| Literature DB >> 35478225 |
Kacey Ronaldson-Bouchard1, Diogo Teles1,2,3, Keith Yeager1, Daniel Naveed Tavakol1, Yimu Zhao1, Alan Chramiec1, Somnath Tagore4, Max Summers1, Sophia Stylianos1, Manuel Tamargo1, Busub Marcus Lee1, Susan P Halligan1, Erbil Hasan Abaci5, Zongyou Guo5, Joanna Jacków5, Alberto Pappalardo5, Jerry Shih6, Rajesh K Soni7, Shivam Sonar8, Carrie German8, Angela M Christiano5,9, Andrea Califano4,7,10,11,12,13, Karen K Hirschi14, Christopher S Chen6, Andrzej Przekwas8, Gordana Vunjak-Novakovic15,16,17.
Abstract
Engineered tissues can be used to model human pathophysiology and test the efficacy and safety of drugs. Yet, to model whole-body physiology and systemic diseases, engineered tissues with preserved phenotypes need to physiologically communicate. Here we report the development and applicability of a tissue-chip system in which matured human heart, liver, bone and skin tissue niches are linked by recirculating vascular flow to allow for the recapitulation of interdependent organ functions. Each tissue is cultured in its own optimized environment and is separated from the common vascular flow by a selectively permeable endothelial barrier. The interlinked tissues maintained their molecular, structural and functional phenotypes over 4 weeks of culture, recapitulated the pharmacokinetic and pharmacodynamic profiles of doxorubicin in humans, allowed for the identification of early miRNA biomarkers of cardiotoxicity, and increased the predictive values of clinically observed miRNA responses relative to tissues cultured in isolation and to fluidically interlinked tissues in the absence of endothelial barriers. Vascularly linked and phenotypically stable matured human tissues may facilitate the clinical applicability of tissue chips.Entities:
Mesh:
Substances:
Year: 2022 PMID: 35478225 PMCID: PMC9250010 DOI: 10.1038/s41551-022-00882-6
Source DB: PubMed Journal: Nat Biomed Eng ISSN: 2157-846X Impact factor: 29.234