| Literature DB >> 34151211 |
Juan Alvarez-Gonzalez1, Adam Yasgar2, Robert W Maul1, Amanda E Rieffer3,4,5, Daniel J Crawford6, Daniel J Salamango3,4,5, Dorjbal Dorjsuren2, Alexey V Zakharov2, Daniel J Jansen2, Ganesha Rai2, Juan Marugan2, Anton Simeonov2, Reuben S Harris3,4,5,7, Rahul M Kohli6, Patricia J Gearhart1.
Abstract
Activation-induced deaminase (AID) not only mutates DNA within the immunoglobulin loci to generate antibody diversity, but it also promotes development of B cell lymphomas. To tame this mutagen, we performed a quantitative high-throughput screen of over 90 000 compounds to see if AID activity could be mitigated. The enzymatic activity was assessed in biochemical assays to detect cytosine deamination and in cellular assays to measure class switch recombination. Three compounds showed promise via inhibition of switching in a transformed B cell line and in murine splenic B cells. These compounds have similar chemical structures, which suggests a shared mechanism of action. Importantly, the inhibitors blocked AID, but not a related cytosine DNA deaminase, APOBEC3B. We further determined that AID was continually expressed for several days after B cell activation to induce switching. This first report of small molecules that inhibit AID can be used to gain regulatory control over base editors.Entities:
Year: 2021 PMID: 34151211 PMCID: PMC8205235 DOI: 10.1021/acsptsci.1c00064
Source DB: PubMed Journal: ACS Pharmacol Transl Sci ISSN: 2575-9108