PUBLICATION

Knockdown of epigenetic transcriptional co-regulator Brd2a disrupts apoptosis and proper formation of hindbrain and midbrain-hindbrain boundary (MHB) region in zebrafish

Authors
Murphy, T., Melville, H., Fradkin, E., Bistany, G., Branigan, G., Olsen, K., Comstock, C.R., Hanby, H., Garbade, E., DiBenedetto, A.J.
ID
ZDB-PUB-170528-4
Date
2017
Source
Mechanisms of Development   146: 10-30 (Journal)
Registered Authors
DiBenedetto, Angela
Keywords
Bromodomain, Cell death, Cerebellum, Embryonic patterning, Engrailed, Midbrain-hindbrain boundary
MeSH Terms
  • Animals
  • Apoptosis/genetics
  • Epigenesis, Genetic/genetics
  • Gene Expression Regulation, Developmental
  • Homeodomain Proteins/genetics
  • Mesencephalon/growth & development
  • Morphogenesis/genetics*
  • Morpholinos/genetics
  • Nerve Tissue Proteins/genetics
  • Neural Tube/growth & development*
  • Protein Serine-Threonine Kinases/genetics*
  • Rhombencephalon/growth & development
  • Somites/growth & development
  • Transcription, Genetic*
  • Zebrafish/genetics
  • Zebrafish/growth & development
  • Zebrafish Proteins/genetics*
(all 17)
PubMed
28549975 Full text @ Mech. Dev.
Abstract
Brd2 is a member of the bromodomain-extraterminal domain (BET) family of proteins and functions as an acetyl-histone-directed transcriptional co-regulator and recruitment scaffold in chromatin modification complexes affecting signal-dependent transcription. While Brd2 acts as a protooncogene in mammalian blood, developmental studies link it to regulation of neuronal apoptosis and epilepsy, and complete knockout of the gene is invariably embryonic lethal. In Drosophila, the Brd2 homolog acts as a maternal effect factor necessary for segment formation and identity and proper expression of homeotic loci, including Ultrabithorax and engrailed. To test the various roles attributed to Brd2 in a single developmental system representing a non-mammalian vertebrate, we conducted a phenotypic characterization of Brd2a deficient zebrafish embryos produced by morpholino knockdown and corroborated by Crispr-Cas9 disruption and small molecule inhibitor treatments. brd2aMO morphants exhibit reduced hindbrain with an ill-defined midbrain-hindbrain boundary (MHB) region; irregular notochord, neural tube, and somites; and abnormalities in ventral trunk and ventral nerve cord interneuron positioning. Using whole mount TUNEL and confocal microscopy, we uncover a significant decrease, then a dramatic increase, of p53-independent cell death at the start and end of segmentation, respectively. In contrast, using qualitative and quantitative analyses of BrdU incorporation, phosphohistone H3-tagging, and flow cytometry, we detect little effect of Brd2a knockdown on overall proliferation levels in embryos. RNA in situ hybridization shows reduced or absent expression of homeobox gene eng2a and paired box gene pax2a, in the hindbrain domain of the MHB region, and an overabundance of pax2a-positive kidney progenitors, in knockdowns. Together, these results suggest an evolutionarily conserved role for Brd2 in the proper formation and/or patterning of segmented tissues, including the vertebrate CNS, where it acts as a bi-modal regulator of apoptosis, and is necessary, directly or indirectly, for proper expression of genes that pattern the MHB and/or regulate differentiation in the anterior hindbrain.
Genes / Markers
Marker Marker Type Name
brd2aGENEbromodomain containing 2a
egr2bGENEearly growth response 2b
en2aGENEengrailed homeobox 2a
hoxa2bGENEhomeobox A2b
hoxb1aGENEhomeobox B1a
otx2bGENEorthodenticle homeobox 2b
pax2aGENEpaired box 2a
tp53GENEtumor protein p53
wnt1GENEwingless-type MMTV integration site family, member 1
1 - 9 of 9
Show
Figures
Figure Gallery (13 images) / 2
Show all Figures
Expression
Phenotype
Fish Conditions Stage Phenotype Figure
ABchemical treatment: apoptosis inducerPrim-5
ABchemical treatment: apoptosis inducerPrim-5
AB + CRISPR1-brd2astandard conditionsPrim-5
AB + CRISPR1-brd2astandard conditionsPrim-5
AB + CRISPR1-brd2astandard conditionsPrim-5
AB + MO3-brd2astandard conditionsBud
AB + MO3-brd2astandard conditions14-19 somites
AB + MO3-brd2astandard conditions14-19 somites
AB + MO3-brd2astandard conditions14-19 somites
AB + MO3-brd2astandard conditions14-19 somites
1 - 10 of 58
Show
Mutations / Transgenics
No data available
Human Disease / Model
No data available
Sequence Targeting Reagents
Target Reagent Reagent Type
brd2aCRISPR1-brd2aCRISPR
brd2aMO3-brd2aMRPHLNO
brd2aMO4-brd2aMRPHLNO
tp53MO4-tp53MRPHLNO
1 - 4 of 4
Show
Fish
Fish
AB
AB/C32
AB + CRISPR1-brd2a
AB + MO3-brd2a
AB + MO3-brd2a + MO4-brd2a
AB + MO3-brd2a + MO4-tp53
AB + MO4-brd2a
AB + MO4-tp53
1 - 8 of 8
Show
Antibodies
Orthology
Engineered Foreign Genes
No data available
Mapping
Your Input Welcome
We welcome your input and comments. Please use this form to recommend updates to the information in ZFIN. We appreciate as much detail as possible and references as appropriate. We will review your comments promptly.
Citation
Murphy, T., Melville, H., Fradkin, E., Bistany, G., Branigan, G., Olsen, K., Comstock, C.R., Hanby, H., Garbade, E., DiBenedetto, A.J. (2017) Knockdown of epigenetic transcriptional co-regulator Brd2a disrupts apoptosis and proper formation of hindbrain and midbrain-hindbrain boundary (MHB) region in zebrafish. Mechanisms of Development. 146:10-30.