Morphofunctional effects of mitotane on mitochondria in human adrenocortical cancer cells

Poli, Giada; Guasti, Daniele; Rapizzi, Elena; Fucci, Rossella; Canu, Letizia; Bandinelli, Alessandra; Cini, Nicoletta; Bani, Danièle; Mannelli, Massimo; Luconi, Michaela

doi:10.1530/erc-13-0150

Cited by 65 publications

(53 citation statements)

References 28 publications

(37 reference statements)

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“…This was confirmed to some extent in cell culture suggesting that down-regulation of the mitochondrial respiratory chain might be involved in the cytotoxic effect of the drug (37,38). We personally have some doubts if the covalent binding of a mitotane intermediate to mitochondrial proteins is actually causative of decreased steroid synthesis and cell death in ACCs as i) in the original report, protein adducts have been mainly found in non-human adrenocortical tissue and only weakly in NCI-H295 cells, ii) these presumed adducts have never been identified, and iii) alterations of the respiratory chain also occur during apoptosis which may be triggered by completely separate pathways.…”

Section: Mitotanementioning

confidence: 63%

EJE PRIZE 2014: Current and evolving treatment options in adrenocortical carcinoma: where do we stand and where do we want to go?

Ronchi

Kroiß

Sbiera

et al. 2014

European Journal of Endocrinology

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Adrenocortical carcinoma (ACC) is not only a rare and heterogeneous disease but also one of the most aggressive endocrine tumors. Despite significant advances in the last decade, its pathogenesis is still only incompletely understood and overall therapeutic means are unsatisfactory. Herein, we provide our personal view of the currently available treatment options and suggest the following research efforts that we consider timely and necessary to improve therapy: i) for better outcome in localized ACCs, surgery should be restricted to experienced centers, which should then collaborate closely to address the key surgical questions (e.g. best approach and extent of surgery) in a multicenter manner. ii) For the development of better systemic therapies, it is crucial to elucidate the exact molecular mechanisms of action of mitotane. iii) A prospective trial is needed to address the role of cytotoxic drugs in the adjuvant setting in aggressive ACCs (e.g. mitotane vs mitotaneC cisplatin). iv) For metastatic ACCs, new regimens should be investigated as first-line therapy. v) Several other issues (e.g. the role of radiotherapy and salvage therapies) might be answered -at least in a first step -by large retrospective multicenter studies. In conclusion, although it is unrealistic to expect that the majority of ACCs can be cured within the next decade, international collaborative efforts (including multiple translational and clinical studies) should allow significant improvement of clinical outcome of this disease. To this end, it might be reasonable to expand the European Network for the Study of Adrenal Tumors (ENSAT) to a truly worldwide international network -INSAT.

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Section: Mitotanementioning

confidence: 63%

EJE PRIZE 2014: Current and evolving treatment options in adrenocortical carcinoma: where do we stand and where do we want to go?

Ronchi

Kroiß

Sbiera

et al. 2014

European Journal of Endocrinology

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“…Many inhibitors of electron transport as well as of F1F0-ATPase cause cell death under conditions that require respiration, but not under glycolytic conditions (Marroquin et al 2007; Poli, et al 2013; Tettamanti, et al 2008). Numerous inhibitors of oxidative phosphorylation have been investigated as potential anti-cancer agents (Rohlena, et al 2013).…”

Section: Discussionmentioning

confidence: 99%

ATR-101 disrupts mitochondrial functions in adrenocortical carcinoma cells and in vivo

Cheng

Kerppola²,

Kerppola

2016

Endocrine-Related Cancer

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Adrenocortical carcinoma (ACC) generally has poor prognosis. Existing treatments provide limited benefit for most patients with locally advanced or metastatic tumors. We investigated the mechanisms for the cytotoxicity, xenograft suppression and adrenalytic activity of ATR-101 (PD132301-02), a prospective agent for ACC treatment. Oral ATR-101 administration inhibited the establishment and impeded the growth of ACC-derived H295R cell xenografts in mice. ATR-101 induced H295R cell apoptosis in culture and in xenografts. ATR-101 caused mitochondrial hyperpolarization, reactive oxygen release and ATP depletion within hours after exposure, followed by cytochrome c release, caspase-3 activation, and membrane permeabilization. The increase in mitochondrial membrane potential occurred concurrently with the decrease in cellular ATP levels. When combined with ATR-101, lipophilic free radical scavengers suppressed the reactive oxygen release, and glycolytic precursors prevented the ATP depletion, abrogating ATR-101 cytotoxicity. ATR-101 directly inhibited F1F0-ATPase activity and suppressed ATP synthesis in mitochondrial fractions. ATR-101 administration to guinea pigs caused oxidized lipofuscin accumulation in the zona fasciculata layer of the adrenal cortex, implicating reactive oxygen release in the adrenalytic effect of ATR-101. These results support the development of ATR-101 and other adrenalytic compounds for the treatment of ACC.

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“…Besides VDAC2, we also detected VDAC1 in the human epithelial thyroid tumours and in the thyroid cell lines. In 2010, Koren et al showed that this isoform is essential for normal growth of tumoural cells, and that silencing VDAC1 expression in T-Rex-293 cells by means of RNA interference reduced ATP production and decreased cell growth (Koren et al, 2010).…”

Section: Discussionmentioning

confidence: 99%

The proteomic 2D-DIGE approach reveals the protein voltage-dependent anion channel 2 as a potential therapeutic target in epithelial thyroid tumours

Mato

Barceló-Batllori

Orera

et al. 2015

Molecular and Cellular Endocrinology

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Morphofunctional effects of mitotane on mitochondria in human adrenocortical cancer cells

Cited by 65 publications

References 28 publications

EJE PRIZE 2014: Current and evolving treatment options in adrenocortical carcinoma: where do we stand and where do we want to go?

EJE PRIZE 2014: Current and evolving treatment options in adrenocortical carcinoma: where do we stand and where do we want to go?

ATR-101 disrupts mitochondrial functions in adrenocortical carcinoma cells and in vivo

The proteomic 2D-DIGE approach reveals the protein voltage-dependent anion channel 2 as a potential therapeutic target in epithelial thyroid tumours

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