Abstract
BackgroundCancer treatment during pregnancy is a growing problem especially now that women delay childbearing. Systemic treatment of these malignancies during pregnancy centers mainly on the anticancer drugs anthracyclines, widely used in treating hematological and breast cancer during pregnancy and sometimes associated with early and late toxicity for the fetus. Owing to concern about their cardiac and neurodevelopmental toxicity more information is needed on which anthracycline to prefer and whether they can safely guarantee a cardiotoxicity-free outcome in the fetus.DiscussionThe major research findings underline anthracycline-induced dose-dependent effects, including cardiotoxicity, many avoidable. Partly because the placenta acts mainly as a barrier, research findings indicate low transplacental anthracycline transfer. Anthracycline-induced teratogenicity depends closely on when patients receive chemotherapy. Anthracycline cardiac toxicity may depend on the association with drugs that inhibit or induce placental P-glycoprotein (P-gp). P-gp-induced drug interactions may alter placental P-gp barrier function and subsequently change fetal exposure. Though many anthracyclines have acceptable safety profiles clinical studies suggest giving idarubicin with special caution. Patients and doctors who care for pregnant women should whenever possible avoid prematurity and hence reduce prematurity-induced medical complications at birth and in the long-term. Information is lacking on long-term anthracycline-induced effects.ConclusionPregnant women receiving anthracycline-based chemotherapy should undergo regular, state-of-the-art diagnostic imaging to detect fetal drug-induced cardiac damage early, and allow alternative therapeutic options. Recognizing drug-induced interactions and understanding the most vulnerable fetuses will help in choosing tailored therapy. Future research on placental transport, blood-brain barrier drug passage and pharmacokinetics will improve the way we manage these difficult-to-treat patients and their fetuses.
Highlights
Cancer treatment during pregnancy is a growing problem especially that women delay childbearing
Some evidence suggests that these radicals are produced via poly (ADP-ribose) polymerase (PARP) and nicotinamide adenine dinucleotide phosphate (NADPH) oxidase causing the caspase hyperactivation that is essential for cell apoptosis or programmed cell death [9]
In a retrospective study conducted in our gynecologic clinic, we suggested explaining to the mother that because many chemotherapeutic regimens including anthracyclines leave the fetus unchanged mothers should whenever possible avoid prematurity so as to reduce prematurity-induced medical complications at birth and in the long-term [57]
Summary
Cancer treatment during pregnancy is a growing problem especially that women delay childbearing. Systemic treatment of these malignancies during pregnancy centers mainly on the anticancer drugs anthracyclines, widely used in treating hematological and breast cancer during pregnancy and sometimes associated with early and late toxicity for the fetus. Given the current general trend for women in developed countries to delay childbearing, treating cancer in pregnant women is a growing problem [2]. Hematological cancers are less frequent than breast cancer in pregnancy [5] Systemic treatment of these malignancies during pregnancy centers mainly on the anticancer drugs anthracyclines. Anthracyclines are widely used in treating hematological and breast cancer during pregnancy and sometimes associated with early and late toxicity for the fetus
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