Bid expression network controls neuronal cell fate during avian ciliary ganglion development
Abstract: Avian ciliary ganglion (CG) development involves a transient execution phase of apoptosis controlling the final number of neurons, but the time-dependent molecular mechanisms for neuronal cell fate are largely unknown. To elucidate the molecular networks regulating important aspects of parasympathetic neuronal development, a genome-wide expression analysis was performed during multiple stages of avian CG development between embryonic days E6 and E14. The transcriptome data showed a well-defined sequence of events, starting from neuronal migration via neuronal fate cell determination, synaptic transmission, and regulation of synaptic plasticity to growth factor associated signaling. In particular, we extracted a neuronal apoptosis network that characterized the cell death execution phase at E8/E9 and apoptotic cell clearance at E14 by combining the gene time series analysis with network synthesis from the chicken interactome. Network analysis identified TP53 as key regulator and predicted involvement of the BH3 interacting domain death agonist (BID). A virus-based RNAi knockdown approach in vivo showed a crucial impact of BID expression on the execution of ontogenetic programmed cell death (PCD). In contrast, Bcl-XL expression did not impact PCD. Therefore, BID-mediated apoptosis represents a novel cue essential for timing within CG maturation
- Standort
-
Deutsche Nationalbibliothek Frankfurt am Main
- Umfang
-
Online-Ressource
- Sprache
-
Englisch
- Anmerkungen
-
Frontiers in physiology. - 9 (2018) , 00797, ISSN: 1664-042X
- Ereignis
-
Veröffentlichung
- (wo)
-
Freiburg
- (wer)
-
Universität
- (wann)
-
2019
- Urheber
-
Koszinowski, Sophie
La Padula, Veronica
Edlich, Frank
Krieglstein, Kerstin
Busch, Hauke
Börries, Melanie
- DOI
-
10.3389/fphys.2018.00797
- URN
-
urn:nbn:de:bsz:25-freidok-1454875
- Rechteinformation
-
Kein Open Access; Der Zugriff auf das Objekt ist unbeschränkt möglich.
- Letzte Aktualisierung
-
14.08.2025, 10:44 MESZ
Datenpartner
Deutsche Nationalbibliothek. Bei Fragen zum Objekt wenden Sie sich bitte an den Datenpartner.
Beteiligte
- Koszinowski, Sophie
- La Padula, Veronica
- Edlich, Frank
- Krieglstein, Kerstin
- Busch, Hauke
- Börries, Melanie
- Universität
Entstanden
- 2019
Ähnliche Objekte (12)
Blind normalization of public high-throughput databases
Pattern formation and synchronization in excitable systems under the influence of spatiotemporal colored noise
Extrazelluläre Effekte des Ca2+-bindenden Proteins S100A1 : grundlegende Experimente zur Morphologie und Funktion neonataler Kardiomyozyten in Abhängigkeit der Kulturbedingungen
Searching of clinical trials made easier in cBioPortal using patients' genetic and clinical profiles
Targeting of apoptotic pathways by SMAC or BH3 mimetics distinctly sensitizes paclitaxel-resistant triple negative breast cancer cells
SNAIL1-mediated downregulation of FOXA proteins facilitates the inactivation of transcriptional enhancer elements at key epithelial genes in colorectal cancer cells
TGF[beta]-induced cytoskeletal remodeling mediates elevation of cell stiffness and invasiveness in NSCLC
Differences in DNA methylation and functional expression in lactase persistent and non-persistent individuals
Boolean modeling reveals the necessity of transcriptional regulation for bistability in PC12 cell differentiation
Extending cBioPortal for therapy recommendation documentation in molecular tumor boards: development and usability study
SNAIL1 employs [beta]‐Catenin‐LEF1 complexes to control colorectal cancer cell invasion and proliferation
MBECS: Microbiome Batch Effects Correction Suite
Blind normalization of public high-throughput databases
Pattern formation and synchronization in excitable systems under the influence of spatiotemporal colored noise
Extrazelluläre Effekte des Ca2+-bindenden Proteins S100A1 : grundlegende Experimente zur Morphologie und Funktion neonataler Kardiomyozyten in Abhängigkeit der Kulturbedingungen
Searching of clinical trials made easier in cBioPortal using patients' genetic and clinical profiles
Targeting of apoptotic pathways by SMAC or BH3 mimetics distinctly sensitizes paclitaxel-resistant triple negative breast cancer cells
SNAIL1-mediated downregulation of FOXA proteins facilitates the inactivation of transcriptional enhancer elements at key epithelial genes in colorectal cancer cells
TGF[beta]-induced cytoskeletal remodeling mediates elevation of cell stiffness and invasiveness in NSCLC
Differences in DNA methylation and functional expression in lactase persistent and non-persistent individuals
Boolean modeling reveals the necessity of transcriptional regulation for bistability in PC12 cell differentiation
Extending cBioPortal for therapy recommendation documentation in molecular tumor boards: development and usability study
SNAIL1 employs [beta]‐Catenin‐LEF1 complexes to control colorectal cancer cell invasion and proliferation
MBECS: Microbiome Batch Effects Correction Suite
Blind normalization of public high-throughput databases
Pattern formation and synchronization in excitable systems under the influence of spatiotemporal colored noise
Extrazelluläre Effekte des Ca2+-bindenden Proteins S100A1 : grundlegende Experimente zur Morphologie und Funktion neonataler Kardiomyozyten in Abhängigkeit der Kulturbedingungen
Searching of clinical trials made easier in cBioPortal using patients' genetic and clinical profiles
Targeting of apoptotic pathways by SMAC or BH3 mimetics distinctly sensitizes paclitaxel-resistant triple negative breast cancer cells
SNAIL1-mediated downregulation of FOXA proteins facilitates the inactivation of transcriptional enhancer elements at key epithelial genes in colorectal cancer cells
TGF[beta]-induced cytoskeletal remodeling mediates elevation of cell stiffness and invasiveness in NSCLC
Differences in DNA methylation and functional expression in lactase persistent and non-persistent individuals
Boolean modeling reveals the necessity of transcriptional regulation for bistability in PC12 cell differentiation
Extending cBioPortal for therapy recommendation documentation in molecular tumor boards: development and usability study
SNAIL1 employs [beta]‐Catenin‐LEF1 complexes to control colorectal cancer cell invasion and proliferation