Primary afferent neurons that convey somatosensory modalities comprise two large, heterogeneous populations: small-diameter neurons that give rise to slowly conducting unmyelinated axonal C fibers and medium-to-large diameter neurons with fast myelinated A fibers. Despite these two major groupings, tools to differentiate between unmyelinated and myelinated primary afferent fibers by genetic targeting have not been available; in particular, whereas numerous mouse driver lines exist to target different C fiber populations, genetic tools that target myelinated primary afferent populations are scarce. Here we describe a knock-in mouse line expressing tamoxifen-dependent CreERT2 under control of the Nefh gene, which encodes neurofilament heavy chain (NFH or NF200), a protein that is highly enriched in myelinated fibers. This mouse enables highly selective and efficient recombination of Cre-dependent reporters for functional and anatomical interrogation of myelinated fibers while excluding unmyelinated C fibers. In combination with other recombinase-expressing mouse lines, this genetic tool will be valuable for intersectional targeting of subpopulations of myelinated primary afferent fibers.
Genetic targeting of myelinated primary afferent neurons using a new Nefh(CreERT2) knock-in mouse.
利用新型 Nefh(CreERT2) 敲入小鼠对有髓初级传入神经元进行基因靶向
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作者:Chen John Cy, Kaczmarczyk Lech, de-Faria Felipe Meira, Szczot Marcin, Jackson Walker S, Larsson Max
| 期刊: | Scientific Reports | 影响因子: | 3.900 |
| 时间: | 2025 | 起止号: | 2025 Mar 29; 15(1):10890 |
| doi: | 10.1038/s41598-025-95874-2 | 种属: | Mouse |
| 研究方向: | 神经科学 | ||
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