660 research outputs found
A 37 kb region upstream of brachyury comprising a notochord enhancer is essential for notochord and tail development
The node-streak border region comprising notochord progenitor cells (NPCs) at the posterior node and neuro-mesodermal progenitor cells (NMPs) in the adjacent epiblast is the prime organizing center for axial elongation in mouse embryos. The T-box transcription factor brachyury (T) is essential for both formation of the notochord and maintenance of NMPs, and thus is a key regulator of trunk and tail development. The T promoter controlling T expression in NMPs and nascent mesoderm has been characterized in detail; however, control elements for T expression in the notochord have not been identified yet. We have generated a series of deletion alleles by CRISPR/Cas9 genome editing in mESCs, and analyzed their effects in mutant mouse embryos. We identified a 37 kb region upstream of T that is essential for notochord function and tailbud outgrowth. Within that region, we discovered a T-binding enhancer required for notochord cell specification and differentiation. Our data reveal a complex regulatory landscape controlling cell type-specific expression and function of T in NMP/nascent mesoderm and node/notochord, allowing proper trunk and tail development
Patterning and gastrulation defects caused by the tw18 lethal are due to loss of Ppp2r1a
The mouse t haplotype, a variant 20 cM genomic region on Chromosome 17,
harbors 16 embryonic control genes identified by recessive lethal mutations
isolated from wild mouse populations. Due to technical constraints so far only
one of these, the tw5 lethal, has been cloned and molecularly characterized.
Here we report the molecular isolation of the tw18 lethal. Embryos carrying
the tw18 lethal die from major gastrulation defects commencing with primitive
streak formation at E6.5. We have used transcriptome and marker gene analyses
to describe the molecular etiology of the tw18 phenotype. We show that both
WNT and Nodal signal transduction are impaired in the mutant epiblast, causing
embryonic patterning defects and failure of primitive streak and mesoderm
formation. By using a candidate gene approach, gene knockout by homologous
recombination and genetic rescue, we have identified the gene causing the tw18
phenotype as Ppp2r1a, encoding the PP2A scaffolding subunit PR65alpha. Our
work highlights the importance of phosphatase 2A in embryonic patterning,
primitive streak formation, gastrulation, and mesoderm formation downstream of
WNT and Nodal signaling
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An Image-Based Genetic Assay Identifies Genes in T1D Susceptibility Loci Controlling Cellular Antiviral Immunity in Mouse
The pathogenesis of complex diseases, such as type 1 diabetes (T1D), derives from interactions between host genetics and environmental factors. Previous studies have suggested that viral infection plays a significant role in initiation of T1D in genetically predisposed individuals. T1D susceptibility loci may therefore be enriched in previously uncharacterized genes functioning in antiviral defense pathways. To identify genes involved in antiviral immunity, we performed an image-based high-throughput genetic screen using short hairpin RNAs (shRNAs) against 161 genes within T1D susceptibility loci. RAW 264.7 cells transduced with shRNAs were infected with GFP-expressing herpes simplex virus type 1 (HSV-1) and fluorescent microscopy was performed to assess the viral infectivity by fluorescence reporter activity. Of the 14 candidates identified with high confidence, two candidates were selected for further investigation, Il27 and Tagap. Administration of recombinant IL-27 during viral infection was found to act synergistically with interferon gamma (IFN-γ) to activate expression of type I IFNs and proinflammatory cytokines, and to enhance the activities of interferon regulatory factor 3 (IRF3). Consistent with a role in antiviral immunity, Tagap-deficient macrophages demonstrated increased viral replication, reduced expression of proinflammatory chemokines and cytokines, and decreased production of IFN-β. Taken together, our unbiased loss-of-function genetic screen identifies genes that play a role in host antiviral immunity and delineates roles for IL-27 and Tagap in the production of antiviral cytokines
Estimating prognosis and palliation based on tumour marker CA 19-9 and quality of life indicators in patients with advanced pancreatic cancer receiving chemotherapy
To investigate the prognostic value of quality of life (QOL) relative to tumour marker carbohydrate antigen (CA) 19-9, and the role of CA 19-9 in estimating palliation in patients with advanced pancreatic cancer receiving chemotherapy
Dopamine transporter (DAT1) and dopamine receptor D4 (DRD4) genotypes differentially impact on electrophysiological correlates of error processing
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Особенности формирования структуры ЗТВ и зон оплавления покрытия на основе стали 10Р6М5 электронным лучом в вакууме
Особенности формирования структуры в зоне оплавления и зоне термического влияния композиционного покрытия на основе стали 10Р6М5 в ходе вакуумного импульсного электронного воздействияEigenschaften der Strukturbildung in der Schmelzzone und die Warmeeinflu?zone, auf der Grundlage der Warme einflus sverbundbeschichtung 10Р6M5 Stahl wahrend der Vakuumbelichtungsgepulster Elektronenstrah
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The tissue-specific lncRNA Fendrr is an essential regulator of heart and body wall development in the mouse
The histone modifying complexes PRC2 and TrxG/MLL play pivotal roles in determining the activation state of genes controlling pluripotency, lineage commitment, and cell differentiation. Long non-coding RNAs (lncRNAs) can bind to either complex, and some have been shown to act as modulators of PRC2 or TrxG/MLL activity. Here we show that the lateral mesoderm-specific lncRNA Fendrr is essential for proper heart and body wall development in the mouse. Embryos lacking Fendrr displayed upregulation of several transcription factors controlling lateral plate or cardiac mesoderm differentiation, accompanied by a drastic reduction in PRC2 occupancy along with decreased H3K27 trimethylation and/or an increase in H3K4 trimethylation at their promoters. Fendrr binds to both the PRC2 and TrxG/MLL complexes, suggesting that it acts as modulator of chromatin signatures that define gene activity. Thus, our work identifies a lncRNA that plays an essential role in fine-tuning the regulatory networks which control the fate of lateral mesoderm derivatives
First Measurement of Chiral Dynamics in \pi^- \gamma -> \pi^- \pi^- \pi^+
The COMPASS collaboration at CERN has investigated the \pi^- \gamma -> \pi^-
\pi^- \pi^+ reaction at center-of-momentum energy below five pion masses,
sqrt(s) < 5 m(\pi), embedded in the Primakoff reaction of 190 GeV pions
impinging on a lead target. Exchange of quasi-real photons is selected by
isolating the sharp Coulomb peak observed at smallest momentum transfers, t' <
0.001 (GeV/c)^2. Using partial-wave analysis techniques, the scattering
intensity of Coulomb production described in terms of chiral dynamics and its
dependence on the 3\pi-invariant mass m(3\pi) = sqrt(s) were extracted. The
absolute cross section was determined in seven bins of with an
overall precision of 20%. At leading order, the result is found to be in good
agreement with the prediction of chiral perturbation theory over the whole
energy range investigated.Comment: 10 pages, 5 figure
Measurement of the Longitudinal Spin Transfer to Lambda and Anti-Lambda Hyperons in Polarised Muon DIS
The longitudinal polarisation transfer from muons to lambda and anti-lambda
hyperons, D_LL, has been studied in deep inelastic scattering off an
unpolarised isoscalar target at the COMPASS experiment at CERN. The spin
transfers to lambda and anti-lambda produced in the current fragmentation
region exhibit different behaviours as a function of x and xF . The measured x
and xF dependences of D^lambda_LL are compatible with zero, while
D^anti-lambda_LL tends to increase with xF, reaching values of 0.4 - 0.5. The
resulting average values are D^lambda_LL = -0.012 +- 0.047 +- 0.024 and
D^anti-lambda_LL = 0.249 +- 0.056 +- 0.049. These results are discussed in the
frame of recent model calculations.Comment: 13 pages, 7 figure
The Nucleoside Diphosphate Kinase Gene Nme3 Acts as Quantitative Trait Locus Promoting Non-Mendelian Inheritance
The t-haplotype, a variant form of the t-complex region on mouse chromosome 17, acts as selfish genetic element and is transmitted at high frequencies (>95%) from heterozygous (t/+) males to their offspring. This phenotype is termed transmission ratio distortion (TRD) and is caused by the interaction of the t-complex responder (Tcr) with several quantitative trait loci (QTL), the t-complex distorters (Tcd1 to Tcd4), all located within the t-haplotype region. Current data suggest that the distorters collectively impair motility of all sperm derived from t/+ males; t-sperm is rescued by the responder, whereas +-sperm remains partially dysfunctional. Recently we have identified two distorters as regulators of RHO small G proteins. Here we show that the nucleoside diphosphate kinase gene Nme3 acts as a QTL on TRD. Reduction of the Nme3 dosage by gene targeting of the wild-type allele enhanced the transmission rate of the t-haplotype and phenocopied distorter function. Genetic and biochemical analysis showed that the t-allele of Nme3 harbors a mutation (P89S) that compromises enzymatic activity of the protein and genetically acts as a hypomorph. Transgenic overexpression of the Nme3 t-allele reduced t-haplotype transmission, proving it to be a distorter. We propose that the NME3 protein interacts with RHO signaling cascades to impair sperm motility through hyperactivation of SMOK, the wild-type form of the responder. This deleterious effect of the distorters is counter-balanced by the responder, SMOKTcr, a dominant-negative protein kinase exclusively expressed in t-sperm, thus permitting selfish behaviour and preferential transmission of the t-haplotype. In addition, the previously reported association of NME family members with RHO signaling in somatic cell motility and metastasis, in conjunction with our data involving RHO signaling in sperm motility, suggests a functional conservation between mechanisms for motility control in somatic cells and spermatozoa
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