Structure–activity relationship studies on a series of Boc-indole derivatives as LXR agonists are described. Compound 1 was identified as an LXR agonist through structure-based virtual screening followed by high-throughput gene profiling. Replacement of the indan linker portion in 1 with an open-chain linker resulted in compounds with similar or improved in vitro potency and cellular functional activity. The Boc group at the N-1 position of the ...
![N-[2-(4-bromophenyl)ethyl]benzenesulfonamide结构式](https://image.chemsrc.com/caspic/123/105938-45-2.png)