Short-Term Administration of HIV Protease Inhibitor Saquinavir Improves Skull Bone Healing with Enhanced Osteoclastogenesis

Haixia Liu; Yun Shen; Bingkun Zhao; Enoch H Poon; Shengcai Qi; Dai Fei Elmer Ker; Timothy R Billiar; Gregory M Cooper; Yuanzhi Xu; Dan Wang

doi:10.1097/PRS.0000000000009734

Short-Term Administration of HIV Protease Inhibitor Saquinavir Improves Skull Bone Healing with Enhanced Osteoclastogenesis

Plast Reconstr Surg. 2022 Dec 1;150(6):1264e-1274e. doi: 10.1097/PRS.0000000000009734. Epub 2022 Sep 19.

Authors

Affiliation

¹ From the Department of Stomatology, Shanghai Tenth People's Hospital, School of Medicine, Tongji University; the Institute for Tissue Engineering and Regenerative Medicine; the Key Laboratory for Regenerative Medicine, Ministry of Education, School of Biomedical Sciences, Faculty of Medicine, Chinese University of Hong Kong; and the Departments of Surgery, Plastic Surgery, and Oral Biology and Bioengineering, University of Pittsburgh.

Abstract

Background: Using immunomodulatory methods to address the challenging issue of craniofacial bone repair may be a potentially effective approach. The protease inhibitor saquinavir has been shown to inhibit the inflammatory response by targeting the toll-like receptor 4/myeloid differentiation primary response complex. Independently, inhibition of toll-like receptor 4 or myeloid differentiation primary response led to enhanced skull bone repair. Therefore, the authors aimed to investigate the effects of saquinavir on skull bone healing.

Methods: The effects of saquinavir on skull bone healing were assessed by means of gene expression, histology, immunohistochemistry, and tomography in a mouse calvarial defect model. Subsequently, the role of saquinavir in cell viability, migration, and osteogenic and osteoclastogenic differentiation was also evaluated in vitro.

Results: One-week saquinavir administration improved skull bone healing based on micro-computed tomographic and histomorphometric analyses. Compared to the vehicle control, 1-week saquinavir treatment (1) enhanced osteoclast infiltration (tartrate-resistant acid phosphatase staining) at day 7, but not at days 14 and 28; (2) induced more CD206 + M2 macrophage infiltration, but not F4/80 + M0 macrophages at days 7, 14, and 28; and (3) elevated osteoclastogenic gene RANKL (quantitative polymerase chain reaction) expression and other osteogenic and cytokine expression. Furthermore, in vitro data showed that saquinavir administration did not influence MC3T3-E1 cell migration or mineralization, whereas higher concentrations of saquinavir inhibited cell viability. Saquinavir treatment also enhanced the osteoclastic differentiation of bone marrow-derived precursors, and partially reversed high-mobility group box 1-driven osteoclastogenesis inhibition and elevated proinflammatory cytokine expression.

Conclusion: The improved skull bone repair following short-term saquinavir treatment may involve enhanced osteoclastogenesis and modulated inflammatory response following skull injury.

Clinical relevance statement: The authors' work demonstrates improved skull bone healing by short-term application of saquinavir, a drug traditionally used in the treatment of acquired immunodeficiency syndrome. As such, saquinavir may be repurposed for skeletal repair.

MeSH terms

Animals
HIV Protease Inhibitors* / metabolism
HIV Protease Inhibitors* / pharmacology
HIV Protease Inhibitors* / therapeutic use
Mice
Osteogenesis
Saquinavir* / metabolism
Saquinavir* / pharmacology
Saquinavir* / therapeutic use
Skull / injuries
Toll-Like Receptor 4 / physiology

Substances

Saquinavir
HIV Protease Inhibitors
Toll-Like Receptor 4