4.7 Article

Macropore Regulation of Hydroxyapatite Osteoinduction via Microfluidic Pathway

Journal

Publisher

MDPI
DOI: 10.3390/ijms231911459

Keywords

calcium phosphate ceramics; macropore structure; osteoinduction; microfluidic pathway; finite element analysis

Funding

  1. National Key Research and Development Program of China [2016YFC1102000]
  2. Science and Technology Innovation Seedling Project of Sichuan Province, China [2021057]
  3. Fundamental Research Funds for the Central Universities [2682021ZTPY003]
  4. Sichuan Science and Technology Program [21MZGC0218]
  5. Degree and graduate Education and teaching Reform Project of SWJTU [YJG5-2022-Y018]

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This study investigated the effect of macropore size and shape on the osteoinductivity of hydroxyapatite ceramics scaffolds. The results showed that scaffolds with spherical macropores and larger pore sizes had higher new bone production and more uniform new bone distribution. Additionally, the mechanical load of the host tissue was found to play a key role in the microfluidic pathway mechanism.
Macroporous characteristics have been shown to play a key role in the osteoinductivity of hydroxyapatite ceramics, but the physics underlying the new bone formation and distribution in such scaffolds still remain elusive. The work here has emphasized the osteoinductive capacity of porous hydroxyapatite scaffolds containing different macroporous sizes (200-400 mu m, 1200-1500 mu m) and geometries (star shape, spherical shape). The assumption is that both the size and shape of a macropore structure may affect the microfluidic pathways in the scaffolds, which results in the different bone formations and distribution. Herein, a mathematical model and an animal experiment were proposed to support this hypothesis. The results showed that the porous scaffolds with the spherical macropores and large pore sizes (1200-1500 mu m) had higher new bone production and more uniform new bone distribution than others. A finite element analysis suggested that the macropore shape affected the distribution of the medium-high velocity flow field, while the macropore size effected microfluid speed and the value of the shear stress in the scaffolds. Additionally, the result of scaffolds implanted into the dorsal muscle having a higher new bone mass than the abdominal cavity suggested that the mechanical load of the host tissue could play a key role in the microfluidic pathway mechanism. All these findings suggested that the osteoinduction of these scaffolds depends on both the microfluid velocity and shear stress generated by the macropore size and shape. This study, therefore, provides new insights into the inherent osteoinductive mechanisms of bioceramics, and may offer clues toward a rational design of bioceramic scaffolds with improved osteoinductivity.

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