Structure–Function Relationship of Thiazolide-Induced Apoptosis in Colorectal Tumor Cells

Brockmann, Anette; Strittmatter, Tobias; May, Sarah; Stemmer, Kerstin; Marx, Andreas; Brunner, Thomas

doi:10.1021/cb500209a

Cited by 15 publications

(16 citation statements)

References 26 publications

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“…Although we have initially seen that thiazolides bind to GSTP1-1 and inhibit the enzymatic activity of GSTP1-1 in vitro , very likely this observation was based on substrate competition. Indeed, we have seen later that enzymatic GSTP1-1 activity is required for thiazolides to kill colorectal tumor cells, and that increased GSH levels enhance thiazolide activity 31 , 32 ( Figure 6a ). Thus, very likely GSTP1-1 couples GSH to thiazolides, and thereby generates active apoptosis-promoting products.…”

Section: Discussionmentioning

confidence: 89%

“…We have previously performed a structure-function study and shown that changes of substituents in the benzene ring do not affect the cell death-promoting activity of thiazolides, whereas removal of the bromide atom from the thiazole ring, as in compound 2, strongly reduces the activity. 32 To investigate the thiazolide-induced apoptosis signaling pathways, we employed RM4819 as an active thiazolide, and compound 2 is inactive control substance to induce apoptosis in the colorectal tumor cell lines Caco-2 and LS174T. Figure 1a (Caco-2 cells) and Supplementary Figure 1 (LS174T cells) show that RM4819 induced cell death in a dose-dependent manner, whereas cells were almost insensitive to compound 2.…”

Section: Resultsmentioning

confidence: 99%

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Thiazolides promote apoptosis in colorectal tumor cells via MAP kinase-induced Bim and Puma activation

et al. 2015

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While many anticancer therapies aim to target the death of tumor cells, sophisticated resistance mechanisms in the tumor cells prevent cell death induction. In particular enzymes of the glutathion-S-transferase (GST) family represent a well-known detoxification mechanism, which limit the effect of chemotherapeutic drugs in tumor cells. Specifically, GST of the class P1 (GSTP1-1) is overexpressed in colorectal tumor cells and renders them resistant to various drugs. Thus, GSTP1-1 has become an important therapeutic target. We have recently shown that thiazolides, a novel class of anti-infectious drugs, induce apoptosis in colorectal tumor cells in a GSTP1-1-dependent manner, thereby bypassing this GSTP1-1-mediated drug resistance. In this study we investigated in detail the underlying mechanism of thiazolide-induced apoptosis induction in colorectal tumor cells. Thiazolides induce the activation of p38 and Jun kinase, which is required for thiazolide-induced cell death. Activation of these MAP kinases results in increased expression of the pro-apoptotic Bcl-2 homologs Bim and Puma, which inducibly bind and sequester Mcl-1 and Bcl-xL leading to the induction of the mitochondrial apoptosis pathway. Of interest, while an increase in intracellular glutathione levels resulted in increased resistance to cisplatin, it sensitized colorectal tumor cells to thiazolide-induced apoptosis by promoting increased Jun kinase activation and Bim induction. Thus, thiazolides may represent an interesting novel class of anti-tumor agents by specifically targeting tumor resistance mechanisms, such as GSTP1-1.

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Section: Discussionmentioning

confidence: 89%

Section: Resultsmentioning

confidence: 99%

Thiazolides promote apoptosis in colorectal tumor cells via MAP kinase-induced Bim and Puma activation

et al. 2015

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“…Of note, we demonstrated that luteolin activated some enzymes of a DNA damage pathway resulting in significant toxicity for OSCC cells. Moreover, although nitazoxanide was previously shown to be efficient against other cancer cells, such as colorectal (31)(32)(33)(34) and breast cancers (35), the antitumoral activity of metixene hydrochloride and nitazoxanide had not previously been demonstrated against oral cancer cells. We report here that luteolin, metixene hydrochloride, and nitazoxanide exhibit dose-and time-dependent selective toxicity in SCC-25 cells.…”

Section: Discussionmentioning

confidence: 99%

Luteolin Impacts on the DNA Damage Pathway in Oral Squamous Cell Carcinoma

Tjioe

Oliveira

Gavard

2016

Nutrition and Cancer

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Oral squamous cell carcinoma (OSCC) exhibited high chemoresistance to current treatments. Here we aimed at identifying and repositioning approved drugs that could be selectively toxic toward OSCC cells. Through a cell-based drug screening of 1,280 chemical molecules, we selected compounds lethal to oral cancer SCC-25 cells, while sparing normal keratinocyte HaCaT cells. Within the chemical library, the natural flavonoid luteolin was identified as a potent cytotoxic agent against oral cancer cells in vitro, along with metixene hydrochloride and nitazoxanide. Of note, they exhibit low toxicity and high efficiency compared to the standard-of-care, such as cisplatin and the epidermal growth factor receptor inhibitor tyrphostin. From a molecular standpoint, luteolin causes phosphorylation of ataxia telangiectasia mutated (ATM) and H2AX in a DNA repair pathway and can be efficiently combined with a checkpoint kinase (CHK) pharmacological inhibitor. Thus, luteolin emerges as a potent cytotoxic and/or adjuvant therapy in oral cancer, as it is a natural compound presenting better effects in vitro compared to conventional chemotherapeutic agents. Future in vivo exploration is next required to provide the proof-of-concept that luteolin could be an efficient anticancer molecule.

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“…Além disso, apresenta baixa toxicidade contra tecidos normais e efeitos colaterais brandos (Broekhuysen et al, 2000;Cohen, 2005). O efeito antitumoral da nitazoxanide foi descrito em câncer colorretal, de mama, linfático, ósseo in vitro e in vivo (Muller et al, 2008;Sidler et al, 2012;Fan-Minogue et al, 2013;Brockmann et al, 2014;Senkowski et al, 2015). A luteolin é um flavonoide pertencente ao subgrupo das flavonas e foi identificada em mais de 300 espécies de plantas e vegetais.…”

Section: Lista De Ilustraçõesunclassified

“…Em 2014, foi publicado outro trabalho demonstrando que o BRM4819 é capaz de induzir a apoptose em três linhagens de câncer colorretal. Esta atividade pró-apoptótica é dependente da ativação da caspase-3 e da expressão do GSTP1 (Brockmann et al, 2014 …”

Section: Nitazoxanideunclassified

Reposicionamento de fármacos no câncer de boca: Identificação de possíveis agentes

Tjioe¹

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Structure–Function Relationship of Thiazolide-Induced Apoptosis in Colorectal Tumor Cells

Cited by 15 publications

References 26 publications

Thiazolides promote apoptosis in colorectal tumor cells via MAP kinase-induced Bim and Puma activation

Thiazolides promote apoptosis in colorectal tumor cells via MAP kinase-induced Bim and Puma activation

Luteolin Impacts on the DNA Damage Pathway in Oral Squamous Cell Carcinoma

Reposicionamento de fármacos no câncer de boca: Identificação de possíveis agentes

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