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C-axis-oriented platelets of crystalline hydroxyapatite in biomimetic intrafibrillar mineralization of polydopamine-functionalized collagen type Iopen access

Authors
Amornkitbamrung, U.[Amornkitbamrung, U.]In, Y.[In, Y.]Wang, Z.[Wang, Z.]Song, J.[Song, J.]Oh, S.H.[Oh, S.H.]Hong, M.-H.[Hong, M.-H.]Shin, H.[Shin, H.]
Issue Date
15-Feb-2022
Publisher
American Chemical Society
Citation
ACS Omega, v.7, no.6, pp.4821 - 4831
Indexed
SCIE
SCOPUS
Journal Title
ACS Omega
Volume
7
Number
6
Start Page
4821
End Page
4831
URI
https://scholarworks.bwise.kr/skku/handle/2021.sw.skku/97132
DOI
10.1021/acsomega.1c05198
ISSN
2470-1343
Abstract
Mineralized collagen fibrils are important basic building blocks of calcified tissues, such as bone and dentin. Polydopamine (PDA) can introduce functional groups, i.e., hydroxyl and amine groups, on the surfaces of type I collagen (Col-I) as possible nucleation sites of calcium phosphate (CaP) crystallization. Molecular bindings in between PDA and Col-I fibrils (Col-PDA) have been found to significantly reduce the interfacial energy. The wetting effect, mainly hydrophilicity due to the functional groups, escalates the degree of mineralization. The assembly of Col-I molecules into fibrils was initiated at the designated number of collagenous molecules and PDA. In contrast to the infiltration of amorphous calcium phosphate (ACP) precursors into the Col-I matrix by polyaspartic acid (pAsp), this collagen assembly process allows nucleation and ACP to exist in advance by PDA in the intrafibrillar matrix. PDA bound to specific sites, i.e., gap and overlap zones, by the regular arrangement of Col-I fibrils enhanced ACP nucleation and thus mineralization. As a result, the c-axis-oriented platelets of crystalline hydroxyapatite in the Col-I fibril matrix were observed in the enhanced mineralization through PDA functionalization. © 2022 The Authors. Published by American Chemical Society
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