A KNOCK-IN <EM>IGFN1</EM><SUP>ICRE</SUP> TRANSGENIC LINE PROVIDES PARTIAL DEVELOPMENTAL ACCESS TO DIRECTION SELECTIVE TYPE-7 BIPOLAR CELLS
Graduate University for Advanced Studies, SOKENDAI
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Date TBA
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Poster Board
PS02-07PM-636
Poster
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Here, we generated an Igfn1iCre knock-in mouse line and characterized Igfn1 positive cell morphology from birth to adult using Cre-dependent tdTomato reporter and viral labeling. We found Igfn1-positive cells first appeared in the outer retina at postnatal day 4 (P4), and later into the inner nuclear layer by P12–P15, predominantly labeling bipolar cells and some amacrine populations. At P15, about 71% of labeled bipolar cells stratified their axons in the S4 sublamina of the inner plexiform layer, consistent with documented BC7 morphology. In the adult retina, the widespread Igfn1-labeling appears slightly dominated in amacrine cells. Finally, to validate these observations, we examined Igfn1 expression in the publicly available Mouse Retina Cell Atlas. This analysis confirmed strong Igfn1 enrichment in BC7 and revealed lower-level expression in additional bipolar subtypes and amacrine cluster, mirroring experimental results.
Overall, these results reveal Igfn1iCre as a potential developmental tool for BC7 access and reveal unexpected, dynamic Igfn1 expression across retina maturation period.
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