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Investigating the Gene Regulatory Networks Linking Neuronal Identity Specification and Differentiation

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dc.contributor.advisor Ozel, Neset
dc.contributor.author PANDEY, KRISH
dc.date.accessioned 2025-05-16T07:42:36Z
dc.date.available 2025-05-16T07:42:36Z
dc.date.issued 2025-05
dc.identifier.citation 71 en_US
dc.identifier.uri http://dr.iiserpune.ac.in:8080/xmlui/handle/123456789/9902
dc.description.abstract Neuronal diversity emerges from the spatial and temporal patterning of neural stem cells by various signaling molecules and transcription factors (TFs). This diversity is subsequently established and maintained by another set of TFs called terminal selectors. In the Drosophila optic lobe, these progenitor patterning factors and the unique terminal selector combinations in post-mitotic neurons have been comprehensively described. To understand how information is relayed between these two regulatory programs, we studied Tm2 and Tm6 neurons, with a focus on SoxNeuro, a highly important neurodevelopmental factor. We find that Tm6 terminal selector SoxN is also detectable but not required in Tm2 neurons. We showed that Erm, a candidate terminal selector for Tm1 neurons, a related type, cannot be detected within them and upon its knockdown, no phenotypic changes are observed. We leveraged a simultaneously performed scRNA and ATAC-seq (multiome) dataset to find differentially accessible enhancers of SoxN and generate a reporter line for a candidate enhancer in Tm6. We find that while it does not label cell types of interest and labels non-target cells, it works differently based upon its directionality. Finally, we studied the role of temporal TFs (tTFs), Esg and Ey, in regulating SoxN in Tm1/2/4/6 neurons during neurogenesis and found that Esg overexpression does not affect the normal patterning of these neurons but Ey, that is known to stop the production of Tm2/6, leads to the production of more Tm4 neurons specifically. Overall, the interface of fate specification and identity differentiation is a complex program that resolves developmental history into unique neuronal identities, understanding which can unlock potential for selectively generating and designing neurons to achieve therapeutic ends. en_US
dc.language.iso en_US en_US
dc.subject Neuroscience en_US
dc.subject Developmental Biology en_US
dc.subject Drosophila en_US
dc.subject Gene Regulatory Networks en_US
dc.subject Fly Optic Lobe en_US
dc.subject Neurodevelopment en_US
dc.subject Patterning en_US
dc.subject Neuronal Diversity en_US
dc.title Investigating the Gene Regulatory Networks Linking Neuronal Identity Specification and Differentiation en_US
dc.type Thesis en_US
dc.type Working Paper en_US
dc.description.embargo Two Years en_US
dc.type.degree BS-MS en_US
dc.contributor.department Dept. of Biology en_US
dc.contributor.registration 20201075 en_US


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  • MS THESES [1970]
    Thesis submitted to IISER Pune in partial fulfilment of the requirements for the BS-MS Dual Degree Programme/MSc. Programme/MS-Exit Programme

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