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出生后基因标记的成熟小鼠嗅觉感觉神经元的存活。

Survival of mature mouse olfactory sensory neurons labeled genetically perinatally.

机构信息

Max Planck Institute of Biophysics, Max-von-Laue-Strasse 3, 60438 Frankfurt, Germany.

出版信息

Mol Cell Neurosci. 2018 Apr;88:258-269. doi: 10.1016/j.mcn.2018.02.005. Epub 2018 Feb 7.

Abstract

The main olfactory epithelium (MOE) of an adult mouse harbors a few million mature olfactory sensory neurons (OSNs), which are traditionally defined as mature by their expression of the olfactory marker protein (OMP). Mature OSNs differentiate in situ from stem cells at the base of the MOE. The consensus view is that mature OSNs have a defined lifespan and then undergo programmed cell death, and that the adult MOE maintains homeostasis by generating new mature OSNs from stem cells. But there is also evidence for mature OSNs that are long-lived. Thus far modern genetic tools have not been applied to quantify survival of a population of OSNs that are mature at a given point in time. Here, a genetic strategy was developed to label irreversibly OMP-expressing OSNs in mice. A gene-targeted OMP-CreERT2 strain was generated in which mature OSNs express an enzymatically inactive version of the Cre recombinase. The fusion protein CreERT2 becomes transiently active when exposed to tamoxifen, and in the presence of a Cre reporter in the genome such as tdRFP, CreERT2-expressing cells become irreversibly labeled. A cohort of mice was generated with the same day of birth by in vitro fertilization and embryo transfer, and injected tamoxifen in their mothers at E18.5 of gestation. I counted RFP immunoreactive cells in the MOE and vomeronasal organ of 36 tamoxifen-exposed OMP-CreERT2 × tdRFP mice from 7 age groups: postnatal day (PD)1.5, PD3.5, PD6.5, 3 weeks, 9 weeks, 6 months, and 12 months. Approximately 7.8% of perinatally labeled cells remain at 12 months, confirming that some mature OSNs are indeed long-lived. The survival curve of the population of perinatally labeled MOE cells can be modeled with a mean half-life of 26 days for the population as a whole, excluding the long-lived cells.

摘要

成年小鼠的主要嗅觉上皮 (MOE) 中含有几百万个成熟的嗅觉感觉神经元 (OSN),这些神经元通常通过表达嗅觉标记蛋白 (OMP) 来定义为成熟。成熟的 OSN 从 MOE 底部的干细胞原位分化。共识观点认为,成熟的 OSN 具有确定的寿命,然后会经历程序性细胞死亡,而成年 MOE 通过从干细胞中产生新的成熟 OSN 来维持体内平衡。但也有证据表明成熟的 OSN 寿命较长。到目前为止,现代遗传工具尚未应用于定量分析在特定时间点成熟的 OSN 群体的存活情况。在这里,开发了一种遗传策略来标记在给定时间点表达不可逆 OMP 的 OSN。生成了一种基因靶向的 OMP-CreERT2 品系,其中成熟的 OSN 表达一种酶失活形式的 Cre 重组酶。当暴露于他莫昔芬时,融合蛋白 CreERT2 会短暂激活,并且在基因组中存在 Cre 报告基因(如 tdRFP)的情况下,CreERT2 表达的细胞会被不可逆地标记。通过体外受精和胚胎移植在同一天生成了一批小鼠,并在妊娠 E18.5 时给它们的母亲注射他莫昔芬。我在 36 只接受他莫昔芬处理的 OMP-CreERT2×tdRFP 小鼠的 MOE 和犁鼻器中计数了 7 个年龄组(出生后第 1.5、3.5、6.5 天、3 周、9 周、6 个月和 12 个月)的 RFP 免疫反应性细胞。大约 7.8% 的围产期标记细胞在 12 个月时仍然存在,这证实了一些成熟的 OSN 确实寿命较长。可以使用整个群体的平均半衰期为 26 天来对围产期标记的 MOE 细胞群体的存活曲线进行建模,排除长寿细胞。

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