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Avp-IRES2-Cre(JAX #023530)和 Vip-IRES-Cre(JAX #010908)模型在生物钟研究中的局限性。

Limitations of the Avp-IRES2-Cre (JAX #023530) and Vip-IRES-Cre (JAX #010908) Models for Chronobiological Investigations.

机构信息

Department of Biology, University of Toronto Mississauga, Mississauga, ON, Canada.

Department of Cell & Systems Biology, University of Toronto, Toronto, ON, Canada.

出版信息

J Biol Rhythms. 2019 Dec;34(6):634-644. doi: 10.1177/0748730419871184. Epub 2019 Aug 27.

DOI:10.1177/0748730419871184
PMID:31452438
Abstract

The principal circadian pacemaker in mammals, the suprachiasmatic nucleus (SCN), expresses a number of neuropeptides that facilitate intercellular synchrony, helping to generate coherent outputs to peripheral clocks throughout the body. In particular, arginine vasopressin (AVP)- and vasoactive intestinal peptide (VIP)-expressing neurons have been recognized as crucial subpopulations within the SCN and have thus been the focus of many chronobiological studies. Here, we analyze the neuropeptide expression of 2 popular transgenic mouse strains commonly used to direct or restrict Cre-mediated recombination to AVP- and VIP-ergic neurons. The Avp-IRES2-Cre (JAX #023530) and Vip-IRES-Cre (JAX #010908) "driver" mouse strains express the Cre recombinase under the control of the endogenous or gene, respectively, allowing scientists either to ablate their gene of interest or to overexpress a transgene in a cell type-specific manner. Although these are potentially very powerful tools for chronobiologists and other scientists studying AVP- and VIP-ergic neurons, we found that neuropeptide expression in these mice is significantly decreased when an IRES(2)-Cre cassette is inserted downstream of the neuropeptide-encoding gene locus. The impact of IRES(2)-Cre cassette insertion on neuropeptide expression may be a confounding factor in many experimental designs. Our findings suggest that extreme caution must be exercised when using these mouse models to avoid misinterpretation of empirical results.

摘要

哺乳动物的主要生物钟起搏器是视交叉上核(SCN),它表达了许多神经肽,这些神经肽有助于细胞间的同步,有助于为全身的外周时钟产生一致的输出。特别是,精氨酸加压素(AVP)和血管活性肠肽(VIP)表达神经元已被认为是 SCN 中的关键亚群,因此成为许多生物钟生物学研究的焦点。在这里,我们分析了两种常用的转基因小鼠品系的神经肽表达情况,这两种小鼠品系通常用于指导或限制 AVP 和 VIP 能神经元的 Cre 介导重组。Avp-IRES2-Cre(JAX #023530)和 Vip-IRES-Cre(JAX #010908)“驱动”小鼠品系分别在内源性 或 基因的控制下表达 Cre 重组酶,允许科学家以细胞类型特异性的方式消除其感兴趣的基因或过表达转基因。尽管这些对于生物钟生物学家和其他研究 AVP 和 VIP 能神经元的科学家来说是非常强大的工具,但我们发现,当 IRES(2)-Cre 盒插入神经肽编码基因座的下游时,这些小鼠的神经肽表达显著降低。IRES(2)-Cre 盒插入对神经肽表达的影响可能是许多实验设计中的一个混杂因素。我们的研究结果表明,在使用这些小鼠模型时必须非常谨慎,以避免对实验结果的误解。

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