Iron Traffics in Circulation Bound to a Siderocalin (Ngal)-Catechol Complex

نویسندگان

  • Guanhu Bao
  • Matthew Clifton
  • Trisha M. Hoette
  • Kiyoshi Mori
  • Shi-Xian Deng
  • Andong Qiu
  • Melanie Viltard
  • David Williams
  • Neal Paragas
  • Thomas Leete
  • Ritwij Kulkarni
  • Xiangpo Li
  • Belinda Lee
  • Avtandil Kalandadze
  • Adam J. Ratner
  • Juan Carlos Pizarro
  • Kai M. Schmidt-Ott
  • Donald W. Landry
  • Kenneth N. Raymond
  • Roland K. Strong
  • Jonathan Barasch
چکیده

The lipocalins are secreted proteins that bind small organic molecules. Scn-Ngal (also known as neutrophil gelatinase associated lipocalin, siderocalin, lipocalin 2) sequesters bacterial iron chelators, called siderophores, and consequently blocks bacterial growth. However, Scn-Ngal is also prominently expressed in aseptic diseases, implying that it binds additional ligands and serves additional functions. Using chemical screens, crystallography and fluorescence methods, we report that Scn-Ngal binds iron together with a small metabolic product called catechol. The formation of the complex blocked the reactivity of iron and permitted its transport once introduced into circulation in vivo. Scn-Ngal then recycled its iron in endosomes by a pH-sensitive mechanism. As catechols derive from bacterial and mammalian metabolism of dietary compounds, the Scn-Ngal-catechol-Fe(III) complex represents an unforeseen microbial-host interaction, which mimics Scn-Ngal-siderophore interactions but instead traffics iron in aseptic tissues. These results identify an endogenous siderophore, which may link the disparate roles of Scn-Ngal in different diseases.

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عنوان ژورنال:

دوره 6  شماره 

صفحات  -

تاریخ انتشار 2010