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10.1111/bcpt.12198

http://scihub22266oqcxt.onion/10.1111/bcpt.12198
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C4051836!4051836!24443875
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suck abstract from ncbi

pmid24443875      Basic+Clin+Pharmacol+Toxicol 2014 ; 115 (1): 24-31
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  • Mapping the Human Toxome by Systems Toxicology #MMPMID24443875
  • Bouhifd M; Hogberg HT; Kleensang A; Maertens A; Zhao L; Hartung T
  • Basic Clin Pharmacol Toxicol 2014[Jul]; 115 (1): 24-31 PMID24443875show ga
  • Toxicity testing typically involves studying adverse health outcomes in animals subjected to high doses of toxicants with subsequent extrapolation to expected human responses at lower doses. The low-throughput of current toxicity testing approaches (which are largely the same for industrial chemicals, pesticides and drugs) has led to a backlog of more than 80,000 chemicals to which human beings are potentially exposed whose potential toxicity remains largely unknown. Employing new testing strategies that employ the use of predictive, high-throughput cell-based assays (of human origin) to evaluate perturbations in key pathways, referred as pathways of toxicity, and to conduct targeted testing against those pathways, we can begin to greatly accelerate our ability to test the vast ?storehouses? of chemical compounds using a rational, risk-based approach to chemical prioritization, and provide test results that are more predictive of human toxicity than current methods. The NIH Transformative Research Grant project Mapping the Human Toxome by Systems Toxicology aims at developing the tools for pathway mapping, annotation and validation as well as the respective knowledge base to share this information.
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