Abstract
BackgroundMaintaining the correct balance of proliferation versus differentiation in retinal progenitor cells (RPCs) is essential for proper development of the retina. The cell cycle regulator cyclin D1 is expressed in RPCs, and mice with a targeted null allele at the cyclin D1 locus (Ccnd1-/-) have microphthalmia and hypocellular retinas, the latter phenotype attributed to reduced RPC proliferation and increased photoreceptor cell death during the postnatal period. How cyclin D1 influences RPC behavior, especially during the embryonic period, is unclear.ResultsIn this study, we show that embryonic RPCs lacking cyclin D1 progress through the cell cycle at a slower rate and exit the cell cycle at a faster rate. Consistent with enhanced cell cycle exit, the relative proportions of cell types born in the embryonic period, such as retinal ganglion cells and photoreceptor cells, are increased. Unexpectedly, cyclin D1 deficiency decreases the proportions of other early born retinal neurons, namely horizontal cells and specific amacrine cell types. We also found that the laminar positioning of horizontal cells and other cell types is altered in the absence of cyclin D1. Genetically replacing cyclin D1 with cyclin D2 is not efficient at correcting the phenotypes due to the cyclin D1 deficiency, which suggests the D-cyclins are not fully redundant. Replacement with cyclin E or inactivation of cyclin-dependent kinase inhibitor p27Kip1 restores the balance of RPCs and retinal cell types to more normal distributions, which suggests that regulation of the retinoblastoma pathway is an important function for cyclin D1 during embryonic retinal development.ConclusionOur findings show that cyclin D1 has important roles in RPC cell cycle regulation and retinal histogenesis. The reduction in the RPC population due to a longer cell cycle time and to an enhanced rate of cell cycle exit are likely to be the primary factors driving retinal hypocellularity and altered output of precursor populations in the embryonic Ccnd1-/- retina.
Highlights
Maintaining the correct balance of proliferation versus differentiation in retinal progenitor cells (RPCs) is essential for proper development of the retina
We found that the cell cycle rate of the cyclin D1 (Ccnd1)-/- RPC population is slower than normal and this population undergoes a faster rate of depletion due to an increased rate of cell cycle exit
We found that a significantly higher percentage of BrdU+ RPCs exit the cell cycle and form retinal ganglion cell (RGC) in the Ccnd1-/- retina from E13.5 to E14.5 (Figure 4J), confirming that enhanced cell cycle exit of Ccnd1/- RPCs leads to increased proportions of early born neurons
Summary
Maintaining the correct balance of proliferation versus differentiation in retinal progenitor cells (RPCs) is essential for proper development of the retina. The vertebrate retina is composed of seven major cell classes that arise from a common source, the retinal progenitor cell (RPC) population. Cones account for approximately 3% and rods approximately 97% of the photoreceptors in the mouse retina, and rod photoreceptors are the most abundant cell class accounting for approximately 70% of all retinal cells [1]. While cell death contributes to the final cell distribution of the adult retina [4,6], the initial allocation of precursor cells (that is, RPCs that exit the cell cycle) to each class is a predominant factor in setting their relative proportions
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