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Download fileCardiotoxicity Hazard and Risk Characterization of ToxCast Chemicals Using Human Induced Pluripotent Stem Cell-Derived Cardiomyocytes from Multiple Donors
journal contribution
posted on 2021-08-27, 15:08 authored by Sarah
D. Burnett, Alexander D. Blanchette, Weihsueh A. Chiu, Ivan RusynHeart
disease remains a significant human health burden worldwide
with a significant fraction of morbidity attributable to environmental
exposures. However, the extent to which the thousands of chemicals
in commerce and the environment may contribute to heart disease morbidity
is largely unknown, because in contrast to pharmaceuticals, environmental
chemicals are seldom tested for potential cardiotoxicity. Human induced
pluripotent stem cell (iPSC)-derived cardiomyocytes have become an
informative in vitro model for cardiotoxicity testing
of drugs with the availability of cells from multiple individuals
allowing in vitro testing of population variability.
In this study, we hypothesized that a panel of iPSC-derived cardiomyocytes
from healthy human donors can be used to screen for the potential
cardiotoxicity hazard and risk of environmental chemicals. We conducted
concentration–response testing of 1029 chemicals (drugs, pesticides,
flame retardants, polycyclic aromatic hydrocarbons (PAHs), plasticizers,
industrial chemicals, food/flavor/fragrance agents, etc.) in iPSC-derived
cardiomyocytes from 5 donors. We used kinetic calcium flux and high-content
imaging to derive quantitative measures as inputs into Bayesian population
concentration–response modeling of the effects of each chemical.
We found that many environmental chemicals pose a hazard to human
cardiomyocytes in vitro with more than half of all
chemicals eliciting positive or negative chronotropic or arrhythmogenic
effects. However, most of the tested environmental chemicals for which
human exposure and high-throughput toxicokinetics data were available
had wide margins of exposure and, thus, do not appear to pose a significant
human health risk in a general population. Still, relatively narrow
margins of exposure (<100) were estimated for some perfuoroalkyl
substances and phthalates, raising concerns that cumulative exposures
may pose a cardiotoxicity risk. Collectively, this study demonstrated
the value of using a population-based human in vitro model for rapid, high-throughput hazard and risk characterization
of chemicals for which little to no cardiotoxicity data are available
from guideline studies in animals.
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polycyclic aromatic hydrocarbonspahs ), plasticizersmultiple individuals allowingenvironment may contributederive quantitative measuresrelatively narrow marginsheart disease morbiditychemicals eliciting positivethroughput toxicokinetics dataexposure (< 100healthy human donorstested environmental chemicalspotential cardiotoxicity hazardpotential cardiotoxicitycardiotoxicity datawide marginsthroughput hazardseldom testedmorbidity attributableenvironmental chemicals5 donorsenvironmental exposureshuman exposurehuman cardiomyocytesbased humanindustrial chemicalscardiotoxicity hazard1029 chemicalsvitro </significant fractionraising concernsperfuoroalkyl substancesnegative chronotropiclargely unknownguideline studiesfragrance agentsflame retardantsetc .)derived cardiomyocytescontent imaging