Your search keyword '"James C. Neil"' showing total 151 results

1. Frequent Infection of Human Cancer Xenografts with Murine Endogenous Retroviruses in Vivo

Author

Asif Naseer, Anne Terry, Kathryn Gilroy, Anna Kilbey, Ciorsdaidh Watts, Nancy Mackay, Margaret Bell, Susan Mason, Karen Blyth, Ewan Cameron, and James C. Neil

Subjects

xenograft, xenotropic, murine leukemia virus, cancer, Microbiology, QR1-502

Abstract

Infection of human cancer xenografts in mice with murine leukemia viruses (MLVs) is a long-standing observation, but the likelihood of infection in vivo and its biological consequences are poorly understood. We therefore conducted a prospective study in commonly used xenograft recipient strains. From BALB/c nude mice engrafted with MCF7 human mammary carcinoma cells, we isolated a virus that was virtually identical to Bxv1, a locus encoding replication-competent xenotropic MLV (XMLV). XMLV was detected in 9/17 (53%) independently isolated explants. XMLV was not found in primary leukemias or in THP1 leukemia cells grown in Bxv1-negative NSG (NOD/SCID/γCnull) mice, although MCF7 explants harbored replication-defective MLV proviruses. To assess the significance of infection for xenograft behavior in vivo, we examined changes in growth and global transcription in MCF7 and the highly susceptible Raji Burkitt lymphoma cell line chronically infected with XMLV. Raji cells showed a stronger transcriptional response that included up-regulation of chemokines and effectors of innate antiviral immunity. In conclusion, the risk of de novo XMLV infection of xenografts is high in Bxv1 positive mice, while infection can have positive or negative effects on xenograft growth potential with significant consequences for interpretation of many xenograft studies.

Published

2015

2. RUNX2 correlates with subtype-specific breast cancer in a human tissue microarray, and ectopic expression of Runx2 perturbs differentiation in the mouse mammary gland

Author

Laura McDonald, Nicola Ferrari, Anne Terry, Margaret Bell, Zahra M. Mohammed, Clare Orange, Alma Jenkins, William J. Muller, Barry A. Gusterson, James C. Neil, Joanne Edwards, Joanna S. Morris, Ewan R. Cameron, and Karen Blyth

Subjects

RUNX2, Breast cancer, Transgenic model, Mammary development, Medicine, Pathology, RB1-214

Abstract

RUNX2, a master regulator of osteogenesis, is oncogenic in the lymphoid lineage; however, little is known about its role in epithelial cancers. Upregulation of RUNX2 in cell lines correlates with increased invasiveness and the capacity to form osteolytic disease in models of breast and prostate cancer. However, most studies have analysed the effects of this gene in a limited number of cell lines and its role in primary breast cancer has not been resolved. Using a human tumour tissue microarray, we show that high RUNX2 expression is significantly associated with oestrogen receptor (ER)/progesterone receptor (PR)/HER2-negative breast cancers and that patients with high RUNX2 expression have a poorer survival rate than those with negative or low expression. We confirm RUNX2 as a gene that has a potentially important functional role in triple-negative breast cancer. To investigate the role of this gene in breast cancer, we made a transgenic model in which Runx2 is specifically expressed in murine mammary epithelium under the control of the mouse mammary tumour virus (MMTV) promoter. We show that ectopic Runx2 perturbs normal development in pubertal and lactating animals, delaying ductal elongation and inhibiting lobular alveolar differentiation. We also show that the Runx2 transgene elicits age-related, pre-neoplastic changes in the mammary epithelium of older transgenic animals, suggesting that elevated RUNX2 expression renders such tissue more susceptible to oncogenic changes and providing further evidence that this gene might have an important, context-dependent role in breast cancer.

Published

2014

3. Supplementary Figure 1 Legend from Runx Regulation of Sphingolipid Metabolism and Survival Signaling

Author

James C. Neil, Ewan R. Cameron, Michael J.O. Wakelam, Qifeng Zhang, Gillian Borland, Alma Jenkins, Anne Terry, and Anna Kilbey

Abstract

Supplementary Figure 1 Legend from Runx Regulation of Sphingolipid Metabolism and Survival Signaling

Published

2023

4. Supplementary Figure 1 from Runx Regulation of Sphingolipid Metabolism and Survival Signaling

Author

James C. Neil, Ewan R. Cameron, Michael J.O. Wakelam, Qifeng Zhang, Gillian Borland, Alma Jenkins, Anne Terry, and Anna Kilbey

Abstract

Supplementary Figure 1 from Runx Regulation of Sphingolipid Metabolism and Survival Signaling

Published

2023

5. Data from Insertional Mutagenesis Reveals Progression Genes and Checkpoints in MYC/Runx2 Lymphomas

Author

James C. Neil, Ewan Cameron, Linda Scobie, Karen Blyth, Linda Hanlon, Nancy Mackay, and Monica Stewart

Abstract

In this study, we have exploited the power of insertional mutagenesis to elucidate tumor progression pathways in mice carrying two oncogenes (MYC/Runx2) that collaborate to drive early lymphoma development. Neonatal infection of these mice with Moloney murine leukemia virus resulted in accelerated tumor onset with associated increases in clonal complexity and lymphoid dissemination. Large-scale analysis of retroviral integration sites in these tumors revealed a profound bias towards a narrow range of target genes, including Jdp2 (Jundm2), D cyclin, and Pim family genes. Remarkably, direct PCR analysis of integration hotspots revealed that every progressing tumor consisted of multiple clones harboring hits at these loci, giving access to large numbers of independent insertion events and uncovering the contrasting mutagenic mechanisms operating at each target gene. Direct PCR analysis showed that high-frequency targeting occurs only in the tumor environment in vivo and is specific for the progression gene set. These results indicate that early lymphomas in MYC/Runx2 mice remain dependent on exogenous growth signals, and that progression can be achieved by constitutive activation of pathways converging on a cell cycle checkpoint that acts as the major rate-limiting step for lymphoma outgrowth. [Cancer Res 2007;67(11):5126–33]

Published

2023

6. Supplementary Table 1 from Insertional Mutagenesis Reveals Progression Genes and Checkpoints in MYC/Runx2 Lymphomas

Author

James C. Neil, Ewan Cameron, Linda Scobie, Karen Blyth, Linda Hanlon, Nancy Mackay, and Monica Stewart

Abstract

Supplementary Table 1 from Insertional Mutagenesis Reveals Progression Genes and Checkpoints in MYC/Runx2 Lymphomas

Published

2023

7. Data from Runx Regulation of Sphingolipid Metabolism and Survival Signaling

Author

James C. Neil, Ewan R. Cameron, Michael J.O. Wakelam, Qifeng Zhang, Gillian Borland, Alma Jenkins, Anne Terry, and Anna Kilbey

Abstract

The Runx genes (Runx1, 2, and 3) regulate cell fate in development and can operate as either oncogenes or tumor suppressors in cancer. The oncogenic potential of ectopic Runx expression has been shown in transgenic mice that develop lymphoma in potent synergy with overexpressed Myc, and in established fibroblasts that display altered morphology and increased tumorigenicity. Candidate oncogenic functions of overexpressed Runx genes include resistance to apoptosis in response to intrinsic and extrinsic stresses. In a search for gene targets responsible for this aspect of Runx phenotype, we have identified three key enzymes in sphingolipid metabolism (Sgpp1, Ugcg, and St3gal5/Siat9) as direct targets for Runx transcriptional regulation in a manner consistent with survival and apoptosis resistance. Consistent with these changes in gene expression, mass spectrometric analysis showed that ectopic Runx reduces intracellular long-chain ceramides in NIH3T3 fibroblasts and elevated extracellular sphingosine 1 phosphate. Runx expression also opposed the activation of c-Jun-NH2-kinase and p38MAPK, key mediators of ceramide-induced death, and suppressed the onset of apoptosis in response to exogenous tumor necrosis factor α. The survival advantage conferred by ectopic Runx could be partially recapitulated by exogenous sphingosine 1 phosphate and was accompanied by reduced phosphorylation of p38MAPK. These results reveal a novel link between transcription factor oncogenes and lipid signaling pathways involved in cancer cell survival and chemoresistance. Cancer Res; 70(14); 5860–9. ©2010 AACR.

Published

2023

8. Gamma-Retrovirus Integration Marks Cell Type-Specific Cancer Genes: A Novel Profiling Tool in Cancer Genomics.

Author

Kathryn L Gilroy, Anne Terry, Asif Naseer, Jeroen de Ridder, Amin Allahyar, Weiwei Wang, Eric Carpenter, Andrew Mason, Gane K-S Wong, Ewan R Cameron, Anna Kilbey, and James C Neil

Subjects

Medicine, Science

Abstract

Retroviruses have been foundational in cancer research since early studies identified proto-oncogenes as targets for insertional mutagenesis. Integration of murine gamma-retroviruses into the host genome favours promoters and enhancers and entails interaction of viral integrase with host BET/bromodomain factors. We report that this integration pattern is conserved in feline leukaemia virus (FeLV), a gamma-retrovirus that infects many human cell types. Analysis of FeLV insertion sites in the MCF-7 mammary carcinoma cell line revealed strong bias towards active chromatin marks with no evidence of significant post-integration growth selection. The most prominent FeLV integration targets had little overlap with the most abundantly expressed transcripts, but were strongly enriched for annotated cancer genes. A meta-analysis based on several gamma-retrovirus integration profiling (GRIP) studies in human cells (CD34+, K562, HepG2) revealed a similar cancer gene bias but also remarkable cell-type specificity, with prominent exceptions including a universal integration hotspot at the long non-coding RNA MALAT1. Comparison of GRIP targets with databases of super-enhancers from the same cell lines showed that these have only limited overlap and that GRIP provides unique insights into the upstream drivers of cell growth. These observations elucidate the oncogenic potency of the gamma-retroviruses and support the wider application of GRIP to identify the genes and growth regulatory circuits that drive distinct cancer types.

Published

2016

9. Collaboration of MYC and RUNX2 in lymphoma simulates T‐cell receptor signaling and attenuates p53 pathway activity

Author

Camille Huser, Ailsa Holroyd, Alma McDonald, Amanda MacCallum, Jodie Hay, Ewan R. Cameron, Anna Kilbey, James C. Neil, and Kathryn Gilroy

Subjects

p53, 0301 basic medicine, Programmed cell death, senescence, Lymphoma, CD30, Blotting, Western, Receptors, Antigen, T-Cell, Core Binding Factor Alpha 1 Subunit, Mice, Transgenic, Thymus Gland, MYC, Biology, Biochemistry, Proto-Oncogene Proteins c-myc, Transcriptome, Mice, 03 medical and health sciences, 0302 clinical medicine, Downregulation and upregulation, Cell Line, Tumor, Transcriptional regulation, Animals, Molecular Biology, Cellular Senescence, Research Articles, Cell Proliferation, SMYD2, Principal Component Analysis, Protein arginine methyltransferase 5, Computational Biology, CD28, Histone-Lysine N-Methyltransferase, Cell Biology, RUNX, Cell biology, 030104 developmental biology, Apoptosis, 030220 oncology & carcinogenesis, Tumor Suppressor Protein p53, Signal Transduction, Research Article

Abstract

MYC and RUNX oncogenes each trigger p53‐mediated failsafe responses when overexpressed in vitro and collaborate with p53 deficiency in vivo. However, together they drive rapid onset lymphoma without mutational loss of p53. This phenomenon was investigated further by transcriptomic analysis of premalignant thymus from RUNX2/MYC transgenic mice. The distinctive contributions of MYC and RUNX to transcriptional control were illustrated by differential enrichment of canonical binding sites and gene ontology analyses. Pathway analysis revealed signatures of MYC, CD3, and CD28 regulation indicative of activation and proliferation, but also strong inhibition of cell death pathways. In silico analysis of discordantly expressed genes revealed Tnfsrf8/CD30, Cish, and Il13 among relevant targets for sustained proliferation and survival. Although TP53 mRNA and protein levels were upregulated, its downstream targets in growth suppression and apoptosis were largely unperturbed. Analysis of genes encoding p53 posttranslational modifiers showed significant upregulation of three genes, Smyd2, Set, and Prmt5. Overexpression of SMYD2 was validated in vivo but the functional analysis was constrained by in vitro loss of p53 in RUNX2/MYC lymphoma cell lines. However, an early role is suggested by the ability of SMYD2 to block senescence‐like growth arrest induced by RUNX overexpression in primary fibroblasts.

Published

2019

10. Insertional mutagenesis and deep profiling reveals gene hierarchies and a Myc/p53-dependent bottleneck in lymphomagenesis.

Author

Camille A Huser, Kathryn L Gilroy, Jeroen de Ridder, Anna Kilbey, Gillian Borland, Nancy Mackay, Alma Jenkins, Margaret Bell, Pawel Herzyk, Louise van der Weyden, David J Adams, Alistair G Rust, Ewan Cameron, and James C Neil

Subjects

Genetics, QH426-470

Abstract

Retroviral insertional mutagenesis (RIM) is a powerful tool for cancer genomics that was combined in this study with deep sequencing (RIM/DS) to facilitate a comprehensive analysis of lymphoma progression. Transgenic mice expressing two potent collaborating oncogenes in the germ line (CD2-MYC, -Runx2) develop rapid onset tumours that can be accelerated and rendered polyclonal by neonatal Moloney murine leukaemia virus (MoMLV) infection. RIM/DS analysis of 28 polyclonal lymphomas identified 771 common insertion sites (CISs) defining a 'progression network' that encompassed a remarkably large fraction of known MoMLV target genes, with further strong indications of oncogenic selection above the background of MoMLV integration preference. Progression driven by RIM was characterised as a Darwinian process of clonal competition engaging proliferation control networks downstream of cytokine and T-cell receptor signalling. Enhancer mode activation accounted for the most efficiently selected CIS target genes, including Ccr7 as the most prominent of a set of chemokine receptors driving paracrine growth stimulation and lymphoma dissemination. Another large target gene subset including candidate tumour suppressors was disrupted by intragenic insertions. A second RIM/DS screen comparing lymphomas of wild-type and parental transgenics showed that CD2-MYC tumours are virtually dependent on activation of Runx family genes in strong preference to other potent Myc collaborating genes (Gfi1, Notch1). Ikzf1 was identified as a novel collaborating gene for Runx2 and illustrated the interface between integration preference and oncogenic selection. Lymphoma target genes for MoMLV can be classified into (a) a small set of master regulators that confer self-renewal; overcoming p53 and other failsafe pathways and (b) a large group of progression genes that control autonomous proliferation in transformed cells. These findings provide insights into retroviral biology, human cancer genetics and the safety of vector-mediated gene therapy.

Published

2014

11. Safety of Retroviral Vectors in Clinical Applications: Lessons from Retroviral Biology and Pathogenesis

Author

James C. Neil

Subjects

0301 basic medicine, Genetic enhancement, Cancer, Computational biology, Biology, medicine.disease, Genome, Viral vector, Insertional mutagenesis, 03 medical and health sciences, Transformation (genetics), 030104 developmental biology, 0302 clinical medicine, 030220 oncology & carcinogenesis, medicine, Vector (molecular biology), Gene

Abstract

The ability of retroviruses to integrate a precise copy of the viral genome into host cell DNA (deoxyribonucleic acid) has been harnessed in the development of retroviral vectors for stable delivery of foreign genes to target cells. Over several decades, these tools have been utilised in human medicine in diverse applications from cell lineage tracing by gene marking to correction of single-gene disorders and therapy of cancer. The unanticipated occurrence of leukaemias due to vector insertional mutagenesis in trials of gene therapy led to an urgent search for safer vectors and delivery systems. The advent of T-cell therapy for cancer has led to renewed interest in retroviral vectors as stable and efficient delivery vehicles and is supported by observations suggesting that mature T cells are relatively resistant to oncogenic transformation by retroviruses. However, this evidence is circumstantial and the long-term risks are poorly understood. Retroviral vector safety is considered here from the perspective of the biology and pathogenesis of their parental viruses. It is suggested that robust cell suicide strategies to remove transduced cells are likely to be important if retroviral vectors are to be adopted widely for delivery of T-cell therapy for cancer and other diseases.

Published

2017

12. Frequent Infection of Human Cancer Xenografts with Murine Endogenous Retroviruses in Vivo

Author

Anne Terry, Anna Kilbey, Asif Naseer, Karen Blyth, Margaret Bell, Ciorsdaidh Watts, Kathryn Gilroy, Ewan R. Cameron, James C. Neil, Nancy Mackay, and Susan M. Mason

Subjects

Chemokine, lcsh:QR1-502, Endogenous retrovirus, Biology, lcsh:Microbiology, Virus, Article, Mice, In vivo, Virology, Neoplasms, Murine leukemia virus, medicine, cancer, Animals, Humans, xenotropic, Prospective Studies, xenograft, Mice, Inbred BALB C, Endogenous Retroviruses, medicine.disease, biology.organism_classification, Raji cell, Leukemia, Infectious Diseases, Cell culture, biology.protein, Heterografts, murine leukemia virus

Abstract

Infection of human cancer xenografts in mice with murine leukemia viruses (MLVs) is a long-standing observation, but the likelihood of infection in vivo and its biological consequences are poorly understood. We therefore conducted a prospective study in commonly used xenograft recipient strains. From BALB/c nude mice engrafted with MCF7 human mammary carcinoma cells, we isolated a virus that was virtually identical to Bxv1, a locus encoding replication-competent xenotropic MLV (XMLV). XMLV was detected in 9/17 (53%) independently isolated explants. XMLV was not found in primary leukemias or in THP1 leukemia cells grown in Bxv1-negative NSG (NOD/SCID/γCnull) mice, although MCF7 explants harbored replication-defective MLV proviruses. To assess the significance of infection for xenograft behavior in vivo, we examined changes in growth and global transcription in MCF7 and the highly susceptible Raji Burkitt lymphoma cell line chronically infected with XMLV. Raji cells showed a stronger transcriptional response that included up-regulation of chemokines and effectors of innate antiviral immunity. In conclusion, the risk of de novo XMLV infection of xenografts is high in Bxv1 positive mice, while infection can have positive or negative effects on xenograft growth potential with significant consequences for interpretation of many xenograft studies.

Published

2015

13. RUNX Proteins in Development and Cancer

Author

Yoram Groner, Yoshiaki Ito, Paul Liu, James C. Neil, Nancy A. Speck, Andre van Wijnen, Yoram Groner, Yoshiaki Ito, Paul Liu, James C. Neil, Nancy A. Speck, and Andre van Wijnen

Subjects

Life sciences, DNA-binding proteins--Cancer--Research

Abstract

This volume provides the reader with an overview of the diverse functions of the RUNX family of genes. As highlighted in the introduction and several of the 29 chapters, humans and other mammals have three RUNX genes that are known to play specific roles in blood, bone and neuronal development. However, their evolutionary history has recently been traced back to unicellular organisms and their involvement in many well-known signaling pathways (Wnt, TGFb, Notch, Hippo) is indicative of a more general function in cell biology. Their documented roles in cell fate decisions include control of proliferation, differentiation, survival, senescence and autophagy. The pleiotropic effects of RUNX in development are mirrored in cancer, where RUNX genes can function as oncogenes that collaborate strongly with Myc family oncogenes or as tumour suppressor genes. In the latter role, they display hallmarks of both ‘gatekeepers'that modulate p53 responses and ‘caretakers'that protect the genome from DNA damage. Several chapters focus on the importance of these genes in leukemia research, where RUNX1 and CBFB are frequently affected by chromosomal translocations that generate fusion oncoproteins, while recent studies suggest wider roles for RUNX modulation in solid cancers. Moreover, RUNX genes are intimately involved in the development and regulation of the immune system, while emerging evidence suggests a role in innate immunity to infectious agents, including HIV. At the biochemical level, the RUNX family can serve as activators or repressors of transcription and as stable mediators of epigenetic memory through mitosis. Not surprisingly, RUNX activity is controlled at multiple levels, this includes miRNAs and a plethora of post-translational modifications. Several chapters highlight the interplay between the three mammalian RUNX genes, where cross-talk and partial functional redundancies are evident. Finally, structural analysis of the RUNX/CBFB interaction has led to the development of small molecule inhibitors that provide exciting new tools to decipher the roles of RUNX in development and as targets for therapy. This volume provides a compendium and reference source that will be of broad interest to cancer researchers, developmental biologists and immunologists.

Published

2017

14. The RUNX Genes as Conditional Oncogenes: Insights from Retroviral Targeting and Mouse Models

Author

James C, Neil, Kathryn, Gilroy, Gillian, Borland, Jodie, Hay, Anne, Terry, and Anna, Kilbey

Subjects

Disease Models, Animal, Mice, Cell Transformation, Neoplastic, Retroviridae, Neoplasms, Animals, Core Binding Factor alpha Subunits, Humans, Oncogenes, Tumor Suppressor Protein p53

Abstract

The observation that the Runx genes act as targets for transcriptional activation by retroviral insertion identified a new family of dominant oncogenes. However, it is now clear that Runx genes are 'conditional' oncogenes whose over-expression is growth inhibitory unless accompanied by another event such as concomitant over-expression of MYC or loss of p53 function. Remarkably, while the oncogenic activities of either MYC or RUNX over-expression are suppressed while p53 is intact, the combination of both neutralises p53 tumour suppression in vivo by as yet unknown mechanisms. Moreover, there is emerging evidence that endogenous, basal RUNX activity is important to maintain the viability and proliferation of MYC-driven lymphoma cells. There is also growing evidence that the human RUNX genes play a similar conditional oncogenic role and are selected for over-expression in end-stage cancers of multiple types. Paradoxically, reduced RUNX activity can also predispose to cell immortalisation and transformation, particularly by mutant Ras. These apparently conflicting observations may be reconciled in a stage-specific model of RUNX involvement in cancer. A question that has yet to be fully addressed is the extent to which the three Runx genes are functionally redundant in cancer promotion and suppression.

Published

2017

15. The RUNX Genes as Conditional Oncogenes: Insights from Retroviral Targeting and Mouse Models

Author

James C. Neil, Anne Terry, Anna Kilbey, Jodie Hay, Kathryn Gilroy, and Gillian Borland

Subjects

0301 basic medicine, Genetics, Senescence, Core Binding Factor alpha Subunits, Oncogene, Cell, Cancer, Endogeny, Biology, medicine.disease, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, 030220 oncology & carcinogenesis, medicine, Cancer research, Gene, Function (biology)

Abstract

The observation that the Runx genes act as targets for transcriptional activation by retroviral insertion identified a new family of dominant oncogenes. However, it is now clear that Runx genes are 'conditional' oncogenes whose over-expression is growth inhibitory unless accompanied by another event such as concomitant over-expression of MYC or loss of p53 function. Remarkably, while the oncogenic activities of either MYC or RUNX over-expression are suppressed while p53 is intact, the combination of both neutralises p53 tumour suppression in vivo by as yet unknown mechanisms. Moreover, there is emerging evidence that endogenous, basal RUNX activity is important to maintain the viability and proliferation of MYC-driven lymphoma cells. There is also growing evidence that the human RUNX genes play a similar conditional oncogenic role and are selected for over-expression in end-stage cancers of multiple types. Paradoxically, reduced RUNX activity can also predispose to cell immortalisation and transformation, particularly by mutant Ras. These apparently conflicting observations may be reconciled in a stage-specific model of RUNX involvement in cancer. A question that has yet to be fully addressed is the extent to which the three Runx genes are functionally redundant in cancer promotion and suppression.

Published

2017

16. Disrupting MLV integrase:BET protein interaction biases integration into quiescent chromatin and delays but does not eliminate tumor activation in a MYC/Runx2 mouse model

Author

Jodie Hay, Margaret Bell, Nancy Mackay, Sriram Aiyer, Alan Engelman, Anna Kilbey, Gillian Borland, Christine A. Kozak, James C. Neil, Rodrigo A. Villanueva, Vasudevan Achuthan, Dylan Fingerman, Monica J. Roth, Kathryn Gilroy, Lorenz Loyola, and Ewan R. Cameron

Subjects

Carcinogenesis, viruses, Genes, myc, Gene Expression, Endogenous retrovirus, Core Binding Factor Alpha 1 Subunit, Artificial Gene Amplification and Extension, medicine.disease_cause, Polymerase Chain Reaction, Biochemistry, Mice, Murine leukemia virus, Medicine and Health Sciences, Biology (General), 0303 health sciences, Mammalian Genomics, DNA methylation, biology, Chromosome Biology, 030302 biochemistry & molecular biology, Animal Models, Genomics, Chromatin, 3. Good health, Integrase, Leukemia Virus, Murine, Nucleic acids, Experimental Organism Systems, Oncology, CpG site, Epigenetics, DNA modification, Chromatin modification, Research Article, QH301-705.5, Virus Integration, Genetic Vectors, Immunology, Mice, Transgenic, Mouse Models, Research and Analysis Methods, Microbiology, 03 medical and health sciences, Model Organisms, Virology, Genetics, medicine, Animals, Humans, Molecular Biology Techniques, Protein Interactions, Molecular Biology, 030304 developmental biology, Leukemia, Experimental, Integrases, Wild type, Biology and Life Sciences, Computational Biology, Proteins, Cell Biology, DNA, RC581-607, Genome Analysis, Genomic Libraries, biology.organism_classification, Molecular biology, Disease Models, Animal, Tumor Virus Infections, Animal Genomics, Animal Studies, biology.protein, Parasitology, Immunologic diseases. Allergy, K562 Cells, Retroviridae Infections

Abstract

Murine leukemia virus (MLV) integrase (IN) lacking the C-terminal tail peptide (TP) loses its interaction with the host bromodomain and extraterminal (BET) proteins and displays decreased integration at promoter/enhancers and transcriptional start sites/CpG islands. MLV lacking the IN TP via an altered open reading frame was used to infect tumorigenesis mouse model (MYC/Runx2) animals to observe integration patterns and phenotypic effects, but viral passage resulted in the restoration of the IN TP through small deletions. Mice subsequently infected with an MLV IN lacking the TP coding sequence (TP-) showed an improved median survival by 15 days compared to wild type (WT) MLV infection. Recombination with polytropic endogenous retrovirus (ERV), Pmv20, was identified in seven mice displaying both fast and slow tumorigenesis, highlighting the strong selection within the mouse to maintain the full-length IN protein. Mapping the genomic locations of MLV in tumors from an infected mouse with no observed recombination with ERVs, TP-16, showed fewer integrations at TSS and CpG islands, compared to integrations observed in WT tumors. However, this mouse succumbed to the tumor in relatively rapid fashion (34 days). Analysis of the top copy number integrants in the TP-16 tumor revealed their proximity to known MLV common insertion site genes while maintaining the MLV IN TP- genotype. Furthermore, integration mapping in K562 cells revealed an insertion preference of MLV IN TP- within chromatin profile states associated with weakly transcribed heterochromatin with fewer integrations at histone marks associated with BET proteins (H3K4me1/2/3, and H3K27Ac). While MLV IN TP- showed a decreased overall rate of tumorigenesis compared to WT virus in the MYC/Runx2 model, MLV integration still occurred at regions associated with oncogenic driver genes independently from the influence of BET proteins, either stochastically or through trans-complementation by functional endogenous Gag-Pol protein., Author summary Many different retroviruses, including murine leukemia virus (MLV), are used as vectors for human gene therapy and cancer immunotherapies (CAR-T) because of their stable and efficient delivery of genetic material into the host DNA. However, this process can result in activation and/or disruption of cellular genes, which has resulted in the outgrowth of tumors in previous clinical trials. Of critical importance is the preferred location within the host genome at which the retrovirus integrates. Our study presents a modified MLV virus that has lost the ability to bind to the host BET proteins, the drivers of insertion at promoter/enhancer regions of highly activated genes. This is the first direct study within an animal model to examine whether infection with this type of modified MLV virus affects tumor progression. We found that the modified virus improved the survival of the well-characterized MYC/Runx2 mouse compared to infections with the wild-type MLV. Most modified viral integrants mapped into less active regions of the genome, but some integration events still occurred near cancer-related genes. Thus, while the modified MLV virus can be a safer vector than the wildtype virus, it still maintains the potential to activate oncogenes. This study provides new insights on how to improve the safety of MLV retroviral vectors.

Published

2019

17. Barriers to Infection of Human Cells by Feline Leukemia Virus: Insights into Resistance to Zoonosis

Author

Anne, Terry, Anna, Kilbey, Asif, Naseer, Laura S, Levy, Shamim, Ahmad, Ciorsdaidh, Watts, Nancy, Mackay, Ewan, Cameron, Sam, Wilson, and James C, Neil

Subjects

viruses, Leukemia Virus, Feline, Virus Integration, APOBEC, Gene Expression, APOBEC-3G Deaminase, Genome, Viral, zoonosis, Virus Replication, restriction factors, Virus-Cell Interactions, Viral Tropism, HEK293 Cells, Species Specificity, Cell Line, Tumor, Zoonoses, Mutation, Cats, Animals, Humans, feline leukemia virus, Disease Susceptibility, Retroviridae Infections

Abstract

The human genome displays a rich fossil record of past gammaretrovirus infections, yet no current epidemic is evident, despite environmental exposure to viruses that infect human cells in vitro. Feline leukemia viruses (FeLVs) rank high on this list, but neither domestic nor workplace exposure has been associated with detectable serological responses. Nonspecific inactivation of gammaretroviruses by serum factors appears insufficient to explain these observations. To investigate further, we explored the susceptibilities of primary and established human cell lines to FeLV-B, the most likely zoonotic variant. Fully permissive infection was common in cancer-derived cell lines but was also a feature of nontransformed keratinocytes and lung fibroblasts. Cells of hematopoietic origin were generally less permissive and formed discrete groups on the basis of high or low intracellular protein expression and virion release. Potent repression was observed in primary human blood mononuclear cells and a subset of leukemia cell lines. However, the early steps of reverse transcription and integration appear to be unimpaired in nonpermissive cells. FeLV-B was subject to G→A hypermutation with a predominant APOBEC3G signature in partially permissive cells but was not mutated in permissive cells or in nonpermissive cells that block secondary viral spread. Distinct cellular barriers that protect primary human blood cells are likely to be important in protection against zoonotic infection with FeLV. IMPORTANCE Domestic exposure to gammaretroviruses such as feline leukemia viruses (FeLVs) occurs worldwide, but the basis of human resistance to infection remains incompletely understood. The potential threat is evident from the human genome sequence, which reveals many past epidemics of gammaretrovirus infection, and from recent cross-species jumps of gammaretroviruses from rodents to primates and marsupials. This study examined resistance to infection at the cellular level with the most prevalent human cell-tropic FeLV variant, FeLV-B. We found that blood cells are uniquely resistant to infection with FeLV-B due to the activity of cellular enzymes that mutate the viral genome. A second block, which appears to suppress viral gene expression after the viral genome has integrated into the host cell genome, was identified. Since cells derived from other normal human cell types are fully supportive of FeLV replication, innate resistance of blood cells could be critical in protecting against cross-species infection.

Published

2016

18. RUNX oncoproteins and miRNA networks

Author

James C. Neil, Jodie Hay, and Gillian Borland

Subjects

0301 basic medicine, Myeloid leukemia, Chromosomal translocation, Biology, Phenotype, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Oncology, 030220 oncology & carcinogenesis, microRNA, Cancer research, Regulatory circuit, Runx1 aml1

Abstract

News on: An AML1-ETO/miR-29b-1 regulatory circuit modulates phenotypic properties of acute myeloid leukemia cells by Zaidi et\ud al. Oncotarget. 2017; 8:39994-40005. https://doi.org/10.18632/oncotarget.18127.

Published

2017

19. Runx2 in normal tissues and cancer cells: A developing story

Author

Camille Huser, Laura McDonald, François Vaillant, Ewan R. Cameron, Karen Blyth, Marie Anne Pringle, Torsten Stein, James C. Neil, and Alma Jenkins

Subjects

Core Binding Factor Alpha 1 Subunit, Biology, Core Binding Factor beta Subunit, Mice, chemistry.chemical_compound, Prostate cancer, medicine, Animals, Humans, Genes, Tumor Suppressor, Neoplasms, Glandular and Epithelial, Neoplasm Metastasis, Molecular Biology, Gene, Transcription factor, Genetics, Oncogene, Oncogenes, Cell Biology, Hematology, medicine.disease, RUNX2, Haematopoiesis, RUNX1, chemistry, Hematologic Neoplasms, Cancer cell, Cancer research, Molecular Medicine

Abstract

The Runx transcription factors are essential for mammalian development, most notably in the haematopoietic and osteogenic lineages. Runx1 and its binding partner, CBFbeta, are frequently targeted in acute leukaemia but evidence is accumulating that all three Runx genes may have a role to play in a wider range of cancers, either as tumour promoters or tumour suppressors. Whilst Runx2 is renowned for its role as a master regulator of bone development we discuss here its expression pattern and putative functions beyond this lineage. Furthermore, we review the evidence that RUNX2 promotes neoplastic development in haematopoietic lineages and in advanced mammary and prostate cancer.

Published

2010

20. Runx Regulation of Sphingolipid Metabolism and Survival Signaling

Author

Qifeng Zhang, Gillian Borland, Alma Jenkins, Anne Terry, Michael J.O. Wakelam, Anna Kilbey, James C. Neil, and Ewan R. Cameron

Subjects

MAPK/ERK pathway, Cancer Research, MAP Kinase Kinase 4, MAP Kinase Signaling System, Biology, medicine.disease_cause, p38 Mitogen-Activated Protein Kinases, Article, Mice, chemistry.chemical_compound, Sphingosine, medicine, Transcriptional regulation, Animals, Sphingosine-1-phosphate, Promoter Regions, Genetic, Transcription factor, Sphingolipids, Binding Sites, Core Binding Factor alpha Subunits, Lipid signaling, Cell biology, Oncology, chemistry, NIH 3T3 Cells, Lysophospholipids, Signal transduction, Carcinogenesis

Abstract

The Runx genes (Runx1, 2, and 3) regulate cell fate in development and can operate as either oncogenes or tumor suppressors in cancer. The oncogenic potential of ectopic Runx expression has been shown in transgenic mice that develop lymphoma in potent synergy with overexpressed Myc, and in established fibroblasts that display altered morphology and increased tumorigenicity. Candidate oncogenic functions of overexpressed Runx genes include resistance to apoptosis in response to intrinsic and extrinsic stresses. In a search for gene targets responsible for this aspect of Runx phenotype, we have identified three key enzymes in sphingolipid metabolism (Sgpp1, Ugcg, and St3gal5/Siat9) as direct targets for Runx transcriptional regulation in a manner consistent with survival and apoptosis resistance. Consistent with these changes in gene expression, mass spectrometric analysis showed that ectopic Runx reduces intracellular long-chain ceramides in NIH3T3 fibroblasts and elevated extracellular sphingosine 1 phosphate. Runx expression also opposed the activation of c-Jun-NH2-kinase and p38MAPK, key mediators of ceramide-induced death, and suppressed the onset of apoptosis in response to exogenous tumor necrosis factor α. The survival advantage conferred by ectopic Runx could be partially recapitulated by exogenous sphingosine 1 phosphate and was accompanied by reduced phosphorylation of p38MAPK. These results reveal a novel link between transcription factor oncogenes and lipid signaling pathways involved in cancer cell survival and chemoresistance. Cancer Res; 70(14); 5860–9. ©2010 AACR.

Published

2010

21. A Novel Model of SCID-X1 Reconstitution Reveals Predisposition to Retrovirus-induced Lymphoma but No Evidence of γC Gene Oncogenicity

Author

Ralph D. Hector, Louise Grant, Anne A Nielsen, Linda Scobie, James C. Neil, Margaret Bell, Sharon Meikle, Karen Blyth, Adrain Philbey, Adrain J Thrasher, and Ewan R. Cameron

Subjects

Lymphoma, T-Lymphocytes, Genetic enhancement, X-Linked Combined Immunodeficiency Diseases, Polymerase Chain Reaction, Mice, 0302 clinical medicine, Drug Discovery, Murine leukemia virus, Promoter Regions, Genetic, B-Lymphocytes, 0303 health sciences, Flow Cytometry, 3. Good health, Leukemia, 030220 oncology & carcinogenesis, Molecular Medicine, Interleukin Receptor Common gamma Subunit, Genetically modified mouse, Genotype, Transgene, Blotting, Western, CD2 Antigens, Mice, Transgenic, Thymus Gland, In Vitro Techniques, Biology, Immunophenotyping, 03 medical and health sciences, Genetics, medicine, Animals, Humans, Molecular Biology, 030304 developmental biology, Pharmacology, Severe combined immunodeficiency, Original Articles, Genetic Therapy, medicine.disease, biology.organism_classification, eye diseases, Retroviridae, Immunology, Ectopic expression, CD8

Abstract

The emergence of leukemia following gene transfer to restore common cytokine receptor gamma chain (gammaC) function in X-linked severe combined immunodeficiency (SCID-X1) has raised important questions with respect to gene therapy safety. To explore the risk factors involved, we tested the oncogenic potential of human gammaC in new strains of transgenic mice expressing the gene under the control of the CD2 promoter and locus control region (LCR). These mice demonstrated mildly perturbed T-cell development, with an increased proportion of thymic CD8 cells, but showed no predisposition to tumor development even on highly tumor prone backgrounds or after gamma-retrovirus infection. The human CD2-gammaC transgene rescued T and B-cell development in gammaC(-/-) mice but with an age-related delay, mimicking postnatal reconstitution in SCID-X1 gene therapy subjects. However, we noted that gammaC(-/-) mice are acutely susceptible to murine leukemia virus (MLV) leukemogenesis, and that this trait was not corrected by the gammaC transgene. We conclude that the SCID-X1 phenotype can be corrected safely by stable ectopic expression of gammaC and that the transgene is not significantly oncogenic when expressed in this context. However, an underlying predisposition conferred by the SCID-X1 background appears to collaborate with insertional mutagenesis to increase the risk of tumor development.

Published

2009

22. RUNX1 and its fusion oncoprotein derivative, RUNX1-ETO, induce senescence-like growth arrest independently of replicative stress

Author

Gordon Peters, Anna Kilbey, Sandy Wotton, Carol Stocking, Anne Terry, James C. Neil, Ewan R. Cameron, Alma Jenkins, and Kamil Wolyniec

Subjects

Male, Senescence, Cancer Research, RUNX1, Oncogene Proteins, Fusion, DNA damage, Blotting, Western, Foreskin, Biology, medicine.disease_cause, p38 Mitogen-Activated Protein Kinases, Article, RUNX1 Translocation Partner 1 Protein, p14arf, hemic and lymphatic diseases, Genetics, medicine, Humans, Molecular Biology, Cells, Cultured, Cellular Senescence, Cyclin-Dependent Kinase Inhibitor p16, Cell Proliferation, Mutation, Reverse Transcriptase Polymerase Chain Reaction, Cell growth, Infant, Newborn, Fibroblasts, Fusion protein, premature senescence, RUNX1-ETO, Core Binding Factor Alpha 2 Subunit, embryonic structures, ras Proteins, Cancer research, Tumor Suppressor Protein p53, Reactive Oxygen Species, Carcinogenesis, Cell aging

Abstract

A role for the RUNX genes in cancer fail-safe processes has been suggested by their induction of senescence-like growth arrest in primary murine fibroblasts and the failure of RAS-induced senescence in Runx2-deficient cells. We now show that RUNX1 induces senescence in human primary fibroblasts. High-affinity DNA binding is necessary but not sufficient, as shown by the functional attenuation of the truncated RUNX1/AML1a isoform and the TEL-RUNX1 fusion oncoprotein. However, a similar phenotype was potently induced by the RUNX1-ETO (AML1-ETO) oncoprotein, despite its dominant-negative potential. A detailed comparison of H-RAS(V12), RUNX1 and RUNX1-ETO senescent phenotypes showed that the RUNX effectors induce earlier growth stasis with only low levels of DNA damage signaling and a lack of chromatin condensation, a marker of irreversible growth arrest. In human fibroblasts, all effectors induced p53 in the absence of detectable p14(Arf), whereas only RUNX1-ETO induced senescence in p16(Ink4a)-null cells. Correlation was noted between induction of p53, reactive oxygen species and phospho-p38, whereas p38(MAPK) inhibition rescued cell growth markedly. These findings indicate a role for replication-independent pathways in RUNX and RUNX1-ETO senescence, and show that the context-specific oncogenic activity of RUNX1 fusion proteins is mirrored in their distinctive interactions with fail-safe responses.

Published

2009

23. Oncogene-induced senescence: An essential role for Runx

Author

Anna Kilbey, Anne Terry, James C. Neil, and Ewan R. Cameron

Subjects

Senescence, Cell cycle checkpoint, Biology, Models, Biological, Article, Cyclin Gene, Stress, Physiological, Animals, Humans, Gene Regulatory Networks, Genes, Tumor Suppressor, Molecular Biology, Cellular Senescence, Cell Proliferation, Cyclin, Cell growth, Core Binding Factor alpha Subunits, Oncogenes, Cell Biology, Embryonic stem cell, Cell biology, ras Proteins, Signal transduction, Cell aging, Signal Transduction, Developmental Biology

Abstract

Oncogene-induced senescence (OIS) is characterised by a stable cell cycle arrest triggered by activated oncogenes and tumour suppressors. Whilst the in vivo relevance of OIS as a mode of tumour suppression is now beyond doubt many key questions with regard to the underlying mechanisms remain unanswered. To address these questions, we first review current knowledge of the essential players and pathways in OIS focussing our discussions mainly on murine cell systems and the paradigm of Ras-induced senescence. We then update experimental evidence for the involvement of the Runx genes that have recently emerged as important mediators of OIS. Of particular interest is the observation that Runx2 disruption renders primary murine embryonic fibroblasts (MEFs) refractory to Ras-induced senescence despite induction of a cascade of growth inhibitors and senescence markers. We suggest that Runx acts downstream of p53 in the "execution phase" of senescence specifically through deregulation of cyclin gene expression. We...

Published

2008

24. Runx2 contributes to the regenerative potential of the mammary epithelium

Author

Theresa Higgins, Susan M. Mason, Owen J. Sansom, Matthew J. Smalley, Alessandra I. Riggio, Ian Rosewell, Karen Blyth, Ayala King, Joanna S. Morris, Nicola Ferrari, Laura McDonald, Ewan R. Cameron, and James C. Neil

Subjects

Pathology, medicine.medical_specialty, Cellular differentiation, Mammary gland, Population, Core Binding Factor Alpha 1 Subunit, Biology, Epithelium, Article, RC0254, Mice, Mammary Glands, Animal, stomatognathic system, medicine, Animals, Humans, Progenitor cell, education, Wnt Signaling Pathway, education.field_of_study, Multidisciplinary, Stem Cells, Wnt signaling pathway, Cell Differentiation, Embryonic stem cell, Cell biology, Gene Expression Regulation, Neoplastic, medicine.anatomical_structure, Mammary Epithelium, Female, Stem cell

Abstract

Although best known for its role in bone development and associated structures the transcription factor RUNX2 is expressed in a wide range of lineages, including those of the mammary gland. Previous studies have indicated that Runx2 can regulate aspects of mammary cell function and influence the properties of cancer cells. In this study we investigate the role of Runx2 in the mammary stem/progenitor population and its relationship with WNT signalling. Results show that RUNX2 protein is differentially expressed throughout embryonic and adult development of the murine mammary gland with high levels of expression in mammary stem-cell enriched cultures. Importantly, functional analysis reveals a role for Runx2 in mammary stem/progenitor cell function in in vitro and in vivo regenerative assays. Furthermore, RUNX2 appears to be associated with WNT signalling in the mammary epithelium and is specifically upregulated in mouse models of WNT-driven breast cancer. Overall our studies reveal a novel function for Runx2 in regulating mammary epithelial cell regenerative potential, possibly acting as a downstream target of WNT signalling.

Published

2015

25. In memoriam--Richard M. Elliott (1954-2015)

Author

Ian Goodfellow, John McLauchlan, Chris Boutell, Stuart T. Nichol, Ralf G. Dietzgen, James C. Neil, Pedro Fernando da Costa Vasconcelos, Janet M. Daly, Geoffrey L. Smith, Friedemann Weber, Pablo R. Murcia, Mark Harris, Márcio Roberto Teixeira Nunes, Hideki Ebihara, Frederick A. Murphy, Brian J. Willett, Margaret J Hosie, John K. Fazakerley, Stephen Higgs, W. Paul Duprex, Benjamin Brennan, John Steel, Dana L. Vanlandingham, Angelina Plyusnina, Arvind H. Patel, Richard Kormelink, Robert A. Lamb, Massimo Palmarini, Bernadette M. Dutia, Alain Kohl, J. Stephen Lodmell, Scott C. Weaver, Anna-Bella Failloux, Reay G. Paterson, Peter Palese, Charles M. Rice, Anthony R. Fooks, Richard E. Randall, John N. Barr, Anice C. Lowen, Alexander Plyusnin, Noël Tordo, Stacey Efstathiou, Robert B. Tesh, Hanu R. Pappu, Michèle Bouloy, Roger Hewson, Robert G. Dalziel, Esther Schnettler, Adolfo García-Sastre, Sara Cherry, Diane E. Ullman, Rennos Fragkoudis, Centre for Virus Research, MRC - University of Glasgow Centre for Virus Research, Institute for Medical Virology [Gießen], Laboratory of Virology [Wageningen], Wageningen University and Research [Wageningen] (WUR), Arbovirus et Insectes Vecteurs - Arboviruses and Insect Vectors, Institut Pasteur [Paris] (IP), The University of Texas Medical Branch (UTMB), The Pirbright Institute, Biotechnology and Biological Sciences Research Council (BBSRC), University of Leeds, Icahn School of Medicine at Mount Sinai [New York] (MSSM), University of Edinburgh, Emory University [Atlanta, GA], University of St Andrews [Scotland], Boston University School of Medicine (BUSM), Boston University [Boston] (BU), Laboratory of Virology and Infectious Disease [New York], Rockefeller University [New York], Laboratory of Virology, Division of Intramural Research [Hamilton], National Institute of Allergy and Infectious Diseases (NIAID) (NIAID), Laboratorio de Arbovirus, Instituto Evandro Chagas, Animal and Plant Health Agency [Weybridge] (APHA), Division of Virology, University of Cambridge [UK] (CAM), Washington State University (WSU), Department of Molecular Biosciences, Northwestern University [Evanston], Biosecurity Research Institute, Kansas State University, Department of Diagnostic Medicine and Pathobiology, University of Queensland [Brisbane], Division of Biological Sciences [Missoula], University of Montana, Centers for Disease Control and Prevention [Atlanta] (CDC), Centers for Disease Control and Prevention, School of Veterinary Medicine and Science [Leicestershire], University of Nottingham, UK (UON), Department of Entomology [Riverside], University of California [Riverside] (UC Riverside), University of California (UC)-University of California (UC), Helsingin yliopisto = Helsingfors universitet = University of Helsinki, National Institute for Biological Standards and Control (NIBSC), Medicines and Healthcare Products Regulatory Agency (MHRA), Public Health England [London], Centre collaborateur de l'OMS Arbovirus et Fièvres Hémorragiques virales - Stratégies antivirales (CC-OMS), University of Pennsylvania, Institut Pasteur [Paris], Institute for Animal Health, the Pirbright Institute, Faculty of Biological Sciences, University of Leeds, University of California [Riverside] (UCR), University of California-University of California, University of Helsinki, and University of Pennsylvania [Philadelphia]

Subjects

MESH: United Kingdom, Bunyaviridae, Laboratory of Virology, Bunyaviridae Infections, Biology, History, 21st Century, Laboratorium voor Virologie, MESH: Bunyaviridae Infections, Portrait, Virology, Humans, Life Science, ComputingMilieux_MISCELLANEOUS, MESH: Bunyaviridae, MESH: Humans, Historical Article, Biography, History, 20th Century, biology.organism_classification, Obituary, United Kingdom, [SDV.MP.VIR]Life Sciences [q-bio]/Microbiology and Parasitology/Virology, MESH: History, 20th Century, EPS, MESH: History, 21st Century, MESH: Virology

Abstract

International audience

Published

2015

26. The runx genes: gain or loss of function in cancer

Author

James C. Neil, Ewan R. Cameron, and Karen Blyth

Subjects

Core Binding Factor alpha Subunits, Transcription, Genetic, General Mathematics, Growth control, Chromosomal translocation, Cell fate determination, Biology, Models, Biological, Translocation, Genetic, Mice, Transforming Growth Factor beta, Transcription (biology), Neoplasms, Animals, Humans, Genes, Tumor Suppressor, Transcription factor, Gene, Loss function, Mice, Knockout, Genetics, Leukemia, Applied Mathematics, food and beverages, Oncogenes, Neoplasm Proteins, DNA-Binding Proteins, Mutation, Transcription Factors

Abstract

The RUNX genes have come to prominence recently because of their roles as essential regulators of cell fate in development and their paradoxical effects in cancer, in which they can function either as tumour-suppressor genes or dominant oncogenes according to context. How can this family of transcription factors have such an ambiguous role in cancer? How and where do these genes impinge on the pathways that regulate growth control and differentiation? And what is the evidence for a wider role for the RUNX genes in non-haematopoietic cancers?

Published

2005

27. The Runx genes: lineage-specific oncogenes and tumor suppressors

Author

Ewan R. Cameron and James C. Neil

Subjects

Cancer Research, Lymphoma, Tumor suppressor gene, Core Binding Factor Alpha 1 Subunit, Biology, medicine.disease_cause, Molecular oncology, Gene product, Insertional mutagenesis, Mice, chemistry.chemical_compound, Proto-Oncogene Proteins, Genetics, medicine, Animals, Humans, Genes, Tumor Suppressor, Molecular Biology, Transcription factor, Genes, Dominant, Core Binding Factor alpha Subunits, Oncogenes, Fusion protein, Neoplasm Proteins, DNA-Binding Proteins, Core Binding Factor Alpha 3 Subunit, Retroviridae, RUNX1, chemistry, Leukemia, Myeloid, Core Binding Factor Alpha 2 Subunit, Cancer research, Carcinogenesis, Retroviridae Infections, Transcription Factors

Abstract

The Runx genes present a challenge to the simple binary classification of cancer genes as oncogenes or tumor suppressors. There is evidence that loss of function of two of the three mammalian Runx genes promotes cancer, but in a highly lineage-restricted manner. In human leukemias, the RUNX1 gene is involved in various chromosomal translocation events that create oncogenic fusion proteins, at least some of which appear to function as dominant-negative inhibitors of the normal gene product. Paradoxically, evidence is mounting that structurally intact Runx genes are also oncogenic when overexpressed. All the three murine genes act as targets for transcriptional activation by retroviral insertional mutagenesis, and the oncogenic potential of Runx2 has been confirmed in transgenic mice. Moreover, the RUNX1 gene is often amplified or overexpressed in cases of acute leukemia. The state of progress in elucidating the oncogenic roles of the Runx genes is the subject of this review, and we draw together recent observations in a tentative model for the effects of Runx deregulation on hematopoietic cell differentiation. We suggest that lineage-specific factors determine the sensitivity to the oncogenic effects of loss or overexpression of Runx factors.

Published

2004

28. Addiction to RUNX in lymphoma

Author

Gillian Borland, Anna Kilbey, and James C. Neil

Subjects

p53, Genetically modified mouse, oncogene addiction, Aging, Core Binding Factor alpha Subunits, Lymphoma, Antineoplastic Agents, Myc, Biology, DNA-binding protein, law.invention, chemistry.chemical_compound, law, Cell Line, Tumor, hemic and lymphatic diseases, Humans, Molecular Targeted Therapy, Gene, Transcription factor, Cell Biology, Oncogene Addiction, Molecular biology, RUNX, Gene Expression Regulation, Neoplastic, Editorial, RUNX1, chemistry, Cancer research, Suppressor, Signal Transduction

Abstract

The three mammalian Runx genes encode transcription factors that play essential but distinct and lineage-specific roles in development. These sequence-specific DNA binding proteins share a common binding cofactor (CBFβ) that confers protein stability and high affinity for target DNA on its RUNX partners. An important link to cancer was first realised through identification of both RUNX1 and CBFB as frequent targets for chromosomal translocations in human leukaemia. Early studies suggested that RUNX1 is a tumour suppressor subject to dominant negative inhibition by its fusion oncoprotein derivatives and to loss-of-function mutations in AML (reviewed in [1]). However, it is now clear that RUNX1 is far from a typical tumour suppressor as, for example, AML cells expressing the RUNX1-ETO fusion require the activity of the unaffected allele for survival [2] while ALL cases frequently over-express RUNX1 and/or display increased copy number [1]. Moreover, early studies on mouse models of lymphoma revealed all three Runx genes as targets for transcriptional activation in MYC transgenic mice, and the ability of over-expressed MYC and Runx to synergise in lymphoma has been amply confirmed in compound transgenics [1].

Published

2016

29. Linkage on chromosome 10 of several murine retroviral integration loci associated with leukaemia

Author

Peter Haviernik, Linda Wolff, Richard Koller, Nighean I. Barr, Rene Opavsky, Stephen M. Festin, and James C. Neil

Subjects

Expressed Sequence Tags, Genetics, Expressed sequence tag, Genes, myb, Sequence analysis, Virus Integration, Molecular Sequence Data, Chromosome Mapping, Locus (genetics), Biology, Provirus, biology.organism_classification, Molecular biology, Cell Line, Leukemia Virus, Murine, Mice, Retrovirus, Leukemia, Myeloid, Virology, Animals, Amino Acid Sequence, Cloning, Molecular, Scaffold/matrix attachment region, Gene, Synteny

Abstract

Mml loci have been identified as provirus integration sites among a subset of monocytic tumours induced by murine leukaemia virus (MuLV) infection of BALB/c and DBA/2 mice. These myeloid leukaemias contain a retrovirus integrated on chromosome 10 in proximity to the c-myb locus; however, c-myb expression was not altered. Detailed physical mapping enabled placement of the retroviral integration sites ∼25 kb (Mml1), ∼51 kb (Mml2), and ∼70 kb (Mml3) upstream of the c-myb locus. Furthermore, the Fti1 (fit-1) locus, a common integration site in feline leukaemia virus-induced T cell lymphomas, was mapped upstream of Mml3. Sequence analysis of Mml1, Mml2 and Mml3 loci (39·6, 16·4 and 5·9 kb, respectively) in conjunction with the BLAST (basic local alignment search tool) homology searches against the expressed sequence tag (EST) database and the use of gene/exon prediction programs revealed potential coding sequences that were not confirmed by Northern analysis or RT–PCR. The sequences between c-myb and Fti1, which were shown to include two potential scaffold/matrix attachment regions (S/MARs), are most likely regulatory in nature. An extended search for transcribed sequences far upstream of Mml3 revealed five genes, four of which were expressed in multiple tissues in mice. These genes could not be linked to tumour formation by the virus but their homologous sequences were found on human chromosome 6, thus allowing extension of the syntenic region on mouse chromosome 10 to approximately 250 kb.

Published

2002

30. Protection against feline immunodeficiency virus using replication defective proviral DNA vaccines with feline interleukin-12 and -18

Author

Jennifer Bruce, Linda Hanlon, Oswald Jarrett, Matthew C. Golder, Stephen P. Dunham, M A Rigby, Nancy Mackay, David A. Harbour, C.A. Cannon, Julie Macdonald, J. Norman Flynn, Norman Spibey, and James C. Neil

Subjects

Feline immunodeficiency virus, Genes, Viral, Molecular Sequence Data, Virulence, Immunodeficiency Virus, Feline, Antibodies, Viral, Virus Replication, Virus, DNA vaccination, Proviruses, Immunity, Feline Acquired Immunodeficiency Syndrome, Vaccines, DNA, Animals, Amino Acid Sequence, Sequence Deletion, Base Sequence, Integrases, General Veterinary, General Immunology and Microbiology, biology, Interleukin-18, Public Health, Environmental and Occupational Health, Defective Viruses, RNA-Directed DNA Polymerase, Viral Vaccines, Provirus, biology.organism_classification, Interleukin-12, Virology, Reverse transcriptase, Infectious Diseases, DNA, Viral, Lentivirus, Cats, Molecular Medicine, T-Lymphocytes, Cytotoxic

Abstract

A molecular clone of the Glasgow-8 isolate of FIV (FIVGL8) was rendered replication defective by an in-frame deletion in either reverse transcriptase (deltaRT) or integrase (deltaIN) genes for use as DNA vaccines. To test the ability of these multi-gene vaccines to protect against two feline immunodeficiency virus (FIV) isolates of differing virulence, cats were immunized using either DNA vaccine alone or co-administered with interleukin-12 (IL-12) and/or interleukin-18 (IL-18) cytokine DNA. Animals were challenged sequentially with FIV-Petaluma (FIVPET) an FIV isolate of relatively low virulence and subsequently with the more virulent FIVGL8. A proportion of vaccinates (5/18 deltaIN and 2/12 deltaRT) were protected against primary challenge with FIV(PET). Five of the vaccinated-protected cats were re-challenged with FIV(PET); four (all deltaIN) remained free of viraemia whilst all naive controls became viraemic. Following subsequent challenge with the more virulent FIVGL8 these four vaccinated-protected animals all became viraemic but showed lower proviral loads than naive cats. This study suggests that while our current DNA vaccines may not produce sterilizing immunity against more virulent isolates of FIV, they may nevertheless significantly reduce the impact of infection.

Published

2002

31. Insertional Mutagenesis and Deep Profiling Reveals Gene Hierarchies and a Myc/p53-Dependent Bottleneck in Lymphomagenesis

Author

Pawel Herzyk, Ewan R. Cameron, David J. Adams, Alma Jenkins, Alistair G. Rust, Kathryn Gilroy, Camille Huser, Louise van der Weyden, Jeroen de Ridder, Nancy Mackay, James C. Neil, Margaret Bell, Anna Kilbey, and Gillian Borland

Subjects

Cancer Research, Lymphoma, Mouse, Carcinogenesis, Genes, myb, QH426-470, Biology, medicine.disease_cause, Deep sequencing, Insertional mutagenesis, Ikaros Transcription Factor, Mice, Chemokine receptor, Model Organisms, Genetics, medicine, Animals, Humans, Gene Regulatory Networks, Enhancer, Molecular Biology, Gene, Genetics (clinical), Ecology, Evolution, Behavior and Systematics, Regulation of gene expression, Gene Expression Profiling, High-Throughput Nucleotide Sequencing, Computational Biology, Genomics, Animal Models, Gene Expression Regulation, Neoplastic, Gene expression profiling, Mutagenesis, Insertional, Germ Cells, Oncology, Cancer research, Medicine, Moloney murine leukemia virus, Tumor Suppressor Protein p53, Sequence Analysis, Research Article

Abstract

Retroviral insertional mutagenesis (RIM) is a powerful tool for cancer genomics that was combined in this study with deep sequencing (RIM/DS) to facilitate a comprehensive analysis of lymphoma progression. Transgenic mice expressing two potent collaborating oncogenes in the germ line (CD2-MYC, -Runx2) develop rapid onset tumours that can be accelerated and rendered polyclonal by neonatal Moloney murine leukaemia virus (MoMLV) infection. RIM/DS analysis of 28 polyclonal lymphomas identified 771 common insertion sites (CISs) defining a ‘progression network’ that encompassed a remarkably large fraction of known MoMLV target genes, with further strong indications of oncogenic selection above the background of MoMLV integration preference. Progression driven by RIM was characterised as a Darwinian process of clonal competition engaging proliferation control networks downstream of cytokine and T-cell receptor signalling. Enhancer mode activation accounted for the most efficiently selected CIS target genes, including Ccr7 as the most prominent of a set of chemokine receptors driving paracrine growth stimulation and lymphoma dissemination. Another large target gene subset including candidate tumour suppressors was disrupted by intragenic insertions. A second RIM/DS screen comparing lymphomas of wild-type and parental transgenics showed that CD2-MYC tumours are virtually dependent on activation of Runx family genes in strong preference to other potent Myc collaborating genes (Gfi1, Notch1). Ikzf1 was identified as a novel collaborating gene for Runx2 and illustrated the interface between integration preference and oncogenic selection. Lymphoma target genes for MoMLV can be classified into (a) a small set of master regulators that confer self-renewal; overcoming p53 and other failsafe pathways and (b) a large group of progression genes that control autonomous proliferation in transformed cells. These findings provide insights into retroviral biology, human cancer genetics and the safety of vector-mediated gene therapy., Author Summary Cancers are known to arise by a series of mutational and non-mutational (epigenetic) events but the advent of cancer genome sequencing highlights the growing challenge of separating important (driver) from irrelevant (passenger) mutations. Retroviruses that induce cancer by inserting into host DNA and thereby altering key genes are valuable tools because they act as ‘tags’ to identify the critical targets. In this study we combined retroviral tagging with next generation sequencing to achieve a comprehensive description of lymphoma development and progression in transgenic mouse model systems. Our study suggests that three events may be sufficient for lymphoma development and identifies a genetic bottleneck at a small gene set that regulates tumour cell self-renewal, including the Myc oncogene and the p53 tumour suppressor. In contrast, many genes can provide the final step where the lymphoma cell acquires the ability to divide independently of external stimuli. As many of the target genes are conserved and play roles in cancers of non-viral origin, this study may provide a paradigm for the gene interactions that underlie cancer biology. It also elucidates the risks entailed in the recent use of retrovirus-based vectors for human gene therapy.

Published

2014

32. Runx2: A novel oncogenic effector revealed by in vivo complementation and retroviral tagging

Author

Anne Terry, Margaret Bell, Ewan R. Cameron, Monica Stewart, Karen Blyth, François Vaillant, Nancy Mackay, and James C. Neil

Subjects

CD4-Positive T-Lymphocytes, Genetically modified mouse, Cancer Research, Saccharomyces cerevisiae Proteins, CD3 Complex, Transgene, CD3, CD2 Antigens, PIM1, Core Binding Factor Alpha 1 Subunit, Mice, Transgenic, CD8-Positive T-Lymphocytes, Protein Serine-Threonine Kinases, Biology, Gene Rearrangement, T-Lymphocyte, Lymphoma, T-Cell, Fungal Proteins, Proto-Oncogene Proteins c-myc, Mice, Proto-Oncogene Proteins c-pim-1, Proto-Oncogene Proteins, Genetics, medicine, Animals, Caenorhabditis elegans Proteins, Molecular Biology, Crosses, Genetic, Homeodomain Proteins, Oncogene, Genetic Complementation Test, Helminth Proteins, Thymus Neoplasms, medicine.disease, Phenotype, Neoplasm Proteins, Lymphoma, DNA-Binding Proteins, Complementation, Retroviridae, Trans-Activators, Cancer research, biology.protein, ATP-Binding Cassette Transporters, Moloney murine leukemia virus, Tumor Suppressor Protein p53, Transcription Factors

Abstract

The Runx2 (Cbfa1, Pebp2alphaA, Aml3) gene was previously identified as a frequent target for transcriptional activation by proviral insertion in T-cell lymphomas of CD2-MYC transgenic mice. We have recently shown that over-expression of the full-length, most highly expressed Runx2 isoform in the thymus perturbs T-cell development, leads to development of spontaneous lymphomas at low frequency and is strongly synergistic with Myc. To gain further insight into the relationship of Runx2 to other lymphomagenic pathways, we tested the effect of combining the CD2-Runx2 transgene either with a Pim1 transgene (E(mu)-Pim1) or with the p53 null genotype, as each of these displays independent synergy with Myc. In both cases we observed synergistic tumour development. However, Runx2 appeared to have a dominant effect on the tumour phenotype in each case, with most tumours conforming to the CD3(+), CD8(+), CD4(+/-) phenotype seen in CD2-Runx2 mice. Neonatal infection of CD2-Runx2 mice with Moloney murine leukaemia virus (Moloney MLV) also led to a dramatic acceleration of tumour onset. Analysis of known Moloney MLV target genes in these lymphomas showed a high frequency of rearrangement at c-Myc or N-Myc (82%), and a significant number at Pim1 or Pim2 (23%), and at Pal1/Gfi1 (18%). These results indicate that Runx2 makes a distinct contribution to T-cell lymphoma development which does not coincide with any of the oncogene complementation groups previously identified by retroviral tagging.

Published

2001

33. Factors influencing cellular immune responses to feline immunodeficiency virus induced by DNA vaccination

Author

Margaret J Hosie, C.A. Cannon, J N Flynn, M A Rigby, Nancy Mackay, James C. Neil, Oswald Jarrett, and Thomas H. Dunsford

Subjects

Cellular immunity, Feline immunodeficiency virus, viruses, Cytomegalovirus, Gene Products, gag, Immunodeficiency Virus, Feline, Biology, Injections, Intramuscular, Virus, DNA vaccination, law.invention, Interferon-gamma, law, Vaccines, DNA, Animals, Promoter Regions, Genetic, CATS, General Veterinary, General Immunology and Microbiology, Terminal Repeat Sequences, Public Health, Environmental and Occupational Health, Gene Products, env, Viral Vaccines, Provirus, biology.organism_classification, Virology, Infectious Diseases, Lentivirus, Immunology, Cats, Recombinant DNA, Molecular Medicine, T-Lymphocytes, Cytotoxic

Abstract

Virus-specific effector cytotoxic T lymphocytes (CTL) were elicited in the peripheral blood of domestic cats following a single intramuscular inoculation of replication defective feline immunodeficiency virus proviral DNA (FIVDeltaRT). Higher levels of virus-specific cytolysis were observed in the blood when cats were co-inoculated with feline gamma-interferon (IFN) DNA. The responses declined by 12 weeks following the first DNA inoculation and were, with the exception of FIV Gag-specific responses in some cats, refractory to repeated DNA inoculations. Nevertheless, a significant proportion of the cats were protected from challenge with homologous virus. The effects of interval between inoculations, route of DNA delivery, and promoter used to regulate viral gene expression on the induction of virus-specific CTLs were evaluated. The highest levels of virus-specific lysis were recorded following intramuscular co-inoculation of FIVDeltaRT and gamma-IFN DNA, where FIV gene expression was under the control of a cytomegalovirus (CMV) promoter. However, the highest levels of protection were observed using the viral 5'LTR as the promoter. These results suggest that a single intramuscular inoculation of FIVDeltaRT DNA together with gamma-IFN DNA may be sufficient to induce virus-specific CTLs and protection.

Published

2000

34. Transcriptional autoregulation of the bone related CBFA1/RUNX2 gene

Author

Je-Yong Choi, Ming Hu, Gary S. Stein, Hicham Drissi, James C. Neil, Stephen N. Jones, Susana M. Chuva de Sousa Lopes, Andre J. Van Wijnen, Quyen Luc, Janet L. Stein, Anne Terry, A. Rauf Shakoori, and Jane B. Lian

Subjects

Gene isoform, SOX4, Epigenetics of physical exercise, Physiology, RUNX2 Gene, Clinical Biochemistry, Response element, Promoter, Cell Biology, PAX6, Biology, Molecular biology, Transcription factor

Abstract

The runt related transcription factor CBFA1 (AML3/PEBP2αA/RUNX2) regulates expression of several bone- and cartilage-related genes and is required for bone formation in vivo. The gene regulatory mechanisms that control activation and repression of CBFA1 gene transcription during osteoblast differentiation and skeletal development are essential for proper execution of the osteogenic program. We have therefore defined functional contributions of 5′ regulatory sequences conserved in rat, mouse and human CBFA1 genes to transcription. Deletion analysis reveals that 0.6 kB of the bone-related rat or mouse CBFA1 promoter (P1, MASNS protein isoform) is sufficient to confer transcriptional activation, and that there are multiple promoter domains which positively and negatively regulate transcription. Progressive deletion of promoter segments between nt −351 and −92 causes a striking 30- to 100-fold combined decrease in promoter activity. Additionally, 5′ UTR sequences repress reporter gene transcription 2- to 3-fold. Our data demonstrate that CBFA1 is a principal DNA binding protein interacting with the 5′ region of the CBFA1 gene in osseous cells, that there are at least three CBFA1 recognition motifs in the rat CBFA1 promoter, and that there are three tandemly repeated CBFA1 sites within the 5′ UTR. We find that forced expression of CBFA1 protein downregulates CBFA1 promoter activity and that a single CBFA1 site is sufficient for transcriptional autosuppression. Thus, our data indicate that the CBFA1 gene is autoregulated in part by negative feedback on its own promoter to stringently control CBFA1 gene expression and function during bone formation. J. Cell. Physiol. 184:341–350, 2000. © 2000 Wiley-Liss, Inc.

Published

2000

35. A full-length Cbfa1 gene product perturbs T-cell development and promotes lymphomagenesis in synergy with MYC

Author

François Vaillant, Anne Terry, James C. Neil, Karen Blyth, Margaret Bell, Monica Stewart, and Ewan R. Cameron

Subjects

Gene isoform, Cancer Research, Lymphoma, T-Lymphocytes, Transgene, T cell, Apoptosis, Core Binding Factor Alpha 1 Subunit, Mice, Transgenic, Biology, medicine.disease_cause, Proto-Oncogene Proteins c-myc, Gene product, Mice, Gene expression, Genetics, medicine, Animals, Transgenes, Molecular Biology, Oncogene, Core Binding Factors, Molecular biology, Neoplasm Proteins, Phenotype, medicine.anatomical_structure, Cancer research, Carcinogenesis, Cell Division, CD8, Transcription Factors

Abstract

The Cbfa1/PEBP2 alpha A/AML3 gene plays an essential role in osteogenesis but is also expressed in the T-cell lineage where it has been implicated in lymphoma development as a target for retroviral insertional mutagenesis. As lymphoma cells with til-1 insertion express at least five distinct Cbfa1 isoforms, it is important to establish which, if any, have intrinsic oncogenic potential. We have generated transgenic mice in which the most abundant lymphoma isoform (G1/p57) is expressed under the control of the CD2 locus control region. Co-precipitation analysis of transgenic thymus revealed high levels of Cbfa1 protein in an abundant complex containing the binding cofactor Cbfb. CD2-Cbfa1-G1 mice displayed abnormal T-cell development, with a pronounced skew towards CD8 SP cells in the thymus and developed a low incidence of spontaneous lymphomas (6% at 12 months) with cells of similar phenotype. Strongly synergistic tumour development was seen when CD2-Cbfa1-G1 mice were crossed with lines carrying myc transgenes (CD2-myc or tamoxifen-regulatable CD2-mycER) and Cbfa1 was found to rescue expression of the CD2-myc transgene in pre-leukaemic mice. However, synergy did not appear to be due to a dominant block of myc-induced apoptosis by Cbfa1 as explanted primary tumours and cell lines from CD2-Cbfa1-G1/CD2-mycER mice showed accelerated death on induction with tamoxifen at similar rates to CD2-mycER controls. Moreover, thymocytes from preleukaemic CD2-Cbfa1-G1 mice showed reduced survival in vitro and increased sensitivity to the inhibitory effects of TGF-beta. This study demonstrates that a full-length Cbf alpha-chain gene can act as an oncogene without fusion to a heterologous protein.

Published

1999

36. Positive and negative regulation of chondrogenesis by splice variants of PEBP2?A/CBF?1 in clonal mouse EC cells, ATDC5

Author

Anne Terry, James C. Neil, Hiromu Ito, Yoshiaki Ito, Takashi Nakamura, Tomohiko Kanno, and Haruhiko Akiyama

Subjects

Gene isoform, Physiology, Enhancer binding, Clinical Biochemistry, Alternative splicing, Regulator, Endogeny, Cell Biology, Biology, Chondrogenesis, Core binding factor, Molecular biology, G alpha subunit

Abstract

The alphaA type of the alpha subunit of the polyomavirus enhancer binding protein 2 (PEBP2alphaA), also called the core binding factor alpha1 (CBFalpha1) or til-1, plays crucial roles in osteogenesis. Little is known, however, about the function of PEBP2alphaA in chondrogenesis. Here, we examined the role of PEBP2alphaA in chondrogenesis of clonal mouse embryonal carcinoma cells, ATDC5, which are committed as chondroprogenitors. We found that as ATDC5 cells condensed and formed cartilaginous nodules, PEBP2alphaA increased, and the level was maintained throughout the process of chondrocytic maturation. When an established dominant negative form of PEBP2alphaA was introduced in undifferentiated ATDC5 cells, the cellular condensation and the subsequent processes were inhibited. This inhibition was overcome with BMP-4 treatment, which increased the endogenous expression of PEBP2alphaA. Thus, the process of chondrogenesis is regulated by the level of PEBP2alphaA activity. Along with the wild-type PEBP2alphaA, a splice variant form, til-1 G2, is naturally expressed in ATDC5 cells. In luciferase reporter assays, til-1 G2 not only exhibited a limited ability to transactivate the osteocalcin promoter but also inhibited the activity achieved by the wild-type PEBP2alphaA. When til-1 G2 was overexpressed by stable transfection in undifferentiated ATDC5 cells, it inhibited the progression of chondrogenesis. Therefore, we conclude that PEBP2alphaA acts as a positive regulator of chondrogenesis, and that this positive effect may be finely tuned by the opposing effect of the til-1 G2 isoform.

Published

1999

37. Feline immunodeficiency virus (FIV)-associated lymphoma: a potential role for immune dysfunction in tumourigenesis

Author

John J. Callanan, Catherine E. Lawrence, E.A Gault, Julia A. Beatty, James C. Neil, C.K Grant, and O Jarrett

Subjects

Male, Feline immunodeficiency virus, Lymphoma, B-Cell, Lymphocyte, Immunology, Enzyme-Linked Immunosorbent Assay, Immunodeficiency Virus, Feline, Biology, Antibodies, Viral, Lymphocyte Activation, Virus, T-Lymphocyte Subsets, Immunity, Feline Acquired Immunodeficiency Syndrome, medicine, Animals, Southern blot, Immunity, Cellular, CATS, General Veterinary, DNA, Neoplasm, biochemical phenomena, metabolism, and nutrition, biology.organism_classification, medicine.disease, Virology, Specific Pathogen-Free Organisms, Lymphoma, medicine.anatomical_structure, Cats, Female, CD8, Interleukin-1

Abstract

To determine the potential role of immune dysfunction in feline immunodeficiency virus (FIV)-associated lymphomagenesis, we present the results of immunological monitoring during the chronic phase of experimental FIV infection in two cats which subsequently developed lymphoma. In one cat, C1, cell-mediated immunity was depressed throughout the monitoring period but particularly from 125-200 weeks post-infection (pi), when this cat demonstrated profoundly impaired lymphocyte blastogenesis and markedly increased interleukin-1 (IL-1) production compared to age-matched, uninfected control cats. Lymphocyte function in the other cat, C2, was preserved to a greater degree. Alterations in the levels of immunoglobulin isotypes M, A and G in CD4+-, CD8+- and CD21+-lymphocyte sub-sets were demonstrated in both cats. Southern blot analysis revealed the presence of integrated FIV-provirus in tumour DNA from C2 but not C1 indicating a possible direct role for the virus in the former case only. In this study we have characterised, for the first time, the FIV-induced immune dysfunction in cats which developed lymphoma, demonstrating potential indirect mechanisms of tumourigenesis.

Published

1998

38. Workshop Summary: Lessons from the Cat: Feline Immunodeficiency Virus as a Tool to Develop Intervention Strategies against Human Immunodeficiency Virus Type 1

Author

James C. Neil, Naoya Yuhki, Michael H. Malim, John H. Elder, Wayne A.F. Tompkins, Janet Yamamoto, James A. Hoxie, Edward A. Hoover, Neils C. Pedersen, Roger H. Miller, Lawrence Mathes, Thomas W. North, Mary B. Tompkins, Ellen Sparger, and Gregg A. Dean

Subjects

Feline immunodeficiency virus, biology, business.industry, Immunology, Human immunodeficiency virus (HIV), biology.organism_classification, medicine.disease_cause, Virology, Infectious Diseases, Intervention (counseling), Medicine, business, Oncovirus

Published

1998

39. Modulation of Feline Immunodeficiency Virus Infection by Stromal Cell-Derived Factor

Author

Nelleke Broere, Brian J. Willett, James A. Hoxie, James C. Neil, Margaret J Hosie, Joseph Hesselgesser, and Julie D. Turner

Subjects

Receptors, CXCR4, Chemokine, Feline immunodeficiency virus, Stromal cell, viruses, Immunology, Gene Expression, Immunodeficiency Virus, Feline, Antiviral Agents, Microbiology, CXCR4, Virus, Cell Line, Virology, Tumor Cells, Cultured, Animals, Humans, Receptor, Syncytium, biology, biology.organism_classification, Molecular biology, Chemokine CXCL12, Recombinant Proteins, Virus-Cell Interactions, Cell culture, Insect Science, Cats, biology.protein, Tetradecanoylphorbol Acetate, Chemokines, Stromal Cells, Chemokines, CXC

Abstract

The α-chemokine receptor CXCR4 has recently been shown to support syncytium formation mediated by strains of feline immunodeficiency virus (FIV) that have been selected for growth in the Crandell feline kidney cell line (CrFK-tropic virus). Given that both human and feline CXCR4 support syncytium formation mediated by FIV, we investigated whether human stromal cell-derived factor (SDF-1) would inhibit infection with FIV. Human SDF-1α and SDF-1β bound with a high affinity ( K D s of 12.0 and 10.4 nM, respectively) to human cells stably expressing feline CXCR4, and treatment of CrFK cells with human SDF-1α resulted in a dose-dependent inhibition of infection by FIV PET . No inhibitory activity was detected when the interleukin-2 (IL-2)-dependent feline T-cell line Mya-1 was used in place of CrFK cells, suggesting the existence of a CXCR4-independent mechanism of infection. Furthermore, neither the human β-chemokines RANTES, MIP-1α, MIP-1β, and MCP-1 nor the α-chemokine IL-8 had an effect on infection of either CrFK or Mya-1 cells with CrFK-tropic virus. Envelope glycoprotein purified from CrFK-tropic virus competed specifically for binding of SDF-1α to feline CXCR4 and CXCR4 expression was reduced in FIV-infected cells, suggesting that the inhibitory activity of SDF-1α in CrFK cells may be the result of steric hindrance of the virus-receptor interaction following the interaction between SDF and CXCR4. Prolonged incubation of CrFK cells with SDF-1α led to an enhancement rather than an inhibition of infection. Flow cytometric analysis revealed that this effect may be due largely to up-regulation of CXCR4 expression by SDF-1α on CrFK cells, an effect mimicked by treatment of the cells with phorbol myristate acetate. The data suggest that infection of feline cells with FIV can be mediated by CXCR4 and that, depending on the assay conditions, infection can be either inhibited or enhanced by SDF-1α. Infection with FIV may therefore prove a valuable model in which to study the development of novel therapeutic interventions for the treatment of AIDS.

Published

1998

40. Vaccination with a feline immunodeficiency virus multiepitopic peptide induces cell-mediated and humoral immune responses in cats, but does not confer protection

Author

J N Flynn, James C. Neil, Oswald Jarrett, and C.A. Cannon

Subjects

Feline immunodeficiency virus, Immunogen, viruses, Molecular Sequence Data, Immunology, Gene Products, gag, Immunodeficiency Virus, Feline, Antibodies, Viral, Major histocompatibility complex, Microbiology, Quillaja Saponins, Epitopes, Immune system, Adjuvants, Immunologic, Viral Envelope Proteins, Feline Acquired Immunodeficiency Syndrome, Virology, Animals, Cytotoxic T cell, Amino Acid Sequence, Antigens, Viral, chemistry.chemical_classification, Immunity, Cellular, Vaccines, Synthetic, CATS, biology, Gene Products, env, Viral Vaccines, Saponins, biology.organism_classification, Epitope mapping, chemistry, Insect Science, Antibody Formation, Cats, biology.protein, Glycoprotein, Research Article, T-Lymphocytes, Cytotoxic

Abstract

Cats were immunized with a 46-residue multiepitopic synthetic peptide of feline immunodeficiency virus (FIV) comprising immunodominant epitopes present in the third variable domain of the envelope glycoprotein, transmembrane glycoprotein (TM), and p24 Gag core protein, using Quil A as an adjuvant. All vaccinated cats developed a humoral response which recognized the synthetic peptide immunogen and the intact viral core and envelope proteins. A FIV Gag- and Env-specific effector cytotoxic T-lymphocyte response was also detected in the peripheral blood of vaccinated cats, which peaked at week 30. This response appeared to be major histocompatibility complex restricted. Epitope mapping studies revealed that both the cellular and humoral immune responses were directed principally to a peptide within the TM glycoprotein, CNQNQFFCK. However, vaccination did not confer protection when cats were challenged with the Petaluma isolate of FIV at week 35.

Published

1997

41. Comparative Efficiency of Feline Immunodeficiency Virus Infection by DNA Inoculation

Author

C.A. Cannon, James C. Neil, Margaret J Hosie, Michael McDonald, Brian J. Willett, M A Rigby, Nancy Mackay, Oswald Jarrett, and Thomas H. Dunsford

Subjects

Feline immunodeficiency virus, viruses, Molecular Sequence Data, Immunology, Gene Products, gag, Immunodeficiency Virus, Feline, Biology, Antibodies, Viral, Recombinant virus, Virus, Plasmid, Proviruses, Virology, Vaccines, DNA, Animals, Seroconversion, Viral Vaccine, Viral Vaccines, Viral Load, biology.organism_classification, Vaccination, Infectious Diseases, DNA, Viral, Cats, Lentivirus Infections, Leukocytes, Mononuclear, Lymph Nodes, Viral load

Abstract

Direct inoculation of genetic material in DNA form is a novel approach to vaccination that has proved efficacious for a number of viral agents. We are interested in the potential of this approach for the delivery of vaccines based on attenuated or replication-defective retroviruses. Toward this goal, we tested the effect of intramuscular inoculation of a plasmid containing the entire genome of feline immunodeficiency virus (FIV-Petaluma, F14 clone). DNA delivery was compared with intramuscular or intraperitoneal inoculation of virus reconstituted from the same molecular clone. The outcome was monitored by serological analysis and quantitative virus load determination over a 31-week period. DNA inoculation was found to be a reliable means of infection, although seroconversion and the rise in PBMC virus load were delayed relative to intramuscular or intraperitoneal inoculation of virus. At 31 weeks, similar levels of proviral DNA were detected in central lymphoid tissue of all infected animals. In conclusion, DNA inoculation of proviral DNA will be of use as a novel method of cell-free virus challenge and may have further potential for the delivery of lentiviral vaccines.

Published

1997

42. til-1: a novel proviral insertion locus for Moloney murine leukaemia virus in lymphomas of CD2-myc transgenic mice

Author

Monica Stewart, James C. Neil, Anne Terry, Ewan R. Cameron, M. O’Hara, and David Onions

Subjects

Genetically modified mouse, Virus Integration, Transgene, T cell, CD2 Antigens, Genes, myc, Mice, Transgenic, Locus (genetics), Biology, Lymphoma, T-Cell, Mice, Proviruses, hemic and lymphatic diseases, Virology, medicine, Animals, Humans, Cloning, Molecular, Gene, Locus control region, Thymic Lymphoma, Genetics, Chromosome Mapping, Molecular biology, Mice, Inbred C57BL, Chromosome 17 (human), medicine.anatomical_structure, Moloney murine leukemia virus

Abstract

Moloney murine leukaemia virus (MoMLV) markedly accelerates thymic lymphoma development in mice carrying a transgene in which the human c-myc gene is linked to the CD2 locus control region. To investigate the mechanism of synergy and identify the genes which collaborate with myc in these clonal tumours, we analysed the sites of MoMLV insertion. Analysis of known viral integration loci revealed only a small number of insertions at bmi-1, pim-1 and ahi-1. Further cloning and hybridization analysis revealed a new common integration locus, designated til-1, which was occupied in 25 out of 77 lymphomas examined, with evidence of multiple clonal insertions in some cases. Mapping relative to established chromosomal markers in interspecific backcross mice located til-1 to mouse chromosome 17, distal to pim-1 and tic-1. These results suggest that the til-1 locus may harbour a novel myc-collaborating gene which acts as a target for activation in T cell lymphomas.

Published

1996

43. Apparent bypass of negative selection in CD8+ tumours in CD2-myc transgenic mice

Author

James C. Neil, Campbell M, L Keanie, David Onions, Ewan R. Cameron, Sally A. Argyle, and Karen Blyth

Subjects

CD4-Positive T-Lymphocytes, Genetically modified mouse, Cancer Research, Receptors, Antigen, T-Cell, alpha-beta, CD2 Antigens, CD4-CD8 Ratio, Genes, myc, Mice, Transgenic, CD8-Positive T-Lymphocytes, Biology, Lymphoma, T-Cell, medicine.disease_cause, Clonal deletion, Mice, Antigen, medicine, Animals, Superantigens, T-cell receptor, T lymphocyte, medicine.disease, Lymphoma, Mice, Inbred C57BL, Cell Transformation, Neoplastic, Phenotype, Oncology, Immunology, Mice, Inbred CBA, Cancer research, Carcinogenesis, CD8, Research Article

Abstract

A role for antigen stimulation in lymphoid neoplasia has been postulated and is supported by indirect evidence that suggests that the interaction of antigen with both T cells and B cells may constitute an epigenetic event that can contribute to tumour induction or tumour progression. Using myc-bearing transgenic mice that develop mainly clonal T-cell lymphomas we have investigated the possibility that endogenous antigen-mediated clonal deletion might be overridden in tumorigenesis. CD2-myc transgenic mice were backcrossed on to a CBA/Ca background to ensure Mtv-mediated deletion of V beta 11-expressing T cells in the resultant offspring. Lymphomas arising from these mice were subsequently screened for V beta 11 expression. There was a clear correlation between the age at which mice developed neoplasia and the tumour phenotype. Mice with CD4- CD8+ tumours succumbed to thymic lymphoma at a significantly younger age than mice developing CD4+ CD8+ tumours. A small number of tumours consisted of the 'forbidden' V beta 11 phenotype, showing that cells vulnerable to transformation could escape negative selection. The majority of the V beta 11-positive tumours were CD4- CD8+ and were only observed in mice showing clinical evidence of tumour development at a relatively young age. The phenotype of these cells and the age at which tumours arose suggests that T cells escaping tolerance may be susceptible to transformation. Images Figure 2

Published

1996

44. Molecular analysis of tumours from feline immunodeficiency virus (FIV)-infected cats: An indirect role for FIV?

Author

John J. Callanan, Anne Terry, James C. Neil, R. Fulton, and Oswald Jarrett

Subjects

Cancer Research, Feline immunodeficiency virus, Genotype, Lymphoma, Virus Integration, animal diseases, viruses, Molecular Sequence Data, Genes, myc, Mast-Cell Sarcoma, Genome, Viral, Immunodeficiency Virus, Feline, Biology, Virus, medicine, Animals, Amino Acid Sequence, Gene Rearrangement, CATS, Base Sequence, Genes, Immunoglobulin, Sequence Homology, Amino Acid, Leukemia Virus, Feline, Lymphoma, Non-Hodgkin, T-cell receptor, virus diseases, Mastocytoma, Gene rearrangement, biochemical phenomena, metabolism, and nutrition, medicine.disease, biology.organism_classification, Virology, Tumor Virus Infections, Phenotype, Oncology, Cats, Lentivirus Infections, biology.protein, Antibody, Retroviridae Infections

Abstract

Five tumours, which arose in cats naturally or experimentally infected with feline immunodeficiency virus (FIV), were examined with molecular probes to establish tumour cell lineage and to screen for integrated viral sequences. Three of the tumours were classed as B-cell lymphomas on the basis of morphology, immunocytochemistry, rearrangement of immunoglobulin heavy chain genes and lack of rearrangement of T-cell receptor (TCR) beta-chain genes. Two of these B-cell tumours arose in specific pathogen-free (SPF) cats experimentally infected with FIV. One case of multi-centric lymphosarcoma came from a cat naturally infected with both FIV and feline leukaemia virus (FeLV). This tumour contained integrated FeLV proviral sequences and was judged to be of T-cell origin on the basis of TCR gene rearrangement. The fifth case was a mast cell tumour. Rearrangement of the c-myc locus was not found in any of the FIV-associated tumours but was shown to be present in a rare immunoblastic B-cell lymphoma which arose in an uninfected SPF cat. None of the FIV-associated tumours showed evidence of integrated FIV sequences by Southern blot hybridisation, despite isolation of infectious virus from in vitro cultures of tumour cells in I case. These results confirm that FIV-associated tumours can occur in the absence of FeLV and suggest that the role of FIV in lymphomagenesis is generally indirect.

Published

1995

45. cDNA cloning and eukaryotic expression of feline CD9

Author

James C. Neil and Brian J. Willett

Subjects

Feline immunodeficiency virus, DNA, Complementary, medicine.drug_class, Molecular Sequence Data, Immunology, Monoclonal antibody, Tetraspanin 29, Epitope, Mice, Rapid amplification of cDNA ends, Antigens, CD, Complementary DNA, medicine, Animals, Humans, Amino Acid Sequence, Cloning, Molecular, Molecular Biology, Peptide sequence, DNA Primers, Membrane Glycoproteins, Base Sequence, Sequence Homology, Amino Acid, biology, Flow Cytometry, biology.organism_classification, Molecular biology, embryonic structures, Cats, biology.protein, Antibody, Sequence Alignment, Conformational epitope

Abstract

A monoclonal antibody (vpg15) has been described which can block infection with feline immunodeficiency virus (FIV) and which recognizes the feline homologue of CD9. In order to study the role of feline CD9 in infection with FIV we have molecularly cloned a cDNA encoding feline CD9 by R.A.C.E (rapid amplification of cDNA ends). The amino acid sequence of feline CD9 displays 95.1, 93.8 and 90.7% homology to human, murine and bovine CD9, respectively. Although feline CD9 appears most homologous to human CD9, it has two important features in common with bovine and murine CD9: the presence of a histidine residue at position 192 which is absent from the corresponding position (194) in human CD9; and the absence of two asparagine residues which are found at positions 51 and 52 of human CD9. Feline CD9 is unique in that it lacks a potential N-linked glycosylation site in the first extracellular loop, a feature common to CD9 of other species. Despite the high degree of sequence homology, significant cross-species variation occurred in the two predicted extracellular loops, notably between amino acids 169 to 180 of the second loop. When feline CD9 was expressed on human and murine cells, it was recognized by both the conformation-dependent feline CD9-specific antibody, vpg15, and the cross-species reactive anti-human CD9 antibody, FMC56, confirming that the feline CD9 clone encoded a protein which was synthesized, transported to the cell surface and expressed in a similar conformation to native feline CD9. However, although the vpg15 antibody did not recognize human CD9 when expressed on human epithelial cells, it reacted with human CD9 when expressed on murine fibroblast cells. It is possible therefore, that the conformational epitope recognized by the vpg15 epitope is sensitive to either species- or tissue-specific post-translational modification.

Published

1995

46. Mutations in the candidate tumour suppressor gene FLJ12973 on chromosome 15q15 are rare in colorectal cancer

Author

Christina M. Fleischmann, Stephen Bevan, James C. Neil, Anne Terry, and Richard S. Houlston

Subjects

Genetics, Chromosomes, Human, Pair 15, Cancer Research, Xeroderma pigmentosum, Deleted in Colorectal Cancer, Colorectal cancer, Colorectal adenoma, Biology, medicine.disease, Oncology, Mutation, medicine, Carcinoma, Humans, Missense mutation, Genes, Tumor Suppressor, Epigenetics, Colorectal Neoplasms, Gene

Abstract

Allele imbalance at chromosome 15q14-q22 is seen in a high proportion of sporadic colorectal cancers encompassing the colorectal adenoma and carcinoma susceptibility locus. The FLJ12973 gene, which has recently been identified as a candidate tumour suppressor, maps to 15q15 and encodes a WD-repeat protein with structural similarity to the small subunit of the xeroderma pigmentosum E (XP-E) complex. To examine the proposition that FLJ12973 is involved in colorectal cancer we analysed 31 tumours for sequence variation. No missense changes or pathogenic mutations – truncating or splice site – were detected in any of the tumours. While epigenetic effects on FLJ12973 cannot be excluded, these results show that it is not a common target for mutations in colorectal cancers.

Published

2003

47. Feline Leukaemia Virus

Author

Oswald Jarrett and James C. Neil

Subjects

biology, animal diseases, viruses, Infectious dose, virus diseases, Endogenous retrovirus, biology.organism_classification, medicine.disease, Virology, Virus, Retrovirus, hemic and lymphatic diseases, Gene duplication, medicine, Immunocompetence, Immunodeficiency, Gammaretrovirus

Abstract

Feline leukaemia virus (FeLV) is a gammaretrovirus that causes a variety of fatal diseases including leukaemia and lymphoma in its host, the domestic cat, and occasionally in large cat species. Many cats become persistently infected and develop disease after an incubation period of several years, during which virus can be transmitted to other cats. Disease is often associated with the generation of FeLV variants with increased pathogenic potential that can arise by mutation of envelope sequences, duplication of transcriptional enhancer elements or recombination with host proto-oncogene sequences. FeLV can also produce variants by recombination with endogenous proviruses related to FeLV that are found in the domestic cat and its close relatives. The prevalence of FeLV infection has been reduced in many cat populations by isolation of infected carriers and more recently by vaccines that augment the natural ability of most cats to control infection. Key Concepts: The outcome of infection by FeLV depends on the infectious dose, age and immunocompetence of the host. Many cats achieve lifelong control, if not elimination of infection. Cats that become persistently viraemic are at risk of a variety of FeLV-related diseases after a latent period of up to several years. The common infectious form, FeLV-A can acquire altered entry receptor specificity by envelope gene mutation (to FeLV-C) or recombination with endogenous FeLV-related proviruses (to FeLV-B). FeLV envelope variants may induce fatal diseases of rapid onset including nonregenerative anaemia (FeLV-C) or wasting and immunodeficiency (FeLV-T). The oncogenic potential of FeLV can evolve by duplication of transcriptional enhancer control elements in the long-terminal repeat or by transduction of host proto-oncogene sequences. Although the immune parameters of vaccine protection remain unclear, FeLV demonstrates the feasibility of effective immunisation against the gamma retroviruses. Commercial FeLV vaccines in recent or current use include inactivated FeLV, infected cell extracts, recombinant envelope protein and live recombinant poxvirus vaccines. Keywords: retrovirus; FeLV; oncogene; transduction; endogenous retrovirus; receptor; transporter; leukaemia; lymphoma; immunodeficiency

Published

2012

48. Genetic determinants of feline leukemia virus-induced lymphoid tumors: patterns of proviral insertion and gene rearrangement

Author

Christos Tsatsanis, James C. Neil, Hajime Tsujimoto, Anne Terry, D. Spandidos, R. Fulton, L. Levy, K. Nishigaki, and David Onions

Subjects

Transcription, Genetic, T-Lymphocytes, viruses, Molecular Sequence Data, Restriction Mapping, Immunology, Genes, myc, Locus (genetics), Genome, Viral, Protein Serine-Threonine Kinases, Biology, Gene Rearrangement, T-Lymphocyte, Lymphoma, T-Cell, Microbiology, Feline leukemia virus, Cell Line, law.invention, Exon, Proto-Oncogene Proteins c-pim-1, Proviruses, law, Proto-Oncogene Proteins, hemic and lymphatic diseases, Virology, Proto-Oncogenes, Tumor Cells, Cultured, medicine, Animals, Gene, DNA Primers, Gene Rearrangement, Base Sequence, Leukemia Virus, Feline, T-cell receptor, Exons, Gene rearrangement, Protein-Tyrosine Kinases, medicine.disease, biology.organism_classification, Molecular biology, Lymphoma, Tumor Virus Infections, Insect Science, Cats, DNA Transposable Elements, Recombinant DNA, Retroviridae Infections, Research Article

Abstract

The genetic basis of feline leukemia virus (FeLV)-induced lymphoma was investigated in a series of 63 lymphoid tumors and tumor cell lines of presumptive T-cell origin. These were examined for virus-induced rearrangements of the c-myc, flvi-2 (bmi-1), fit-1, and pim-1 loci, for T-cell receptor (TCR) gene rearrangements, and for the presence of env recombinant FeLV (FeLV-B). The myc locus was most frequently affected in naturally occurring lymphomas (32%; n = 38) either by transduction (21%) or by proviral insertion (11%). Proviral insertions were also common at flvi-2 (24%). The two other loci were occupied in a smaller number of the naturally occurring tumors (fit-1, 8%; pim-1, 5%). Examination of the entire set of tumors showed that significant numbers were affected at two (19%) or three (5%) of the loci. Occupation of the fit-1 locus was observed most frequently in tumors induced by FeLV-myc strains, while flvi-2 insertions occurred with similar frequency in the presence or absence of obvious c-myc activation. These results suggest a hierarchy of mutational events in the genesis of feline T-cell lymphomas by FeLV and implicate insertion at fit-1 as a late progression step. The strongest links observed were with T-cell development, as monitored by rearrangement status of the TCR beta-chain gene, which was positively associated with activation of myc (P < 0.001), and with proviral insertion at flvi-2 (P = 0.02). This analysis also revealed a genetically distinct subset of thymic lymphomas with unrearranged TCR beta-chain genes in which the known target loci were involved very infrequently. The presence of env recombinant FeLV (FeLV-B) showed a negative correlation with proviral insertion at fit-1, possibly due to the rapid onset of these tumors. These results shed further light on the multistep process of FeLV leukemogenesis and the relationships between lymphoid cell maturation and susceptibility to FeLV transformation.

Published

1994

49. The generation of monoclonal antibodies recognising novel epitopes by immunisation with solid matrix antigen-antibody complexes reveals a polymorphic determinant on feline CD4

Author

Brian J. Willett, Richard E. Randall, Oswald Jarrett, David Klatzmann, Margaret J Hosie, Mara Rocchi, Amyeric de Parseval, James C. Neil, and E. Peri

Subjects

Staphylococcus aureus, Feline immunodeficiency virus, CD4 antigen, medicine.drug_class, Immunology, Antigen-Antibody Complex, Biosensing Techniques, Monoclonal antibody, Epitope, Cell Line, Epitopes, chemistry.chemical_compound, Antigen, medicine, Animals, Immunology and Allergy, biology, Antibodies, Monoclonal, Flow Cytometry, biology.organism_classification, Precipitin, Precipitin Tests, Virology, Molecular biology, Epitope mapping, chemistry, CD4 Antigens, Cats, biology.protein, Immunization, Antibody, Epitope Mapping

Abstract

Monoclonal antibodies were generated against the feline homologue of CD4 (fCD4) by immunisation of mice with solid matrix antigen-antibody complexes of monoclonal antibody Fel7 (anti-fCD4) and formalin-fixed Staphylococcus A (SMAA-fCD4). The resulting fusion produced nine monoclonal antibodies each of which recognised a major population of feline lymphocytes and which immunoprecipitated a 55 kDa ligand from the feline T lymphosarcoma cell line 3201. Epitope mapping of the antibodies against soluble fCD4 by surface plasmon resonance indicated that the antibodies recognised five separate epitopes distinct from that defined by the Fel7 antibody used to prepare the SMAA-fCD4. These data demonstrate that SMAA complexes are an efficient means of generating monoclonal antibodies recognising novel epitopes on an antigen. One monoclonal antibody (vpg39) recognised an epitope that was expressed variably between cats, being either present or completely absent. Analysis of peripheral blood lymphocytes from specific pathogen free cats suggested that failure to react with the vpg39 antibody was an inherited trait.

Published

1994

50. Induction of feline immunodeficiency virus-specific cytotoxic T cells in vivo with carrier-free synthetic peptide

Author

C Jarrett, Julia A. Beatty, J N Flynn, M Mackett, C.A. Cannon, M A Rigby, and James C. Neil

Subjects

Cellular immunity, Feline immunodeficiency virus, Immunogen, CD8 Antigens, animal diseases, viruses, Molecular Sequence Data, Immunology, Gene Products, gag, Immunodeficiency Virus, Feline, Antibodies, Viral, Lymphocyte Activation, Microbiology, Epitope, Immune system, T-Lymphocyte Subsets, Virology, Animals, Cytotoxic T cell, Amino Acid Sequence, QR355, Vaccines, Synthetic, biology, virus diseases, biochemical phenomena, metabolism, and nutrition, biology.organism_classification, Molecular biology, Insect Science, Lentivirus, Cats, biology.protein, SF600, Antibody, Peptides, T-Lymphocytes, Cytotoxic, Research Article

Abstract

The role of cellular immunity in the establishment and progression of immunosuppressive lentivirus infection remains equivocal. To develop a model system with which these aspects of the host immune response can be studied experimentally, we examined the response of cats to a hybrid peptide containing predicted T-and B-cell epitopes from the gag and env genes of feline immunodeficiency virus (FIV). Cats were immunized with an unmodified 17-residue peptide incorporating residues 196 to 208 (from gag capsid protein p24) and 395 to 398 (from env glycoprotein gp120) of the FIV Glasgow-8 strain by using Quil A as an adjuvant. Virus-specific lymphocytotoxicity was measured by chromium-51 release assays. The target cells were autologous or allogeneic skin fibroblasts either infected with recombinant FIV gag vaccinia virus or pulsed with FIV peptides. Effector cells were either fresh peripheral blood mononuclear cells or T-cell lines stimulated with FIV peptides in vitro. Cytotoxic effector cells from immunized cats lysed autologous, but not allogeneic, target cells when they were either infected with recombinant FIV gag vaccinia virus or pulsed with synthetic peptides comprising residues 196 to 205 or 200 to 208 plus 395. Depletion of CD8+ T cells, from the effector cell population abrogated the lymphocytotoxicity. Immunized cats developed an antibody response to the 17-residue peptide immunogen and to recombinant p24. However, no antibodies which recognized smaller constituent peptides could be detected. This response correlated with peptide-induced T-cell proliferation in vitro. This study demonstrates that cytotoxic T lymphocytes specific for FIV can be induced following immunization with an unmodified short synthetic peptide and defines a system in which the protective or pathological role of such responses can be examined.

Published

1994