Project description:Identification of genes regulated by the transcription factor HNF4a2 Experiment Overall Design: We used microarrays to identify genes regulated by the transcription factor HNF4a2. HEK293 cell lines containing doxycyclin-inducible wilt type or mutant forms of HNF4a2m which were introduced by FRT/FLP mediated recombination into FLP-In T-REx 293 cells (Invitrogen) were treated for 24 hours with 1 µg/ml doxycyclin. Gene expression profiles of induced and noninduced cells were compared to identify HNF4 regulated targets.

Project description:We explore the transcriptional response of mammalian cells undergoing various insults to Golgi homeostasis. HEK293 cells (Flp-In T-REx 293 cells) stably containing a doxycycline-inducible Golgi-localized HaloTag2 construct (GA-HT2) were treated with the ionophore nigericin, the glycosylation inhibitor xyloside, or were induced by doxycycline and treated with the hydrophobic tag HyT36 to induce destabilization of GA-HT2. We found that while nigericin and xyloside induce global transcriptional changes, destabilization of GA-HT2 induces a Golgi-specific response.

Project description:Here we investigated the effects of CEBPA transcription factor expression on myeloid NB4 cells. The sequence of rat CEBPA was C-terminally fused to a promiscuous biotin ligase tag (BirA*) and NB4 cell lines were engineered to express the fusion protein under the control of a doxycycline inducible promoter. Three different NB4 cell lines were investigated that expressed (i) BirA* tag alone (ii) full length CEBPA isoform (P42) fused to BirA* (iii) truncated CEBPA isoform (P30) fused to BirA*. Cells were seeded in media supplemented with or without doxycycline.

Project description:To gain insights into the interactome of wild-type (WT) and S102P mutant GATAD1, we utilized the BioID method, which enables the study of protein-protein interactions. Specifically, we performed BioID proximity labeling experiments in stable Flp-In cells expressing different GATAD1 variants fused to BirA*_FLAG. These variants included BirA*_FLAG_GATAD1-WT, BirA*_FLAG_GATAD1-S102P, BirA*_FLAG_GATAD1-S102D, and BirA*_FLAG_GATAD1-S102A. By employing this approach, we aimed to characterize the protein interactors associated with these GATAD1 variants and gain insights into the functional consequences of the S102P mutation.

Project description:hnRNP M and Rbfox proteins are subunits of the Large Assembly of Splicing Regulators (LASR). The purpose of this study is to investigate how these two splicing factors affect each others' role in regulating splice site choices in pre-mRNA. hnRNP M is knocked down by RNAi in Flp-In T-REx 293 cells (Invitrogen), whereas Rbfox1 is expressed inducibly under tetracycline control from construct integrated into the genome at the FRT site. Using this system, splicing and expression profiles of cells expressing and/or lacking these proteins are compared on a whole genome level by RNA-seq technology.

Project description:RNAi-seq of stable Flp-In™ T-Rex Hela cells that inducibly expressed PP1-NIPP1 and mutants.

Project description:Flp-In T-REx-293 cells transfected with non-targeting control siRNA or UPF1-specific siRNA as indicated and used for total RNA-seq.

Project description:BioID Controls for Flp-In T-REx HEK293 cells are the following; Empty Vector: VL_20151116_COT_01_HEK293_pcDNA5EV_HB VL_20151116_COT_02_HEK293_pcDNA5EV_HB VL_20151116_COT_03_HEK293_pcDNA5EV_HB VL_20151116_COT_04_HEK293_pcDNA5EV_HB BirA-Flag-EGFP: VL_20150825_COT_05_HB VL_20150825_COT_06_HB VL_20150825_COT_07_HB VL_20150825_COT_08_HB BirA-Flag-EGFP-CAAX: VL_20181019_COT_01_HB VL_20181019_COT_02_HB VL_20181019_COT_03_HB VL_20181019_COT_04_HB BioID samples for Flp-In T-REx HEK293 cells are the following; RAC1_WT: 2186_ZL_RAC1_WT_BR1_Velos1_P103_HB 2308_ZL_RAC1_WT_BR2_Velos1_HB RHOG_WT: VL_20170123_COT_01_HB VL_20170123_COT_02_HB RHOA_WT: VL_20160323_COT_04new2_HB VL_20180104_COT_01_HB CDC42_WT: VL_20180104_COT_03_HB VL_20180104_COT_04_HB RAC1_G15A: VL_20180105_COT_01_2_HB VL_20180105_COT_02_HB CDC42_G15A: VL_20180105_COT_03_HB VL_20180105_COT_04_HB RHOG_G15A: VL_20180108_COT_01_HB VL_20180108_COT_02_HB RHOA_G17A: VL_20180108_COT_03_HB VL_20180108_COT_04_HB CDC42_G12V: 2189_ZL_CDC42_G12V_BR1_Velos1_P103_HB 2263_ZL_CDC42_G12V_BR2_Velos1_HB RAC1_G12V: 1871_RAC1_G12V_BirA_Flag_HEK293_2-2_HB VL_20150825_COT_02_HB RAC2_G12V: 2199_ZL_RAC2_G12V_BR1_Velos1_P103_HB 2323_ZL_RAC2_G12V_BR2_Velos1_HB RAC3_G12V: 2200_ZL_RAC3_G12V_BR1_Velos1_P103_HB 2321_ZL_RAC3_G12V_BR2_Velos1_HB RHOA_G14V: 2190_ZL_RHOA_G14V_BR1_Velos1_P103_HB 2262_ZL_RHOA_G14V_BR2_Velos1_HB RHOB_G14V: 2191_ZL_RHOB_G14V_BR1_Velos1_P103_HB 2261_ZL_RHOB_G14V_BR2_Velos1_HB RHOBTB1_WT: 2201_ZL_RHOBTB1_WT_BR1_Velos1_P103_HB 2320_ZL_RHOBTB1_WT_BR2_Velos1_HB RHOBTB2_WT: 2202_ZL_RHOBTB2_WT_BR1_Velos1_P103_HB 2318_ZL_RHOBTB2_WT_BR2_Velos1_HB RHOC_G14V: 2192_ZL_RHOC_G14V_BR1_Velos1_P103_HB 2260_ZL_RHOC_G14V_BR2_Velos1_HB RHOD_G26V: 2193_ZL_RHOD_G26V_BR1_Velos1_P103_HB 2259_ZL_RHOD_G26V_BR2_Velos1_HB RHOF_G28V: 2246_ZL_RHOF_G28V_BR1_2194ReRun_Velos1_P103_HB 2258_ZL_RHOF_G28V_BR2_Velos1_HB RHOG_G12V: 2306_ZL_RHOG_G12V_BR2_Velos1_HB VL_20170123_COT_03_HB RHOH_WT: 2203_ZL_RHOH_WT_BR1_Velos1_P103_HB 2317_ZL_RHOH_WT_BR2_Velos1_HB RHOJ_G40V: 2195_ZL_RHOJ_G40V_BR1_Velos1_P103_HB 2257_ZL_RHOJ_G40V_BR2_Velos1_HB RHOQ_G18V: 2196_ZL_RHOQ_G18V_BR1_Velos1_P103_HB 2338_ZL_RHOQ_G18V_BR2_Velos1_HB RHOU_G58V: 2250_ZL_RHOU_G58v_BR1_2197ReRun_Velos1_P103_HB 2337_ZL_RHOU_G58V_BR2_Velos1_HB RHOV_G40V: 2198_ZL_RHOV_G40V_BR1_Velos1_P103_HB 2324_ZL_RHOV_G40V_BR2_Velos1_HB RND1_WT: 2249_ZL_RND1_WT_BR1_Velos1_P103_HB 2313_ZL_RND1_WT_BR2_Velos1_HB RND2_WT: 2247_ZL_RND2_WT_BR1_Velos1_P103_HB 2315_ZL_RND2_WT_BR2_Velos1_HB RND3_WT: VL_20151116_COT_05_HB VL_20151116_COT_06_HB BioID Controls for Flp-In T-REx HeLa cells are the following; Empty Vector: QE_20180917_COT_01_HB QE_20180917_COT_02_HB QE_20180917_COT_03_HB QE_20180917_COT_04_HB BirA-Flag-EGFP: QE_20151030_COT_02_HB QE_20151030_COT_03_HB QE_20151030_COT_04_HB QE_20151030_COT_05_HB BirA-Flag-EGFP-CAAX: QE_20181022_COT_01_HB QE_20181022_COT_02_HB QE_20181022_COT_03_HB QE_20181022_COT_04_HB BioID samples for Flp-In T-REx HeLa cells are the following; CDC42_G15A: QE_20171218_COT_05_HB QE_20171218_COT_06_HB CDC42_WT: QE_20171218_COT_01_HB QE_20171218_COT_02_HB RAC1_G15A: QE_20171218_COT_03_HB QE_20171218_COT_04_HB RAC1_WT: QE_20151102_COT_01_HB QE_20151102_COT_02_HB RHOA_G17A: QE_20171218_COT_07_HB QE_20171218_COT_08_HB RHOA_WT: QE_20171201_COT_07_HB QE_20171201_COT_08_HB RHOG_G15A: QE_20171220_COT_01_HB QE_20171220_COT_02_HB RHOG_WT: QE_20161215_COT_01_HB QE_20161215_COT_02_HB CDC42_G12V: QE_20171201_COT_09_HB QE_20171201_COT_10_HB RAC1_G12V: QE_20151030_COT_06_HB QE_20151030_COT_07_HB RAC2_G12V: QE_20180105_COT_05_HB QE_20180105_COT_06_HB RAC3_G12V: QE_20180105_COT_07_HB QE_20180105_COT_08_HB RHOA_G14V: QE_20171205_COT_17_HB QE_20171205_COT_18_HB RHOB_G14V: QE_20180105_COT_01_HB QE_20180105_COT_02_HB RHOBTB1_WT: QE_20180108_COT_07_HB QE_20180108_COT_08_HB RHOBTB2_WT: QE_20171205_COT_19_HB QE_20171205_COT_20_HB RHOC_G14V: QE_20180105_COT_03_HB QE_20180105_COT_04_HB RHOD_G26V: QE_20180108_COT_05_HB QE_20180108_COT_06_HB RHOF_G28V: QE_20171130_COT_05_HB QE_20171130_COT_06_HB RHOG_G12V: QE_20161215_COT_03_HB QE_20161215_COT_04_HB RHOH_WT: QE_20171204_COT_15_HB QE_20171204_COT_16_HB RHOJ_G40V: QE_20171130_COT_03_HB QE_20171130_COT_04_HB RHOQ_G18V: QE_20180105_COT_09_HB QE_20180105_COT_10_HB RHOU_G58V: QE_20171204_COT_11_HB QE_20171204_COT_12_new_HB RHOV_G40V: QE_20171130_COT_01_HB QE_20171130_COT_02_HB RND1_WT: QE_20180108_COT_01_HB QE_20180108_COT_02_HB RND2_WT: QE_20171204_COT_13_HB QE_20171204_COT_14_HB RND3_WT: QE_20180108_COT_03_HB QE_20180108_COT_04_HB

Project description:PHYHD1 is a 2-oxoglutarate-dependent dioxygenase. To shed light on the cellular function of human PHYHD1, we performed a BioID screening experiment to map proteins linked to PHYHD1 functionally. For that, we used HEK293T cells transiently expressing either BirA* or BirA*-tagged PHYHD1 in the absence or presence of biotin.

Project description:A 2-hour heat-shock at 37C was used to activate hs-FLP and an actin5C-FRT-stop-FRT-GAL4 transgene in larvae carrying any possible combination of the genetic elements UAS-Myc, UAS-Atu-IR, Max-/-. 48 hours later 16-27 wing imaginal discs were isolated from wandering L3 larvae and polyA-RNA was processed for sequencing.