Modulation of yeast F-actin structure by a mutation in the nucleotide-binding cleft

Albina Orlova; Xin Chen; Peter A Rubenstein; Edward H Egelman

doi:10.1006/jmbi.1997.1163

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Modulation of yeast F-actin structure by a mutation in the nucleotide-binding cleft

Journal article

Peer reviewed

Modulation of yeast F-actin structure by a mutation in the nucleotide-binding cleft

Albina Orlova, Xin Chen, Peter A Rubenstein and Edward H Egelman

Journal of molecular biology, Vol.271(2), pp.235-243

1997

DOI: 10.1006/jmbi.1997.1163

PMID: 9268655

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Abstract

Although the actin sequence is very highly conserved across evolution, tissue-specific expression of different isoforms in high eukaryotes suggests that different isoforms carry out different functions. However, little information exists about either the differences in filaments made from different actins or the effects on filament structure caused by the various mutations in actin that have been introduced to gain insight into actin function. Using electron microscopy and three-dimensional reconstruction, we have studied the differences in the filaments made by yeast and rabbit skeletal muscle actin, two proteins with 88% homologous sequences, and we have assessed the changes in filament structure caused by the introduction of the S14A mutation into yeast actin. Elimination of the S14 hydroxyl group, assumed to bind to the γ-phosphate of actin-bound ATP, results in a 40 to 60-fold decrease in actin’s affinity for ATP. We show that yeast actin displays less extensive contacts between the two long-pitch helical strands than does muscle actin, and displays the large cooperativity within filaments previously observed for muscle actin. Finally, we demonstrate that the S14A mutation narrows the cleft between the two lobes of the actin subunit and strengthens the inter-strand connections in F-actin.

Electron Microscopy

actin

polymers

image analysis

yeast

Details

Title: Subtitle: Modulation of yeast F-actin structure by a mutation in the nucleotide-binding cleft
Creators: Albina Orlova - Department of Cell Biology and Neuroanatomy, University of Minnesota Medical School Minneapolis, MN 55455, USA
Xin Chen - Department of Biochemistry University of Iowa College of Medicine, Iowa City IA 52242-1104, USA
Peter A Rubenstein - Department of Biochemistry University of Iowa College of Medicine, Iowa City IA 52242-1104, USA
Edward H Egelman - Department of Cell Biology and Neuroanatomy, University of Minnesota Medical School Minneapolis, MN 55455, USA
Resource Type: Journal article
Publication Details: Journal of molecular biology, Vol.271(2), pp.235-243
DOI: 10.1006/jmbi.1997.1163
PMID: 9268655
NLM abbreviation: J Mol Biol
ISSN: 0022-2836
eISSN: 1089-8638
Publisher: Elsevier Ltd
Language: English
Date published: 1997
Academic Unit: Stead Family Department of Pediatrics; Biochemistry and Molecular Biology; Internal Medicine
Record Identifier: 9984024410302771

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