Osteoclast depletion with clodronate liposomes delays fracture healing in mice

Hao, Lin; O’Connor, J. P.

doi:10.1002/jor.23440

Cited by 29 publications

(30 citation statements)

References 49 publications

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“…injection of clo-lip or a PBS-lip control, and the extent of macrophage depletion was investigated. As clo-lip administration is known to induce apoptosis of all phagocytic cells, including osteoclasts [24], zoledronate was administered to a third group of mice as an osteoclast-depletion control [33]. Flow cytometric analysis revealed a 70% reduction in the total CD11b + F4/80 + monocyte/macrophage population within the BM of clo-lip–treated animals compared with controls (Figure 1 A ).…”

Section: Resultsmentioning

confidence: 99%

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Clodronate-Liposome Mediated Macrophage Depletion Abrogates Multiple Myeloma Tumor Establishment In Vivo

et al. 2019

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Multiple myeloma is a fatal plasma cell malignancy that is reliant on the bone marrow microenvironment. The bone marrow is comprised of numerous cells of mesenchymal and hemopoietic origin. Of these, macrophages have been implicated to play a role in myeloma disease progression, angiogenesis, and drug resistance; however, the role of macrophages in myeloma disease establishment remains unknown. In this study, the antimyeloma efficacy of clodronate-liposome treatment, which globally and transiently depletes macrophages, was evaluated in the well-established C57BL/KaLwRijHsd murine model of myeloma. Our studies show, for the first time, that clodronate-liposome pretreatment abrogates myeloma tumor development in vivo . Clodronate-liposome administration resulted in depletion of CD169 + bone marrow–resident macrophages. Flow cytometric analysis revealed that clodronate-liposome pretreatment impaired myeloma plasma cell homing and retention within the bone marrow 24 hours postmyeloma plasma cell inoculation. This was attributed in part to decreased levels of macrophage-derived insulin-like growth factor 1. Moreover, a single dose of clodronate-liposome led to a significant reduction in myeloma tumor burden in KaLwRij mice with established disease. Collectively, these findings support a role for CD169-expressing bone marrow–resident macrophages in myeloma disease establishment and progression and demonstrate the potential of targeting macrophages as a therapy for myeloma patients.

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Section: Resultsmentioning

confidence: 99%

“…Encapsulation of clodronate in lipid vesicles specifically targets clodronate to phagocytic macrophages that engulf and degrade the liposome, leading to clodronate accumulation and subsequent cellular apoptosis [23]. Unlike free clodronate, clodronate-liposomes (clo-lip) globally deplete macrophages and other phagocytic cells [23], [24].…”

Section: Introductionmentioning

confidence: 99%

Clodronate-Liposome Mediated Macrophage Depletion Abrogates Multiple Myeloma Tumor Establishment In Vivo

et al. 2019

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“…However, reports regarding effects of clodronate are conflicting, including no changes in bone mineral density in a callus [ 11 ], 30% increase in bone mineral density [ 10 ], increased calcium content within the callus [ 12 ], and decreased healing callus strength [ 13 ]. Recently, it has been shown that osteoclasts are a necessary component of efficient endochondral ossification during fracture repair in mice [ 14 ]; therefore, it is possible that clodronate may impair normal bone healing in horses, which calls for careful consideration when used in a clinical setting.…”

Section: Introductionmentioning

confidence: 99%

Tiludronate and clodronate do not affect bone structure or remodeling kinetics over a 60 day randomized trial

et al. 2018

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BackgroundTiludronate and clodronate are FDA-approved bisphosphonate drug therapies for navicular disease in horses. Although clinical studies have determined their ability to reduce lameness associated with skeletal disorders in horses, data regarding the effect on bone structure and remodeling is lacking. Additionally, due to off-label use of these drugs in young performance horses, effects on bone in young horses need to be investigated. Therefore, the purpose of this randomized, experimental pilot study was to determine the effect of tiludronate and clodronate on normal bone cells, structure and remodeling after 60 days in clinically normal, young horses. Additionally, the effect of clodronate on bone healing 60 days after an induced defect was investigated.ResultsAll horses tolerated surgery well, with no post-surgery lameness and all acquired biopsies being adequate for analyses. Overall, tiludronate and clodronate did not significantly alter any bone structure or remodeling parameters, as evaluated by microCT and dynamic histomorphometry. Tiludronate did not extensively impact bone formation or resorption parameters as evaluated by static histomorphometry. Similarly, clodronate did not affect bone formation or resorption after 60 days. Sixty days post-defect, healing was minimally affected by clodronate.ConclusionsTiludronate and clodronate do not appear to significantly impact bone tissue on a structural or cellular level using standard dose and administration schedules.

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“…In contrast, liposomal drug delivery can also be detrimental on bone healing as shown by Lin and O'Connor. The authors detected impaired fracture healing of femoral defects after treatment with clodronate-encapsulated liposomes ( Figure 2) over an investigation period of 28 days [166]. Liposomes or micelles are suitable site-directed drug carriers, particularly for water-insoluble drugs due to surface-decorated bone-targeting moieties.…”

Section: Liposomes and Micellesmentioning

confidence: 99%

Adjuvant Drug-Assisted Bone Healing: Advances and Challenges in Drug Delivery Approaches

et al. 2020

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Bone defects of critical size after compound fractures, infections, or tumor resections are a challenge in treatment. Particularly, this applies to bone defects in patients with impaired bone healing due to frequently occurring metabolic diseases (above all diabetes mellitus and osteoporosis), chronic inflammation, and cancer. Adjuvant therapeutic agents such as recombinant growth factors, lipid mediators, antibiotics, antiphlogistics, and proangiogenics as well as other promising anti-resorptive and anabolic molecules contribute to improving bone healing in these disorders, especially when they are released in a targeted and controlled manner during crucial bone healing phases. In this regard, the development of smart biocompatible and biostable polymers such as implant coatings, scaffolds, or particle-based materials for drug release is crucial. Innovative chemical, physico- and biochemical approaches for controlled tailor-made degradation or the stimulus-responsive release of substances from these materials, and more, are advantageous. In this review, we discuss current developments, progress, but also pitfalls and setbacks of such approaches in supporting or controlling bone healing. The focus is on the critical evaluation of recent preclinical studies investigating different carrier systems, dual- or co-delivery systems as well as triggered- or targeted delivery systems for release of a panoply of drugs.

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Osteoclast depletion with clodronate liposomes delays fracture healing in mice

Cited by 29 publications

References 49 publications

Clodronate-Liposome Mediated Macrophage Depletion Abrogates Multiple Myeloma Tumor Establishment In Vivo

Clodronate-Liposome Mediated Macrophage Depletion Abrogates Multiple Myeloma Tumor Establishment In Vivo

Tiludronate and clodronate do not affect bone structure or remodeling kinetics over a 60 day randomized trial

Adjuvant Drug-Assisted Bone Healing: Advances and Challenges in Drug Delivery Approaches

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