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3D assessment of intervertebral disc degeneration in zebrafish identifies changes in bone density that prime disc disease

机译:3D assessment of intervertebral disc degeneration in zebrafish identifies changes in bone density that prime disc disease

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摘要

Back pain is a common condition with a high social impact and represents a global health burden.Intervertebral disc disease(IVDD)is one of the major causes of back pain;no therapeutics are currently available to reverse this disease.The impact of bone mineral density(BMD)on IVDD has been controversial,with some studies suggesting osteoporosis as causative for IVDD and others suggesting it as protective for IVDD.Functional studies to evaluate the influence of genetic components of BMD in IVDD could highlight opportunities for drug development and repurposing.By taking a holistic 3D approach,we established an aging zebrafish model for spontaneous IVDD.Increased BMD in aging,detected by automated computational analysis,is caused by bone deformities at the endplates.However,aged zebrafish spines showed changes in bone morphology,microstructure,mineral heterogeneity,and increased fragility that resembled osteoporosis.Elements of the discs recapitulated IVDD symptoms found in humans:the intervertebral ligament(equivalent to the annulus fibrosus)showed disorganized collagen fibers and herniation,while the disc center(nucleus pulposus equivalent)showed dehydration and cellular abnormalities.We manipulated BMD in young zebrafish by mutating sp7 and cathepsin K,leading to low and high BMD,respectively.Remarkably,we detected IVDD in both groups,demonstrating that low BMD does not protect against IVDD,and we found a strong correlation between high BMD and IVDD.Deep learning was applied to high-resolution synchrotroniCJ image data to analyze osteocyte 3D lacunar distribution and morphology,revealing a role of sp7 in controlling the osteocyte lacunar 3D profile.Our findings suggest potential avenues through which bone quality can be targeted to identify beneficial therapeutics for IVDD.

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  • 来源
    《骨研究:英文》 |2021年第004期|P.521-536|共16页
  • 作者单位

    School of Physiology Pharmacology and Neuroscience Biomedical Sciences University of Bristol Bristol UK;

    School of Physics HH Wills Physics Laboratory University of Bristol Bristol UK;

    School of Physiology Pharmacology and Neuroscience Biomedical Sciences University of Bristol Bristol UK;

    School of Physics HH Wills Physics Laboratory University of Bristol Bristol UKCentre for Nanoscience and Quantum Information University of Bristol Bristol UKBristol Centre for Functional Nanomaterials University of Bristol Bristol UK;

    Department of Anthropology and Archaeology University of Bristol Bristol UKDepartment of Mechanical Engineering University of Bristol Bristol UK;

    Clinical Genetics Department Human Genetics and Genome Research Division Center of Excellence for Human Genetics National Research Centre Cairo Egypt;

    Clinical Genetics Department Human Genetics and Genome Research Division Center of Excellence for Human Genetics National Research Centre Cairo Egypt;

    Clinical Genetics Department Human Genetics and Genome Research Division Center of Excellence for Human Genetics National Research Centre Cairo Egypt;

    lnstituto de Investigaciones Biomedicas de Madrid and Ciber de Enfermedades Raras(CIBERER) Madrid Spain;

    Wolfson Bioimaging Facility Biomedical Sciences University of Bristol Bristol UK;

    School of Physics HH Wills Physics Laboratory University of Bristol Bristol UKSchool of Chemistry University of Bristol Bristol UK;

    Evolutionary Developmental Biology Department of Biology Ghent University Ghent Belgium;

    School of Physiology Pharmacology and Neuroscience Biomedical Sciences University of Bristol Bristol UK;

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  • 原文格式 PDF
  • 正文语种 chi
  • 中图分类 内分泌腺疾病及代谢病;
  • 关键词

    intervertebral; degeneration; protective;

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