Exploring the biochemical mechanisms of cytotoxic gold compounds: a proteomic study

Magherini, Francesca; Modesti, Alessandra; Bini, Luca; Puglia, Michele; Landini, Ida; Nobili, Stefania; Mini, Enrico; Cinellu, Maria Agostina; Gabbiani, Chiara; Messori, Luigi

doi:10.1007/s00775-010-0624-3

Cited by 62 publications

(60 citation statements)

References 55 publications

(65 reference statements)

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“…Concerning the A2780/S, the results pointed out that the mode of action of Auoxo6 is strictly related to that of auranofin. Both gold compounds trigger caspase 3 activation and apoptosis and the affected proteins are involved in cell redox homeostasis and stress response [28]. Conversely, in the A2780/R cell line, Auranofin affected the expression of proteasome apparatus proteins whereas Auoxo6 modified the expression of proteins related to mRNA trafficking and stability [29].…”

Section: Introductionmentioning

confidence: 99%

Proteomic analysis of A2780/S ovarian cancer cell response to the cytotoxic organogold(III) compound Aubipyc

Gamberi

Massai

Magherini

et al. 2014

Journal of Proteomics

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Aubipy c is an organogold(III) compound endowed with encouraging anti-proliferative properties in vitro that is being evaluated pre-clinically as a prospective anticancer agent. A classical proteomic approach is exploited here to elucidate the mechanisms of its biological actions in A2780 human ovarian cancer cells. Based on 2-D gel electrophoresis separation and subsequent mass spectrometry identification, a considerable number of differentially expressed proteins were highlighted in A2780 cancer cells treated with Aubipy c . Bioinformatic analysis of the groups of up-regulated and down-regulated proteins pointed out that Aubipy c primarily perturbs mitochondrial processes and the glycolytic pathway. Notably, some major alterations in the glycolytic pathway were validated through Western blot and metabolic investigations. Biological significanceThis is the first proteomic analysis regarding Aubipy c cytotoxicity in A2780/S ovarian cancer cell line. Aubipy c is a promising gold(III) compound which manifests an appreciable cytotoxicity toward the cell line A2780, being able to overcome resistance to platinum. The proteomic study revealed for Aubipy c different cellular alterations with respect to cisplatin as well as to other gold compound such as auranofin. Remarkably, the bioinformatic analysis of proteomic data pointed out that Aubipy c treatment affected, directly or indirectly, several glycolytic enzymes. These data suggest a new mechanism of action for this gold drug and might have an impact on the use of gold-based drug in cancer treatment.

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Section: Introductionmentioning

confidence: 99%

Proteomic analysis of A2780/S ovarian cancer cell response to the cytotoxic organogold(III) compound Aubipyc

Gamberi

Massai

Magherini

et al. 2014

Journal of Proteomics

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“…Among this group, we found another intermediate node, an actin-related protein involved in cytoskeleton organization [28] (ACTR6-Q9GZN1). The protein SMN2 (Q16637) is a node between two input proteins involved in splicing: the Heterogeneous nuclear ribonucleoprotein H (P31943) [2], and the Serine-threonine kinase receptor-associated protein (Q9Y3F4) [1]. The SMN2 protein plays an essential role in spliceosomal assembly, and is required for pre-mRNA splicing [29].…”

Section: Bioinformatic Analysis Of Proteomic Datamentioning

confidence: 99%

“…Proteomic results have the potential to provide new insight into the molecular mechanisms of this group of molecules at the cellular level [2]. More than 99% of currently approved clinical drugs are organic compounds.…”

Section: Introductionmentioning

confidence: 99%

“…cell line (A2780/S), after treatment with four different cytotoxic gold compounds, namely: Auranofin [2], Auoxo6 [2], AuL12 [1] and Au2Phen [1]. In a very recent paper, we have used for the first time, 2D-DIGE to investigate the mode of action of two anticancer ruthenium compounds, namely NAMI-A and RAPTA-T in A2780/S human cancer cells [18].…”

Section: Introductionmentioning

confidence: 99%

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New Insights into the Molecular Mechanisms of Selected Anticancer Metal Compounds through Bioinformatic Analysis of Proteomic Data

Gamberi¹

2013

J Proteomics Bioinform

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“…Very recently, we have exploited a classical proteomic approach to gain a deeper insight into the mechanism of two cytotoxic gold compounds, namely Auoxo6, a binuclear gold(III) complex showing a very favourable cytotoxic profile, and auranofin, a clinically established gold(I) antiarthritic drug, causing relevant tumor cell growth inhibition in vitro [56]. First, the 72h cytotoxicity profiles of Auoxo6 and auranofin were carefully recorded against A2780 human ovarian carcinoma cells, either sensitive or resistant to cisplatin.…”

Section: B) Proteomic Analysis Of Cellular Responses To Metallodrugsmentioning

confidence: 99%

Proteomic and Metallomic Strategies for Understanding the Mode of Action of Anticancer Metallodrugs

Gabbiani¹,

Magherini²,

Modesti³

et al. 2010

ACAMC

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Since the discovery of cisplatin and its introduction in the clinics, metal compounds have been intensely investigated in view of their possible application in cancer therapy. In this frame, a deeper understanding of their mode of action, still rather obscure, might turn crucial for the design and the obtainment of new and better anticancer agents. Due to the extreme complexity of the biological systems, it is now widely accepted that innovative and information-rich methods are absolutely needed to afford such a goal. Recently, both proteomic and metallomic strategies were successfully implemented for the elucidation of specific mechanistic features of anticancer metallodrugs within an innovative "Systems Biology" perspective. Particular attention was paid to the following issues: i) proteomic studies of the molecular basis of platinum resistance; ii) proteomic analysis of cellular responses to cytotoxic metallodrugs; iii) metallomic studies of the transformation and fate of metallodrugs in cellular systems. Notably, those pioneering studies, that are reviewed here, allowed a significant progress in the understanding of the molecular mechanisms of metal based drugs at the cellular level. A further extension of those studies and a closer integration of proteomic and metallomic strategies and technologies might realistically lead to rapid and significant advancements in the mechanistic knowledge of anticancer metallodrugs.

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Exploring the biochemical mechanisms of cytotoxic gold compounds: a proteomic study

Cited by 62 publications

References 55 publications

Proteomic analysis of A2780/S ovarian cancer cell response to the cytotoxic organogold(III) compound Aubipyc

Proteomic analysis of A2780/S ovarian cancer cell response to the cytotoxic organogold(III) compound Aubipyc

New Insights into the Molecular Mechanisms of Selected Anticancer Metal Compounds through Bioinformatic Analysis of Proteomic Data

Proteomic and Metallomic Strategies for Understanding the Mode of Action of Anticancer Metallodrugs

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