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西亚试剂:Crystal structure of human mitoNEET reveals distinct groups

发布时间:2025-12-04

Crystal structure of human mitoNEET reveals distinct groups of iron–sulfur proteins

( 2Fe-2S | thiazolidinediones | mitochondria )

Jinzhong Lin *{dagger}, Tao Zhou *, Keqiong Ye {dagger}{ddagger}, and Jinfeng Wang *{ddagger}

*National Laboratory of Biomacromolecules, Center for Structural and Molecular Biology, Institute of Biophysics, Chinese Academy of Sciences, Beijing 100101, China; and {dagger}National Institute of Biological Sciences, Beijing 102206, China

 

Edited by Richard H. Holm, Harvard University, Cambridge, MA, and approved July 15, 2007 (received for review March 16, 2007 )

MitoNEET is a protein of unknown function present in the mitochondrial membrane that was recently shown to bind specifically the antidiabetic drug pioglizatone. Here, we report the crystal structure of the soluble domain (residues 32–108) of human mitoNEET at 1.8-Å resolution. The structure reveals an intertwined homodimer, and each subunit was observed to bind a [2Fe-2S] cluster. The [2Fe-2S] ligation pattern of three cysteines and one histidine differs from the known pattern of four cysteines in most cases or two cysteines and two histidines as observed in Rieske proteins. The [2Fe-2S] cluster is packed in a modular structure formed by 17 consecutive residues. The cluster-binding motif is conserved in at least seven distinct groups of proteins from bacteria, archaea, and eukaryotes, which show a consensus sequence of (hb)-C-X1-C-X2-(S/T)-X3-P-(hb)-C-D-X2-H, where hb represents a hydrophobic residue; we term this a CCCH-type [2Fe-2S] binding motif. The nine conserved residues in the motif contribute to iron ligation and structure stabilization. UV-visible absorption spectra indicated that mitoNEET can exist in oxidized and reduced states. Our study suggests an electron transfer function for mitoNEET and for other proteins containing the CCCH motif.

 

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