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Publication : Distribution, development, and identity of retinal ganglion cells labeled in the Sert-Cre reporter mouse.

First Author  Su J Year  2024
Journal  J Comp Neurol Volume  532
Issue  3 Pages  e25606
PubMed ID  38544361 Mgi Jnum  J:346779
Mgi Id  MGI:7618928 Doi  10.1002/cne.25606
Citation  Su J, et al. (2024) Distribution, development, and identity of retinal ganglion cells labeled in the Sert-Cre reporter mouse. J Comp Neurol 532(3):e25606
abstractText  The mouse retina contains over 40 types of retinal ganglion cells (RGCs) that differ in morphology, function, or gene expression. RGCs also differ by whether their axons target the brain.s ipsilateral or contralateral hemisphere. Contralaterally projecting RGCs (contraRGCs) are widespread in mouse retina, whereas ipsilateral projecting RGCs (ipsiRGCs) are confined to the ventro-temporal (VT) crescent of retina. In this study, we employed the Sert-Cre transgenic line, which had been reported to selectively label ipsiRGCs, to study ipsiRGCs during development. Although the number of Cre-expressing ipsiRGCs did not significantly increase with postnatal age, the region of retina that they occupied did, and by adulthood represented ~30% of the retinal surface. Unexpectedly, genetic ablation of Sert-Cre cells failed to fully disrupt ipsilateral projecting retinal axons, suggesting that not all ipsiRGCs generated Cre in Sert-Cre mice. To test this hypothesis, we retrogradely labeled ipsiRGCs in Sert-Cre mice which revealed that not all ipsiRGCs are labeled in Sert-Cre mice and a small population of contraRGCs flanking the VT crescent generates Cre in this line. These results do not negate the usefulness of the Sert-Cre mouse but do raise important caveats to the interpretation of such studies.
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