Conformational Flexibility in Calcitonin: the Dynamic Properties of Human and Salmon Calcitonin in Solution

Overview

Journal J Biomol NMR

Publisher Springer

Specialties Molecular Biology
Nuclear Medicine

Date 1999 Mar 10

PMID 10070757

Citations 12

Authors

P Amodeo

A Motta

G Strazzullo

M A Castiglione Morelli

Affiliations

Soon will be listed here.

Abstract

We have studied the dynamic properties of human (h) and salmon (s) calcitonin (CT) in solution. For both hormones, distance geometry in torsion-angle space has been used to generate three-dimensional structures consistent with NMR data obtained in sodium dodecyl sulfate micelles. For sCT and hCT we used, respectively, 356 and 275 interproton distances together with hydrogen-bonds as restraints. To better characterize their flexibility and dynamic properties two fully unrestrained 1100-ps molecular dynamics (MD) simulations in methanol were performed on the lowest-energy structures of both hormones. Statistical analyses of average geometric parameters and of their fluctuations performed in the last 1000 ps of the MD run show typical helical values for residues 9-19 of sCT during the whole trajectory. For hCT a shorter helix was observed involving residues 13-21, with a constant helical region in the range 13-19. Angular order parameters S(phi) and S(psi) indicate that hCT exhibits a higher flexibility, distributed along the whole chain, including the helix, while the only flexible amino acid residues in sCT connect three well-defined domains. Finally, our study shows that simulated annealing in torsion-angle space can efficiently be extended to NMR-based three-dimensional structure calculations of helical polypeptides. Furthermore, provided that a sufficient number of NMR restraints describes the system, the method allows the detection of equilibria in solution. This identification occurs through the generation of 'spurious' high-energy structures, which, for right-handed alpha-helices, are likely to be represented by left-handed alpha-helices.

Citing Articles

Molecular Insights into the Effects of F16L and F19L Substitutions on the Conformation and Aggregation Dynamics of Human Calcitonin.

Huang F, Huang J, Yan J, Liu Y, Lian J, Sun Q J Chem Inf Model. 2024; 64(11):4500-4510.

PMID: 38745385 PMC: 11349047. DOI: 10.1021/acs.jcim.4c00553.

Unraveling the underlying mechanisms of reduced amyloidogenic properties in human calcitonin via double mutations.

Chang Y, Pan P, Tu L Protein Sci. 2024; 33(4):e4952.

PMID: 38501491 PMC: 10949316. DOI: 10.1002/pro.4952.

Deciphering the influence of Y12L and N17H substitutions on the conformation and oligomerization of human calcitonin.

Yan J, Wang Y, Fan X, Zou Y, Ding F, Huang F Soft Matter. 2024; 20(3):693-703.

PMID: 38164981 PMC: 10845004. DOI: 10.1039/d3sm01332d.

Investigating the inhibitory property of DM hCT on hCT fibrillization via its relevant peptide fragments.

Chuang Y, Chang Y, Tu L Protein Sci. 2023; 32(8):e4711.

PMID: 37354016 PMC: 10360389. DOI: 10.1002/pro.4711.

Structural Perturbation of Monomers Determines the Amyloid Aggregation Propensity of Calcitonin Variants.

Liu Y, Wang Y, Zhang Y, Zou Y, Wei G, Ding F J Chem Inf Model. 2022; 63(1):308-320.

PMID: 36456917 PMC: 9839651. DOI: 10.1021/acs.jcim.2c01202.

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