3b32 Citations

Thermodynamics and conformational change governing domain-domain interactions of calmodulin.

O'Donnell SE, Newman RA, Witt TJ, Hultman R, Froehlig JR, Christensen AP, Shea MA
Methods Enzymol 466 503-26 (2009)
Cited: 11 times
EuropePMC logo PMID: 21609874

Abstract

Calmodulin (CaM) is a small (148 amino acid), ubiquitously expressed eukaryotic protein essential for Ca(2+) regulation and signaling. This highly acidic polypeptide (pI<4) has two homologous domains (N and C), each consisting of two EF-hand Ca(2+)-binding sites. Despite significant homology, the domains have intrinsic differences in their Ca(2+)-binding properties and separable roles in regulating physiological targets such as kinases and ion channels. In mammalian full-length CaM, sites III and IV in the C-domain bind Ca(2+) cooperatively with ~10-fold higher affinity than sites I and II in the N-domain. However, the difference is only twofold when CaM is severed at residue 75, indicating that anticooperative interactions occur in full-length CaM. The Ca(2+)-binding properties of sites I and II are regulated by several factors including the interplay of interdomain linker residues far from the binding sites. Our prior thermodynamic studies showed that these residues inhibit thermal denaturation and decrease calcium affinity. Based on high-resolution structures and NMR spectra, there appear to be interactions between charged residues in the sequence 75-80 and those near the amino terminus of CaM. To explore electrostatic contributions to interdomain interactions in CaM, KCl was used to perturb the Ca(2+)-binding affinity, thermal stability, and hydrodynamic size of a nested set of recombinant mammalian CaM (rCaM) fragments terminating at residues 75, 80, 85, or 90. Potassium chloride is known to decrease Ca(2+)-binding affinity of full-length CaM. It may act directly by competition with acidic side chains that chelate Ca(2+) in the binding sites, and indirectly elsewhere in the molecule by changing tertiary constraints and conformation. In all proteins studied, KCl decreased Ca(2+)-affinity, decreased Stokes radius, and increased thermal stability, but not monotonically. Crystallographic structures of Ca(2+)-saturated rCaM(1-75) (3B32.pdb) and rCaM(1-90) (3IFK.pdb) were determined, offering cautionary notes about the effect of packing interactions on flexible linkers. This chapter describes an array of methods for characterizing system-specific thermodynamic properties that in concert govern structure and function.

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  2. Pathomimetic avatars reveal divergent roles of microenvironment in invasive transition of ductal carcinoma in situ. Sameni M, Cavallo-Medved D, Franco OE, Chalasani A, Ji K, Aggarwal N, Anbalagan A, Chen X, Mattingly RR, Hayward SW, Sloane BF. Breast Cancer Res 19 56 (2017)
  3. Thermodynamics and conformational change governing domain-domain interactions of calmodulin. O'Donnell SE, Newman RA, Witt TJ, Hultman R, Froehlig JR, Christensen AP, Shea MA. Methods Enzymol 466 503-526 (2009)


Articles citing this publication (8)

  1. Effect of Ca2+ on the promiscuous target-protein binding of calmodulin. Westerlund AM, Delemotte L. PLoS Comput Biol 14 e1006072 (2018)
  2. Protein Conformational Changes Are Detected and Resolved Site Specifically by Second-Harmonic Generation. Moree B, Connell K, Mortensen RB, Liu CT, Benkovic SJ, Salafsky J. Biophys J 109 806-815 (2015)
  3. FH8--a small EF-hand protein from Fasciola hepatica. Fraga H, Faria TQ, Pinto F, Almeida A, Brito RM, Damas AM. FEBS J 277 5072-5085 (2010)
  4. The Neuronal Calcium Sensor protein Acrocalcin: a potential target of calmodulin regulation during development in the coral Acropora millepora. Reyes-Bermudez A, Miller DJ, Sprungala S. PLoS One 7 e51689 (2012)
  5. Comparing allosteric transitions in the domains of calmodulin through coarse-grained simulations. Nandigrami P, Portman JJ. J Chem Phys 144 105102 (2016)
  6. Electron paramagnetic resonance spectroscopy of nitroxide-labeled calmodulin. Bowman PB, Puett D. Protein J 33 267-277 (2014)
  7. Improved Synthesis of 2-Trifluoromethyl-10-aminopropylphenothiazine: Making 2-Trifluoromethyl-10-aminopropylphenothiazine Readily Available for Calmodulin Purification. Johnson JW, Cain KW, Dunlap TB, Naumiec GR. ACS Omega 3 16309-16313 (2018)
  8. Mapping site-specific changes that affect stability of the N-terminal domain of calmodulin. Krause ME, Martin TT, Laurence JS. Mol Pharm 9 734-743 (2012)


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