Forward Genetic Screens in Zebrafish Identify Pre-mRNA-Processing Pathways Regulating Early T Cell Development

Iwanami, Norimasa; Sikora, Katarzyna; Richter, Andreas S.; Mönnich, Maren; Guerri, Lucia; Soza‐Ried, Cristian; Lawir, Divine Fondzenyuy; Mateos, Fernando; Hess, Isabell; O’Meara, Connor P.; Schorpp, Michael; Boehm, Thomas

doi:10.1016/j.celrep.2016.11.003

Cited by 27 publications

(56 citation statements)

References 44 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…In pro-B cells, PI3K signaling supresses the function of FOXO-1 that is required for the correct splicing of Ikzf1 , a transcription factors which enables VDJ recombination in cooperation with PAX5 ( 126 ). Forward genetic screens in zebrafish have extended the list of RBPs involved in pre-mRNA-processing in T cells in thymus and they support the idea that global splicing pathways control lymphoid development ( 127 ). Expression of the splicing factors FUS, SC35, hnRPNPL, and hnRPNPLL is important for B- and T-cell development and for T-cell activation ( 128 , 129 ).…”

Section: Rbps In Development Of the Immune Systemmentioning

confidence: 76%

Uncovering the Role of RNA-Binding Proteins in Gene Expression in the Immune System

Díaz-Muñoz

Turner

2018

Front. Immunol.

View full text Add to dashboard Cite

Fighting external pathogens requires an ever-changing immune system that relies on tight regulation of gene expression. Transcriptional control is the first step to build efficient responses while preventing immunodeficiencies and autoimmunity. Post-transcriptional regulation of RNA editing, location, stability, and translation are the other key steps for final gene expression, and they are all controlled by RNA-binding proteins (RBPs). Nowadays we have a deep understanding of how transcription factors control the immune system but recent evidences suggest that post-transcriptional regulation by RBPs is equally important for both development and activation of immune responses. Here, we review current knowledge about how post-transcriptional control by RBPs shapes our immune system and discuss the perspective of RBPs being the key players of a hidden immune cell epitranscriptome.

show abstract

Section: Rbps In Development Of the Immune Systemmentioning

confidence: 76%

Uncovering the Role of RNA-Binding Proteins in Gene Expression in the Immune System

Díaz-Muñoz

Turner

2018

Front. Immunol.

View full text Add to dashboard Cite

show abstract

“…In a forward genetic screen for aberrant T cell development, we identified a large number of recessive mutations, all characterized by reduced numbers of rag1-expressing immature thymocytes in larvae 5 days after fertilization (dpf) 23,24 . The mutation in the IY071 line 23 (Fig. 1a) affected the gene encoding the maintenance DNA methyltransferase DNMT1.…”

Section: Resultsmentioning

confidence: 99%

“…The recessive viable dnmt1 allele (dnmt1 t25501 ) exhibits a missense mutation (N1391K) in the target recognition domain (TRD) of the catalytic domain of the enzyme (Fig. 1b) 23 ; since a previously identified dnmt1 mutant allele is embryonic lethal 20 , we consider the dnmt1 t25501 allele to be a hypomorph. The mutation in dnmt1 t25501 occurs in an evolutionarily conserved region of the protein (equivalent to N1510K in the mouse protein) (Fig.…”

Section: Resultsmentioning

confidence: 99%

See 1 more Smart Citation

Transgenerational inheritance of impaired larval T cell development in zebrafish

et al. 2020

Self Cite

View full text Add to dashboard Cite

Evidence for transgenerational inheritance of epigenetic information in vertebrates is scarce. Aberrant patterns of DNA methylation in gametes may set the stage for transmission into future generations. Here, we describe a viable hypomorphic allele of dnmt1 in zebrafish that causes widespread demethylation of CpG dinucleotides in sperm and somatic tissues. We find that homozygous mutants are essentially normal, with the exception of drastically impaired lymphopoiesis, affecting both larval and adult phases of T cell development. The phenotype of impaired larval (but not adult) T cell development is transmitted to subsequent generations by genotypically wildtype fish. We further find that about 200 differentially methylated regions in sperm DNA of transmitting and non-transmitting males, including hypermethylated sites associated with runx3 and rptor genes, whose reduced activities are associated with impaired larval T cell development. Our results indicate a particular sensitivity of larval T cell development to transgenerationally inherited epimutations.

show abstract

“…The teleost fishes, zebrafish ( Danio rerio ) and medaka ( Oryzias latipes ), offer a number of attractive features for studying T-cell development ( 9 , 35 – 38 ). Forward and reverse genetic approaches have been applied to characterize mechanisms underlying T-cell development in these model organisms ( 38 – 40 ). Apart from their strength as genetic model systems, the most important advantage of these fish is the optical access they provide.…”

Section: Long-term In Vivo Imaging In Fish Permitsmentioning

confidence: 99%

Making Thymus Visible: Understanding T-Cell Development from a New Perspective

Aghaallaei

Bajoghli

2018

Front. Immunol.

View full text Add to dashboard Cite

T-cell development is coupled with a highly ordered migratory pattern. Lymphoid progenitors must follow a precise journey; starting from the hematopoietic tissue, they move toward the thymus and then migrate into and out of distinct thymic microenvironments, where they receive signals and cues required for their differentiation into naïve T-cells. Knowing where, when, and how these cells make directional “decisions” is key to understanding T-cell development. Such insights can be gained by directly observing developing T-cells within their environment under various conditions and following specific experimental manipulations. In the last decade, several model systems have been developed to address temporal and spatial aspects of T-cell development using imaging approaches. In this perspective article, we discuss the advantages and limitations of these systems and highlight a particularly powerful in vivo model that has been recently established. This model system enables the migratory behavior of all thymocytes to be studied simultaneously in a noninvasive and quantitative manner, making it possible to perform systems-level studies that reveal fundamental principles governing T-cell dynamics during development and in disease.

show abstract

Forward Genetic Screens in Zebrafish Identify Pre-mRNA-Processing Pathways Regulating Early T Cell Development

Cited by 27 publications

References 44 publications

Uncovering the Role of RNA-Binding Proteins in Gene Expression in the Immune System

Uncovering the Role of RNA-Binding Proteins in Gene Expression in the Immune System

Transgenerational inheritance of impaired larval T cell development in zebrafish

Making Thymus Visible: Understanding T-Cell Development from a New Perspective

Contact Info

Product

Resources

About