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An intrinsically disordered motif mediates diverse actions of monomeric C-reactive protein

  • Hai Yun Li
  • , Jing Wang
  • , Fan Meng
  • , Zhe Kun Jia
  • , Yang Su
  • , Qi Feng Bai
  • , Ling Ling Lv
  • , Fu Rong Ma
  • , Lawrence A. Potempa
  • , Yong Bin Yan
  • , Shang Rong Ji
  • , Yi Wu
  • Tsinghua University
  • Lanzhou University
  • Roosevelt University Chicago

科研成果: 期刊稿件文章同行评审

53 引用 (Scopus)

摘要

Most proinflammatory actions of C-reactive protein (CRP) are only expressed following dissociation of its native pentameric assembly into monomeric form (mCRP). However, little is known about what underlies the greatly enhanced activities of mCRP. Here we show that a single sequence motif, i.e. cholesterol binding sequence (CBS; a.a. 35-47), is responsible for mediating the interactions of mCRP with diverse ligands. The binding of mCRP to lipoprotein component ApoB, to complement component C1q, to extracellular matrix components fibronectin and collagen, to blood coagulation component fibrinogen, and to membrane lipid component cholesterol, are all found to be markedly inhibited by the synthetic CBS peptide but not by other CRP sequences tested. Likewise, mutating CBS in mCRP also greatly impairs these interactions. Functional experiments further reveal that CBS peptide significantly reduces the effects of mCRP on activation of endothelial cells in vitro and on acute induction of IL-6 in mice. The potency and specificity of CBS are critically determined by the N-terminal residues Cys-36, Leu-37, and His-38; while the versatility of CBS appears to originate from its intrinsically disordered conformation polymorphism. Together, these data unexpectedly identify CBS as the major recognition site of mCRP and suggest that this motif may be exploited to tune the proinflammatory actions of mCRP.

源语言英语
页(从-至)8795-8804
页数10
期刊Journal of Biological Chemistry
291
16
DOI
出版状态已出版 - 15 4月 2016

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