| Literature DB >> 30981691 |
Renren Bai1, Xiaokang Jie2, Jian Sun2, Zhongxing Liang3, Younghyoun Yoon3, Amber Feng3, Yoonhyeun Oum3, Wenyan Yu2, Rui Wu2, Bin Sun4, Eric Salgado3, Yuanyuan Xie5, Hyunsuk Shim6.
Abstract
The CXCR4/CXCL12 axis plays prominent roles in tumor metastasis and inflammation. CXCR4 has been shown to be involved in a variety of inflammation-related diseases. Therefore, CXCR4 is a promising potential target to develop novel anti-inflammatory agents. Taking our previously discovered CXCR4 modulator RB-108 as the lead compound, a series of derivatives were synthesized structurally modifying and optimizing the amide and sulfamide side chains. The derivatives successfully maintained potent CXCR4 binding affinity. Furthermore, compounds IIb, IIc, IIIg, IIIj, and IIIm were all efficacious in inhibiting the invasion of CXCR4-positive cells, displaying a much more potent effect than the lead compound RB-108. Notably, compound IIIm significantly decreased carrageenan-induced swollen volume and paw thickness in a mouse paw edema model. More importantly, IIIm exhibited satisfying PK profiles with a half-life of 4.77 h in an SD rat model. In summary, we have developed compound IIIm as a new candidate for further investigation based on the lead compound RB-108.Entities:
Keywords: Anti-inflammation; CXCR4 modulators; Inflammatory cell recruitment; RB-108; Structural modification
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Year: 2019 PMID: 30981691 PMCID: PMC6488424 DOI: 10.1016/j.ejmech.2019.03.065
Source DB: PubMed Journal: Eur J Med Chem ISSN: 0223-5234 Impact factor: 6.514