Tissue Specific Roles for the Ribosome Biogenesis Factor Wdr43 in Zebrafish Development

Zhao, Chengtian; Andreeva, Viktoria; Gibert, Yann; LaBonty, Melissa; Lattanzi, Victoria J.; Prabhudesai, Shubhangi; Zhou, Yi; Zon, Leonard I.; McCann, Kathleen L.; Baserga, Susan J.; Yelick, Pamela C.

doi:10.1371/journal.pgen.1004074

Cited by 44 publications

(65 citation statements)

References 64 publications

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“…The fan mutant embryos exhibited increased apoptosis and reduced proliferation of the developing CNC. Furthermore, fan mutant embryos have decreased steady-state levels of prerRNAs and pre-rRNA processing defects (Zhao et al 2014), as expected from previous studies of the molecular function Utp5/ WDR43 (Gallagher et al 2004;Prieto and McStay 2007). Apoptosis mediated by p53 due to defects in ribosome biogenesis is conserved across species.…”

Section: Utp5/wdr43 and Diseasesupporting

confidence: 72%

“…Since depletion or dysfunction of Utp5 or any of its interacting partners in the t-Utp/UTPA subcomplex results in defects in pre-rRNA transcription and processing (Gallagher et al 2004) and because ribosome biogenesis defects result in craniofacial dysmorphology, all the protein-protein interactions of Utp5/WDR43 are likely to have significance in the development of craniofacial structures. This hypothesis is supported by a zebrafish mutant with a premature stop codon in WDR43, which results in a C-terminal truncation that abrogates the interaction between WDR43 and UTP15 and the interaction between WDR43 and UTP4 (Zhao et al 2014). The same mutation in WDR43 that disrupts protein-protein interactions also causes severe craniofacial defects.…”

Section: Discovery and Role Of Utp5 In The Yeast Saccharomyces Cerevimentioning

confidence: 95%

“…A study that systemically tested whether human proteins could complement their yeast orthologs did not test Utp5/WDR43 (Kachroo et al 2015), although its functional conservation suggests that human WDR43 may complement yeast Utp5. Furthermore, injection of human Wdr43 mRNA partially rescues the zebrafish fantome (fan) / wdr43 mutant craniofacial phenotype (Zhao et al 2014). Overall, there is ample evidence to support a functional conservation for the role of Utp5/WDR43 from yeast to humans.…”

Section: Role and Conservation Of Utp5/ Wdr43 In Other Eukaryotesmentioning

confidence: 96%

“…Black arrows indicate an interaction found by PCA (Tarassov et al 2008), yeast 2-hybrid (Uetz et al 2000;, in vitro reconstitution (Poll et al 2014) and that the interaction is conserved for the human orthologs of the proteins (Sato et al 2013). Blue crosses indicate protein-protein interactions that are disrupted in fantome mutant zebrafish and result in craniofacial defects (Zhao et al 2014). …”

Section: Role and Conservation Of Utp5/ Wdr43 In Other Eukaryotesmentioning

confidence: 99%

“…Despite possible alternative functions for these proteins associated with craniofacial defects, all of them are required for efficient transcription of pre-rRNA, thus offering a strong argument that defects in ribosome synthesis-and the likely consequential disruptions in messenger RNA (mRNA) translation and protein synthesis-lie at the heart of the etiology of defective craniofacial development. For this review, we focus our discussion concerning the relationship between ribosome biogenesis and craniofacial development on the protein WDR43, also called Utp5, whose significance in craniofacial development has only recently been identified (Zhao et al 2014). Many erudite reviews have explored the connection between other ribosome biogenesis proteins and craniofacial development (Sakai and Trainor 2009;Trainor and Andrews 2013;van Gijn et al 2013;Ross and Zarbalis 2014;Trainor and Merrill 2014).…”

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confidence: 99%

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The Contributions of the Ribosome Biogenesis Protein Utp5/WDR43 to Craniofacial Development

2016

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Fairly recently, it was recognized that human ribosomopathies-developmental defects caused by mutations in ribosome biogenesis proteins-can exhibit tissue-specific defects rather than the expected global defects. This apparent anomaly-that seemingly ubiquitously expressed and required ribosomal proteins can have distinct functions in cell and tissue differentiation-has spurred new areas of research focused on better understanding translational mechanisms, biogenesis, and function in diverse cell types. This renewed appreciation for, and need to better understand, roles for ribosomal proteins in human development and disease has identified surprising similarities and differences in a variety of human ribosomopathies. Here, we discuss ribosomal protein functions in health and disease, focusing on the ribosome biogenesis protein Utp5/WDR43. New and exciting research in this field is anticipated to provide insight into a variety of previously understudied craniofacial dysostoses and result in significantly improved knowledge and understanding of roles for translational machinery in human craniofacial development and disease.

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Section: Utp5/wdr43 and Diseasesupporting

confidence: 72%

Section: Discovery and Role Of Utp5 In The Yeast Saccharomyces Cerevimentioning

confidence: 95%

Section: Role and Conservation Of Utp5/ Wdr43 In Other Eukaryotesmentioning

confidence: 96%

Section: Role and Conservation Of Utp5/ Wdr43 In Other Eukaryotesmentioning

confidence: 99%

mentioning

confidence: 99%

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The Contributions of the Ribosome Biogenesis Protein Utp5/WDR43 to Craniofacial Development

2016

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Zebrafish models of orofacial clefts

Duncan

Mukherjee

Cornell

et al. 2017

Developmental Dynamics

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Zebrafish is a model organism that affords experimental advantages toward investigating the normal function of genes associated with congenital birth defects. Here we summarize zebrafish studies of genes implicated in orofacial cleft (OFC). The most common use of zebrafish in this context has been to explore the normal function an OFC-associated gene product in craniofacial morphogenesis by inhibiting expression of its zebrafish ortholog. The most frequently deployed method has been to inject embryos with antisense morpholino oligonucleotides targeting the desired transcript. However improvements in targeted mutagenesis strategies have led to widespread adoption of CRISPR/Cas9 technology. A second application of zebrafish has been for functional assays of gene variants found in OFC patients; such in vivo assays are valuable because the success of in silico methods for testing allele severity has been mixed. Finally, zebrafish have been used to test the tissue specificity of enhancers that harbor single nucleotide polymorphisms (SNPs) associated with risk for OFC. We review examples of each of these approaches in the context of genes that are implicated in syndromic and non-syndromic OFC.

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Bop1 is required to establish precursor domains of craniofacial tissues

Keer,

Neilson,

Cousin

et al. 2023

Genesis

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SummaryBop1 can promote cell proliferation and is a component of the Pes1‐Bop1‐WDR12 (PeBoW) complex that regulates ribosomal RNA processing and biogenesis. In embryos, however, bop1 mRNA is highly enriched in the neural plate, cranial neural crest and placodes, and potentially may interact with Six1, which also is expressed in these tissues. Recent work demonstrated that during development, Bop1 is required for establishing the size of the tadpole brain, retina and cranial cartilages, as well as controlling neural tissue gene expression levels. Herein, we extend this work by assessing the effects of Bop1 knockdown at neural plate and larval stages. Loss of Bop1 expanded neural plate gene expression domains (sox2, sox11, irx1) and reduced neural crest (foxd3, sox9), placode (six1, sox11, irx1, sox9) and epidermal (dlx5) expression domains. At larval stages, Bop1 knockdown reduced the expression of several otic vesicle genes (six1, pax2, irx1, sox9, dlx5, otx2, tbx1) and branchial arch genes that are required for chondrogenesis (sox9, tbx1, dlx5). The latter was not the result of impaired neural crest migration. Together these observations indicate that Bop1 is a multifunctional protein that in addition to its well‐known role in ribosomal biogenesis functions during early development to establish the craniofacial precursor domains.

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Tissue Specific Roles for the Ribosome Biogenesis Factor Wdr43 in Zebrafish Development

Cited by 44 publications

References 64 publications

The Contributions of the Ribosome Biogenesis Protein Utp5/WDR43 to Craniofacial Development

The Contributions of the Ribosome Biogenesis Protein Utp5/WDR43 to Craniofacial Development

Zebrafish models of orofacial clefts

Bop1 is required to establish precursor domains of craniofacial tissues

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