Your search keyword '"Flavell, A. J."' showing total 22 results

1. Screening of a large Rubinstein–Taybi cohort identified many novel variants and emphasizes the importance of the CREBBP histone acetyltransferase domain.

Author

Cross, Esther, Duncan‐Flavell, Philippa J., Howarth, Rachel J., Hobbs, James I., Thomas, Nicholas Simon, and Bunyan, David J.

Abstract

Pathogenic variants within the CREBBP and EP300 genes account for the majority of individuals with Rubinstein–Taybi syndrome (RSTS). Data are presented from a large cohort of 395 individuals referred for diagnostic testing of CREBBP, and of the 19 CREBBP missense variants classified as likely pathogenic in this study, 17 were within the histone acetyltransferase (HAT) domain, providing evidence that this domain is critical to the normal function of the CREBBP protein (CBP). The data presented here, combined with other published results, suggest that the presence of a missense variant within the CBP HAT domain can be considered as moderate evidence of pathogenicity in the context of official variant interpretation guidelines. Within our study cohort, 129 had a pathogenic or likely pathogenic CREBBP variant and 5 had a variant of uncertain significance (VUS) which warranted familial studies. 147 of the remaining probands were also screened for EP300 and a further 16 pathogenic or likely pathogenic variants were identified, plus one VUS. Therefore, this analysis has provided a molecular diagnosis in at least 145 individuals with RSTS (37%) and identified a wide range of variants (n = 133) of which 103 were novel. [ABSTRACT FROM AUTHOR]

Published

2020

2. Chromatin state analysis of the barley epigenome reveals a higher-order structure defined by H3K27me1 and H3K27me3 abundance.

Author

Baker, Katie, Dhillon, Taniya, Colas, Isabelle, Cook, Nicola, Milne, Iain, Milne, Linda, Bayer, Micha, and Flavell, Andrew J.

Subjects

CHROMATIN, HISTONE genetics, EPIGENETICS, IMMUNOPRECIPITATION, GENE expression, RETROTRANSPOSONS

Abstract

Combinations of histones carrying different covalent modifications are a major component of epigenetic variation. We have mapped nine modified histones in the barley seedling epigenome by chromatin immunoprecipitation next-generation sequencing (Ch IP-seq). The chromosomal distributions of the modifications group them into four different classes, and members of a given class also tend to coincide at the local DNA level, suggesting that global distribution patterns reflect local epigenetic environments. We used this peak sharing to define 10 chromatin states representing local epigenetic environments in the barley genome. Five states map mainly to genes and five to intergenic regions. Two genic states involving H3K36me3 are preferentially associated with constitutive gene expression, while an H3K27me3-containing genic state is associated with differentially expressed genes. The 10 states display striking distribution patterns that divide barley chromosomes into three distinct global environments. First, telomere-proximal regions contain high densities of H3K27me3 covering both genes and intergenic DNA, together with very low levels of the repressive H3K27me1 modification. Flanking these are gene-rich interior regions that are rich in active chromatin states and have greatly decreased levels of H3K27me3 and increasing amounts of H3K27me1 and H3K9me2. Lastly, H3K27me3-depleted pericentromeric regions contain gene islands with active chromatin states separated by extensive retrotransposon-rich regions that are associated with abundant H3K27me1 and H3K9me2 modifications. We propose an epigenomic framework for barley whereby intergenic H3K27me3 specifies facultative heterochromatin in the telomere-proximal regions and H3K27me1 is diagnostic for constitutive heterochromatin elsewhere in the barley genome. [ABSTRACT FROM AUTHOR]

Published

2015

3. The low-recombining pericentromeric region of barley restricts gene diversity and evolution but not gene expression.

Author

Baker, Katie, Bayer, Micha, Cook, Nicola, Dreißig, Steven, Dhillon, Taniya, Russell, Joanne, Hedley, Pete E., Morris, Jenny, Ramsay, Luke, Colas, Isabelle, Waugh, Robbie, Steffenson, Brian, Milne, Iain, Stephen, Gordon, Marshall, David, and Flavell, Andrew J.

Subjects

BARLEY genetics, GENE expression in plants, PLANT genomes, CHROMOSOME duplication, RECOMBINANT DNA, HETEROCHROMATIN, PLANTS

Abstract

The low-recombining pericentromeric region of the barley genome contains roughly a quarter of the genes of the species, embedded in low-recombining DNA that is rich in repeats and repressive chromatin signatures. We have investigated the effects of pericentromeric region residency upon the expression, diversity and evolution of these genes. We observe no significant difference in average transcript level or developmental RNA specificity between the barley pericentromeric region and the rest of the genome. In contrast, all of the evolutionary parameters studied here show evidence of compromised gene evolution in this region. First, genes within the pericentromeric region of wild barley show reduced diversity and significantly weakened purifying selection compared with the rest of the genome. Second, gene duplicates (ohnolog pairs) derived from the cereal whole-genome duplication event ca. 60MYa have been completely eliminated from the barley pericentromeric region. Third, local gene duplication in the pericentromeric region is reduced by 29% relative to the rest of the genome. Thus, the pericentromeric region of barley is a permissive environment for gene expression but has restricted gene evolution in a sizeable fraction of barley's genes. [ABSTRACT FROM AUTHOR]

Published

2014

4. Barley whole exome capture: a tool for genomic research in the genus Hordeum and beyond.

Author

Mascher, Martin, Richmond, Todd A., Gerhardt, Daniel J., Himmelbach, Axel, Clissold, Leah, Sampath, Dharanya, Ayling, Sarah, Steuernagel, Burkhard, Pfeifer, Matthias, D'Ascenzo, Mark, Akhunov, Eduard D., Hedley, Pete E., Gonzales, Ana M., Morrell, Peter L., Kilian, Benjamin, Blattner, Frank R., Scholz, Uwe, Mayer, Klaus F.X., Flavell, Andrew J., and Muehlbauer, Gary J.

Subjects

HORDEUM, PLANT genomes, PLANT diversity, PLANT cellular signal transduction, PLANT genetics, NUCLEOTIDE sequence, GENE targeting

Abstract

Advanced resources for genome-assisted research in barley ( Hordeum vulgare) including a whole-genome shotgun assembly and an integrated physical map have recently become available. These have made possible studies that aim to assess genetic diversity or to isolate single genes by whole-genome resequencing and in silico variant detection. However such an approach remains expensive given the 5 Gb size of the barley genome. Targeted sequencing of the m RNA-coding exome reduces barley genomic complexity more than 50-fold, thus dramatically reducing this heavy sequencing and analysis load. We have developed and employed an in-solution hybridization-based sequence capture platform to selectively enrich for a 61.6 megabase coding sequence target that includes predicted genes from the genome assembly of the cultivar Morex as well as publicly available full-length c DNAs and de novo assembled RNA-Seq consensus sequence contigs. The platform provides a highly specific capture with substantial and reproducible enrichment of targeted exons, both for cultivated barley and related species. We show that this exome capture platform provides a clear path towards a broader and deeper understanding of the natural variation residing in the m RNA-coding part of the barley genome and will thus constitute a valuable resource for applications such as mapping-by-sequencing and genetic diversity analyzes. [ABSTRACT FROM AUTHOR]

Published

2013

5. Locus-dependent selection in crop-wild hybrids of lettuce under field conditions and its implication for GM crop development.

Author

Hooftman, Danny A. P., Flavell, Andrew J., Jansen, Hans, den Nijs, Hans C. M., Syed, Naeem H., Sørensen, Anker P., Orozco-ter Wengel, Pablo, and van de Wiel, Clemens C. M.

Subjects

*PLANT hybridization, *TRANSGENIC plants, *LOCUS (Genetics), *PLANT habitats, *LINKAGE disequilibrium, *LETTUCE

Abstract

Gene escape from crops has gained much attention in the last two decades, as transgenes introgressing into wild populations could affect the latter's ecological characteristics. However, different genes have different likelihoods of introgression. The mixture of selective forces provided by natural conditions creates an adaptive mosaic of alleles from both parental species. We investigated segregation patterns after hybridization between lettuce ( Lactuca sativa) and its wild relative, L. serriola. Three generations of hybrids (S1, BC1, and BC1S1) were grown in habitats mimicking the wild parent's habitat. As control, we harvested S1 seedlings grown under controlled conditions, providing very limited possibility for selection. We used 89 AFLP loci, as well as more recently developed dominant markers, 115 retrotransposon markers (SSAP), and 28 NBS loci linked to resistance genes. For many loci, allele frequencies were biased in plants exposed to natural field conditions, including over-representation of crop alleles for various loci. Furthermore, Linkage disequilibrium was locally changed, allegedly by selection caused by the natural field conditions, providing ample opportunity for genetic hitchhiking. Our study indicates that when developing genetically modified crops, a judicious selection of insertion sites, based on knowledge of selective (dis)advantages of the surrounding crop genome under field conditions, could diminish transgene persistence. [ABSTRACT FROM AUTHOR]

Published

2011

6. Analysis of >1000 single nucleotide polymorphisms in geographically matched samples of landrace and wild barley indicates secondary contact and chromosome-level differences in diversity around domestication genes.

Author

Russell, Joanne, Dawson, Ian K., Flavell, Andrew J., Steffenson, Brian, Weltzien, Eva, Booth, Allan, Ceccarelli, Salvatore, Grando, Stefania, and Waugh, Robbie

Subjects

NUCLEOTIDES, BARLEY genetics, GENETIC polymorphisms, CHROMOSOMES, CELL nuclei

Abstract

Summary [ABSTRACT FROM AUTHOR]

Published

2011

7. Splenic stromal cells mediate IL-7 independent adult lymphoid tissue inducer cell survival.

Author

Hou, Tie Zheng, Mustafa, Mohammad Z., Flavell, Sarah J., Barrington, Fern, Jenkinson, Eric J., Anderson, Graham, Lane, Peter J. L., Withers, David R., and Buckley, Christopher D.

Published

2010

8. Pichia pastoris as a host for secretion of toxic saporin chimeras.

Author

Lombardi, Alessio, Bursomanno, Sara, Lopardo, Teresa, Traini, Roberta, Colombatti, Marco, Ippoliti, Rodolfo, Flavell, David J., Flavell, Sopsamorn U., Ceriotti, Aldo, and Fabbrini, Maria Serena

Subjects

CANCER treatment, PROTEINS, ENDOPLASMIC reticulum, PROTEIN folding, UROKINASE, PICHIA pastoris, PLANT toxins

Abstract

Most of the targeting moieties, such as antibody fragments or growth factor domains, used to construct targeted toxins for anticancer therapy derive from secretory proteins. These normally fold in the oxidative environment of the endoplasmic reticulum, and hence their folding in bacterial cells can be quite inefficient. For instance, only low amounts of properly folded antimetastatic chimera constituted by the amino-terminal fragment of human urokinase (ATF) fused to the plant ribosome-inactivating protein saporin could be recovered. ATF-saporin was instead secreted efficiently when expressed in eukaryotic cells protected from autointoxication with neutralizing anti-saporin antibodies. Pichia pastoris is a microbial eukaryotic host where these domains can fold into a transport-competent conformation and reach the extracellular medium. We show here that despite some host toxicity codon-usage optimization greatly increased the expression levels of active saporin but not those of an active-site mutant SAP-KQ in GS115 (his4) strain. The lack of any toxicity associated with expression of the latter confirmed that toxicity is due to saporin catalytic activity. Nevertheless, GS115 (his4) cells in flask culture secreted 3.5 mg/L of a histidine-tagged ATF-saporin chimera showing an IC50 of 6 x 10-11 M against U937 cells, thus demonstrating the suitability of this expression platform for secretion of toxic saporin-based chimeras. [ABSTRACT FROM AUTHOR]

Published

2010

9. Fibroblasts as novel therapeutic targets in chronic inflammation.

Author

Flavell, S. J., Hou, T. Z., Lax, S., Filer, A. D., Salmon, M., and Buckley, C. D.

Subjects

*INFLAMMATION, *FIBROBLASTS, *TROPISMS, *CELLS, *PHARMACOLOGY

Abstract

A characteristic feature of many chronic inflammatory diseases is their persistence and predilection for certain sites. The molecular basis for such tissue tropism and failure of the inflammatory response to resolve has until relative recently remained obscure. Recent studies have strongly implicated fibroblasts as cells which contribute to disease persistence and which help define anatomical location. Therefore fibroblasts make an attractive therapeutic target as they help orchestrate the inflammatory infiltrate. Current anti-inflammatory therapies target immune cells in an attempt to inhibit the production of pro-inflammatory mediators. However an equally important target is the active induction of pro-resolution programmes responsible for the resolution of inflammation. Fibroblasts are likely to be an important source of these anti-inflammatory mediators. Therapeutic manipulation of fibroblasts and their biologically active products is an emerging concept in treating cancer and is likely to provide a novel method to achieve improved control of chronic inflammatory disease.British Journal of Pharmacology (2008) 153, S241–S246; doi:10.1038/sj.bjp.0707487; published online 29 October 2007 [ABSTRACT FROM AUTHOR]

Published

2008

10. The anti-CD20 antibody rituximab augments the immunospecific therapeutic effectiveness of an anti-CD19 immunotoxin directed against human B-cell lymphoma.

Author

Flavell, David J., Warnes, Sarah L., Bryson, Christine J., Field, Sarah A., Noss, Armorel L., Packham, Graham, and Flavell, Sopsamorn U.

Subjects

*RITUXIMAB, *LYMPHOMAS, *ANTINEOPLASTIC agents, *CELLS, *APOPTOSIS, *ANTIBODY-toxin conjugates

Abstract

The chimaeric anti-CD20 antibody rituximab (Rituxan) sensitises lymphoma cells to small molecule cytotoxic drugs and to protein toxins. We have explored the augmentive effect of rituximab on the anti-CD19 immunotoxin BU12-SAPORIN in a model of human lymphoma. Intact rituximab and its F(ab)2 derivative both augmented the immunospecific protein synthesis inhibitory effects of BU12-SAPORIN in a complement-independent manner. A combination of rituximab + BU12-SAPORIN completely abolished the proliferation of Ramos cells in vitro and also induced a significantly greater degree of apoptosis in these cells. Treatment with rituximab, BU12-SAPORIN or a combination of both induced poly(ADPribose) polymerase and caspase 3 cleavage, although this was always consistently greater in combination-treated cells. zVAD almost completely inhibited apoptosis in rituximab- or BU12-SAPORIN-treated cells but only partially in combination-treated cells. In severe combined immunodeficient (SCID)-Ramos mice the combination of rituximab + BU12-SAPORIN was significantly better therapeutically than either single agent. The immunological fidelity of the therapeutic effect because of combination treatment was demonstrated through the failure of rituximab to augment an irrelevant anti-CD7 immunotoxin. The therapeutic efficacy of rituximab and combination treatment was reduced in SCID-Ramos mice depleted of serum complement while natural killer cell depletion failed to show any convincing role for antibody-dependent cellular cytotoxicity. This study shows a clear therapeutic advantage from using rituximab to immunospecifically augment immunotoxin cytotoxicity warranting further investigation. [ABSTRACT FROM AUTHOR]

Published

2006

11. Saporin and ricin A chain follow different intracellular routes to enter the cytosol of intoxicated cells.

Author

Vago, Riccardo, Marsden, Catherine J., Lord, J. Michael, Ippoliti, Rodolfo, Flavell, David J., Flavell, Sopsamorn-U, Ceriotti, Aldo, and Fabbrini, M. Serena

Subjects

RICIN, PLANT toxins, CYTOSOL, CELLS, ENDOCYTOSIS, ENDOPLASMIC reticulum

Abstract

Several protein toxins, such as the potent plant toxin ricin, enter mammalian cells by endocytosis and undergo retrograde transport via the Golgi complex to reach the endoplasmic reticulum (ER). In this compartment the catalytic moieties exploit the ER-associated degradation (ERAD) pathway to reach their cytosolic targets. Bacterial toxins such as cholera toxin or Pseudomonas exotoxin A carry KDEL or KDEL-like C-terminal tetrapeptides for efficient delivery to the ER. Chimeric toxins containing monomeric plant ribosome-inactivating proteins linked to various targeting moieties are highly cytotoxic, but it remains unclear how these molecules travel within the target cell to reach cytosolic ribosomes. We investigated the intracellular pathways of saporin, a monomeric plant ribosome-inactivating protein that can enter cells by receptor-mediated endocytosis. Saporin toxicity was not affected by treatment with Brefeldin A or chloroquine, indicating that this toxin follows a Golgi-independent pathway to the cytosol and does not require a low pH for membrane translocation. In intoxicated Vero or HeLa cells, ricin but not saporin could be clearly visualized in the Golgi complex using immunofluorescence. The saporin signal was not evident in the Golgi, but was found to partially overlap with that of a late endosome/lysosome marker. Consistently, the toxicities of saporin or saporin-based targeted chimeric polypeptides were not enhanced by the addition of ER retrieval sequences. Thus, the intracellular movement of saporin differs from that followed by ricin and other protein toxins that rely on Golgi-mediated retrograde transport to reach their retrotranslocation site. [ABSTRACT FROM AUTHOR]

Published

2005

12. Rapid isolation of plant Ty1-copia group retrotransposon LTR sequences for molecular marker studies.

Author

Pearce, Stephen R, Stuart-Rogers, Caroline, Knox, Maggie R, Kumar, Amar, Ellis, T. H. Noel, and Flavell, Andrew J

Subjects

TRANSPOSONS, FAVA bean, PEA genetics, NORWAY spruce, POLYMERASE chain reaction, GENETICS

Abstract

Summary The terminal sequences of long-terminal repeat (LTR) retrotransposons are a source of powerful molecular markers for linkage mapping and biodiversity studies. The major factor limiting the widespread application of LTR retrotransposon-based molecular markers is the availability of new retrotransposon terminal sequences. We describe a PCR-based method for the rapid isolation of LTR sequences of Ty1-copia group retrotransposons from the genomic DNA of potentially any higher plant species. To demonstrate the utility of this technique, we have identified a variety of new retrotransposon LTR sequences from pea, broad bean and Norway spruce. Primers specific for three pea LTRs have been used to reveal polymorphisms associated with the correspond- ing retrotransposons within the Pisum genus. [ABSTRACT FROM AUTHOR]

Published

1999

13. Retrotransposon-based insertion polymorphisms (RBIP) for high throughput marker analysis.

Author

Flavell, Andrew J., Knox, Maggie R., Pearce, Stephen R., and Ellis, T. H. Noel

Subjects

*POLYMERASE chain reaction, *PLANT gene mapping

Abstract

SummaryTwo assays based upon PCR detection of a polymorphic PDR1 retrotransposon insertion in Pisum sativum have been developed. Both methods involve PCR with primers derived from the transposon and flanking DNA. The first method uses a dot assay for PCR product detection which could be fully automated for handling thousands of samples. The second method, which is designed to handle lower numbers, requires a single PCR and gel lane per sample. Both methods yield co-dominant markers, with presence and absence of the transposon insertion independently scorable, and both could in principle be applied to any transposable element in any plant species. [ABSTRACT FROM AUTHOR]

Published

1998

14. MODELLING HUMAN LEUKEMIA AND LYMPHOMA IN SEVERE COMBINED IMMUNODEFICIENT (SCID) MICE: PRACTICAL APPLICATIONS.

Author

FLAVELL, DAVID J.

Published

1996

15. Comparison of the performance of anti-CD7 and anti-CD38 bispecific antibodies and immunotoxins for the delivery of saporin to a human T-cell acute lymphoblastic leukemia cell line.

Author

Flavell, David J., Cooper, Sue, Okayama, Keiko, Emery, Loretta, and Flavell, Sopsamorn U.

Published

1995

16. Identification of peanut agglutinin binding glycoproteins restricted to Hodgkin's disease-derived cell lines.

Author

Flavell, D. J., Jones, D. B., and Wright, D. H.

Published

1989

17. Therapy of human B-cell lymphoma bearing scid mice is more effective with anti-CD19-and anti-CD38-saporin immunotoxins used in combination than with either immunotoxin used alone.

Author

Flavell, David J., Boehm, Deborah A., Emery, Loretta, Moss, Armorel, Ramsay, Alan, and Flavell, Sopsamorn U.

Published

1995

18. Therapy of human T-cell acute lymphoblastic leukaemia in severe combined immunodeficient mice with two different anti-CD7-saporin immunotoxins containing hindered or non-hindered disulphide cross-linkers.

Author

Flavell, David J., Boehm, Deborah A., Okayama, Keiko, Kohler, Janice A., and Flavell, Sopsamor N. U.

Published

1994

19. The anti-mitozantrone monoclonal antibody NO-1, protects acute leukaemia cell lines from the cytotoxic effects of mitozantrone.

Author

Flavell, S. U. and Flavell, D. J.

Published

1991

20. Opisthorchis viverrini: pathogenesis of infection in immunodeprived hamsters.

Author

FLAVELL, D. J. and FLAVELL, S. U.

Published

1986

21. High-dose mitoxantrone and etoposide conditioning in autologous bone marrow transplantation for relapsed Hodgkin's disease.

Author

Lim, S.H., Baglin, T.P., Flavell, D. J., Flavell, S. U., Wimperis, J. Z., and Marcus, R. E.

Published

1992

22. Monoclonal antibodies. Peter C. L. Beverley (Ed.). Churchill Livingstone, 1986. No. of pages: 275. Price: £42.00. ISBN 0443 029903.

Author

Flavell, David J.

Published

1989