Your search keyword '"Jullian E"' showing total 7 results

1. Mutant K-ras2 in serum

Author

Andreyev, HJN Benamouzig, R Beranek, M Clarke, P and Cunningham, D Norman, AR Giaretti, W de Goeij, AFPM and Iacopetta, BJ Jullian, E Krtolica, K Lee, JQ Wang, ST and Lees, N Al-Mulla, F Muller, O Pauly, M Pricolo, V and Russo, A Troungos, C Urosevic, N Ward, R

Published

2003

2. Kirsten ras mutations in patients with colorectal cancer: the 'RASCAL II' study

Author

Andreyev, HJN Norman, AR Cunningham, D Oates, J Dix, BR and Iacopetta, BJ Young, J Walsh, T Ward, R Hawkins, N and Beranek, M Jandik, P Benamouzig, R Jullian, E and Laurent-Puig, P Olschwang, S Muller, O Hoffmann, I and Rabes, HM Zietz, C Troungos, C Valavanis, C Yuen, ST and Ho, JWC Croke, CT O'Donoghue, DP Giaretti, W Rapallo, A and Russo, A Bazan, V Tanaka, M Omura, K Azuma, T and Ohkusa, T Fujimori, T Ono, Y Pauly, M Faber, C and Glaesener, R de Goeij, AFPM Arends, JW Andersen, SN and Lovig, T Breivik, J Gaudernack, G Clausen, OPF De Angelis, P Meling, GI Rognum, TO Smith, R Goh, HS and Font, A Rosell, R Sun, XF Zhang, H Benhattar, J and Losi, L Lee, JQ Wang, ST Clarke, PA Bell, S Quirke, P Bubb, VJ Piris, J Cruickshank, NR Morton, D Fox, JC Al-Mulla, F Lees, N Hall, CN Snary, D Wilkinson, K Dillon, D Costa, J Pricolo, VE Finkelstein, SD and Thebo, JS Senagore, AJ Halter, SA Wadler, S Malik, S and Krtolica, K Urosevic, N

Abstract

Researchers worldwide with information about the Kirsten ras (Ki-ras) tumour genotype and outcome of patients with colorectal cancer were invited to provide that data in a schematized format for inclusion in a collaborative database called RASCAL (The Kirsten ras in-colorectal-cancer collaborative group). Our results from 2721 such patients have been presented previously and for the first time in any common cancer, showed conclusively that different gene mutations have different impacts on outcome, even when the mutations occur at the same site on the genome. To explore the effect of Ki-ras mutations at different stages of colorectal cancer, more patients were recruited to the database, which was reanalysed when information on 4268 patients from 42 centres in 21 countries had been entered. After predetermined exclusion criteria were applied, data on 3439 patients were entered into a multivariate analysis. This found that of the 12 possible mutations on codons 12 and 13 of Kirsten ras, only one mutation on codon 12, glycine to valine, found in 8.6% of all patients, had a statistically significant impact on failure-free survival (P = 0.004, HR 1.3) and overall survival (P = 0.008, HR 1.29). This mutation appeared to have a greater impact on outcome in Dukes’ C cancers (failure-free survival. P = 0.008, HR 1.5; overall survival P = 0.02, HR 1.45) than in Dukes’ B tumours (failure-free survival, P = 0.46, HR 1.12; overall survival P = 0.36, HR 1.15). Ki-ras mutations may occur early in the development of pre-cancerous adenomas in the colon and rectum. However, this collaborative study suggests that not only is the presence of a codon 12 glycine to valine mutation important for cancer progression but also that it may predispose to more aggressive biological behaviour in patients with advanced colorectal cancer. (C) 2001 Cancer Research Campaign.

Published

2001

3. C-fos and c-myc modulation, mitogenic effect and Ia expression in the P388D1 murine macrophage line treated by immunomodifiers

Author

Le Discorde, Magali, Le Garrec, Y. C., Jullian, E. H., Michel, P. J., Pompidou, A. J., Laboratoire Histologie, Cytogénétique et Institut de Pathologie Moléculaire, Université Paris Descartes - Paris 5 (UPD5), and Le Discorde, Magali

Subjects

DNA Replication, Lipopolysaccharides, Genes, MHC Class II, Genes, myc, MESH: Adjuvants, Immunologic, MESH: DNA Replication, MESH: Genes, fos, Interferon-gamma, Mice, Adjuvants, Immunologic, MESH: Endotoxins, Tumor Cells, Cultured, [SDV.BBM] Life Sciences [q-bio]/Biochemistry, Molecular Biology, Animals, MESH: Animals, [SDV.BBM]Life Sciences [q-bio]/Biochemistry, Molecular Biology, MESH: Tumor Cells, Cultured, MESH: Mice, MESH: Tetradecanoylphorbol Acetate, MESH: Genes, myc, Leukemia P388, Genes, fos, MESH: Macrophage Activation, MESH: Gene Expression Regulation, Neoplastic, Macrophage Activation, Recombinant Proteins, MESH: Genes, MHC Class II, Endotoxins, Gene Expression Regulation, Neoplastic, MESH: Interferon-gamma, Recombinant, MESH: Leukemia P388, Tetradecanoylphorbol Acetate, MESH: Lipopolysaccharides

Abstract

The aim of the present study was to investigate whether the early modulation of the c-fos and c-myc oncogenes could give some orientation to the impact of immunomodulators on the monocyte-macrophage lineage. In order to work in a homogeneous system we used the P388D1 mouse macrophage cell-line which is considered as an almost mature macrophage. When P388D1 cells were stimulated by LPS, interferon-gamma or the association of both compounds, no direct correlation could be found between the modulation of DNA synthesis and the early expression of the c-fos and c-myc oncogenes. The positive regulation of Ia antigen expression seemed to correlate with the absence of induction of c-fos oncogene.

Published

1992

4. Identification of water-soluble gamma-glutamyl-Se-methylselenocysteine in yeast-based selenium supplements by reversed-phase HPLC with ICP-MS and electrospray tandem MS detection

Author

Heidi Goenaga Infante, Ruth Hearn, Gavin O'Connor, Raimund Wahlen, Margaret P. Rayman, Jullian E. Spallholz, and Tim Catterick

Subjects

Electrospray, Aqueous solution, Chromatography, Formic acid, chemistry.chemical_element, Reversed-phase chromatography, High-performance liquid chromatography, Yeast, Analytical Chemistry, chemistry.chemical_compound, chemistry, Yeast extract, Spectroscopy, Selenium

Abstract

Identification of gamma-glutamyl-Se-methylselenocysteine (γ-glutamyl-SeMC) in water-soluble yeast fractions was accomplished by on-line reversed-phase (RP) HPLC with ICP-MS and electrospray ionisation (ESI) tandem MS. The sample was leached with water using accelerated solvent extraction (ASE) and the aqueous extracts were directly analysed using on-line RP HPLC-ICP-MS. HPLC was carried out with 0.1% formic acid in methanol–water (2 + 98, v/v) solution. Se-specific detection of the chromatographic effluent by ICP-MS allowed identification of γ-glutamyl-SeMC on the basis of comparison of retention times with a matching standard. Aqueous extracts of three different Se–yeast supplements (1291, 1550 and 1983 μg g−1 Se in the dry sample) were analysed by HPLC-ICP-MS for their γ-glutamyl-SeMC content (as Se). A significant variation of the Se speciation in the water extracts appeared to occur with an increase in the total Se concentration from 1550 to 1983 μg g−1. Apparently, the contribution of water-soluble SeMC and selenomethionine (SeMet) increased whereas the contribution of Se incorporated into γ-glutamyl-SeMC decreased with the increasing total Se content. Verification of the presence of γ-glutamyl-SeMC in the water-soluble yeast extract, on the basis of molecular mass determination for the [M + H]+ 80Se ions (m/z 313) and detection of its product ions using on-line RP HPLC-ESI-MS/MS, is reported here for the first time. This was achieved without the need for a cleanup of the aqueous yeast extract. The presence of γ-glutamyl-SeMC might be relevant to the anticarcinogenic potential of selenised yeast since this species is believed to serve primarily as a carrier of SeMC, which appears to be easily converted in animals and possibly humans to methylselenol. This Se metabolite is thought to be an effective anticarcinogen.

Published

2005

5. [Role of human papillomavirus in esophageal carcinogenesis]

Author

ROBERT BENAMOUZIG and Jullian E

Subjects

Esophageal Neoplasms, Humans, Cell Transformation, Viral, Immunohistochemistry, Papillomaviridae, In Situ Hybridization

6. A PRKAR1A Mutation Associated with Primary Pigmented Nodular Adrenocortical Disease in 12 Kindreds

Author

Fernande René-Corail, E. Jullian, Philippe Chanson, Bernard Conte-Devolx, Xavier Bertagna, Alfonso Gentil, Miguel Lucas, Frédérique Tissier, J. Aidan Carney, Anelia Horvath, Hervé Lefebvre, Constantine A. Stratakis, Jérôme Bertherat, Sosipatros Boikos, Fritz-Line Cephise-Velayoudom, Marie-Christine Vantyghem, Lionel Groussin, Carl D. Malchoff, [Groussin,L, Jullian,E, Rene-Corail,F, Tissier,F, Bertagna,X, Bertherat,J] Institut National de la Santé et de la Recherche Médicale, Centre National de la Recherche Scientifique Unité Mixte de Recherche. Institut Cochin, Université René-Descartes, Paris, France. [Groussin,L, Bertherat,J] Department of Endocrinology, Centre de Référence Maladies Rares de la Surrénale, Hôpital Cochin, Paris, France. [Horvath,A, Boikos,S, Stratakis,CA] Section on Endocrinology and Genetics, Developmental Endocrinology Branch, National Institute of Child Health and Human Development, National Institutes of Health, Bethesda, Maryland. [Lefebvre,H] Department of Endocrinology, Centre Hospitalier Universitaire de Rouen, France.[Cephise-Velayoudom,FL, Vantyghem,MC] Department of Endocrinology, Clinique Marc Linquette-Centre Hospitalier Universitaire, Lille, France. [Chanson,P] Department of Endocrinology, Kremlin Bicetre, France. [Conte-Devolx,B] Department of Endocrinology, Hôpital de la Timone Marseille, France. [Lucas,M] Department of Molecular Biology Hospital Universitario Virgen Macarena, Seville, Spain. [Gentil,A] Department of Endocrinology, Hospital Universitario Virgen Macarena, Seville, Spain.[Malchoff,CD] Department of Medicine, University of Connecticut Health Center, Farmington, Connecticut. [Tissier,F] Department of Pathology , Hôpital Cochin, Paris, France. [Carney,JA] Emeritus Staff, Department of Laboratory Medicine and Pathology, Mayo Clinic, Rochester, Minnesota., and This work was supported by the Groupement d’Intérêt Scientifique-Institut National de la Santé et de la Recherche Médicale Institut des Maladies Rares and the Plan Hospitalier de Recherche Clinique (AOM 02068 to the Comete Network coordinated by Professor P. F. Plouin), and in part by National Institutes of Health intramural project Z01-HD- 000642-04 (to C.A.S.).

Subjects

Male, Pathology, Endocrinology, Diabetes and Metabolism, Clinical Biochemistry, Penetrance, Diseases::Endocrine System Diseases::Adrenal Gland Diseases::Adrenocortical Hyperfunction::Cushing Syndrome [Medical Subject Headings], Chemicals and Drugs::Enzymes and Coenzymes::Enzymes::Transferases::Phosphotransferases::Phosphotransferases (Alcohol Group Acceptor)::Protein Kinases::Protein-Serine-Threonine Kinases::Cyclic Nucleotide-Regulated Protein Kinases::Cyclic AMP-Dependent Protein Kinases::Cyclic AMP-Dependent Protein Kinase Type I::Cyclic AMP-Dependent Protein Kinase RIalpha Subunit [Medical Subject Headings], Biochemistry, Cushing syndrome, Chemicals and Drugs::Heterocyclic Compounds::Heterocyclic Compounds, 1-Ring::Piperidines::Piperidones::Cycloheximide [Medical Subject Headings], Endocrinology, Cycloheximide, PRKAR1A, Cushing Syndrome, Cells, Cultured, Protein Synthesis Inhibitors, PRKAR1A Gene Mutation, primary pigmented nodular adrenocortical, Founder Effect, Pedigree, Phenotype, Mutation (genetic algorithm), Female, Phenomena and Processes::Genetic Phenomena::Genotype [Medical Subject Headings], Adrenal Cortex Diseases, Adult, medicine.medical_specialty, Adolescent, Genotype, Cyclic AMP-Dependent Protein Kinase RIalpha Subunit, Context (language use), Biology, Chemicals and Drugs::Enzymes and Coenzymes::Enzymes::Transferases::Phosphotransferases::Phosphotransferases (Alcohol Group Acceptor)::Protein Kinases::Protein-Serine-Threonine Kinases::Cyclic Nucleotide-Regulated Protein Kinases::Cyclic AMP-Dependent Protein Kinases [Medical Subject Headings], Internal medicine, medicine, Humans, RNA, Messenger, Diseases::Endocrine System Diseases::Adrenal Gland Diseases::Adrenal Cortex Diseases [Medical Subject Headings], Carney complex, disease, Biochemistry (medical), DNA, Chemicals and Drugs::Nucleic Acids, Nucleotides, and Nucleosides::Nucleic Acids::RNA::RNA, Messenger [Medical Subject Headings], medicine.disease, Phenomena and Processes::Genetic Phenomena::Founder Effect [Medical Subject Headings], Cyclic AMP-Dependent Protein Kinases, Introns, Haplotypes, Anatomy::Cells::Cells, Cultured [Medical Subject Headings], Mutation, mutation, Primary pigmented nodular adrenocortical disease

Abstract

CONTEXT: Primary pigmented nodular adrenocortical disease (PPNAD), a rare cause of corticotropin-independent Cushing syndrome, can be part of Carney complex (CNC), an autosomal dominant multiple neoplasia syndrome characterized by spotty skin pigmentation, cardiac myxomas, and endocrine tumors or be isolated (i). Germline PRKAR1A-inactivating mutations have been observed in both CNC and iPPNAD, but with no apparent genotype-phenotype correlation. OBJECTIVE:The objectives of the study were a detailed phenotyping for CNC manifestations in 12 kindreds bearing the same PRKAR1A mutation and a study of the consequences of the mutation and a potential founder effect. DESIGN: The study consisted of descriptive case reports. SETTING: The study was conducted at two referral centers. PATIENTS: The patients described in this study were referred for PRKAR1A gene mutation analysis because of a diagnosis of apparently iPPNAD. RESULTS: We describe a 6-bp polypyrimidine tract deletion [exon 7 IVS del (-7-->-2)] in 12 unrelated kindreds that were referred for Cushing syndrome due to PPNAD. Nine of the patients had no family history; in two, there was a family history of iPPNAD. Only one patient met the criteria for CNC. Relatives carrying the same mutation had no manifestations of CNC or PPNAD, suggesting a low penetrance of this PRKAR1A defect. A founder effect was excluded by extensive genotyping of chromosome 17 markers. CONCLUSIONS: In conclusion, a small intronic deletion of the PRKAR1A gene is a low-penetrance cause of mainly iPPNAD; it is the first PRKAR1A genetic defect to have an association with a specific phenotype. Yes

Published

2006

7. Kirsten ras mutations in patients with colorectal cancer: the 'RASCAL II' study

Author

J. Breivik, E. Jullian, Nicholas J. Hawkins, S. A. Halter, J. S. Thebo, Viviana Bazan, C. Troungos, Deborah A. Dillon, R. Glaesener, P.M. De Angelis, C. Valavanis, J. C. Fox, R. Smith, C. Faber, Y. Ono, K. Wilkinson, Hong Zhang, Jenq Chang Lee, N. Urosevic, Vivien J. Bubb, K. Krtolica, Jacqui Oates, Pierre Laurent-Puig, Toshifumi Ohkusa, Takahiro Fujimori, D. P. O'Donoghue, K. Omura, Paul A. Clarke, Ingrid Hoffmann, A. R. Norman, M. Pauly, Jose Costa, S T Yuen, David Cunningham, H S Goh, V. E. Pricolo, Sandra M. Bell, Shan Tair Wang, Anthony J. Senagore, Oliver Müller, N. R. Cruickshank, P. Jandik, Jwc Ho, M. Tanaka, G. I. Meling, T. O. Rognum, S Malik, Walter Giaretti, J. Piris, Robyn L. Ward, A. Rapallo, H. M. Rabes, A. Font, N. Lees, C. N. Hall, C. T. Croke, S. N. Andersen, Robert Benamouzig, Rafael Rosell, Jan-Willem Arends, S. Wadler, T. Azuma, S. D. Finkelstein, D. Snary, Barry Iacopetta, Dion Morton, Sylviane Olschwang, Fahd Al-Mulla, Gustav Gaudernack, Antonio Russo, C. Zietz, Xiao-Feng Sun, H J N Andreyev, T. Walsh, Philip Quirke, T. Lovig, M. Beranek, B. R. Dix, J. Young, Ole Petter F. Clausen, L. Losi, A.F.P.M. de Goeij, J. Benhattar, Andreyev, HJN, Norman, AR, Cunningham, D, Oates, J, Dix, BR, Iacopetta, BJ, Young, J, Walsh, T, Ward, R, Hawkins, N, Beranek, M, Jandik, P, Benamouzig, R, Jullian, E, Laurent-Puig, P, Olschwang, S, Muller, O, Hoffmann, I, Rabes, HM, Zietz, C, Troungos, C, Valavanis, C, Yuen, ST, Ho, JWC, Croke, CT, O’Donoghue, DP, Giaretti, W, Rapallo, A, Russo, A, Bazan, V, Tanaka, M, Omura, K, Azuma, T, Ohkusa, T, Fujimori, T, Ono, Y, Pauly, M, FabeR, C, Glaesener, R, de Goeij, AFPM, Arends, JW, Andersen, SN, Lövig, T, Breivik, J, Gaudernack, G, Clausen, OPF, De Angelis, P, Meling, GI, Rognum, TO, Smith, R, Goh, H-S, Font, A, Rosell, R, Sun, XF, Zhang, H, Benhattar, J, Losi, L, Lee, JQ, Wang, ST, Clarke, PA, Bell, S, Quirke, P, Bubb, VJ, Piris, J, Cruickshank,NR, Morton, D, Fox, JC, Al-Mulla, F, Lees, N, Hall, CN, Snary, D, K Wilkinson, VJ, Dillon, D, Costa, J, Pricolo, VE, Finkelstein, SD, Thebo, JS, Senagore, AJ, Halter, SA, Wadler, S, Malik, S, Krtolica, K, and Urosevic, N

Subjects

Male, Oncology, Cancer Research, Pathology, Multivariate analysis, Databases, Factual, Settore MED/06 - Oncologia Medica, Colorectal cancer, Gene mutation, medicine.disease_cause, 0302 clinical medicine, Genotype, Colorectal cancer, Ki-ras, mutation, Registries, Aged, 80 and over, 0303 health sciences, Mutation, Valine, Middle Aged, 3. Good health, KRAS Mutation Analysis, medicine.anatomical_structure, Presented by the Kirsten ras in-colorectal-cancer collaborative group, 030220 oncology & carcinogenesis, Female, Colorectal Neoplasms, Adult, medicine.medical_specialty, Adolescent, overall survival, Mutation, Missense, Rectum, colorectal cancer, Disease-Free Survival, 03 medical and health sciences, Internal medicine, medicine, Humans, Point Mutation, K-ras, Codon, prognosis, Aged, Neoplasm Staging, Proportional Hazards Models, 030304 developmental biology, business.industry, Cancer, medicine.disease, Survival Analysis, Genes, ras, Multivariate Analysis, business

Abstract

Researchers worldwide with information about the Kirsten ras (Ki-ras) tumour genotype and outcome of patients with colorectal cancer were invited to provide that data in a schematized format for inclusion in a collaborative database called RASCAL (The Kirsten ras in-colorectal-cancer collaborative group). Our results from 2721 such patients have been presented previously and for the first time in any common cancer, showed conclusively that different gene mutations have different impacts on outcome, even when the mutations occur at the same site on the genome. To explore the effect of Ki-ras mutations at different stages of colorectal cancer, more patients were recruited to the database, which was reanalysed when information on 4268 patients from 42 centres in 21 countries had been entered. After predetermined exclusion criteria were applied, data on 3439 patients were entered into a multivariate analysis. This found that of the 12 possible mutations on codons 12 and 13 of Kirsten ras, only one mutation on codon 12, glycine to valine, found in 8.6% of all patients, had a statistically significant impact on failure-free survival (P = 0.004, HR 1.3) and overall survival (P = 0.008, HR 1.29). This mutation appeared to have a greater impact on outcome in Dukes’ C cancers (failure-free survival, P = 0.008, HR 1.5; overall survival P = 0.02, HR 1.45) than in Dukes’ B tumours (failure-free survival, P = 0.46, HR 1.12; overall survival P = 0.36, HR 1.15). Ki-ras mutations may occur early in the development of pre-cancerous adenomas in the colon and rectum. However, this collaborative study suggests that not only is the presence of a codon 12 glycine to valine mutation important for cancer progression but also that it may predispose to more aggressive biological behaviour in patients with advanced colorectal cancer. © 2001 Cancer Research Campaign http://www.bjcancer.com