CD11c-cre 转基因小鼠造血细胞中 Cre 重组酶的差异表达

IF 1.6 4区 医学 Q4 BIOCHEMICAL RESEARCH METHODS
Claire Murat , Sylvie Guerder
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引用次数: 0

摘要

在这项研究中,我们深入分析了鲍里斯-雷齐斯(Boris Reizis)研究小组培育的、被广泛使用的 CD11c-Cre 转基因小鼠中 Cre 的表达情况。与之前的观察不同,我们利用高灵敏度的 Rosa-26-floxed-tdTomato 报告小鼠系,从造血干细胞开始,在多个造血系细胞中发现了 Cre 的不同表达。事实上,我们发现,在 CD11c-Cre 驱动小鼠中,Cre 如预期的那样在髓树突状细胞前体的 cDC 亚系细胞和 pDC 中表达,但也在相当一部分造血干细胞和普通淋巴祖细胞中表达,因此,在所有白细胞中的表达率为 50%。因此,这项研究表明,在选择用于鉴定 Cre 驱动小鼠中 Cre 表达的报告小鼠时应谨慎,并考虑报告系统的敏感性。这项研究还表明,一些使用 CD11c-Cre 转基因小鼠的报道可能需要在仔细评估其模型中 Cre 介导的细胞类型特异性的基础上重新考虑。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Variegate expression of Cre recombinase in hematopoietic cells in CD11c-cre transgenic mice

In this study, we performed an in-depth analysis of Cre expression in the widely used CD11c-Cre transgenic mice generated by the group of Boris Reizis. In contrast to previous observation, using the highly sensitive Rosa-26-floxed-tdTomato reporter mouse line, we show variegated expression of Cre in multiple hematopoietic linage cells starting in hematopoietic stem cells. Indeed, we found that in the CD11c-Cre driver mice, Cre is expressed in cDC linage cells and pDC starting from the myeloid dendritic cell precursor, as expected, but also in a substantial fraction of hematopoietic stem cells and common lymphoid progenitors and, consequently, in >50% of all leukocytes. Hence, this study indicates that the reporter mice used to characterize Cre expression in Cre-driver mice should be selected with caution and considering the sensitivity of the reporter system. This study also suggests that the interpretation of some reports using this CD11c-Cre transgenic mice may need to be re-considered based on a careful evaluation of the cell type-specificity of Cre-mediated in their model.

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来源期刊
CiteScore
4.10
自引率
0.00%
发文量
120
审稿时长
3 months
期刊介绍: The Journal of Immunological Methods is devoted to covering techniques for: (1) Quantitating and detecting antibodies and/or antigens. (2) Purifying immunoglobulins, lymphokines and other molecules of the immune system. (3) Isolating antigens and other substances important in immunological processes. (4) Labelling antigens and antibodies. (5) Localizing antigens and/or antibodies in tissues and cells. (6) Detecting, and fractionating immunocompetent cells. (7) Assaying for cellular immunity. (8) Documenting cell-cell interactions. (9) Initiating immunity and unresponsiveness. (10) Transplanting tissues. (11) Studying items closely related to immunity such as complement, reticuloendothelial system and others. (12) Molecular techniques for studying immune cells and their receptors. (13) Imaging of the immune system. (14) Methods for production or their fragments in eukaryotic and prokaryotic cells. In addition the journal will publish articles on novel methods for analysing the organization, structure and expression of genes for immunologically important molecules such as immunoglobulins, T cell receptors and accessory molecules involved in antigen recognition, processing and presentation. Submitted full length manuscripts should describe new methods of broad applicability to immunology and not simply the application of an established method to a particular substance - although papers describing such applications may be considered for publication as a short Technical Note. Review articles will also be published by the Journal of Immunological Methods. In general these manuscripts are by solicitation however anyone interested in submitting a review can contact the Reviews Editor and provide an outline of the proposed review.
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