Structural basis for oxygen degradation domain selectivity of the HIF prolyl hydroxylases.

Rasheduzzaman Chowdhury,Ivanhoe K. H. Leung,Ya-Min Tian,Martine I. Abboud,Wei Ge,Carmen Domene,François-Xavier Cantrelle,Isabelle Landrieu,Adam P. Hardy,Christopher W. Pugh,Peter J. Ratcliffe,Timothy D. W. Claridge,Christopher J. Schofield

Structural basis for oxygen degradation domain selectivity of the HIF prolyl hydroxylases.

2016

Rasheduzzaman Chowdhury
Ivanhoe K. H. Leung
Ya-Min Tian
Martine I. Abboud
Wei Ge
Carmen Domene
François-Xavier Cantrelle
Isabelle Landrieu
Adam P. Hardy
Christopher W. Pugh
Peter J. Ratcliffe
Timothy D. W. Claridge
Christopher J. Schofield

The response to hypoxia involves multiple genes regulated by the hypoxia inducible transcription factors (HIFs), whose stability is regulated by prolyl hydroxylation. Here the authors provide a molecular basis for the substrate selectivity of the HIF prolyl hydroxylases that can be altered in erythrocytosis and cancer.

Keywords:

Transcription factor
Proline
Hypoxia-Inducible Factor-Proline Dioxygenases
Oxidoreductase
Biochemistry
Hydroxylation
Plasma protein binding
Protein domain
Biology
Hypoxia (medical)
Isozyme
Hypoxia-Inducible Factor 1
Gene isoform

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