RESUMO
Nanoplastic-lipid interaction is vital to understanding the nanoscale mechanism of plastic adsorption and aggregation on a lipid membrane surface. However, a single-particle mechanistic picture of the nanoplastic transport process on a lipid surface remains unclear. Here, we report a salt-dependent non-Gaussian transport mechanism of polystyrene particles on a supported 1-palmitoyl-2-oleoyl-glycero-3-phosphocholine (POPC) lipid bilayer surface. Particle stickiness on the POPC surface increases with salt concentration, where the particles stay longer at the surface and diffuse to shorter distances. Additionally, a non-Gaussian diffusion state dominates the transport process at high salt concentrations. Our current study provides insight into the transport mechanism of polystyrene (PS) particles on supported lipid membranes, which is essential to understanding fundamental questions regarding the adsorption mechanisms of nanoplastics on lipid surfaces.
Assuntos
Bicamadas Lipídicas , Fosfatidilcolinas , Poliestirenos , Cloreto de Sódio , Bicamadas Lipídicas/química , Fosfatidilcolinas/química , Poliestirenos/química , Cloreto de Sódio/química , Propriedades de Superfície , Adsorção , DifusãoRESUMO
Restriction endonucleases (REs) cleave DNA at specific site in presence of Mg2+ ion. Experiments further emphasize the role of hydration in metal ion specificity and sequence specificity of DNA cleavage. However, the relation between hydration and specificity has not been understood till date. This leads us to study via all-atom molecular dynamics (MD) simulations how the hydration around the scissile phosphate group changes in presence of Mg2+ and Ca2+ and depend on the DNA sequence. We observe the least number of hydrogen bonds around the scissile phosphate group in presence of Mg2+ ion. We further find that the hydrogen bonds decrease at the scissile phosphate on mutating one base pair in the cleavage region of the DNA in Mg2+ loaded EcoRI-DNA complex. We also perform steered MD simulations and observe that the rate of decrease of fraction of hydrogen bonds is slower in the mutated complex than the unmutated complex.
Assuntos
DNA , Silício , Desoxirribonuclease EcoRI/química , Desoxirribonuclease EcoRI/genética , Desoxirribonuclease EcoRI/metabolismo , Sítios de Ligação , Sequência de Bases , DNA/química , Fosfatos , Especificidade por Substrato , CinéticaRESUMO
ZnO is bio-safe and hence, may be a potential candidate for direct use as a glucose sensor. This requires an understanding of the interaction of glucose with four common surfaces, (101Ì0), (112Ì0), (0001) and (0001Ì) of ZnO. We carry out molecular dynamics (MD) simulations enhanced by umbrella sampling of a glucose molecule in a solvent over a hydrated ZnO slab. The slab is obtained by quantum mechanical optimization. We observe that hydration layers formed above the surfaces affect the approach of glucose to the surfaces. Potential of mean force (PMF) calculations show that the (101Ì0) surface shows the strongest adsorption of adsorption free energy -6.81 kJ mol-1 towards glucose. Thus, we offer a theoretical understanding on the interactions at the nano-bio junction of glucose and ZnO surfaces. Our study suggests that the (101Ì0) surface may be used to fabricate a direct glucose sensor.
RESUMO
Restriction endonucleases protect bacterial cells against bacteriophage infection by cleaving the incoming foreign DNA into fragments. In presence of Mg2+ ions, EcoRV is able to cleave the DNA but not in presence of Ca2+ , although the protein binds to DNA in presence of both metal ions. We make an attempt to understand this difference using conformational thermodynamics. We calculate the changes in conformational free energy and entropy of conformational degrees of freedom, like DNA base pair steps and dihedral angles of protein residues in Mg2+ (A)-EcoRV-DNA complex compared to Ca2+ (S)-EcoRV-DNA complex using all-atom molecular dynamics (MD) trajectories of the complexes. We find that despite conformational stability and order in both complexes, the individual degrees of freedom behave differently in the presence of two different metal ions. The base pairs in cleavage region are highly disordered in Ca2+ (S)-EcoRV-DNA compared to Mg2+ (A)-EcoRV-DNA. One of the acidic residues ASP90, coordinating to the metal ion in the vicinity of the cleavage site, is conformationally destabilized and disordered, while basic residue LYS92 gets conformational stability and order in Ca2+ (S) bound complex than in Mg2+ (A) bound complex. The enhanced fluctuations hinder placement of the metal ion in the vicinity of the scissile phosphate of DNA. Similar loss of conformational stability and order in the cleavage region is observed by the replacement of the metal ion. Considering the placement of the metal ion near scissile phosphate as requirement for cleavage action, our results suggest that the changes in conformational stability and order of the base pair steps and the protein residues lead to cofactor sensitivity of the enzyme. Our method based on fluctuations of microscopic conformational variables can be applied to understand enzyme activities in other protein-DNA systems.
