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转染了人淀粉样前体蛋白启动子 - 乳糖酶基因报告基因构建体的转基因小鼠。

Mice transgenic for a human amyloid precursor protein promoter-lacZ reporter construct.

作者信息

Wright K L, Morgan D G, Yu X, Goss J R, Salbaum J M, Duff K, Gordon M N

机构信息

Department of Pharmacology, University of South Florida College of Medicine, Tampa 33612-4799, USA.

出版信息

J Mol Neurosci. 1999 Aug-Oct;13(1-2):111-20. doi: 10.1385/jmn:13:1-2:111.

Abstract

Transgenic mouse lines were generated that expressed a 2-kb amyloid precursor protein (APP) promoter/beta-galactosidase reporter gene construction. In brain, hippocampal pyramidal neurons, neurons in the deeper layers of cerebral cortex, and neurons in several thalamic nuclei were heavily labeled by beta-galactosidase histochemistry. In general, molecular layers and white matter regions did not express the reporter gene. When compared with in situ hybridization for endogenous murine APP RNA, the striatum and outer layers of cerebral cortex had little reporter expression. Thus, the match between reporter expression and endogenous APP expression in brain was not perfect. A similar mismatch between the relative expression of the reporter gene and endogenous APP RNA distribution was found in homogenates from several organs. Although prior work in transgenic mice found similar mismatches in reporter gene distribution, none had tested the APP promoter construct in response to neuronal injury. Kainic acid injections successfully increased murine APP expression in the transgenic mice, but had no effect on the reporter gene expression. Based on these data and those collected by others, we conclude that the 2-kb region upstream of the APP transcription initiation site contains some elements responsible for the tissue-specific expression of this gene, but does not contain all the cis-acting elements sufficient for either the differential tissue distribution of this gene or the regulation of this gene subsequent to neural damage.

摘要

构建了表达2kb淀粉样前体蛋白(APP)启动子/β-半乳糖苷酶报告基因的转基因小鼠品系。在脑中,海马锥体细胞、大脑皮质深层的神经元以及几个丘脑核中的神经元通过β-半乳糖苷酶组织化学被大量标记。一般来说,分子层和白质区域不表达报告基因。与内源性小鼠APP RNA的原位杂交相比,纹状体和大脑皮质外层的报告基因表达很少。因此,报告基因表达与脑中内源性APP表达之间的匹配并不完美。在几个器官的匀浆中也发现了报告基因相对表达与内源性APP RNA分布之间类似的不匹配。尽管之前在转基因小鼠中的研究发现报告基因分布存在类似的不匹配,但没有人测试过APP启动子构建体对神经元损伤的反应。海藻酸注射成功增加了转基因小鼠中内源性APP的表达,但对报告基因表达没有影响。基于这些数据以及其他人收集的数据,我们得出结论,APP转录起始位点上游的2kb区域包含一些负责该基因组织特异性表达的元件,但不包含足以实现该基因差异组织分布或神经损伤后该基因调控的所有顺式作用元件。

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