Modeling periodontal host-microbe interactions using vascularized gingival connective tissue equivalents

Hardik Makkar; Chwee Teck Lim; Kai Soo Tan; Gopu Sriram

doi:10.1088/1758-5090/ace935

Modeling periodontal host-microbe interactions using vascularized gingival connective tissue equivalents

Biofabrication. 2023 Aug 2;15(4). doi: 10.1088/1758-5090/ace935.

Authors

Hardik Makkar¹, Chwee Teck Lim^{2

3

4}, Kai Soo Tan^{1

5}, Gopu Sriram^{1

5}

Affiliations

¹ Faculty of Dentistry, National University of Singapore, Singapore 119085, Singapore.
² Institute for Health Innovation and Technology (iHealthtech), National University of Singapore, Singapore 117599, Singapore.
³ Department of Biomedical Engineering, National University of Singapore, Singapore 117583, Singapore.
⁴ Mechanobiology Institute, National University of Singapore, Singapore 117411, Singapore.
⁵ ORCHIDS: Oral Care Health Innovations and Designs Singapore, National University of Singapore, Singapore 119085, Singapore.

PMID: 37473752
DOI: 10.1088/1758-5090/ace935

Abstract

Gingival connective tissue and its vasculature play a crucial role in the host's immune response against the periodontal microbiome and serve as a bridge between the oral and systemic environments. However, there is a lack of representative models that mimic the complex features of vascularized gingival connective tissue and its interaction with the periodontal microbiome, hindering our understanding of periodontal health and disease. Towards this pursuit, we present the characterization of vascularized gingival connective tissue equivalents (CTEs) as a model to study the interactions between oral biofilm colonizers and gingival tissues in healthy and diseased states. Whole-mount immunolabeling and label-free confocal reflectance microscopy of human fibrin-based matrix embedded with gingival fibroblasts and microvascular endothelial cells demonstrated the generation of bi-cellular vascularized gingival CTEs. Next, we investigated the response of the vascularized gingival CTEs to early, intermediate, and late oral biofilm colonizers. Despite colonization, the early colonizers did not elicit any significant change in the production of the cytokines and chemokines by the CTEs representative of the commensal and homeostatic state. In contrast, intermediate and late colonizers representing a transition to a diseased state exhibited connective tissue and vascular invasion, and elicited a differential immune response accompanied by increased monocyte migration. The culture supernatants produced by the vascularized gingival CTEs in response to early and intermediate colonizers polarized macrophages towards an immunomodulatory M2-like phenotype which activates and protects the host, while the late colonizers polarized towards a pro-inflammatory M1-like phenotype. Lastly,in silicoanalysis showed a high strength of associations between the proteins and transcripts investigated with periodontitis and vascular diseases. In conclusion, the vascularized gingival CTEs provide a biomimeticin vitroplatform to study host-microbiome interactions and innate immune response in periodontal health and diseased states, which potentially paves the way toward the development and assessment of novel periodontal therapeutics.

Keywords: 3D culture; connective tissue; gingiva; host-microbe interaction; innate immune response; microvasculature; periodontitis.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Connective Tissue / metabolism
Endothelial Cells* / metabolism
Gingiva / metabolism
Host Microbial Interactions
Humans
Periodontitis* / metabolism