Doxycycline preserves chondrocyte viability and function in human and calf articular cartilage ex vivo

Li, Yue; Vuong, Brian; Yao, Hongwei; Owens, Brett D.

doi:10.14814/phy2.14571

Cited by 5 publications

(6 citation statements)

References 38 publications

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“…Other studies did not demonstrate this same chondrotoxicity. 18,19 For instance, Yue et al 23 found that doxycycline decreased chondrocyte apoptosis, increased type II collagen synthesis, and increased mechanical integrity. Doxycycline has also been shown to protect the articular environment through decreased expression of catabolic cytokines.…”

Section: Resultsmentioning

confidence: 99%

Review of Intra-Articular Use of Antibiotics and Antiseptic Irrigation and Their Systematic Association with Chondrolysis

Post,

Blankespoor,

Ierulli

et al. 2023

kjm

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Introduction. Intra-articular antibiotics have been proposed as a treatment for septic arthritis to allow for high local concentrations without subjecting a patient to the toxicity/side effects of systemic therapy. However, there is concern for chondrotoxicity with intra-articular use of these solutions in high concentrations. The purpose of this systematic review was to evaluate the intra-articular use of antibiotics and antiseptic solutions, and to determine their association with chondrolysis following in vitro or in vivo administration. Methods. A systematic review was conducted following PRISMA guidelines through PubMed, Clinical Key, OVID, and Google Scholar. Studies in English were included if they evaluated for chondrotoxicity following antibiotic exposure. Results. The initial search resulted in 228 studies, with 36 meeting criteria. Overall, 7 of the 24 (29%) agents were non-chondrotoxic: minocycline, tetracycline, chloramphenicol, teicoplanin, pefloxacin, linezolid, polymyxin-bacitracin. Eight (33%) agents had inconsistent results: doxycycline, ceftriaxone, gentamicin, vancomycin, ciprofloxacin, ofloxacin, chlorhexidine, and povidone iodine. Chondrotoxicity was evident with 9 (38%) agents, all of which were also dose-dependently chondrotoxic based on reported estimated half maximal inhibitory concentrations (est.IC50): amikacin (est. IC50 = 0.31-2.74 mg/mL), neomycin (0.82), cefazolin (1.67-3.95), ceftazidime (3.16-3.59), ampicillin-sulbactam (8.64 - >25), penicillin (11.61), amoxicillin (14.01), imipenem (>25), and tobramycin (>25). Additionally, chondroprotective effects of doxycycline and minocycline were reported. Conclusions. This systematic review identified agents that may be used in the treatment of septic arthritis. Nine agents should be avoided due to their dose-dependent chondrotoxic effects. Further studies are needed to clarify the safety of these medications for human intra-articular use.

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Section: Resultsmentioning

confidence: 99%

Review of Intra-Articular Use of Antibiotics and Antiseptic Irrigation and Their Systematic Association with Chondrolysis

Post,

Blankespoor,

Ierulli

et al. 2023

kjm

View full text Add to dashboard Cite

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“…Chondrocyte viability plays a critical role in maintaining the biochemical and biomechanical properties necessary to prevent stenosis or collapse in tracheal replacement, however the preservation of chondrocyte viability remains a challenge in tracheal tissue engineering. 19,41,42 Modulation of decellularization protocol, such as optimization of decellularization time, can preserve viability of chondrocytes in DTS. 19 We also observed a higher mortality rate of hosts receiving DTS than that of STG control (p = 0.0490).…”

Section: Discussionmentioning

confidence: 99%

Regeneration of partially decellularized tracheal scaffolds in a mouse model of orthotopic tracheal replacement

et al. 2021

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Decellularized tracheal scaffolds offer a potential solution for the repair of long-segment tracheal defects. However, complete decellularization of trachea is complicated by tracheal collapse. We created a partially decellularized tracheal scaffold (DTS) and characterized regeneration in a mouse model of tracheal transplantation. All cell populations except chondrocytes were eliminated from DTS. DTS maintained graft integrity as well as its predominant extracellular matrix (ECM) proteins. We then assessed the performance of DTS in vivo. Grafts formed a functional epithelium by study endpoint (28 days). While initial chondrocyte viability was low, this was found to improve in vivo. We then used atomic force microscopy to quantify micromechanical properties of DTS, demonstrating that orthotopic implantation and graft regeneration lead to the restoration of native tracheal rigidity. We conclude that DTS preserves the cartilage ECM, supports neo-epithelialization, endothelialization and chondrocyte viability, and can serve as a potential solution for long-segment tracheal defects.

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“…Chondrocytes are responsible for the maintenance of the graft matrisome; the viability of these cells could prove to play a critical role in graft performance. [28][29][30] Beyond decellularization, graft viability is related to ischemia time and storage conditions; these factors can limit the creation of a donor tissue bank. Wellestablished approaches of cryopreservation methods to biobank organs have been developed to enhance viability.…”

Section: Discussionmentioning

confidence: 99%

“…Graft chondrocyte viability is now a new and important consideration. Chondrocytes are responsible for the maintenance of the graft matrisome; the viability of these cells could prove to play a critical role in graft performance 28–30 . Beyond decellularization, graft viability is related to ischemia time and storage conditions; these factors can limit the creation of a donor tissue bank.…”

Section: Discussionmentioning

confidence: 99%

A Multimodal Approach to Quantify Chondrocyte Viability for Airway Tissue Engineering

et al. 2022

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Objectives/Hypothesis Partially decellularized tracheal scaffolds have emerged as a potential solution for long‐segment tracheal defects. These grafts have exhibited regenerative capacity and the preservation of native mechanical properties resulting from the elimination of all highly immunogenic cell types while sparing weakly immunogenic cartilage. With partial decellularization, new considerations must be made about the viability of preserved chondrocytes. In this study, we propose a multimodal approach for quantifying chondrocyte viability for airway tissue engineering. Methods Tracheal segments (5 mm) were harvested from C57BL/6 mice, and immediately stored in phosphate‐buffered saline at −20°C (PBS‐20) or biobanked via cryopreservation. Stored and control (fresh) tracheal grafts were implanted as syngeneic tracheal grafts (STG) for 3 months. STG was scanned with micro‐computed tomography (μCT) in vivo. STG subjected to different conditions (fresh, PBS‐20, or biobanked) were characterized with live/dead assay, terminal deoxynucleotidyl transferase dUTP nick end labeling (TUNEL), and von Kossa staining. Results Live/dead assay detected higher chondrocyte viability in biobanked conditions compared to PBS‐20. TUNEL staining indicated that storage conditions did not alter the proportion of apoptotic cells. Biobanking exhibited a lower calcification area than PBS‐20 in 3‐month post‐implanted grafts. Higher radiographic density (Hounsfield units) measured by μCT correlated with more calcification within the tracheal cartilage. Conclusions We propose a strategy to assess chondrocyte viability that integrates with vivo imaging and histologic techniques, leveraging their respective strengths and weaknesses. These techniques will support the rational design of partially decellularized tracheal scaffolds. Level of Evidence N/A Laryngoscope, 133:512–520, 2023

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Doxycycline preserves chondrocyte viability and function in human and calf articular cartilage ex vivo

Cited by 5 publications

References 38 publications

Review of Intra-Articular Use of Antibiotics and Antiseptic Irrigation and Their Systematic Association with Chondrolysis

Review of Intra-Articular Use of Antibiotics and Antiseptic Irrigation and Their Systematic Association with Chondrolysis

Regeneration of partially decellularized tracheal scaffolds in a mouse model of orthotopic tracheal replacement

A Multimodal Approach to Quantify Chondrocyte Viability for Airway Tissue Engineering

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