Research output: Contribution to journal › Article › peer-review
Spatiotemporal changes in atomic and molecular architecture of mineralized bone under pathogenic conditions. / Павлычев, Андрей Алексеевич; Брыкалова, Ксения Олеговна; Чёрный, Александр Андреевич; Корнеев, Анатолий Вячеславович; Корнилов, Николай Николаевич.
In: Crystals, Vol. 13, No. 3, 381, 23.02.2023.Research output: Contribution to journal › Article › peer-review
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TY - JOUR
T1 - Spatiotemporal changes in atomic and molecular architecture of mineralized bone under pathogenic conditions
AU - Павлычев, Андрей Алексеевич
AU - Брыкалова, Ксения Олеговна
AU - Чёрный, Александр Андреевич
AU - Корнеев, Анатолий Вячеславович
AU - Корнилов, Николай Николаевич
PY - 2023/2/23
Y1 - 2023/2/23
N2 - Mechanisms responsible for spatiotemporal changes in the atomic-molecular architecture of the human femur in intact and osteoarthritis-affected areas were studied using high-resolution X-ray diffraction and spectroscopic techniques. Comparison of the experimental data demonstrates strong deviations of core electron-binding energies, lattice constants of hydroxyapatite crystal cells, linear sizes of crystallites, and degrees of crystallinity for both intact and osteoarthritic areas. The quantitative values of these characteristics and their standard deviations in each area are measured and presented. A systematic analysis of the site-dependent deviations was carried out within the framework of the 3D superlattice model. It is argued that the main mechanism responsible for the deviations arises primarily as a result of carbonization and catalytic reactions at the mineral-cartilage interface. The impact of the mechanism is enhanced in the vicinities of the area of sclerosed bone, but not inside the area where mechanical loads are maximum. Restoration of the atomic-molecular architecture of mineralized bone in the sclerosis area is revealed. Statistical aspects of the spatiotemporal changes in mineralized bone under pathogenic conditions are discussed.
AB - Mechanisms responsible for spatiotemporal changes in the atomic-molecular architecture of the human femur in intact and osteoarthritis-affected areas were studied using high-resolution X-ray diffraction and spectroscopic techniques. Comparison of the experimental data demonstrates strong deviations of core electron-binding energies, lattice constants of hydroxyapatite crystal cells, linear sizes of crystallites, and degrees of crystallinity for both intact and osteoarthritic areas. The quantitative values of these characteristics and their standard deviations in each area are measured and presented. A systematic analysis of the site-dependent deviations was carried out within the framework of the 3D superlattice model. It is argued that the main mechanism responsible for the deviations arises primarily as a result of carbonization and catalytic reactions at the mineral-cartilage interface. The impact of the mechanism is enhanced in the vicinities of the area of sclerosed bone, but not inside the area where mechanical loads are maximum. Restoration of the atomic-molecular architecture of mineralized bone in the sclerosis area is revealed. Statistical aspects of the spatiotemporal changes in mineralized bone under pathogenic conditions are discussed.
UR - https://www.mendeley.com/catalogue/23f0b53b-7bed-3786-afcb-01be6e17b80a/
U2 - 10.3390/cryst13030381
DO - 10.3390/cryst13030381
M3 - Article
VL - 13
JO - Crystals
JF - Crystals
SN - 2073-4352
IS - 3
M1 - 381
ER -
ID: 103268781