The metabolic profile of mitoxantrone and its relation with mitoxantrone-induced cardiotoxicity

Rossato, Luciana; Costa, Vera Marisa; Pinho, Paula Guedes de; Arbo, Marcelo Dutra; Freitas, Víctor de; Vilain, Laure; Bastos, Maria de Lourdes; Palmeira, Carlos M.; Remião, Fernando

doi:10.1007/s00204-013-1040-6

Cited by 48 publications

(64 citation statements)

References 29 publications

(80 reference statements)

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“…ethyl]amino]-1,2,3,4,7,12-hexahydronaphto- [2,3]-quinoxaline-7-12-dione), which has proven antitumour effects and has been related to MTX toxicity [5,10]. Recently, we demonstrated that, as it happens with MTX, the naphthoquinoxaline metabolite also distributes to highly perfused tissues and accumulates in organs such as liver and heart in rats [5].…”

Section: -Dihydroxy-4-[2-hydroxyethyl]-6-[[2-[[2-hydroxyethyl]amino]mentioning

confidence: 99%

“…Recently, we demonstrated that, as it happens with MTX, the naphthoquinoxaline metabolite also distributes to highly perfused tissues and accumulates in organs such as liver and heart in rats [5]. The liver is subjected to a prolonged exposure to MTX and, possibly, to this toxic metabolite that may contribute to its direct hepatotoxicity.…”

Section: -Dihydroxy-4-[2-hydroxyethyl]-6-[[2-[[2-hydroxyethyl]amino]mentioning

confidence: 99%

“…Additionally, MTX is a substrate of membrane efflux pumps, namely the transporter breast cancer resistance protein (BCRP), which could interfere in MTX biodisposition [4]. However, the doses commonly employed range between 12-14 mg/m 2 and the maximum recommended cumulative dose is 140 mg/m 2 [1].One of the most serious adverse events related to MTX therapy is the late and irreversible cardiotoxicity [1], whose underlying mechanisms have been studied by us [5][6][7]. It is known that cardiotoxic drugs such as MTX can cause acute liver failure as a result of a primary congestive heart failure with low cardiac output and consequent reduced hepatic blood flow [8].…”

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Cumulative Mitoxantrone‐Induced Haematological and Hepatic Adverse Effects in a Subchronic In vivo Study

Rossato

Costa

Dallegrave

et al. 2013

Basic Clin Pharma Tox

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Mitoxantrone (MTX) is an antineoplastic agent that can induce hepato-and haematotoxicity. This work aimed to investigate the occurrence of cumulative early and late MTX-induced hepatic and haematological disturbances in an vivo model. A control group and two groups treated with three cycles of 2.5 mg/kg MTX at days 0, 10 and 20 were formed. One of the treated groups suffered euthanasia on day 22 (MTX22) to evaluate early MTX toxic effects, while the other suffered euthanasia on day 48 (MTX48), to allow the evaluation of MTX late effects. An early immunosuppression with a drop in the IgG levels was observed, causing a slight decrease in the plasma total protein content. The early bone marrow depression was followed by signs of recovery in MTX48. The genotoxic potential of MTX was demonstrated by the presence of several micronuclei in MTX22 leucocytes. Increases in plasma iron and cholesterol levels in the MTX22 rats were observed, while in both groups increases in the unconjugated bilirubin, C4 complement, and decreases in the triglycerides, alanine aminotransferase, alkaline phosphatase and transferrin were found in plasma samples. On MTX 48, the liver histology showed more hepatotoxic signs, the hepatic levels of reduced and oxidized glutathione were increased, and ATP hepatic levels were decreased. However, the hepatic total protein levels were decreased only in the livers of MTX22 group. Results demonstrated the MTX genotoxic effects, haemato-and direct hepatotoxicity. While the haematological toxicity is ameliorated with time, the same was not observed in the hepatic injury.Mitoxantrone (MTX) is an anticancer and immunosuppressive drug that has been used in the treatment of tumours such as acute leukaemia, lymphoma, prostatic and breast cancer [1] and in the active forms of relapsing-remitting or secondary progressive multiple sclerosis [2]. MTX acts as an intercalating agent that causes double breaks in DNA by stabilization of a complex formed between DNA and topoisomerase II [1,3]. The regimen of MTX administration varies depending on disease progression and the clinical condition of the patient. Additionally, MTX is a substrate of membrane efflux pumps, namely the transporter breast cancer resistance protein (BCRP), which could interfere in MTX biodisposition [4]. However, the doses commonly employed range between 12-14 mg/m 2 and the maximum recommended cumulative dose is 140 mg/m 2 [1].One of the most serious adverse events related to MTX therapy is the late and irreversible cardiotoxicity [1], whose underlying mechanisms have been studied by us [5][6][7]. It is known that cardiotoxic drugs such as MTX can cause acute liver failure as a result of a primary congestive heart failure with low cardiac output and consequent reduced hepatic blood flow [8]. However, the precise origin of liver failure, due to a direct effect or secondary to the cardiomyopathy, is not easy to define, because clinical signs of cardiac decompensating can be undetected in a first moment delaying the diagnosis [8]. Additi...

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Section: -Dihydroxy-4-[2-hydroxyethyl]-6-[[2-[[2-hydroxyethyl]amino]mentioning

confidence: 99%

Section: -Dihydroxy-4-[2-hydroxyethyl]-6-[[2-[[2-hydroxyethyl]amino]mentioning

confidence: 99%

mentioning

confidence: 99%

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Cumulative Mitoxantrone‐Induced Haematological and Hepatic Adverse Effects in a Subchronic In vivo Study

Rossato

Costa

Dallegrave

et al. 2013

Basic Clin Pharma Tox

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“…Nevertheless, fumonisins have attracted relatively little attention in toxicological research. Currently, hepatotoxicity (Campos et al 2014;Liu et al 2014;Godoy et al 2009Godoy et al , 2013Godoy et al , 2015Schyschka et al 2013;Schliess et al 2014;Grinberg et al 2014), nephrotoxicity (Yang et al 2014;Yu et al 2013;Early et al 2013;Kitada et al 2006;Ruíz-López et al 2006;Bulacio and Torres 2013) and cardiotoxicity (Fujisawa et al 2014;Maayah et al 2014;Ferreiro et al 2014;Rossato et al 2013) represent cutting-edge topics in toxicology. Recently, lists of reference compounds have been recommended for establishment of in vitro systems of repeated dose toxicity (Jennings et al 2014;Hengstler et al 2014).…”

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confidence: 99%

Highlight report: metabolism and toxicity by fumonisins

Degen

2015

Arch Toxicol

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“…Moreover, zebrafish-based test systems have been studied as an alternative method to identify hepatotoxic compounds (Driessen et al 2013;Scholz 2013). Compared to the high number of studies based on in vitro systems the fraction of in vivo studies published in the Archives of Toxicology has become relatively small (Rossato et al 2013;Yu et al 2013;Early et al 2013;Cordova et al 2013;Saito et al 2013;Hammad et al 2014). Moreover, studies systematically comparing the functions of in vitro systems to the in vivo situation are rare Heise et al 2012).…”

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confidence: 99%