Abstract
In several cancers, the efflux and resistance against doxorubicin (DOX), an effective anticancer drug, are associated with cellular iron deficiency and overexpression of the mitochondrial exporter ABCB8. Conversely, decreased ABCB8 expression and disrupted iron homeostasis in the heart have been implicated in DOX-associated cardiotoxicity. While studies have demonstrated that altered iron status can modulate the susceptibility to DOX cardiotoxicity, the exact molecular mechanisms have not been clearly understood. Here, we hypothesized that iron stores influence cardiac ABCB8 expression and consequently cardiac retention and toxicity of DOX. First, we found that ABCB8 deficiency in cardiomyocytes decreased DOX efflux, increased DOX-induced toxicity, and decreased cell viability. Conversely, intracellular DOX retention and toxicity were ameliorated by ABCB8 overexpression. To determine if altered cardiac iron status modifies ABCB8 expression, we treated cardiomyocytes with high iron or iron chelators. Western blot and qPCR analyses revealed that ABCB8 levels were decreased in iron overload and increased in iron deficiency. Subsequently, DOX retention and toxicity were increased in cardiomyocytes with iron overload, whereas iron deficiency ameliorated these effects. Next, we validated our results using a mouse model of hereditary hemochromatosis (HH), a genetic iron overload disorder. HH mice exhibited decreased ABCB8 expression and increased DOX retention and toxicity. These changes were abolished by the treatment of HH mice with a low-iron diet. Finally, cardiac-specific overexpression of ABCB8 in HH mice prevented cardiac DOX accumulation and abrogated DOX-induced cardiotoxicity without altering iron overload in the heart. Together, our results demonstrate that ABCB8 mediates DOX efflux and that iron regulates DOX retention and toxicity by altering cardiac ABCB8 expression. Our study identifies a novel role of iron in DOX-induced cardiotoxicity and suggests potential therapeutic intervention for DOX and anthracycline-based cancer pharmacology.
Highlights
Doxorubicin (DOX) is an effective anticancer agent, it is non-selective towards cells and accumulates in other organs, primarily the heart, exerting off-target toxicities
We found that intracellular DOX retention is potentiated in ATP binding cassette subfamily B8 (ABCB8)-deficient cardiomyocytes and decreased in ABCB8 overexpression
We note that our results are not congruent with those by Ichikawa et al, who reported that DOX retention does not differ in cardiomyocytes with altered ABCB8 expression (Ichikawa et al, 2014)
Summary
Doxorubicin (DOX) is an effective anticancer agent, it is non-selective towards cells and accumulates in other organs, primarily the heart, exerting off-target toxicities. It has been known that ABC (ATP-binding cassette) protein expression significantly correlates with chemosensitivity in cancer (Clarke et al, 2005; Noguchi et al, 2014). These proteins (summarized in (Mohammad et al, 2018)) are active transporters which utilize ATP to translocate substrates across cellular and subcellular membranes and have been extensively studied since their overexpression is linked to increased cellular DOX efflux and resistance in several cancers (Szakács et al, 2006; Martin et al, 2014). There is a need to identify novel DOX efflux transporters to efficiently correct DOX-induced cardiotoxicity
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