Microbe-Dependent Exacerbated Alveolar Bone Destruction in Heterozygous Cherubism Mice

Mizuho Kittaka; Tetsuya Yoshimoto; Collin Schlosser; Mikihito Kajiya; Hidemi Kurihara; Ernst J Reichenberger; Yasuyoshi Ueki

doi:10.1002/jbm4.10352

Microbe-Dependent Exacerbated Alveolar Bone Destruction in Heterozygous Cherubism Mice

JBMR Plus. 2020 Apr 14;4(6):e10352. doi: 10.1002/jbm4.10352. eCollection 2020 Jun.

Authors

Mizuho Kittaka^{1

2}, Tetsuya Yoshimoto^{1

2}, Collin Schlosser³, Mikihito Kajiya⁴, Hidemi Kurihara⁴, Ernst J Reichenberger⁵, Yasuyoshi Ueki^{1

2}

Affiliations

¹ Department of Biomedical Sciences and Comprehensive Care Indiana University School of Dentistry Indianapolis IN USA.
² Indiana Center for Musculoskeletal Health Indiana University School of Medicine Indianapolis IN USA.
³ Department of Orthodontics and Dentofacial Orthopedics University of Missouri-Kansas City, School of Dentistry Kansas City MO USA.
⁴ Department of Periodontal Medicine, Applied Life Sciences Institute of Biomedical & Health Sciences, Graduate School of Biomedical & Health Sciences, Hiroshima University Hiroshima Japan.
⁵ Department of Reconstructive Sciences, School of Dental Medicine University of Connecticut Health Farmington CT USA.

Abstract

Cherubism (OMIM#118400) is a craniofacial disorder characterized by destructive jaw expansion. Gain-of-function mutations in SH3-domain binding protein 2 (SH3BP2) are responsible for this rare disorder. We have previously shown that homozygous knock-in (KI) mice (Sh3bp2 ^KI/KI ) recapitulate human cherubism by developing inflammatory lesions in the jaw. However, it remains unknown why heterozygous KI mice (Sh3bp2 ^KI/+ ) do not recapitulate the excessive jawbone destruction in human cherubism, even though all mutations are heterozygous in humans. We hypothesized that Sh3bp2 ^KI/+ mice need to be challenged for developing exacerbated jawbone destruction and that bacterial stimulation in the oral cavity may be involved in the mechanism. In this study, we applied a ligature-induced periodontitis model to Sh3bp2 ^KI/+ mice to induce inflammatory alveolar bone destruction. Ligature placement induced alveolar bone resorption with gingival inflammation. Quantification of alveolar bone volume revealed that Sh3bp2 ^KI/+ mice developed more severe bone loss (male: 43.0% ± 10.6%, female: 42.6% ± 10.4%) compared with Sh3bp2 ^+/+ mice (male: 25.8% ± 4.0%, female: 30.9% ± 6.5%). Measurement of bone loss by the cement-enamel junction-alveolar bone crest distance showed no difference between Sh3bp2 ^KI/+ and Sh3bp2 ^+/+ mice. The number of osteoclasts on the alveolar bone surface was higher in male Sh3bp2 ^KI/+ mice, but not in females, compared with Sh3bp2 ^+/+ mice. In contrast, inflammatory cytokine levels in gingiva were comparable between Sh3bp2 ^KI/+ and Sh3bp2 ^+/+ mice with ligatures. Genetic deletion of the spleen tyrosine kinase in myeloid cells and antibiotic treatment suppressed alveolar bone loss in Sh3bp2 ^KI/+ mice, suggesting that increased osteoclast differentiation and function mediated by SYK and accumulation of oral bacteria are responsible for the increased alveolar bone loss in Sh3bp2 ^KI/+ mice with ligature-induced periodontitis. High amounts of oral bacterial load caused by insufficient oral hygiene could be a trigger for the initiation of jawbone destruction in human cherubism. © 2020 The Authors. JBMR Plus published by Wiley Periodicals, Inc. on behalf of American Society for Bone and Mineral Research.

Keywords: CHERUBISM; ORAL MICROBES; OSTEOCLASTS; PERIODONTITIS; SH3BP2.

Abstract

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