Publication | Open Access
Polycomb group (PcG) proteins and Pax6 cooperate to inhibit <i>in vivo</i> reprogramming of the developing <i>Drosophila</i> eye
22
Citations
51
References
2018
Year
GeneticsMolecular GeneticsDistinct Pcg ComplexesTranscriptional RegulationWing FatePolycomb GroupCell DivisionDevelopmental GeneticsMorphogenesisInvertebrate VisionGene ExpressionCell BiologyGene FunctionBiologyPattern FormationCell LineageDevelopmental BiologyEvolutionary Developmental BiologyNatural SciencesCell Fate DeterminationMedicineCell Development
ABSTRACT How different cells and tissues commit to and determine their fates has been a central question in developmental biology since the seminal embryological experiments conducted by Wilhelm Roux and Hans Driesch in sea urchins and frogs. Here, we demonstrate that Polycomb group (PcG) proteins maintain Drosophila eye specification by suppressing the activation of alternative fate choices. The loss of PcG in the developing eye results in a cellular reprogramming event in which the eye is redirected to a wing fate. This fate transformation occurs with either the individual loss of Polycomb proteins or the simultaneous reduction of the Pleiohomeotic repressive complex and Pax6. Interestingly, the requirement for retinal selector genes is limited to Pax6, as the removal of more downstream members does not lead to the eye-wing transformation. We also show that distinct PcG complexes are required during different developmental windows throughout eye formation. These findings build on earlier observations that the eye can be reprogrammed to initiate head epidermis, antennal and leg development.
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