Literature DB >> 23334161

Conformational change and human cytochrome c function: mutation of residue 41 modulates caspase activation and destabilizes Met-80 coordination.

Tracy M Josephs1, Matthew D Liptak, Gillian Hughes, Alexandra Lo, Rebecca M Smith, Sigurd M Wilbanks, Kara L Bren, Elizabeth C Ledgerwood.   

Abstract

Cytochrome c is a highly conserved protein, with 20 residues identical in all eukaryotic cytochromes c. Gly-41 is one of these invariant residues, and is the position of the only reported naturally occurring mutation in cytochrome c (human G41S). The basis, if any, for the conservation of Gly-41 is unknown. The mutation of Gly-41 to Ser enhances the apoptotic activity of cytochrome c without altering its role in mitochondrial electron transport. Here we have studied additional residue 41 variants and determined their effects on cytochrome c functions and conformation. A G41T mutation decreased the ability of cytochrome c to induce caspase activation and decreased the redox potential, whereas a G41A mutation had no impact on caspase induction but the redox potential increased. All residue 41 variants decreased the pK (a) of a structural transition of oxidized cytochrome c to the alkaline conformation, and this correlated with a destabilization of the interaction of Met-80 with the heme iron(III) at physiological pH. In reduced cytochrome c the G41T and G41S mutations had distinct effects on a network of hydrogen bonds involving Met-80, and in G41T the conformational mobility of two Ω-loops was altered. These results suggest the impact of residue 41 on the conformation of cytochrome c influences its ability to act in both of its physiological roles, electron transport and caspase activation.

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Year:  2013        PMID: 23334161      PMCID: PMC3582831          DOI: 10.1007/s00775-012-0973-1

Source DB:  PubMed          Journal:  J Biol Inorg Chem        ISSN: 0949-8257            Impact factor:   3.358


  48 in total

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5.  The Human Cytochrome c Domain-Swapped Dimer Facilitates Tight Regulation of Intrinsic Apoptosis.

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Authors:  Shiloh M Nold; Haotian Lei; Tung-Chung Mou; Bruce E Bowler
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7.  Disruption of cytochrome c heme coordination is responsible for mitochondrial injury during ischemia.

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8.  Disruption of a hydrogen bond network in human versus spider monkey cytochrome c affects heme crevice stability.

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