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Improvements and Limitations of Humanized Mouse Models for HIV Research: NIH/NIAID “Meet the Experts” 2015 Workshop Summary

机译:艾滋病毒研究人性化小鼠模型的改善与限制:NIH / NIAID“符合专家”2015讲习班摘要

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摘要

The number of humanized mouse models for the human immunodeficiency virus (HIV)/acquired immunodeficiency syndrome (AIDS) and other infectious diseases has expanded rapidly over the past 8 years. Highly immunodeficient mouse strains, such as NOD/SCID/gamma chainnull (NSG, NOG), support better human hematopoietic cell engraftment. Another improvement is the derivation of highly immunodeficient mice, transgenic with human leukocyte antigens (HLAs) and cytokines that supported development of HLA-restricted human T cells and heightened human myeloid cell engraftment. Humanized mice are also used to study the HIV reservoir using new imaging techniques. Despite these advances, there are still limitations in HIV immune responses and deficits in lymphoid structures in these models in addition to xenogeneic graft-versus-host responses. To understand and disseminate the improvements and limitations of humanized mouse models to the scientific community, the NIH sponsored and convened a meeting on April 15, 2015 to discuss the state of knowledge concerning these questions and best practices for selecting a humanized mouse model for a particular scientific investigation. This report summarizes the findings of the NIH meeting.
机译:人类免疫缺陷病毒(HIV)/获得的免疫缺陷综合征(艾滋病)和其他传染病的人源化小鼠模型的数量在过去的8年里迅速扩大。高度免疫缺陷的小鼠菌株,例如NOD / SCID / Gamma Chainnull(NSG,NOG),支持更好的人造血细胞植入。另一种改进是高度免疫缺陷小鼠的衍生物,具有人白细胞抗原(HLA)和细胞因子的转基因,所述细胞因子支持HLA限制的人T细胞和提高人髓细胞植入。人源化小鼠还用于使用新的成像技术研究HIV储层。尽管有这些进展,除了异种移植物与宿主反应外,这些模型中的淋巴结结构和淋巴结结构缺陷仍存在局限性。理解和传播人性化小鼠模型对科学界的改善和限制,2015年4月15日赞助和召开会议,讨论了关于这些问题的知识状态以及为特定选择人性化小鼠模型的最佳实践科学调查。本报告总结了NIH会议的调查结果。

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