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Revealing Two-State Protein-Protein Interaction of Calmodulin by Single-Molecule Spectroscopy

Journal Article · · Journal of the American Chemical Society, 128(31):10034-10042
DOI:https://doi.org/10.1021/ja057005m· OSTI ID:891118
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We report a single-molecule fluorescence resonance energy transfer (FRET) and polarization study of conformational dynamics of calmodulin (CaM) interacting with a target peptide, C28W of 28 amino-acid oligomer. The C28W peptide represents the essential binding sequence domain of the Ca-ATPase protein interacting with CaM, which is important in cellular signaling for the regulation of energy in metabolism. However, the mechanism of the CaM-C28W recognition complex formation is still unclear. The amino-terminal (N-terminal) domain of the CaM was labeled with a fluorescein-based arsenical hairpin binder (F1AsH) that enables our unambiguously probing the CaM N-terminal target-binding domain motions at a millisecond timescale without convolution of the probe-dye random motions. By analyzing the distribution of FRET efficiency between F1AsH labeled CaM and Texas Red labeled C28W and the polarization fluctuation dynamics and distributions of the CaM N-terminal domain, we reveal slow (at sub-second time scale) binding-unbinding motions of the N-terminal domain of the CaM in CaM-C28W complexes, which is a strong evidence of a two-state binding interaction of CaM-mediated cell signaling.

Research Organization:
Pacific Northwest National Laboratory (PNNL), Richland, WA (US), Environmental Molecular Sciences Laboratory (EMSL)
Sponsoring Organization:
USDOE
DOE Contract Number:
AC05-76RL01830
OSTI ID:
891118
Report Number(s):
PNNL-SA-46564; 6509
Journal Information:
Journal of the American Chemical Society, 128(31):10034-10042, Journal Name: Journal of the American Chemical Society, 128(31):10034-10042
Country of Publication:
United States
Language:
English

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Related Subjects

59 BASIC BIOLOGICAL SCIENCES
BINDERS
CALMODULIN
DISTRIBUTION
EFFICIENCY
ENERGY TRANSFER
Environmental Molecular Sciences Laboratory
FLUCTUATIONS
FLUORESCENCE
METABOLISM
PEPTIDES
POLARIZATION
PROTEINS
REGULATIONS
RESONANCE
SPECTROSCOPY
TARGETS