Structural Dynamics of Human Telomeric G-Quadruplex Loops Studied by Molecular Dynamics Simulations

Zhu, Hong; Xiao, Shiyan; Liang, Haojun

doi:10.1371/journal.pone.0071380

Cited by 30 publications

(35 citation statements)

References 46 publications

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“…In MD simulation, parmbsc0 combined FF99SB force field within AMBER12 software was applied, which has been validated for G-quadruplex structures by many nanoseconds state-of-theart molecular dynamics simulations. [24][25][26][27] The system was firstly energy minimized by the steepest descent method for 5000 steps with the AMBER sander module, during which K + and waters were free to move while G-quadruplex was restricted by a harmonic constraint of 100 kcal/mol per A. A following conjugate gradient minimization was then conducted for 5000 steps with no constraint on any component.…”

Section: Molecular Dynamics Simulationmentioning

confidence: 99%

Characterization of potassium binding with human telomeres

Wang

Liu

2015

Clin Exp Pharma Physio

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Human telomeres are G-rich tandem repeats that assume G-quadruplex structures at the ends of chromosomes. Stabilization of telomeric G-quadruplex represents a significant drug target for inhibiting the telomerase activity that is required in about 85% of cancers. Metal ions have been revealed as important stabilizers to DNA G-quadruplexes, but their binding process with human telomeric G-quadruplex remains unclear. In this report, we show that K traverses into the G-tetrads centre of two G-tetrad layers through the half-capped top pathway constructed by the two edge-wise loop bases. The binding is mediated by the electrostatic interactions between K and the nearby bases of G-tetrads. However, direct traverse of K into the interior of G-quadruplex is negatively regulated by the steric hindrance of water molecules. Once K enters the G-quadruplex, stabilization of the in-plane or sandwiched conformation of the telomeric G-quadruplex-K complex is maintained by surrounding water molecules. These findings provide insights into the atomic interactions between K and telomere G-tetrads for targeted drug design.

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Section: Molecular Dynamics Simulationmentioning

confidence: 99%

Characterization of potassium binding with human telomeres

Wang

Liu

2015

Clin Exp Pharma Physio

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“…[1][2][3][4][5][6][7][8][9][10][11] Human telomeres containing tandem repeats of sequence d(TTAGGG) at their extreme 3 0 -end are the complexes of DNA and proteins located at the ends of the chromosome, which play important roles in protecting chromosomes from fusion and degradation. 17,18 Until now, numerous methods have been used to analyze the structure of the human telomeric G-quadruplex in vitro, such as high-resolution solution state NMR, 5,[8][9][10]19 single crystal diffraction, 20 molecular dynamics (MD) simulations, [21][22][23] circular dichroism (CD), 7,22,[24][25][26] fluorescence, 7,27 differential scanning calorimetry (DSC), 28,29 mass spectrometry, 30,31 photon correlation spectroscopy, 32 atomic force microscopy (AFM), [33][34][35] analytical ultracentrifugation (AUC) 7,36-39 and so on. 17,18 Until now, numerous methods have been used to analyze the structure of the human telomeric G-quadruplex in vitro, such as high-resolution solution state NMR, 5,[8][9][10]19 single crystal diffraction, 20 molecular dynamics (MD) simulations, [21]…”

Section: Introductionmentioning

confidence: 99%

The effects of monovalent metal ions on the conformation of human telomere DNA using analytical ultracentrifugation

Gao

2016

Soft Matter

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A human telomere DNA segment (HT-DNA) can fold into a G-quadruplex in the presence of some monovalent cations. These cations can interact with the phosphate groups of the DNA segment and/or with the O6 oxygen atom of guanines, which are called non-specific interactions and specific interactions, respectively. However, until now how these two interactions affect the structure of HT-DNA has not been well understood. In this study, a combination of analytical ultracentrifugation (AUC) and circular dichroism (CD) was used to explore the effects of these two interactions on the structure of a 22-mer single-stranded DNA with a sequence of 5'-AGGG(TTAGGG)3-3'. The results showed that the standard sedimentation coefficient (s20,w) of HT-DNA starts to increase when the concentration of potassium ions (CK(+)) is higher than 10.0 µM due to the formation of a G-quadruplex through specific interactions. Whereas, for a control DNA, a higher CK(+) value of 1.0 mM was needed for increasing s20,w due to non-specific interactions. Moreover, potassium ions could promote the formation of the G-quadruplex much more easily than lithium, sodium and cesium ions, presumably due to its appropriate size in the dehydrated state and easier dehydration. The molar mass of DNA at different cation concentrations was nearly a constant and close to the theoretical value of the molar mass of monomeric HT-DNA, indicating that what we observed is the structural change of individual DNA chains.

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“…Thus, atomistic simulations, able to predict the structural/dynamical properties of nanostructures before experiments, can give useful information concerning the stability of the assembly obtained starting from the predesigned sequences. During the past few years molecular dynamics (MD) atomistic simulations have been successfully used to characterize the structure and the dynamics of Seeman DNA nanostructures, to investigate the properties of a truncated octahedral DNA nano‐cage family, to probe the stability and the dynamical properties of DNA nanocircles, supercoiled DNA structures, or human telomeric G‐quadruplex loops and to investigate the temperature dependent encapsulation mechanism of a DNA nanostructure …”

Section: Introductionmentioning

confidence: 99%

Influence of the single‐strand linker composition on the structural/dynamical properties of a truncated octahedral DNA nano‐cage family

et al. 2014

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The structural/dynamical properties of three truncated octahedral DNA nano-cages composed by identical double helices but single strand linkers with different composition, namely 7 thymidines, 7 adenines, and 7 alternated thymidines and adenines, have been investigated through classical molecular dynamics simulations. Trajectories have been analyzed to investigate the role of the linkers in defining nano-cages stability and flexibility, including possible influence on the internal cages motions. The data indicate that the cages behavior is almost identical and that the structural/dynamical parameters measured along the trajectories are not particularly affected by the presence of different bases. These results demonstrate that the constraints imposed by the nano-structure geometry are the main factor in modulating these properties

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Structural Dynamics of Human Telomeric G-Quadruplex Loops Studied by Molecular Dynamics Simulations

Cited by 30 publications

References 46 publications

Characterization of potassium binding with human telomeres

Characterization of potassium binding with human telomeres

The effects of monovalent metal ions on the conformation of human telomere DNA using analytical ultracentrifugation

Influence of the single‐strand linker composition on the structural/dynamical properties of a truncated octahedral DNA nano‐cage family

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