Fetal Rat Hearts Do Not Display Acute Cardiotoxicity in Response to Maternal Doxorubicin Treatment

Gzirí, Mina Mhallem; Pokreisz, Péter; Vos, Rita De; Verbeken, Eric; Debiève, Frédéric; Mertens, Luc; Janssens, Stefan; Amant, Frédéric

doi:10.1124/jpet.113.205419

Cited by 10 publications

(5 citation statements)

References 35 publications

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“…LV wall thinning combined with a 14% reduction in LVIDd also led to significant reductions in EF, FS, SV and EDV in Dox treated mice in this study. Similar changes in cardiac geometry and hemodynamic parameters were also noted in animal models of Dox induced acute cardiotoxicity [ 52 , 53 , 54 , 55 ]. For instance, a single injection of Dox (20 mg/Kg) led to significant reductions in LVPWd dimension and fractional shortening (FS) in pregnant rats as early as 48-h time point [ 52 ].…”

Section: Discussionsupporting

confidence: 55%

“…Similar changes in cardiac geometry and hemodynamic parameters were also noted in animal models of Dox induced acute cardiotoxicity [ 52 , 53 , 54 , 55 ]. For instance, a single injection of Dox (20 mg/Kg) led to significant reductions in LVPWd dimension and fractional shortening (FS) in pregnant rats as early as 48-h time point [ 52 ]. In mice subjected to acute Dox treatment (20–25 mg/Kg), significant reductions in LVIDd, LVIDs, FS and cardiac output were noted 4–5 days after drug treatment [ 54 , 55 ].…”

Section: Discussionsupporting

confidence: 55%

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Regulation of Transplanted Cell Homing by FGF1 and PDGFB after Doxorubicin Myocardial Injury

Baguma-Nibasheka

Feridooni

Zhang

et al. 2021

Cells

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There is no effective treatment for the total recovery of myocardial injury caused by an anticancer drug, doxorubicin (Dox). In this study, using a Dox-induced cardiac injury model, we compared the cardioprotective effects of ventricular cells harvested from 11.5-day old embryonic mice (E11.5) with those from E14.5 embryos. Our results indicate that tail-vein-infused E11.5 ventricular cells are more efficient at homing into the injured adult myocardium, and are more angiogenic, than E14.5 ventricular cells. In addition, E11.5 cells were shown to mitigate the cardiomyopathic effects of Dox. In vitro, E11.5 ventricular cells were more migratory than E14.5 cells, and RT-qPCR analysis revealed that they express significantly higher levels of cytokine receptors Fgfr1, Fgfr2, Pdgfra, Pdgfrb and Kit. Remarkably, mRNA levels for Fgf1, Fgf2, Pdgfa and Pdgfb were also found to be elevated in the Dox-injured adult heart, as were the FGF1 and PDGFB protein levels. Addition of exogenous FGF1 or PDGFB was able to enhance E11.5 ventricular cell migration in vitro, and, whereas their neutralizing antibodies decreased cell migration. These results indicate that therapies raising the levels of FGF1 and PDGFB receptors in donor cells and or corresponding ligands in an injured heart could improve the efficacy of cell-based interventions for myocardial repair.

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Section: Discussionsupporting

confidence: 55%

Section: Discussionsupporting

confidence: 55%

Regulation of Transplanted Cell Homing by FGF1 and PDGFB after Doxorubicin Myocardial Injury

Baguma-Nibasheka

Feridooni

Zhang

et al. 2021

Cells

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“…Available data provide only limited experimental and clinical data on the transplacental transfer of these chemotherapeutics in pregnant women; in a baboon model, fetal plasma concentrations of doxorubicin, epirubicin and paclitaxel were about 7.5 %, 4.0 %, and 1.4 %, of the respective maternal concentrations [ 32 ]. Fetal blood samples from pregnant rats receiving doxorubicin showed a plasmatic concentration that was 6.2 % that of the mother; interestingly, neither Doppler analysis nor heart microstructure or cellular DNA turnover and apoptosis were influenced by doxorubicin exposure [ 33 ].…”

Section: Discussionmentioning

confidence: 99%

Epirubicin: a new entry in the list of fetal cardiotoxic drugs? Intrauterine death of one fetus in a twin pregnancy. Case report and review of literature

Framarino-dei-Malatesta

Perrone

Giancotti

et al. 2015

BMC Cancer

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BackgroundCurrent knowledge indicate that epirubicin administration in late pregnancy is almost devoid of any fetal cardiotoxicity. We report a twin pregnancy complicated by breast cancer in which epirubicin administration was causatively linked to the death of one twin who was small for gestational age (SGA) and in a condition of oligohydramnios and determined the onset of a transient cardiotoxicity of the surviving fetus/newborn.Case presentationA 38-year-old caucasic woman with a dichorionic twin pregnancy was referred to our center at 20 and 1/7 weeks for a suspected breast cancer, later confirmed by the histopathology report. At 31 and 3/7 weeks, after the second chemotherapy cycle, ultrasound examination evidenced the demise of one twin while cardiac examination revealed a monophasic diastolic ventricular filling, i.e. a diastolic dysfunction of the surviving fetus who was delivered the following day due to the occurrence of grade II placental abruption. The role of epirubicin cardiotoxicity in the death of the first twin was supported by post-mortem cardiac and placental examination and by the absence of structural or genomic abnormalities that may indicate an alternative etiology of fetal demise. The occurrence of epirubicin cardiotoxicity in the surviving newborn was confirmed by the report of high levels of troponin and transient left ventricular septal hypokinesia.ConclusionBased on our findings we suggest that epirubicin administration in pregnancy should be preceded by the screening of some fetal conditions like SGA and oligohydramnios that may increase its cardiotoxicity and that, during treatment, the diastolic function of the fetal right ventricle should be specifically monitored by a pediatric cardiologist; also, epirubicin and desamethasone for lung maturation should not be closely administered since placental effects of glucocorticoids may increase epirubicin toxicity.

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“…In animal experiments, fetal rat hearts exposed to doxorubicin did not show acute cardiotoxicity in response to maternal treatment, with intact microstructure, unaltered number of apoptotic cells and preserved cell proliferation [50]. A small study in humans confirms no fetal cardiac dysfunction after anthracycline exposure during pregnancy [51].…”

Section: Doxorubicinmentioning

confidence: 97%

Exploring the safety of chemotherapy for treating breast cancer during pregnancy

Lambertini

Kamal

Peccatori

et al. 2015

Expert Opinion on Drug Safety

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The rule of thumb of chemotherapy - avoiding first trimester exposure and starting therapy in the second trimester - can be considered applicable for classic agents that are used in managing pregnant breast cancer patients. Anthracycline-based regimens are considered the standard of care in managing BCP. Recently, a growing amount of data suggests the safety of taxanes during pregnancy. Pregnancy in cancer patients should be considered as "high risk": once the systemic treatment is initiated, regular fetal monitoring is highly recommended. Emerging data are available on the relative long-term safety secondary to anthracycline exposure during pregnancy. A continued monitoring of the health of individuals with prenatal exposure to chemotherapy into adulthood is recommended for the possible occurrence of long-term side effects.

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Fetal Rat Hearts Do Not Display Acute Cardiotoxicity in Response to Maternal Doxorubicin Treatment

Cited by 10 publications

References 35 publications

Regulation of Transplanted Cell Homing by FGF1 and PDGFB after Doxorubicin Myocardial Injury

Regulation of Transplanted Cell Homing by FGF1 and PDGFB after Doxorubicin Myocardial Injury

Epirubicin: a new entry in the list of fetal cardiotoxic drugs? Intrauterine death of one fetus in a twin pregnancy. Case report and review of literature

Exploring the safety of chemotherapy for treating breast cancer during pregnancy

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