Your search keyword '"Taylor, Graham P"' showing total 11 results

1. Glucose Metabolism and Oxygen Availability Govern Reactivation of the Latent Human Retrovirus HTLV-1.

Author

Kulkarni, Anurag, Mateus, Manuel, Thinnes, Cyrille, McCullagh, James S., Schofield, Christopher J., Taylor, Graham P., Bangham, Charles R. M., Kulkarni, Anurag, Mateus, Manuel, Thinnes, Cyrille, McCullagh, James S., Schofield, Christopher J., Taylor, Graham P., and Bangham, Charles R. M.

Abstract

The human retrovirus HTLV-1 causes a hematological malignancy or neuroinflammatory disease in approximately 10% of infected individuals. HTLV-1 primarily infects CD4(+) T lymphocytes and persists as a provirus integrated in their genome. HTLV-1 appears transcriptionally latent in freshly isolated cells; however, the chronically active anti-HTLV-1 cytotoxic T cell response observed in infected individuals indicates frequent proviral expression in vivo. The kinetics and regulation of HTLV-1 proviral expression in vivo are poorly understood. By using hypoxia, small-molecule hypoxia mimics, and inhibitors of specific metabolic pathways, we show that physiologically relevant levels of hypoxia, as routinely encountered by circulating T cells in the lymphoid organs and bone marrow, significantly enhance HTLV-1 reactivation from latency. Furthermore, culturing naturally infected CD4(+) T cells in glucose-free medium or chemical inhibition of glycolysis or the mitochondrial electron transport chain strongly suppresses HTLV-1 plus-strand transcription. We conclude that glucose metabolism and oxygen tension regulate HTLV-1 proviral latency and reactivation in vivo.

Published

2017

2. Glucose Metabolism and Oxygen Availability Govern Reactivation of the Latent Human Retrovirus HTLV-1.

Author

Kulkarni, Anurag, Mateus, Manuel, Thinnes, Cyrille, McCullagh, James S., Schofield, Christopher J., Taylor, Graham P., Bangham, Charles R. M., Kulkarni, Anurag, Mateus, Manuel, Thinnes, Cyrille, McCullagh, James S., Schofield, Christopher J., Taylor, Graham P., and Bangham, Charles R. M.

Abstract

The human retrovirus HTLV-1 causes a hematological malignancy or neuroinflammatory disease in approximately 10% of infected individuals. HTLV-1 primarily infects CD4(+) T lymphocytes and persists as a provirus integrated in their genome. HTLV-1 appears transcriptionally latent in freshly isolated cells; however, the chronically active anti-HTLV-1 cytotoxic T cell response observed in infected individuals indicates frequent proviral expression in vivo. The kinetics and regulation of HTLV-1 proviral expression in vivo are poorly understood. By using hypoxia, small-molecule hypoxia mimics, and inhibitors of specific metabolic pathways, we show that physiologically relevant levels of hypoxia, as routinely encountered by circulating T cells in the lymphoid organs and bone marrow, significantly enhance HTLV-1 reactivation from latency. Furthermore, culturing naturally infected CD4(+) T cells in glucose-free medium or chemical inhibition of glycolysis or the mitochondrial electron transport chain strongly suppresses HTLV-1 plus-strand transcription. We conclude that glucose metabolism and oxygen tension regulate HTLV-1 proviral latency and reactivation in vivo.

Published

2017

3. CADM1/TSLC1 Identifies HTLV-1-Infected Cells and Determines Their Susceptibility to CTL-Mediated Lysis

Author

Manivannan, Kiruthika, Rowan, Aileen G., Tanaka, Yuetsu, Taylor, Graham P., Bangham, Charles R. M., Manivannan, Kiruthika, Rowan, Aileen G., Tanaka, Yuetsu, Taylor, Graham P., and Bangham, Charles R. M.

Abstract

Human T cell lymphotropic virus-1 (HTLV-1) primarily infects CD4+ T cells, causing inflammatory disorders or a T cell malignancy in 5% to 10% of carriers. The cytotoxic T lymphocyte (CTL) response is a key factor that controls the viral load and thus the risk of disease. The ability to detect the viral protein Tax in primary cells has made it possible to estimate the rate at which Tax-expressing infected cells are eliminated by CTLs in persistently infected people. However, most HTLV-1-infected cells are Tax– at a given time, and their immunophenotype is poorly defined. Here, we aimed to identify a cell-surface molecule expressed by both Tax+ and Tax– HTLV-1-infected cells and use it to analyse the CTL response in fresh peripheral blood mononuclear cells. Cell adhesion molecule 1 (CADM1/ TSLC1) was the best single marker of HTLV-1 infection, identifying HTLV-1-infected cells with greater sensitivity and specificity than CD25, CCR4 or ICAM-1. CADM1+ CD4+ T cells carried a median of 65% of proviral copies in peripheral blood. In a cohort of 23 individuals, we quantified the rate of CTL-mediated killing of Tax+ and Tax− CADM1+ cells. We show that CADM1 expression is associated with enhanced susceptibility of infected cells to CTL lysis: despite the immunodominance of Tax in the CTL response, Tax+ CADM1– cells were inefficiently lysed by CTLs. Upregulation of the CADM1 ligand CRTAM on CD8+ T cells correlated with efficient lysis of infected cells. Tax– CADM1+ cells were lysed at a very low rate by autologous CTLs, however, were efficiently killed when loaded with exogenous peptide antigen. High expression of CADM1 on most HTLV-1-infected cells in the face of enhanced CTL counterselection implies that CADM1 confers a strong benefit on the virus.

Published

2016

4. T Cell Receptor Vβ Staining Identifies the Malignant Clone in Adult T cell Leukemia and Reveals Killing of Leukemia Cells by Autologous CD8^+ T cells

Author

Rowan, Aileen G., Witkover, Aviva, Melamed, Anat, Tanaka, Yuetsu, Cook, Lucy B. M., Fields, Paul, Taylor, Graham P., Bangham, Charles R. M., Rowan, Aileen G., Witkover, Aviva, Melamed, Anat, Tanaka, Yuetsu, Cook, Lucy B. M., Fields, Paul, Taylor, Graham P., and Bangham, Charles R. M.

Abstract

There is growing evidence that CD8^+ cytotoxic T lymphocyte (CTL) responses can contribute to long-term remission of many malignancies. The etiological agent of adult T-cell leukemia/lymphoma (ATL), human T lymphotropic virus type-1 (HTLV-1), contains highly immunogenic CTL epitopes, but ATL patients typically have low frequencies of cytokine-producing HTLV-1-specific CD8^+ cells in the circulation. It remains unclear whether patients with ATL possess CTLs that can kill the malignant HTLV-1 infected clone. Here we used flow cytometric staining of TCRVβ and cell adhesion molecule-1 (CADM1) to identify monoclonal populations of HTLV-1-infected T cells in the peripheral blood of patients with ATL. Thus, we quantified the rate of CD8^+-mediated killing of the putative malignant clone in ex vivo blood samples. We observed that CD8^+ cells from ATL patients were unable to lyse autologous ATL clones when tested directly ex vivo. However, short in vitro culture restored the ability of CD8^+ cells to kill ex vivo ATL clones in some donors. The capacity of CD8^+ cells to lyse HTLV-1 infected cells which expressed the viral sense strand gene products was significantly enhanced after in vitro culture, and donors with an ATL clone that expressed the HTLV-1 Tax gene were most likely to make a detectable lytic CD^8+ response to the ATL cells. We conclude that some patients with ATL possess functional tumour-specific CTLs which could be exploited to contribute to control of the disease.

Published

2016

5. Clonality of HTLV-2 in natural infection.

Author

Melamed, Anat, Melamed, Anat, Witkover, Aviva D, Laydon, Daniel J, Brown, Rachael, Ladell, Kristin, Miners, Kelly, Rowan, Aileen G, Gormley, Niall, Price, David A, Taylor, Graham P, Murphy, Edward L, Bangham, Charles RM, Melamed, Anat, Melamed, Anat, Witkover, Aviva D, Laydon, Daniel J, Brown, Rachael, Ladell, Kristin, Miners, Kelly, Rowan, Aileen G, Gormley, Niall, Price, David A, Taylor, Graham P, Murphy, Edward L, and Bangham, Charles RM

Abstract

Human T-lymphotropic virus type 1 (HTLV-1) and type 2 (HTLV-2) both cause lifelong persistent infections, but differ in their clinical outcomes. HTLV-1 infection causes a chronic or acute T-lymphocytic malignancy in up to 5% of infected individuals whereas HTLV-2 has not been unequivocally linked to a T-cell malignancy. Virus-driven clonal proliferation of infected cells both in vitro and in vivo has been demonstrated in HTLV-1 infection. However, T-cell clonality in HTLV-2 infection has not been rigorously characterized. In this study we used a high-throughput approach in conjunction with flow cytometric sorting to identify and quantify HTLV-2-infected T-cell clones in 28 individuals with natural infection. We show that while genome-wide integration site preferences in vivo were similar to those found in HTLV-1 infection, expansion of HTLV-2-infected clones did not demonstrate the same significant association with the genomic environment of the integrated provirus. The proviral load in HTLV-2 is almost confined to CD8+ T-cells and is composed of a small number of often highly expanded clones. The HTLV-2 load correlated significantly with the degree of dispersion of the clone frequency distribution, which was highly stable over ∼8 years. These results suggest that there are significant differences in the selection forces that control the clonal expansion of virus-infected cells in HTLV-1 and HTLV-2 infection. In addition, our data demonstrate that strong virus-driven proliferation per se does not predispose to malignant transformation in oncoretroviral infections.

Published

2014

6. Clonality of HTLV-2 in natural infection.

Author

Melamed, Anat, Ross, Susan R1, Melamed, Anat, Witkover, Aviva D, Laydon, Daniel J, Brown, Rachael, Ladell, Kristin, Miners, Kelly, Rowan, Aileen G, Gormley, Niall, Price, David A, Taylor, Graham P, Murphy, Edward L, Bangham, Charles RM, Melamed, Anat, Ross, Susan R1, Melamed, Anat, Witkover, Aviva D, Laydon, Daniel J, Brown, Rachael, Ladell, Kristin, Miners, Kelly, Rowan, Aileen G, Gormley, Niall, Price, David A, Taylor, Graham P, Murphy, Edward L, and Bangham, Charles RM

Abstract

Human T-lymphotropic virus type 1 (HTLV-1) and type 2 (HTLV-2) both cause lifelong persistent infections, but differ in their clinical outcomes. HTLV-1 infection causes a chronic or acute T-lymphocytic malignancy in up to 5% of infected individuals whereas HTLV-2 has not been unequivocally linked to a T-cell malignancy. Virus-driven clonal proliferation of infected cells both in vitro and in vivo has been demonstrated in HTLV-1 infection. However, T-cell clonality in HTLV-2 infection has not been rigorously characterized. In this study we used a high-throughput approach in conjunction with flow cytometric sorting to identify and quantify HTLV-2-infected T-cell clones in 28 individuals with natural infection. We show that while genome-wide integration site preferences in vivo were similar to those found in HTLV-1 infection, expansion of HTLV-2-infected clones did not demonstrate the same significant association with the genomic environment of the integrated provirus. The proviral load in HTLV-2 is almost confined to CD8+ T-cells and is composed of a small number of often highly expanded clones. The HTLV-2 load correlated significantly with the degree of dispersion of the clone frequency distribution, which was highly stable over ∼8 years. These results suggest that there are significant differences in the selection forces that control the clonal expansion of virus-infected cells in HTLV-1 and HTLV-2 infection. In addition, our data demonstrate that strong virus-driven proliferation per se does not predispose to malignant transformation in oncoretroviral infections.

Published

2014

7. Proposal for diagnostic criteria of tropical spastic paraparesis/HTLV-I-associated myelopathy (TSP/HAM).

Author

De Castro-Costa, Carlos M, De Castro-Costa, Carlos M, Araújo, Abelardo QC, Barreto, Márcio M, Takayanagui, Osvaldo M, Sohler, Marzia P, da Silva, Eduardo LM, de Paula, Sônia MB, Ishak, Ricardo, Ribas, João GR, Rovirosa, Luis C, Carton, Herwig, Gotuzzo, Eduardo, Hall, William W, Montano, Silvia, Murphy, Edward L, Oger, Joel, Remondegui, Carlos, Taylor, Graham P, De Castro-Costa, Carlos M, De Castro-Costa, Carlos M, Araújo, Abelardo QC, Barreto, Márcio M, Takayanagui, Osvaldo M, Sohler, Marzia P, da Silva, Eduardo LM, de Paula, Sônia MB, Ishak, Ricardo, Ribas, João GR, Rovirosa, Luis C, Carton, Herwig, Gotuzzo, Eduardo, Hall, William W, Montano, Silvia, Murphy, Edward L, Oger, Joel, Remondegui, Carlos, and Taylor, Graham P

Abstract

After the first description of TSP/HAM in 1985 and the elaboration of WHO's diagnostic criteria in 1988, the experience of the professionals in this field has increased so that a critical reappraisal of these diagnostic guidelines was considered timely. Brazilian neurologists and observers from other countries met recently to discuss and propose a modified model for diagnosing TSP/HAM with levels of ascertainment as definite, probable, and possible, according to myelopathic symptoms, serological findings, and/or detection of HTLV-I DNA and exclusion of other disorders.

Published

2006

8. Proposal for diagnostic criteria of tropical spastic paraparesis/HTLV-I-associated myelopathy (TSP/HAM).

Author

De Castro-Costa, Carlos M, De Castro-Costa, Carlos M, Araújo, Abelardo QC, Barreto, Márcio M, Takayanagui, Osvaldo M, Sohler, Marzia P, da Silva, Eduardo LM, de Paula, Sônia MB, Ishak, Ricardo, Ribas, João GR, Rovirosa, Luis C, Carton, Herwig, Gotuzzo, Eduardo, Hall, William W, Montano, Silvia, Murphy, Edward L, Oger, Joel, Remondegui, Carlos, Taylor, Graham P, De Castro-Costa, Carlos M, De Castro-Costa, Carlos M, Araújo, Abelardo QC, Barreto, Márcio M, Takayanagui, Osvaldo M, Sohler, Marzia P, da Silva, Eduardo LM, de Paula, Sônia MB, Ishak, Ricardo, Ribas, João GR, Rovirosa, Luis C, Carton, Herwig, Gotuzzo, Eduardo, Hall, William W, Montano, Silvia, Murphy, Edward L, Oger, Joel, Remondegui, Carlos, and Taylor, Graham P

Abstract

After the first description of TSP/HAM in 1985 and the elaboration of WHO's diagnostic criteria in 1988, the experience of the professionals in this field has increased so that a critical reappraisal of these diagnostic guidelines was considered timely. Brazilian neurologists and observers from other countries met recently to discuss and propose a modified model for diagnosing TSP/HAM with levels of ascertainment as definite, probable, and possible, according to myelopathic symptoms, serological findings, and/or detection of HTLV-I DNA and exclusion of other disorders.

Published

2006

9. International Retrovirology Association brings together scientists and clinicians to bridge discoveries about human T-lymphotropic viruses from the laboratory to clinical trials.

Author

Murphy, Edward, Murphy, Edward, Jacobson, Steven, Franchini, Genoveffa, Taylor, Graham P, Hanchard, Barrie, Morgan, Owen, Lairmore, Michael, Murphy, Edward, Murphy, Edward, Jacobson, Steven, Franchini, Genoveffa, Taylor, Graham P, Hanchard, Barrie, Morgan, Owen, and Lairmore, Michael

Abstract

Human T-lymphotropic virus type 1 (HTLV-1) and HTLV-2 were among the first human retroviruses discovered in the early 1980's. The International Retrovirology Association is an organized effort that fostered the efforts of scientists and clinicians to form interdisciplinary groups to study this group of retroviruses and their related diseases. The Association promotes excellent science, patient education, and fosters the training of young scientists to promote "bench-to-bedside" research. The International Conference on Human Retrovirology: HTLV and Related Viruses sponsored by the Association supports clinicians and researchers in the exchange of research findings and stimulation of new research directions. This years conference will be held from June 22 to 25, in Montego Bay, Jamaica http://www.htlvconference.org.jm/. Since its inception in 1988, these conferences have provided a highly interactive forum for the global community of HTLV scientists. This is of particular importance as HTLV research enters its third decade and a new generation of scientists takes over this important work. Many of the scientists attending the meeting will be from developing countries where HTLV is endemic, consistent with the history of international collaborations that have characterized HTLV research. The International Conference on Human Retrovirology provides a unique opportunity for researchers of all disciplines interested in HTLV infections to meet their peers and to address the questions facing clinicians and scientists who study retroviruses, like HTLV.

Published

2005

10. The seroepidemiology of human T-lymphotropic viruses: types I and II in Europe: a prospective study of pregnant women.

Author

UCL - MD/MIGE - Département de microbiologie, d'immunologie et de génétique, Taylor, Graham P, Bodéus, Monique, Courtois, Françoise, Pauli, Georg, Del Mistro, Annarosa, Machuca, Ana, Padua, Elizabeth, Andersson, Soren, Goubau, Patrick, Chieco-Bianchi, Luigi, Soriano, Vincent, Coste, Joliette, Ades, Anthony E, Weber, Jonathan N, UCL - MD/MIGE - Département de microbiologie, d'immunologie et de génétique, Taylor, Graham P, Bodéus, Monique, Courtois, Françoise, Pauli, Georg, Del Mistro, Annarosa, Machuca, Ana, Padua, Elizabeth, Andersson, Soren, Goubau, Patrick, Chieco-Bianchi, Luigi, Soriano, Vincent, Coste, Joliette, Ades, Anthony E, and Weber, Jonathan N

Abstract

BACKGROUND: Up to 20 million persons are infected with the human retroviruses human T-lymphotropic virus (HTLV)-I and HTLV-II globally. Most data on the seroprevalence of HTLV-I and HTLV-II in Europe are from studies of low-risk blood donors or high-risk injection drug users (IDUs). Little is known about the general population. METHODS: A prospective anonymous study of HTLV-I and HTLV-II seroprevalence among 234,078 pregnant women in Belgium, France, Germany, Italy, Portugal, Spain, and the United Kingdom was conducted. Maternal antibody status was determined by standard methods using sera obtained for routine antenatal infection screens or eluted from infant heel prick dried blood spots obtained for routine neonatal metabolic screens. RESULTS: Anti-HTLV-I/II antibodies were detected and confirmed in 96 pregnant women (4.4 per 10,000, 95% confidence interval [CI]: 3.5-5.2). Of these, 73 were anti-HTLV-I, 17 were anti-HTLV-II, and 6 were specifically anti-HTLV but untyped. The seroprevalence ranged from 0.7 per 10,000 in Germany to 11.5 per 10,000 in France. CONCLUSIONS: Pregnant women better reflect the general population than blood donors or IDUs. The seroprevalence of HTLV-I and HTLV-II in Western Europe is 6-fold higher among pregnant women (4.4 per 10,000) than among blood donors (0.07 per 10,000). These data provide a robust baseline against which changes in HTLV-I and HTLV-II seroprevalence in Europe can be measured.

Published

2005

11. International Retrovirology Association brings together scientists and clinicians to bridge discoveries about human T-lymphotropic viruses from the laboratory to clinical trials.

Author

Murphy, Edward, Murphy, Edward, Jacobson, Steven, Franchini, Genoveffa, Taylor, Graham P, Hanchard, Barrie, Morgan, Owen, Lairmore, Michael, Murphy, Edward, Murphy, Edward, Jacobson, Steven, Franchini, Genoveffa, Taylor, Graham P, Hanchard, Barrie, Morgan, Owen, and Lairmore, Michael

Abstract

Human T-lymphotropic virus type 1 (HTLV-1) and HTLV-2 were among the first human retroviruses discovered in the early 1980's. The International Retrovirology Association is an organized effort that fostered the efforts of scientists and clinicians to form interdisciplinary groups to study this group of retroviruses and their related diseases. The Association promotes excellent science, patient education, and fosters the training of young scientists to promote "bench-to-bedside" research. The International Conference on Human Retrovirology: HTLV and Related Viruses sponsored by the Association supports clinicians and researchers in the exchange of research findings and stimulation of new research directions. This years conference will be held from June 22 to 25, in Montego Bay, Jamaica http://www.htlvconference.org.jm/. Since its inception in 1988, these conferences have provided a highly interactive forum for the global community of HTLV scientists. This is of particular importance as HTLV research enters its third decade and a new generation of scientists takes over this important work. Many of the scientists attending the meeting will be from developing countries where HTLV is endemic, consistent with the history of international collaborations that have characterized HTLV research. The International Conference on Human Retrovirology provides a unique opportunity for researchers of all disciplines interested in HTLV infections to meet their peers and to address the questions facing clinicians and scientists who study retroviruses, like HTLV.

Published

2005