The interplay between hemostasis and immune response in biomaterial development for osteogenesis

, Ma, Yaping, , , Zhang, Yi, Lu, Haiping, Zhao, Qingyu, Cao, Jin, Wu, Chengtie, Wang, Xin, & (2022) The interplay between hemostasis and immune response in biomaterial development for osteogenesis. Materials Today, 54, pp. 202-224.

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Description

Treatment of large bone defects, particularly bone non-union, remains a clinical challenge. The gold-standard bone substitute continues to be an autologous bone graft, which is difficult to be replaced with synthetic biomaterials. Considering these aspects, strategies should be formulated to develop advanced materials for functional bone regeneration. Recent studies have revealed that hematoma (the first tissue structure formed at the bone injury site) plays an essential role in bone healing. Hematoma consists of a fibrin clot, infiltrated immune cells, and tissue progenitor cells. It bridges the bone defect and provides a microenvironment for the interplay between hemostasis and the immune systems. Moreover, an ideal fibrin structure with appropriate fiber thickness and density could facilitate bone regeneration, and biomaterial implantation could affect fibrin structure. Meanwhile, immunoregulation plays an essential role in bone healing. In particular, materials inducing a shift from inflammatory to anti-inflammatory phenotypes in immune cells show enhanced osteoinductivity. More importantly, the interaction between hemostasis and the immune system should play a vital part in bone regeneration by determining both fibrin structure and bone healing microenvironment. Coagulants-triggered inflammation could, in turn, facilitate coagulation cascades, which form positive feedback to amplify both processes. Meanwhile, anti-coagulants neutralize coagulation and inhibit inflammation and thereby control the coagulation and inflammation to prevent thrombosis. The balance between coagulation–inflammation and anti-coagulation–anti-inflammation plays a determinant role in the fibrin structure and fibrinolysis process. The inflammation could be “quenched” gradually during this process, whereby a highly effective microenvironment for bone regeneration can be generated. Presently, there are limited biomaterial studies targeting the bone-healing hematoma, particularly the hemostasis–immune interplay. Considering this, this review summarizes the current materials for hemostasis and immunomodulation, and the critical role of the hemostasis–immune interaction in bone regeneration. It also proposes potential strategies to develop materials with the capacity to generate a highly effective bone healing hematoma, by modulating the hemostasis–immune interplay to maintain the balance between coagulation–inflammation and anti-coagulation–anti-inflammation.

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ID Code: 228951
Item Type: Contribution to Journal (Review article)
Refereed: Yes
ORCID iD:
Xiao, Lanorcid.org/0000-0002-5227-9352
Crawford, Rossorcid.org/0000-0001-6079-1316
Mendhi, Jayantiorcid.org/0000-0003-0696-011X
Xiao, Yinorcid.org/0000-0003-1785-3491
Additional Information: Funding Information: This work was supported by the NHMRC Idea Grant (APP2000647) of Australia, JRC (2019) from Queensland Department of Environment and Science, ITI Research Grant 1260_2017, Young Researcher Grant (19-066) from the Osteology Foundation, Switzerland, QUT Centre for Biomedical Technologies ECR/MCR grant scheme 2021, the National Natural Science Foundation of China (Grant no. 31960209, 82060620 and 31760266), the Training Project for High-Level Innovative Talents in Guizhou Province (Grant no. fzc20200612), a Project from Guizhou Science and Technology Fund (Grant no. (2020)1Y093), and a Project from Zunyi Science and Technology Fund (Grant no. Zun Shi Ke He HZ Zi 2021-40).
Measurements or Duration: 23 pages
Keywords: Bone regeneration, Bone substitutive biomaterials, Coagulation, Fibrinolysis, Osteoimmunomodulation
DOI: 10.1016/j.mattod.2022.02.010
ISSN: 1369-7021
Pure ID: 107182463
Divisions: Current > Research Centres > Centre for Biomedical Technologies
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Current > QUT Faculties and Divisions > Faculty of Engineering
Current > Schools > School of Mechanical, Medical & Process Engineering
Funding Information: This work was supported by the NHMRC Idea Grant (APP2000647) of Australia, JRC (2019) from Queensland Department of Environment and Science, ITI Research Grant 1260_2017, Young Researcher Grant (19-066) from the Osteology Foundation, Switzerland, QUT Centre for Biomedical Technologies ECR/MCR grant scheme 2021, the National Natural Science Foundation of China (Grant no. 31960209, 82060620 and 31760266), the Training Project for High-Level Innovative Talents in Guizhou Province (Grant no. fzc20200612), a Project from Guizhou Science and Technology Fund (Grant no. (2020)1Y093), and a Project from Zunyi Science and Technology Fund (Grant no. Zun Shi Ke He HZ Zi 2021-40).
Funding:
Copyright Owner: Crown Copyright
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Deposited On: 22 Mar 2022 04:49
Last Modified: 12 Jul 2024 07:36