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Advantages and limitations of mouse models to deplete dendritic cells

机译:小鼠模型的优点和局限性耗尽树突细胞

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摘要

Dendritic cells (DCs) play a key role in regulating innate and adaptive immunity. Our understanding of DC biology has benefited from studies in CD11c.DTR and CD11c.DOG mouse models that use the CD11c promoter to express a diphtheria toxin (DT) receptor transgene to inducibly deplete CD11c+ cells. Other models to inducibly deplete specific DC subsets upon administration of DT have also been generated. However, most models suffer from limitations such as depletion of additional cell types or the requirement to be used as radiation chimeras. Moreover, CD11c.DTR and CD11c.DOG mice have recently been reported to display neutrophilia and monocytosis upon DT injection. We discuss here some of the limitations that should be taken into consideration when interpreting results obtained with mouse models of DC ablation.
机译:树突状细胞(dc)起着关键的作用天然免疫与适应性免疫调节。理解直流生物学受益匪浅在CD11c研究。使用CD11c启动子表达白喉毒素(DT)受体转基因诱导耗尽CD11c +细胞。诱导耗尽特定的直流子集DT管理局也已生成。然而,大多数模型受到限制作为额外的损耗或细胞类型要求被用作辐射嵌合体。此外,CD11c。最近报道显示嗜中性和单核细胞增多症DT注入。这里应该采取的一些局限性考虑当解释结果获得直流电消融的小鼠模型。

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