Developing a zebrafish model of bisphosphonate induced osteonecrosis of jaw to define cellular and molecular mechanisms

Developing a zebrafish model of bisphosphonate induced osteonecrosis of jaw to define cellular and molecular mechanisms

Bisphosphonates are critical drugs of the orthopaedic clinic, which act by inhibiting osteoclast resorptive activity and thus promote bone density. They are commonly used for treating Osteogenesis Imperfecta (OI), Paget’s disease, osteoporosis, and bone metastasis. In particular, the global rise in...

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Main Author: Ethiraj, Lalith Prabha
Other Authors: Tom James Carney
Format: Thesis-Doctor of Philosophy
Language:English
Published: Nanyang Technological University 2023
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Science::Medicine
Online Access:https://hdl.handle.net/10356/168636
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spelling sg-ntu-dr.10356-1686362023-07-04T01:52:12Z Developing a zebrafish model of bisphosphonate induced osteonecrosis of jaw to define cellular and molecular mechanisms Ethiraj, Lalith Prabha Tom James Carney Lee Kong Chian School of Medicine (LKCMedicine) tcarney@ntu.edu.sg Science::Medicine Bisphosphonates are critical drugs of the orthopaedic clinic, which act by inhibiting osteoclast resorptive activity and thus promote bone density. They are commonly used for treating Osteogenesis Imperfecta (OI), Paget’s disease, osteoporosis, and bone metastasis. In particular, the global rise in the incidence of the latter two diseases has led to significantly expanded bisphosphonate use in recent years. This has seen a concomitant increase in the incidence of Bisphosphonate Related Osteonecrosis of Jaw (BRONJ), a rare but potentially serious side effect of bisphosphonate use. Patients affected by BRONJ show paradoxical necrotic lesions in the jaw and loss of teeth with a considerable reduction in quality of life. The rarity of BRONJ limits the power of human studies, and the underlying mechanism remains unclear. Treatment options are extremely limited and mostly surgical. This necessitates the need for animal models to determine the cellular and molecular mechanisms involved. Current mammalian models of BRONJ require surgical removal of teeth to instigate ONJ, limiting throughput, and their current clinical translational impact is questionable. In previous studies, we demonstrated bisphosphonate efficacy in zebrafish OI and fracture models. I have developed colorimetric and fluorescent Tartrate Resistant Acid Phosphatase (TRAP) staining approaches to assess and quantify osteoclast activity in the fracture model and on the tooth-bearing ceratobranchial bone. This allowed me to demonstrate a high spontaneous osteoclastic activity around the base of the zebrafish pharyngeal teeth and its suppression with bisphosphonate treatment. Surprisingly, I also noted necrotic lesions in the jaw of all adult zebrafish following extended treatment with bisphosphonate. This led to teeth-bone disjunction and was reminiscent of the BRONJ seen in the clinic. This establishes zebrafish as a robust and accessible model of BRONJ. There is convincing evidence of an immunological contribution to BRONJ progression. Using the newly established zebrafish BRONJ model, I assayed the innate immune response through a combination of fluorescent dyes and transgenic lines. A biphasic immune response was observed. There was an initial infiltration of neutrophils which ablated after 3 weeks, and activated macrophages were observed pooling at the teeth bone junction at later stages. Concomitant with this was an early downregulation of NF-κB signalling, followed by marked NF-κB signalling upregulation at later time points. I tested if the osteoclast/macrophage lineage was necessary for BRONJ. Genetic ablation of these cells using the csf1ra mutant entirely abolished BRONJ onset following alendronate treatment. Furthermore, I showed 9 pharmacological inhibition of NF-κB signalling was fully protective against BRONJ in zebrafish. In sum, I developed a robust zebrafish model of BRONJ and used it to generate preliminary insights into immune contribution to the pathology and finally identified a signalling pathway that can be targeted for treatment or prevention. Future uses of this model is to identify, describe and ameliorate BRONJ in the clinic, are discussed. Doctor of Philosophy 2023-06-13T07:31:25Z 2023-06-13T07:31:25Z 2023 Thesis-Doctor of Philosophy Ethiraj, L. P. (2023). Developing a zebrafish model of bisphosphonate induced osteonecrosis of jaw to define cellular and molecular mechanisms. Doctoral thesis, Nanyang Technological University, Singapore. https://hdl.handle.net/10356/168636 https://hdl.handle.net/10356/168636 10.32657/10356/168636 en This work is licensed under a Creative Commons Attribution-NonCommercial 4.0 International License (CC BY-NC 4.0). application/pdf Nanyang Technological University
institution Nanyang Technological University
building NTU Library
continent Asia
country Singapore
Singapore
content_provider NTU Library
collection DR-NTU
language English
topic Science::Medicine
spellingShingle Science::Medicine
Ethiraj, Lalith Prabha
Developing a zebrafish model of bisphosphonate induced osteonecrosis of jaw to define cellular and molecular mechanisms
description Bisphosphonates are critical drugs of the orthopaedic clinic, which act by inhibiting osteoclast resorptive activity and thus promote bone density. They are commonly used for treating Osteogenesis Imperfecta (OI), Paget’s disease, osteoporosis, and bone metastasis. In particular, the global rise in the incidence of the latter two diseases has led to significantly expanded bisphosphonate use in recent years. This has seen a concomitant increase in the incidence of Bisphosphonate Related Osteonecrosis of Jaw (BRONJ), a rare but potentially serious side effect of bisphosphonate use. Patients affected by BRONJ show paradoxical necrotic lesions in the jaw and loss of teeth with a considerable reduction in quality of life. The rarity of BRONJ limits the power of human studies, and the underlying mechanism remains unclear. Treatment options are extremely limited and mostly surgical. This necessitates the need for animal models to determine the cellular and molecular mechanisms involved. Current mammalian models of BRONJ require surgical removal of teeth to instigate ONJ, limiting throughput, and their current clinical translational impact is questionable. In previous studies, we demonstrated bisphosphonate efficacy in zebrafish OI and fracture models. I have developed colorimetric and fluorescent Tartrate Resistant Acid Phosphatase (TRAP) staining approaches to assess and quantify osteoclast activity in the fracture model and on the tooth-bearing ceratobranchial bone. This allowed me to demonstrate a high spontaneous osteoclastic activity around the base of the zebrafish pharyngeal teeth and its suppression with bisphosphonate treatment. Surprisingly, I also noted necrotic lesions in the jaw of all adult zebrafish following extended treatment with bisphosphonate. This led to teeth-bone disjunction and was reminiscent of the BRONJ seen in the clinic. This establishes zebrafish as a robust and accessible model of BRONJ. There is convincing evidence of an immunological contribution to BRONJ progression. Using the newly established zebrafish BRONJ model, I assayed the innate immune response through a combination of fluorescent dyes and transgenic lines. A biphasic immune response was observed. There was an initial infiltration of neutrophils which ablated after 3 weeks, and activated macrophages were observed pooling at the teeth bone junction at later stages. Concomitant with this was an early downregulation of NF-κB signalling, followed by marked NF-κB signalling upregulation at later time points. I tested if the osteoclast/macrophage lineage was necessary for BRONJ. Genetic ablation of these cells using the csf1ra mutant entirely abolished BRONJ onset following alendronate treatment. Furthermore, I showed 9 pharmacological inhibition of NF-κB signalling was fully protective against BRONJ in zebrafish. In sum, I developed a robust zebrafish model of BRONJ and used it to generate preliminary insights into immune contribution to the pathology and finally identified a signalling pathway that can be targeted for treatment or prevention. Future uses of this model is to identify, describe and ameliorate BRONJ in the clinic, are discussed.
author2 Tom James Carney
author_facet Tom James Carney
Ethiraj, Lalith Prabha
format Thesis-Doctor of Philosophy
author Ethiraj, Lalith Prabha
author_sort Ethiraj, Lalith Prabha
title Developing a zebrafish model of bisphosphonate induced osteonecrosis of jaw to define cellular and molecular mechanisms
title_short Developing a zebrafish model of bisphosphonate induced osteonecrosis of jaw to define cellular and molecular mechanisms
title_full Developing a zebrafish model of bisphosphonate induced osteonecrosis of jaw to define cellular and molecular mechanisms
title_fullStr Developing a zebrafish model of bisphosphonate induced osteonecrosis of jaw to define cellular and molecular mechanisms
title_full_unstemmed Developing a zebrafish model of bisphosphonate induced osteonecrosis of jaw to define cellular and molecular mechanisms
title_sort developing a zebrafish model of bisphosphonate induced osteonecrosis of jaw to define cellular and molecular mechanisms
publisher Nanyang Technological University
publishDate 2023
url https://hdl.handle.net/10356/168636
_version_ 1772827015672496128

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