Assessment of drug induced developmental toxicity using human embryonic stem cells

Mehta, Ashish; Konala, Vijay Bhaskar Reddy; Khanna, Aparna; Majumdar, Anish Sen

doi:10.1016/j.cellbi.2008.08.012

Cited by 41 publications

(43 citation statements)

References 33 publications

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“…For instance, it was shown that while retinoic acid (RA) and 13-cis RA (13RA) exerted cytotoxic effects on hESCs, only the former compound induced cytotoxicity in mESCs despite both compounds being well-known agents of embryotoxicity 94 . However, testing for cytotoxicity is not a sufficient end-point to establish reproductive toxicity and hence incorporation of biomarkers to monitor changes in early lineage transcripts and cardiac development has been proposed 91,95 . In comparison to animal models, hPSCs have proven their effectiveness as an embryotoxic test system 96 .…”

Section: Human Pscs and Embryotoxicitymentioning

confidence: 99%

“…In an attempt to address species variation, hPSCs have been proposed as suitable models for investigating embryotoxicity 91,93,94 . For instance, it was shown that while retinoic acid (RA) and 13-cis RA (13RA) exerted cytotoxic effects on hESCs, only the former compound induced cytotoxicity in mESCs despite both compounds being well-known agents of embryotoxicity 94 .…”

Section: Human Pscs and Embryotoxicitymentioning

confidence: 99%

“…Acceptance of the mEST along with the WEC and MM test by the regulatory commission was therefore expected 78 ; however, the Scientific Advisory Committee (ESAC) of the ECVAM felt that these in vitro test systems were not adequate 79 . While several strategies have been implemented in attempts to improve mEST [80][81][82][83][84][85][86][87][88][89][90] , a major concern which remains is the species variation as it would be challenging to evaluate or interpret test results in a human context 91,92 .…”

Section: Human Pscs and Embryotoxicitymentioning

confidence: 99%

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Human Pluripotent Stem Cells and Drug Discovery: A New Beginning

Verma¹,

Mehta²,

Flora³

2016

Def. Life. Sc. Jl.

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Human pluripotent stem cells (hPSCs) offer unique opportunities to discover and develop a new generation of drugs. Their ability to differentiate into virtually any cell type renders them a cost-effective, renewable source of tissue-specific cell types capable of predicting human responses towards novel chemical entities. Using these improved in vitro models based on physiologically relevant human cell types could result in identifying highly precise and safe compounds, thereby reducing drug attrition rates. Moreover, ability to develop humanised disease models for patient-stratified drug screening makes hPSCs an impeccable tool in translational medicine. In this mini-review we focus on the positives and negatives of utilising hPSC-derived cell types as drug discovery platforms with special emphasis on cardio-, hepato-and embryotoxicity.

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Section: Human Pscs and Embryotoxicitymentioning

confidence: 99%

Section: Human Pscs and Embryotoxicitymentioning

confidence: 99%

Section: Human Pscs and Embryotoxicitymentioning

confidence: 99%

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Human Pluripotent Stem Cells and Drug Discovery: A New Beginning

Verma¹,

Mehta²,

Flora³

2016

Def. Life. Sc. Jl.

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“…A second interesting study has evaluated the potential of hESC to provide information on toxic chemicals using two non-embryotoxic, two weakly embryotoxic, and two strongly embryotoxic chemicals [46]. Cytotoxic indices were determined using cells representing the embryo (hESC), fetus (human embryoid bodies) and adults (human foreskin fibroblasts).…”

Section: Examples Of Studies That Have Been Donementioning

confidence: 99%

Mouse and Human Embryonic Stem Cells: Can They Improve Human Health by Preventing Disease?

Talbot

Lin²

2011

CTMC

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Given the vast number of chemicals that are released into the environment each year, it is imperative that we develop new predictive models to identify toxicants before unavoidable exposure harms the health of humans and other organisms. In vitro models are especially attractive in predictive toxicology as they can greatly reduce assay costs and animal usage while identifying those chemicals that may require further in vivo evaluation. With the derivation of both mouse and human embryonic stem cells, new opportunities have developed that could revolutionize the field of predictive toxicology. Stem cells themselves can be used to model pre-implantation development, or they can be used during or after differentiation model the earliest stages of development. Because embryos and fetuses are usually more sensitive to environmental toxicants than adults, stem cells provide an unique tool for studying the prenatal phase in our life cycle. The embryonic stem cell test (EST), which has been validated for use with mouse ESC (mESC), is an accurate predictor of embryotoxic compounds, particularly those that are highly embryotoxic. Human embryonic stem cells (hESCs), although not yet incorporated into a validated test, are a particularly attractive platform for toxicological testing as they can give us direct information on humans and avoid concerns about species variation in response. This review discusses toxicological studies and strategies that have been used with embryonic stem cells during the past five years and possible directions that could lead to improvements in the development of predictive assays in the future.

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“…The authors concluded that although this initial assay showed promise, additional research would be needed to standardize a human EST. Mehta et al [2008] attempted to increase the predictivity of the test by examining gene expression of each of the three germ layers as the endpoint of differentiation in a single hESC line. The authors concluded that the "implementation of the EST in regulatory test guidelines would demonstrate the importance of in vitro assays as valuable components of the risk/hazard assessment process" [Mehta et al 2008].…”

Section: Mouse Embryonic Stem Cell Test (Mest)mentioning

confidence: 99%