High-throughput micro-CT analysis identifies sex-dependent biomarkers of erosive arthritis in TNF-Tg mice and differential response to anti-TNF therapy

High-throughput micro-CT analysis identifies sex-dependent biomarkers of erosive arthritis in TNF-Tg mice and differential response to anti-TNF therapy

Development of reliable disease activity biomarkers is critical for diagnostics, prognostics, and novel drug development. Although computed tomography (CT) is the gold-standard for quantification of bone erosions, there are no consensus approaches or rationales for utilization of specific outcome me...

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Veröffentlicht in:PloS one 2024-07, Vol.19 (7), p.e0305623
Hauptverfasser: Kenney, H Mark, Chen, Kiana L, Schnur, Lindsay, Fox, Jeffrey I, Wood, Ronald W, Xing, Lianping, Ritchlin, Christopher T, Rahimi, Homaira, Schwarz, Edward M, Awad, Hani A
Format: Artikel
Sprache:eng
Schlagworte:
Animal models
Animals
Ankle
Arthritis
Biological markers
Biology and Life Sciences
Biomarkers
Bone density
Bones
Calcaneus
Computed tomography
CT imaging
Disease Models, Animal
Diseases
Drug development
Effectiveness
Engineering and Technology
Female
Females
Genetic engineering
Health aspects
Histology
Image analysis
Image processing
Immunoglobulin G
Inflammation
Joint diseases
Joints (anatomy)
Magnetic resonance imaging
Male
Males
Medicine and Health Sciences
Mice
Mice, Inbred C57BL
Mice, Transgenic
Monoclonal antibodies
Osteoclasts
Pathogenesis
Research and Analysis Methods
Segmentation
Sex Characteristics
Sex Factors
Sexual dimorphism
Soil erosion
Synovitis
Talus
Transgenic mice
Tumor necrosis factor
Tumor Necrosis Factor-alpha - antagonists & inhibitors
X-Ray Microtomography - methods
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Zusammenfassung:Development of reliable disease activity biomarkers is critical for diagnostics, prognostics, and novel drug development. Although computed tomography (CT) is the gold-standard for quantification of bone erosions, there are no consensus approaches or rationales for utilization of specific outcome measures of erosive arthritis in complex joints. In the case of preclinical models, such as sexually dimorphic tumor necrosis factor transgenic (TNF-Tg) mice, disease severity is routinely quantified in the ankle through manual segmentation of the talus or small regions of adjacent bones primarily due to the ease in measurement. Herein, we sought to determine the particular hindpaw bones that represent reliable biomarkers of sex-dependent disease progression to guide future investigation and analysis. Hindpaw micro-CT was performed on wild-type (n = 4 male, n = 4 female) and TNF-Tg (n = 4 male, n = 7 female) mice at monthly intervals from 2-5 (females) and 2-8-months (males) of age, since female TNF-Tg mice exhibit early mortality from cardiopulmonary disease at approximately 5-6-months. Further, 8-month-old WT (n = 4) and TNF-Tg males treated with anti-TNF monoclonal antibodies (n = 5) or IgG placebo isotype controls (n = 6) for 6-weeks were imaged with micro-CT every 3-weeks. For image analysis, we utilized our recently developed high-throughput and semi-automated segmentation strategy in Amira software. Synovial and osteoclast histology of ankle joints was quantified using Visiopharm. First, we demonstrated that the accuracy of automated segmentation, determined through analysis of ~9000 individual bones by a single user, was comparable in wild-type and TNF-Tg hindpaws before correction (79.2±8.9% vs 80.1±5.1%, p = 0.52). Compared to other bone compartments, the tarsal region demonstrated a sudden, specific, and significant bone volume reduction in female TNF-Tg mice, but not in males, by 5-months (4-months 4.3± 0.22 vs 5-months 3.4± 0.62 mm3, p
ISSN:1932-6203
1932-6203
DOI:10.1371/journal.pone.0305623