A conserved maternal-specific repressive domain in Zelda revealed by Cas9-mediated mutagenesis in Drosophila melanogaster

Hamm, Danielle C.; Larson, Elizabeth D; Nevil, Markus; Marshall, Kelsey E.; Bondra, Eliana R.; Harrison, Melissa M.

doi:10.1371/journal.pgen.1007120

Cited by 40 publications

(51 citation statements)

References 45 publications

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“…The highly anomalous nature of the movement of Zld that differs from that of chromatin associated His2B and Bcd suggests that its motion depends at least in part on interactions off of DNA. Most of the amino acid sequence of Zld consists of intrinsically disordered domains, some of which are required for its function (Hamm et al 2017) . We and others have shown that intrinsically disordered domains mediate weak, multivalent proteinprotein interactions between regulatory factors (Chong et al 2018; Boehning et al 2018; Kovar 2011; Burke et al 2015; Altmeyer et al 2015; Xiang et al 2015; Friedman et al 2007) that lead to the selective enrichment of factors in hubs (Chong et al 2018; Boehning et al 2018 .…”

Section: Our Observation That Zld and Bcd Form Hubs Of Locally High Cmentioning

confidence: 99%

“…However, how it accomplishes this remains unclear. Zelda has a cluster of four C2H2 Znfingers near the Cterminus that mediate its DNA binding activity and 2 additional ZFs near the Nterminus which have been implicated in controlling its activation potential (Hamm et al 2017) , but most of the rest of the protein consists of varying types of lowcomplexity sequence.…”

Section: Introductionmentioning

confidence: 99%

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Dynamic multifactor hubs interact transiently with sites of active transcription inDrosophilaembryos

Mir

Stadler

Ortiz

et al. 2018

Preprint

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The regulation of transcription requires the coordination of numerous activities on DNA, yet it remains poorly understood how transcription factors facilitate these multiple functions. Here we use lattice lightsheet microscopy to integrate singlemolecule and highspeed 4D imaging in developing Drosophila embryos to study the nuclear organization and interactions of the key patterning factors Zelda and Bicoid. In contrast to previous studies suggesting stable, cooperative binding, we show that both factors interact with DNA with surprisingly high offrates. We find that both factors form dynamic subnuclear hubs, and that Bicoid binding is enriched within Zelda hubs. Remarkably, these hubs are both short lived and interact only transiently with sites of active Bicoid dependent transcription. Based on our observations we hypothesize that, beyond simply forming bridges between DNA and the transcription machinery, transcription factors can organize other proteins into hubs that transiently drive multiple activities at their gene targets. 1 15 20 25 30 35

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Section: Our Observation That Zld and Bcd Form Hubs Of Locally High Cmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Dynamic multifactor hubs interact transiently with sites of active transcription inDrosophilaembryos

Mir

Stadler

Ortiz

et al. 2018

Preprint

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“…To better understand this surprising result, we examined Zld dynamics in living embryos and particularly during mitosis ( Figure 4). We took advantage of an endogenously tagged fluorescent version of Zld 24 . The GFP-zld flies are homozygous viable, thereby showing that the GFP-tagged version of Zld retains wild-type physiological properties.…”

Section: Quantitative Kinetic Analysis Reveals the Dynamic Propertiesmentioning

confidence: 99%

“…RNAi were expressed following crosses between this recombinant and UASp-shRNA-w (BL35573) or UASp-shRNA-zld 21 , virgin females expressing RNAi, MCP-GFP-His2Av-mRFP were crossed with MS2 containing transgenic constructs. The GFP-zld strain was obtained by CRISPR 24 . GFP-ash1 26 and His2Av-mRFP (BL23651).…”

Section: Drosophila Stocks and Geneticsmentioning

confidence: 99%

Temporal Control of Transcription by Zelda in living Drosophila embryos

Dufourt

Trullo

Hunter

et al. 2018

Preprint

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Abstract/introPioneer factors have the exquisite ability to engage their target sites at nucleosomal DNA, which leads to a local remodeling of chromatin and the establishment of a transcriptional competence. However, the direct impact of enhancer priming by pioneer factors on the temporal control of gene expression and on mitotic memory remains elusive. In Drosophila embryos, the maternally deposited activator Zelda (Zld) exhibits key pioneer factor properties and indeed regulates the awakening of the zygotic genome. The analysis of thousands of endogenous Zld bound regions in various genetic contexts, as well as the study of isolated synthetic enhancers with static approaches, led to the proposal that Zld could act as a quantitative developmental timer. Here we employ quantitative live imaging methods and mathematical modeling to directly test the effect of Zld on temporal coordination in gene activation and on mitotic memory. Using an automatic tracking software, we quantified the timing of activation in hundreds of nuclei and their progeny in Drosophila embryos. We demonstrate that increasing the number of Zld binding sites accelerates the kinetics of transcriptional activation regardless of their past transcriptional state. In spite of its known pioneering activities, we show that Zld is not a mitotic bookmarker and is neither necessary nor sufficient to foster mitotic memory. Fluorescent recovery after photo-bleaching and fluorescent correlation spectroscopy experiments reveal that, Zld is highly dynamic and exhibits transient binding to chromatin. We propose that Zld low binding rates could be compensated for by local accumulation of Zld in nuclear microenvironments in vivo, thus allowing rapid and coordinated gene activation.All rights reserved. No reuse allowed without permission.(which was not peer-reviewed) is the author/funder, who has granted bioRxiv a license to display the preprint in perpetuity.The copyright holder for this preprint . http://dx.doi.org/10.1101/282426 doi: bioRxiv preprint first posted online Mar. 14, 2018; 2 Results and Discussion Zelda fosters temporal transcriptional coordinationIn the blastoderm embryo, two redundant enhancers control snail (sna) gene expression, a proximal (primary) and a distal (shadow enhancer) 1,2 . Both enhancers are bound by Zelda (Zld) at early nuclear cycles 3,4 . Expression driven by the long intact shadow enhancer (sna-shadow) leads to rapid transcriptional activation, precluding analysis of the impact of Zld on fine-tuning the timing of this activation ( Figure S1, A-B). We therefore used a previously described truncated version of the sna shadow enhancer (snaE) that leads to a stochastic activation, compatible with mitotic memory tracking 5 .To follow transcriptional dynamics in a quantitative manner, we created a series of enhancer

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“…The functional study of Zelda domains was approached using a Cas9 engineering system to obtain D. melanogaster insects with point mutations in the Zinc finger 1, in the acidic patch, or in the Zinc finger 2 (JAZ) [16]. Mutations in the Zinc finger 1 or in the acidic patch did not affect the viability of the insects, whereas mutations in the Zinc finger 2 (JAZ) led to a maternal-effect lethal phenotype [16]. A transcriptomic analysis of mutated flies showed that the Zinc finger 2 (JAZ) acts as a maternal repressive domain during embryo development, being associated with the transcriptional regulation of the zygotic Zelda targets and with the clearance of maternal transcripts [16].…”

Section: Introductionmentioning

confidence: 99%

Zelda and the maternal‐to‐zygotic transition in cockroaches

2019

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In the endopterygote Drosophila melanogaster, Zelda is an activator of the zygotic genome during the maternal‐to‐zygotic transition (MZT). Zelda binds cis‐regulatory elements (TAGteam heptamers), making chromatin accessible for gene transcription. Zelda has been studied in other endopterygotes: Apis mellifera and Tribolium castaneum, and the paraneopteran Rhodnius prolixus. We studied Zelda in the cockroach Blattella germanica, a hemimetabolan, short germ‐band, and polyneopteran species. B. germanica Zelda has the complete set of functional domains, which is typical of species displaying ancestral features concerning embryogenesis. Interestingly, we found D. melanogaster TAGteam heptamers in the B. germanica genome. The canonical one, CAGGTAG, is present at a similar proportion in the genome of these two species and in the genome of other insects, suggesting that the genome admits as many CAGGTAG motifs as its length allows. Zelda‐depleted embryos of B. germanica show defects involving blastoderm formation and abdomen development, and genes contributing to these processes are down‐regulated. We conclude that in B. germanica, Zelda strictly activates the zygotic genome, within the MZT, a role conserved in more derived endopterygote insects. In B. germanica, zelda is expressed during MZT, whereas in D. melanogaster and T. castaneum it is expressed beyond this transition. In these species and A. mellifera, Zelda has functions even in postembryonic development. The expansion of zelda expression beyond the MZT in endopterygotes might be related with the evolutionary innovation of holometabolan metamorphosis. Databases The RNA‐seq datasets of B. germanica, D. melanogaster, and T. castaneum are accessible at the GEO databases https://www.ncbi.nlm.nih.gov/geo/query/acc.cgi?acc=GSE99785, https://www.ncbi.nlm.nih.gov/geo/query/acc.cgi?acc=GSE18068, https://www.ncbi.nlm.nih.gov/geo/query/acc.cgi?acc=GSE63770, and https://www.ncbi.nlm.nih.gov/geo/query/acc.cgi?acc=GSE84253. In addition, the RNA‐seq library from T. castaneum adult females is available at SRA: SRX021963. The B. germanica reference genome is available as BioProject PRJNA203136.

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A conserved maternal-specific repressive domain in Zelda revealed by Cas9-mediated mutagenesis in Drosophila melanogaster

Cited by 40 publications

References 45 publications

Dynamic multifactor hubs interact transiently with sites of active transcription inDrosophilaembryos

Dynamic multifactor hubs interact transiently with sites of active transcription inDrosophilaembryos

Temporal Control of Transcription by Zelda in living Drosophila embryos

Zelda and the maternal‐to‐zygotic transition in cockroaches

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