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Crystallography-guided discovery of carbazole-based retinoic acid-related orphan receptor gamma-t (RORγt) modulators: insights into different protein behaviors with “short” and “long” inverse agonists

  • Ming cheng Yu
  • , Feng Yang
  • , Xiao yu Ding
  • , Nan nan Sun
  • , Zheng yuan Jiang
  • , Ya fei Huang
  • , Yu rong Yan
  • , Chen Zhu
  • , Qiong Xie
  • , Zhi feng Chen
  • , Si qi Guo
  • , Hua liang Jiang
  • , Kai xian Chen
  • , Cheng Luo
  • , Xiao min Luo*
  • , Shi jie Chen*
  • , Yong hui Wang*
  • *此作品的通讯作者
  • Fudan University
  • CAS - Shanghai Institute of Materia Medica
  • University of Chinese Academy of Sciences
  • Fudan Zhangjiang Institute

科研成果: 期刊稿件文章同行评审

摘要

A series of 6-substituted carbazole-based retinoic acid-related orphan receptor gamma-t (RORγt) modulators were discovered through 6-position modification guided by insights from the crystallographic profiles of the “short” inverse agonist 6. With the increase in the size of the 6-position substituents, the “short” inverse agonist 6 first reversed its function to agonists and then to “long” inverse agonists. The cocrystal structures of RORγt complexed with the representative “short” inverse agonist 6 (PDB: 6LOB), the agonist 7d (PDB: 6LOA) and the “long” inverse agonist 7h (PDB: 6LO9) were revealed by X-ray analysis. However, minor differences were found in the binding modes of “short” inverse agonist 6 and “long” inverse agonist 7h. To further reveal the molecular mechanisms of different RORγt inverse agonists, we performed molecular dynamics simulations and found that “short” or “long” inverse agonists led to different behaviors of helixes H11, H11’, and H12 of RORγt. The “short” inverse agonist 6 destabilizes H11’ and dislocates H12, while the “long” inverse agonist 7h separates H11 and unwinds H12. The results indicate that the two types of inverse agonists may behave differently in downstream signaling, which may help identify novel inverse agonists with different regulatory mechanisms.

源语言英语
页(从-至)1524-1534
页数11
期刊Acta Pharmacologica Sinica
42
9
DOI
出版状态已出版 - 9月 2021
已对外发布

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