Your search keyword '"Thymidine Kinase -- genetics"' showing total 12 results

1. Heterogeneity and evolution of thymidine kinase and DNA polymerase mutants of herpes simplex virus type 1: Implications for antiviral therapy

Author

Andrei, Graciela, Georgala, Aspasia, Topalis, Dimitri, Fiten, Pierre, Aoun, Michel, Opdenakker, Ghislain, Snoeck, Robert, Andrei, Graciela, Georgala, Aspasia, Topalis, Dimitri, Fiten, Pierre, Aoun, Michel, Opdenakker, Ghislain, and Snoeck, Robert

Abstract

Background. Infections caused by acyclovir-resistant isolates of herpes simplex virus (HSV) after hematopoietic stem cell transplantation (HSCT) are an emerging concern. An understanding of the evolutionary aspects of HSV infection is crucial to the design of effective therapeutic and control strategies.Methods. Eight sequential HSV-1 isolates were recovered from an HSCT patient who suffered from recurrent herpetic gingivostomatitis and was treated alternatively with acyclovir, ganciclovir, and foscavir. The diverse spectra and temporal changes of HSV drug resistance were determined phenotypically (drug-resistance profiling) and genotypically (sequencing of the viral thymidine kinase and DNA polymerase genes).Results. Analysis of 60 clones recovered from the different isolates demonstrated that most of these isolates were heterogeneous mixtures of variants, indicating the simultaneous infection with different drug-resistant viruses. The phenotype/genotype of several clones associated with resistance to acyclovir and/or foscavir were identified. Two novel mutations (E798K and I922T) in the viral DNA polymerase could be linked to drug resistance.Conclusions. The heterogeneity within the viral populations and the temporal changes of drug-resistant viruses found in this HSCT recipient were remarkable, showing a rapid evolution of HSV-1. Drug-resistance surveillance is highly recommended among immunocompromised patients to manage the clinical syndrome and to avoid the emergence of multidrug-resistant isolates. © 2013 The Author., SCOPUS: ar.j, info:eu-repo/semantics/published

Published

2013

2. Transcription factor binding sites in the pol gene intragenic regulatory region of HIV-1 are important for virus infectivity

Author

Arsène Burny, Yves Collette, Dominique Demonte, Véronique Goffin, Yvan de Launoit, Stéphane de Walque, Carine Van Lint, and Caroline Vanhulle

Subjects

Gene Expression Regulation, Viral, Transcriptional Activation, Sp1 Transcription Factor, DNA Mutational Analysis, Gene Products, pol, Biology, Response Elements, Virus Replication, DNA-binding protein, Thymidine Kinase, Article, Sp1 Transcription Factor -- metabolism, Cell Line, Mice, HIV-1 -- physiology, Proto-Oncogene Proteins, HIV-1 -- genetics, Genetics, Trans-Activators -- metabolism, Animals, Humans, Point Mutation, Binding site, Promoter Regions, Genetic, Transcription factor, ChIA-PET, Transcription Factors -- metabolism, Sp1 transcription factor, Binding Sites, Gene Products, pol -- genetics, Thymidine Kinase -- genetics, Zinc Fingers, Sciences bio-médicales et agricoles, Molecular biology, Chromatin, DNA binding site, DNA-Binding Proteins, Transcription Factors -- chemistry, Proto-Oncogene Proteins -- metabolism, Sp3 Transcription Factor, Gene Products, tat, HIV-1, Trans-Activators, Gene Products, tat -- metabolism, tat Gene Products, Human Immunodeficiency Virus, Chromatin immunoprecipitation, DNA-Binding Proteins -- metabolism, Transcription Factors, Octamer Transcription Factor-1

Abstract

We have previously identified in the pol gene of human immunodeficiency virus type 1 (HIV-1) a new positive transcriptional regulatory element (nt 4481-4982) containing recognition sites for nuclear proteins (sites B, C, D and a GC-box) [C. Van Lint, J. Ghysdael, P. Paras, Jr, A. Burny and E. Verdin (1994) J. Virol. 68, 2632-2648]. In this study, we have further physically characterized each binding site and have shown that the transcription factors Oct-1, Oct-2, PU.1, Sp1 and Sp3 interact in vitro with the pol region. Chromatin immunoprecipitation assays using HIV-infected cell lines demonstrated in the context of chromatin that Sp1, Sp3, Oct-1 and PU.1 are recruited to the HS7 region in vivo. For each site, we have identified mutations abolishing factor binding to their cognate DNA sequences without altering the underlying amino acid sequence of the integrase. By transient transfection assays, we have demonstrated the involvement of the pol binding sites in the transcriptional enhancing activity of the intragenic region. Our functional results with multimerized wild-type and mutated pol binding sites separately (i.e. in the absence of the other sites) have demonstrated that the PU.1, Sp1, Sp3 and Oct-1 transcription factors regulate the transcriptional activity of a heterologous promoter through their respective HS7 binding sites. Finally, we have investigated the physiological role of the HS7 binding sites in HIV-1 replication and have shown that these sites are important for viral infectivity., Journal Article, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published

2005

3. Transcription factor binding sites in the pol gene intragenic regulatory region of HIV-1 are important for virus infectivity.

Author

Goffin, Véronique, Demonte, Dominique, Vanhulle, Caroline, De Walque, Stéphane, De Launoit, Yvan, Burny, Arsène, Collette, Yves, Van Lint, Carine, Goffin, Véronique, Demonte, Dominique, Vanhulle, Caroline, De Walque, Stéphane, De Launoit, Yvan, Burny, Arsène, Collette, Yves, and Van Lint, Carine

Abstract

We have previously identified in the pol gene of human immunodeficiency virus type 1 (HIV-1) a new positive transcriptional regulatory element (nt 4481-4982) containing recognition sites for nuclear proteins (sites B, C, D and a GC-box) [C. Van Lint, J. Ghysdael, P. Paras, Jr, A. Burny and E. Verdin (1994) J. Virol. 68, 2632-2648]. In this study, we have further physically characterized each binding site and have shown that the transcription factors Oct-1, Oct-2, PU.1, Sp1 and Sp3 interact in vitro with the pol region. Chromatin immunoprecipitation assays using HIV-infected cell lines demonstrated in the context of chromatin that Sp1, Sp3, Oct-1 and PU.1 are recruited to the HS7 region in vivo. For each site, we have identified mutations abolishing factor binding to their cognate DNA sequences without altering the underlying amino acid sequence of the integrase. By transient transfection assays, we have demonstrated the involvement of the pol binding sites in the transcriptional enhancing activity of the intragenic region. Our functional results with multimerized wild-type and mutated pol binding sites separately (i.e. in the absence of the other sites) have demonstrated that the PU.1, Sp1, Sp3 and Oct-1 transcription factors regulate the transcriptional activity of a heterologous promoter through their respective HS7 binding sites. Finally, we have investigated the physiological role of the HS7 binding sites in HIV-1 replication and have shown that these sites are important for viral infectivity., Journal Article, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published

2005

4. Tumor-selective gene transduction and cell killing with an oncotropic autonomous parvovirus-based vector.

Author

Dupont, Florence, Avalosse, Bernard, Karim, A, Mine, Natacha, Bosseler, M, Maron, A, Van Den Broeke, Anne, Ghanem, Ghanem Elias, Burny, Arsène, Zeicher, M, Dupont, Florence, Avalosse, Bernard, Karim, A, Mine, Natacha, Bosseler, M, Maron, A, Van Den Broeke, Anne, Ghanem, Ghanem Elias, Burny, Arsène, and Zeicher, M

Abstract

A recombinant MVMp of the fibrotropic strain of minute virus of mice (MVMp) expressing the chloramphenicol acetyltransferase reporter gene was used to infect a series of biologically relevant cultured cells, normal or tumor-derived, including normal melanocytes versus melanoma cells, normal mammary epithelial cells versus breast adenocarcinoma cells, and normal neurons or astrocytes versus glioma cells. As a reference cell system we used normal human fibroblasts versus the SV40-transformed fibroblast cell line NB324K. After infection, we observed good expression of the reporter gene in the different tumor cell types, but only poor expression if any in the corresponding normal cells. We also constructed a recombinant MVMp expressing the green fluorescent protein reporter gene and assessed by flow cytometry the efficiency of gene transduction into the different target cells. At a multiplicity of infection of 30, we observed substantial transduction of the gene into most of the tumor cell types tested, but only marginal transduction into normal cells under the same experimental conditions. Finally, we demonstrated that a recombinant MVMp expressing the herpes simplex virus thymidine kinase gene can, in vitro, cause efficient killing of most tumor cell types in the presence of ganciclovir, whilst affecting normal proliferating cells only marginally if at all. However, in the same experimental condition, breast tumor cells appeared to be resistant to GCV-mediated cytotoxicity, possibly because these cells are not susceptible to the bystander effect. Our data suggest that MVMp-based vectors could prove useful as selective vehicles for anticancer gene therapy, particularly for in vivo delivery of cytotoxic effector genes into tumor cells., Comparative Study, Journal Article, info:eu-repo/semantics/published

Published

2000

5. A phase 1-2 clinical trial of gene therapy for recurrent glioblastoma multiforme by tumor transduction with the herpes simplex thymidine kinase gene followed by ganciclovir.

Author

Shand, N., Weber, F, Mariani, Luigi, Bernstein, Mark, Gianella-Borradori, Athos, Long, Z., Sorensen, AG, Barbier, Nicolas Serge, GLI328 European-canadian study group, Shand, N., Weber, F, Mariani, Luigi, Bernstein, Mark, Gianella-Borradori, Athos, Long, Z., Sorensen, AG, Barbier, Nicolas Serge, and GLI328 European-canadian study group

Abstract

This study has investigated the effects of herpes simplex thymidine kinase gene (HSV-tk) transfer followed by ganciclovir treatment as adjuvant gene therapy to surgical resection in patients with recurrent glioblastoma multiforme (GBM). The study was open and single-arm, and aimed at assessing the feasibility and safety of the technique and indications of antitumor activity. In 48 patients a suspension of retroviral vector-producing cells (VPCs) was administered by intracerebral injection immediately after tumor resection. Intravenous ganciclovir was infused daily 14 to 27 days after surgery. Patients were monitored for adverse events and for life by regular biosafety assaying. Tumor changes were monitored by magnetic resonance imaging (MRI). Reflux during injection was a frequent occurrence but serious adverse events during the treatment period (days 1-27) were few and of a nature not unexpected in this population. One patient experienced transient neurological disorders associated with postganciclovir MRI enhancement. There was no evidence of replication-competent retrovirus in peripheral blood leukocytes or in tissue samples of reresection or autopsy. Vector DNA was shown in the leukocytes of some patients but not in autopsy gonadal samples. The median survival time was 8.6 months, and the 12-month survival rate was 13 of 48 (27%). On MRI studies, tumor recurrence was absent in seven patients for at least 6 months and for at least 12 months in two patients, one of whom remains recurrence free at more than 24 months. Treatment-characteristic images of injection tracks and intracavity hemoglobin were apparent. In conclusion, the gene therapy is feasible and appears to be satisfactorily safe as an adjuvant to the surgical resection of recurrent GBM, but any benefit appears to be marginal. Investigation of the precise effectiveness of this gene therapy requires prospective, controlled studies., Clinical Trial, Clinical Trial, Phase I, Clinical Trial, Phase II, Journal Article, Multicenter Study, info:eu-repo/semantics/published

Published

1999

6. Gene therapy of rat C6 glioma using adenovirus-mediated transfer of the herpes simplex virus thymidine kinase gene: long-term follow-up by magnetic resonance imaging

Author

Maron, A., Gustin, T., Le Roux, A., Mottet, I., Dedieu, J. -F, Jean-Pierre Brion, Demeure, R., Perricaudet, M., and Octave, J. -N

Subjects

Male, Time Factors, Genes, Viral, viruses, Genetic Vectors, Gene Transfer Techniques, Thymidine Kinase -- genetics, Simplexvirus -- genetics, Sciences bio-médicales et agricoles, Brain Neoplasms -- genetics, Magnetic Resonance Imaging, Glioma -- genetics, Rats, Brain Neoplasms -- pathology, Glioma -- pathology, Glioma -- therapy, Gene Therapy -- methods, Animals, Rats, Wistar, Brain Neoplasms -- therapy, Adenoviridae -- genetics, Ganciclovir -- therapeutic use

Abstract

The herpes simplex virus thymidine kinase gene was transferred into C6 glioma cells by infection with a recombinant adenovirus. In vitro, a 10 microM ganciclovir concentration was able to kill 100% of the infected cells. For in vivo experiments, brain tumors were established by stereotactic injection of C6 glioma cells in the caudate nucleus of rats. Five days later, the recombinant adenovirus was inoculated into the tumors and the animals were treated by intraperitoneal injections of ganciclovir for 14 days. At the end of ganciclovir therapy, histological examination revealed a 28-fold decrease in tumor volumes in the treated animals, as compared with control animals. In long-term studies, the mean survival time of the treated animals were four-fold longer than that of control ones. Magnetic resonance imaging demonstrated an apparent complete tumor regression in 62% of the animals. However, late tumor recurrence was observed in the treated animals. Repeated inoculation of C6 glioma cells in the contralateral hemisphere of long-term surviving animals resulted in either tumor rejection or slowly growing tumors. These findings demonstrate the potential efficacy of adenovirus-mediated transfer of the herpes simplex virus thymidine kinase gene and ganciclovir administration in the treatment of rat gliomas., Journal Article, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published

1996

7. Gene therapy for glioblastoma [correction of gliobestome] multiform: in vivo tumor transduction with the herpes simplex thymidine kinase gene followed by ganciclovir.

Author

Stockhammer, Günther, Brotchi, Jacques, Leblanc, Richard, Bernstein, Mark, Schackert, Gabriele, Weber, F, Ostertag, C, Mulder, N H, Mellstedt, Håkan, Seiler, Rolf Walter, Yonekawa, Yasuhiro, Twerdy, K, Kostron, Herwig, De Witte, Olivier, Lambermont, Micheline, Velu, Thierry, Laneuville, Pierre, Villemure, Jean Guy, Rutka, James, Warnke, P, Laseur, Marian, Mooij, Jan Jakob, Boëthius, Jörgen, Mariani, Luigi, Gianella-Borradori, Athos, Stockhammer, Günther, Brotchi, Jacques, Leblanc, Richard, Bernstein, Mark, Schackert, Gabriele, Weber, F, Ostertag, C, Mulder, N H, Mellstedt, Håkan, Seiler, Rolf Walter, Yonekawa, Yasuhiro, Twerdy, K, Kostron, Herwig, De Witte, Olivier, Lambermont, Micheline, Velu, Thierry, Laneuville, Pierre, Villemure, Jean Guy, Rutka, James, Warnke, P, Laseur, Marian, Mooij, Jan Jakob, Boëthius, Jörgen, Mariani, Luigi, and Gianella-Borradori, Athos

Abstract

Clinical Trial, Clinical Trial, Phase II, Journal Article, Multicenter Study, info:eu-repo/semantics/published

Published

1997

8. Gene therapy of rat C6 glioma using adenovirus-mediated transfer of the herpes simplex virus thymidine kinase gene: long-term follow-up by magnetic resonance imaging.

Author

Maron, A, Gustin, T, Le Roux, A, Mottet, I, Dedieu, J F, Brion, Jean Pierre, Demeure, Roger, Perricaudet, M, Octave, Jean Noël, Maron, A, Gustin, T, Le Roux, A, Mottet, I, Dedieu, J F, Brion, Jean Pierre, Demeure, Roger, Perricaudet, M, and Octave, Jean Noël

Abstract

The herpes simplex virus thymidine kinase gene was transferred into C6 glioma cells by infection with a recombinant adenovirus. In vitro, a 10 microM ganciclovir concentration was able to kill 100% of the infected cells. For in vivo experiments, brain tumors were established by stereotactic injection of C6 glioma cells in the caudate nucleus of rats. Five days later, the recombinant adenovirus was inoculated into the tumors and the animals were treated by intraperitoneal injections of ganciclovir for 14 days. At the end of ganciclovir therapy, histological examination revealed a 28-fold decrease in tumor volumes in the treated animals, as compared with control animals. In long-term studies, the mean survival time of the treated animals were four-fold longer than that of control ones. Magnetic resonance imaging demonstrated an apparent complete tumor regression in 62% of the animals. However, late tumor recurrence was observed in the treated animals. Repeated inoculation of C6 glioma cells in the contralateral hemisphere of long-term surviving animals resulted in either tumor rejection or slowly growing tumors. These findings demonstrate the potential efficacy of adenovirus-mediated transfer of the herpes simplex virus thymidine kinase gene and ganciclovir administration in the treatment of rat gliomas., Journal Article, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published

1996

9. Identification of a thyroid-specific and cAMP-responsive enhancer in the upstream sequences of the human thyroglobulin promoter

Author

Berg, Véronique, Vassart, Gilbert, Christophe, Daniel, Berg, Véronique, Vassart, Gilbert, and Christophe, Daniel

Abstract

Functional analysis of remote 5'-flanking sequences from the human thyroglobulin gene in primary cultured dog thyrocytes led to the identification of a partly cAMP-responsive enhancer, located between -3.6 to -2.2 kb from the transcriptional start site. Deletion analysis of the 1.4 kb-long region localised the enhancer activity in a 0.5 kb-long fragment (located between -3.2 and -2.7 kb relative to transcription start), which could be divided into two functional sub-fragments of 0.2 and 0.3 kb. A potential binding site for the CREB/ATF transcription factors was found in the 0.3 kb element. The complete enhancer region had no detectable activity when assayed in Hela cells, suggesting that it constituted a thyroid-specific regulatory element. Accordingly, footprinting experiments revealed the presence of several binding sites for Thyroid Transcription Factor-1 (TTF-1) in both the 0.2 and 0.3 kb elements., Journal Article, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published

1996

10. Models of thyroid goiter and tumors in transgenic mice.

Author

Ledent, Catherine, Parmentier, Marc, Vassart, Gilbert, Dumont, Jacques Emile, Ledent, Catherine, Parmentier, Marc, Vassart, Gilbert, and Dumont, Jacques Emile

Abstract

Journal Article, Research Support, Non-U.S. Gov't, Review, SCOPUS: ar.j, info:eu-repo/semantics/published

Published

1994

11. Specific ablation of thyroid follicle cells in adult transgenic mice.

Author

Wallace, Helen, Ledent, Catherine, Vassart, Gilbert, Bishop, J. O., al-Shawi, R, Wallace, Helen, Ledent, Catherine, Vassart, Gilbert, Bishop, J. O., and al-Shawi, R

Abstract

The coding region of the herpes simplex type 1 virus thymidine kinase gene was coupled to the promoter of the bovine thyroglobulin gene and introduced into the genome of mice. The viral thymidine kinase (HSV1-TK) was expressed mainly in the thyroid glands and testis. Upon treatment of transgenic females with the antiherpetic agent Ganciclovir the thyroid regressed, while the parathyroid gland was unaffected. The number of thyroid follicle cells was greatly reduced after 3 days, and they were completely absent after 7 days of treatment. After 14 days, the levels of circulating T4 and T3 were below the limits of detection, total soluble protein recovered from the thyroid and parathyroid glands together was 10% of the control value, and the level of thyroid HSV1-TK was more than 100-fold lower than that in transgenic controls. Levels of circulating PTH and calcitonin remained normal. At the time of treatment the mice were adults. Thus, the thyroid follicle cells were selectively ablated after normal development with a functional thyroid gland. When treatment with Ganciclovir was terminated after 14 days, no circulating T4 or T3 or other indications of thyroid regeneration were detected for a subsequent period of 90 days. During this time the mice gained weight more slowly than controls, at a rate consistent with the suppression of GH synthesis by thyroid deficiency. The production of mouse major urinary protein (MUP) ceased in the treated mice and was completely restored by the administration of T4. MUP production was not restored by GH, demonstrating that the expression of the Mup genes requires T4 in addition to GH., Journal Article, Research Support, Non-U.S. Gov't, SCOPUS: ar.j, info:eu-repo/semantics/published

Published

1991

12. Identification and characterization of an enhancer in the coding region of the genome of human immunodeficiency virus type 1

Author

Verdin, Eric, Becker, Nathalie, Bex, Françoise, Droogmans, Louis, Burny, Arsène, Verdin, Eric, Becker, Nathalie, Bex, Françoise, Droogmans, Louis, and Burny, Arsène

Abstract

Transcription of human immunodeficiency virus type 1 (HIV-1) is regulated by cis-acting DNA elements located in the viral long terminal repeats, by viral transregulatory proteins, and by cellular transcription factors acting in concert to modulate the degree of viral expression. We demonstrate that a DNA fragment corresponding to the central portion of the HIV-1 genome exhibits enhancer activity when cloned upstream of the thymidine kinase promoter of herpes simplex virus. This enhancer is inducible by phorbol 12-myristate 13-acetate in HeLa cells and is independent of its position and orientation with respect to the promoter. We have mapped the activity of the enhancer to two independent domains encompassing nucleotides 4079-4342 (end of the pol gene) and nucleotides 4781-6026 (vif gene and first coding exon of tat). This intragenic enhancer and its subdomains demonstrate cellular specificity because they are only active in specific cell lines. The presence of similar intragenic enhancer elements in other retroviruses suggests that they might be a conserved feature of this family of viruses., info:eu-repo/semantics/published

Published

1990