Notice
This is not the latest version of this item. The latest version can be found at:https://dspace.mit.edu/handle/1721.1/142801.2
Identification of NQO2 As a Protein Target in Small Molecule Modulation of Hepatocellular Function
DownloadAccepted version (1.236Mb)
Open Access Policy
Open Access Policy
Creative Commons Attribution-Noncommercial-Share Alike
Terms of use
Metadata
Show full item recordAbstract
The utility of in vitro human disease models is mainly dependent on the availability and functional maturity of tissue-specific cell types. We have previously screened for and identified small molecules that can enhance hepatocyte function in vitro. Here, we characterize the functional effects of one of the hits, FH1, on primary human hepatocytes in vitro, and also in vivo on primary hepatocytes in a zebrafish model. Furthermore, we conducted an analogue screen to establish the structure-activity relationship of FH1. We performed affinity-purification proteomics that identified NQO2 to be a potential binding target for this small molecule, revealing a possible link between inflammatory signaling and hepatocellular function in zebrafish and human hepatocyte model systems.
Date issued
2021Journal
ACS Chemical Biology
Publisher
American Chemical Society (ACS)
Citation
Schepers, Arnout G, Shan, Jing, Cox, Andrew G, Huang, Ada, Evans, Helen et al. 2021. "Identification of NQO2 As a Protein Target in Small Molecule Modulation of Hepatocellular Function." ACS Chemical Biology, 16 (9).
Version: Author's final manuscript