Microtechnology-based organ systems and whole-body models for drug screening

Authors
Lee, Seung HwanHa, Sang KeunChoi, InwookChoi, NakwonPark, Tai HyunSung, Jong Hwan
Issue Date
2016-06
Publisher
WILEY-V C H VERLAG GMBH
Citation
BIOTECHNOLOGY JOURNAL, v.11, no.6, pp.746 - 756
Abstract
After drug administration, the drugs are absorbed, distributed, metabolized, and excreted (ADME). Because ADME processes affect drug efficacy, various in vitro models have been developed based on the ADME processes. Although these models have been widely accepted as a tool for predicting the effects of drugs, the differences between in vivo and in vitro systems result in high attrition rates of drugs during the development process and remain a major limitation. Recent advances in microtechnology enable more accurate mimicking of the in vivo environment, where cellular behavior and physiological responses to drugs are more realistic; this has led to the development of novel in vitro systems, known as "organ-on-a-chip" systems. The development of organ-on-a-chip systems has progressed to include the reproduction of multiple organ interactions, which is an important step towards "body-on-a-chip" systems that will ultimately predict whole-body responses to drugs. In this review, we summarize the application of microtechnology for the development of in vitro systems that accurately mimic in vivo environments and reconstruct multiple organ models.
Keywords
CELL-CULTURE ANALOG; CUT LIVER SLICES; ON-A-CHIP; IN-VITRO; INTESTINAL SCAFFOLDS; CACO-2 MONOLAYERS; BIOREACTOR; METABOLISM; TOXICITY; PERMEABILITY; CELL-CULTURE ANALOG; CUT LIVER SLICES; ON-A-CHIP; IN-VITRO; INTESTINAL SCAFFOLDS; CACO-2 MONOLAYERS; BIOREACTOR; METABOLISM; TOXICITY; PERMEABILITY; In vitro systems; Microfluidics; Microtechnology; Multiple organ interaction; Organ-on-a-chip
ISSN
1860-6768
URI
https://pubs.kist.re.kr/handle/201004/123998
DOI
10.1002/biot.201500551
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KIST Article > 2016
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