuberculosis in a Synergistic Manner

Dalecki

Haeili

Shah

et al. 2015

Antimicrob Agents Chemother

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“…These candidate anticancer drugs are currently under clinical investigations for various types of cancer. Due to the growing demand for the existing drugs in anticancer drug discovery, a number of collections of existing drugs are now available commercially or noncommercially, which are amenable for high throughput screening (Chong et al 2006;Diamandis et al 2007;Doudican et al 2008;Huang et al 2011;Hothi et al 2012;Robinson et al 2013;Czyz et al 2014;Ketley et al 2014;Mei et al 2014) (Table 3).…”

Section: Experimental Models Of Cscs and Drug Repositioningmentioning

confidence: 99%

Existing drugs and their application in drug discovery targeting cancer stem cells

Lv¹,

Shim²

2015

Arch. Pharm. Res.

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Despite standard cancer therapies such as chemotherapy and targeted therapy have shown some efficacies, the cancer in many cases eventually relapses and metastasizes upon stopping the treatment. There is a small subpopulation of cancer cells within tumor, with specific characters similar to those found in stem cells. This group of cancer cells is known as tumor-initiating or cancer stem cells (CSCs), which have an ability to self-renew and give rise to cancer cell progeny. CSCs are related with drug resistance, metastasis and relapse of cancer, hence emerging as a crucial drug target for eliminating cancer. Rapid advancement of CSC biology has enabled researchers to isolate and culture CSCs in vitro, making the cells amenable to high-throughput drug screening. Recently, drug repositioning, which utilizes existing drugs to develop potential new indications, has been gaining popularity as an alternative approach for the drug discovery. As existing drugs have favorable bioavailability and safety profiles, drug repositioning is now actively exploited for prompt development of therapeutics for many serious diseases, such as cancer. In this review, we will introduce latest examples of attempted drug repositioning targeting CSCs and discuss potential use of the repositioned drugs for cancer therapy.

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High-throughput screen identifies disulfiram as a potential therapeutic for triple-negative breast cancer cells: Interaction with IQ motif-containing factors

Cited by 44 publications

References 87 publications

Drug Affinity Responsive Target Stability (DARTS) for Small-Molecule Target Identification

Drug Affinity Responsive Target Stability (DARTS) for Small-Molecule Target Identification

Disulfiram and Copper Ions Kill Mycobacterium tuberculosis in a Synergistic Manner

Existing drugs and their application in drug discovery targeting cancer stem cells

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