Please use this identifier to cite or link to this item: http://hdl.handle.net/10603/431977
Title: Identification and characteriation of novel tumor suppressors using in vivo tumor model in drosophila melanogaster
Researcher: NAGARKAR, SANKET
Guide(s): SHASHIDHARA, L.S.
Keywords: Genetics and Heredity
Life Sciences
Molecular Biology and Genetics
University: Indian Institute of Science Education and Research (IISER) Pune
Completed Date: 2020
Abstract: Cancer is a disease that hitch hikes growth regulatory network and causes uncontrollable cell proliferation and metastasis which is usually fatal Genetic alterations in cancer cells enable such hitch hiking of regulatory networks These alterations allow cancer cells to acquire abilities to grow and metastasize which together with other enabling characteristics of cancer form the hallmarks of cancer Cancer cells gradually acquire multiple hallmark characteristics defining cancer progression as a multi step process Disease progression and accumulating genetic alterations suggest cooperative mechanisms underlying progression of disease which is also supported by experimental evidence Thus it is of fundamental importance to identify causal genetic alterations in different cancer types This has motivated a large number of genome wide omics studies which have revealed a plethora of genomic transcriptomic changes in cancer tissues Resultant large data has presented a bigger challenge of identifying relevant causal factors To understand the cooperative mechanisms underlying tumorigenesis we carried out a genome wide screen in Drosophila tumor model for epithelial cancers We used epithelial growth factor EGFR and Yorkie Yki as oncogenic drivers and depleted one gene at a time using RNAi mediated knock down in each of these contexts We have identified several novel putative tumor suppressors depletion of which enhance effects of EGFR and Yki resulting in massive overgrowth of wing imaginal discs Interestingly we identified components of the Negative Elongation Factor Complex NELF as tumor suppressors specifically in context of Yki These findings were particularly intriguing because Yki is a co activator of transcription while the NELF complex is required for promoter proximal pausing PPP PPP as the name suggests occurs in region proximal to transcription start site and has been shown to be a critical regulatory mechanism in transcription of genes in response to stimuli before elongation phase and after promo newline newline
Pagination: NA
URI: http://hdl.handle.net/10603/431977
Appears in Departments:Department of Biology

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