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Is Chemokine Receptor CCR9 Required for Synovitis in Rheumatoid Arthritis? Deficiency of CCR9 in a Murine Model of Antigen-Induced Arthritis
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作者 Alison Cartwright Sophie King +1 位作者 Jim Middleton Oksana Kehoe 《Open Journal of Rheumatology and Autoimmune Diseases》 2012年第4期77-84,共8页
Objectives: Monocytes/macrophages accumulate in the synovial membrane in rheumatoid arthritis and play a key role in disease pathogenesis, contributing to inflammation, cartilage destruction and bone erosion. Identifi... Objectives: Monocytes/macrophages accumulate in the synovial membrane in rheumatoid arthritis and play a key role in disease pathogenesis, contributing to inflammation, cartilage destruction and bone erosion. Identification of molecules involved in monocyte/macrophage recruitment in inflammation is crucial for development of therapeutic interventions. Chemokine receptor CCR9 is up-regulated on these cells in peripheral blood and synovium of rheumatoid patients. This study investigated the course of antigen-induced arthritis in CCR9 deficient C57BL/6 mice in comparison to wild type animals to determine whether CCR9 is critical for disease severity and progression. Methods: Methylated bovine serum albumin was used for induction of uni-lateral arthritis by direct injection into the knee joints of preimmunized animals. Arthritis is confined to the injected joint allowing comparison with the normal opposing joint. Clinical severity of arthritis was assessed by measuring swelling in the arthritic joint in comparison to the normal joint. Histological analysis was performed to assess the extent of leukocyte infiltration and cartilage depletion. Results: Levels of swelling were not significantly different between wild type and CCR9 deficient mice. Similarly there was no significant difference in histological severity of arthritis when comparing CCR9-deficient mice to wild type mice. Conclusions: CCR9 was not required for development of synovial inflammation and cartilage destruction in the anti-gen-induced model of arthritis in C57BL/6 mice in this study. This may reflect a true lack of a pathogenic role of CCR9 on monocyte/macrophage function in vivo or it may reflect differences in the current antigen-induced arthritis model when compared to human RA. 展开更多
关键词 CHEMOKINE Receptor ccr9 RHEUMATOID ARTHRITIS Inflammation Antigen-Induced ARTHRITIS Mouse mod-el Monocytes/Macrophages
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中国国家大学科技园创新孵化效率的地区和技术差距研究 被引量:1
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作者 陈明慧 李倩 郭江江 《浙江师范大学学报(社会科学版)》 2023年第1期58-69,共12页
如何衡量和提高国家大学科技园的创新孵化效率是当前国家大学科技园发展过程中亟待解决的难题。文章基于全国27个省(区、市)的国家大学科技园数据,采用Meta-frontier CCR模型和Malmquist生产率指数法,对中国国家大学科技园创新孵化效率... 如何衡量和提高国家大学科技园的创新孵化效率是当前国家大学科技园发展过程中亟待解决的难题。文章基于全国27个省(区、市)的国家大学科技园数据,采用Meta-frontier CCR模型和Malmquist生产率指数法,对中国国家大学科技园创新孵化效率进行了系统的实证研究。研究结果表明:我国国家大学科技园创新孵化效率整体前景良好,但各地区内部差异化、发展不平衡问题较为严重;技术差距比(TGR)衡量的技术差距结果显示,东部和西部地区的国家大学科技园技术差距比相对稳定,逐渐趋向于1,中部和东北部地区则波动较大;动态分解结果表明,东部地区国家大学科技园创新孵化效率提升的动力来自技术效率,其余地区则主要由规模效率主导。 展开更多
关键词 国家大学科技园 创新孵化效率 meta-frontier ccr模型 Malmquist生产率指数法
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