Search

Your search keyword '"J F, Prud'homme"' showing total 12 results
Start Over Author "J F, Prud'homme"
12 results on '"J F, Prud'homme"'

1. Noninherited maternal antigens do not play a role in rheumatoid arthritis susceptibility in Europe. European Consortium on Rheumatoid Arthritis Families

Author

P, Barrera, A, Balsa, H, Alves, R, Westhovens, K, Maenaut, F, Cornélis, P, Fritz, T, Bardin, G, de Almeida, A, Lopes-Vaz, D, Pascual Salcedo, E G, de la Concha, T R, Radstake, L B, van de Putte, P, Migliorini, J F, Prud'homme, D, Charron, M, Spyropoulou, A, Mendes, M, Spaepen, M, Martinez, V, Lepage, and C, Stravopoulos

Subjects
Adult, Arthritis, Rheumatoid, Cohort Studies, Europe, Family Health, Male, Histocompatibility Testing, Prevalence, Humans, Female, HLA-DR Antigens, Alleles, Netherlands
Abstract

It has been proposed that noninherited maternal antigens (NIMA) (HLA-DR antigens) might play a role in susceptibility to rheumatoid arthritis (RA), especially in patients who are not genetically predisposed, such as those who are HLA-DR4 and/or shared epitope (SE) negative. The present study was undertaken to test the NIMA hypothesis in a large cohort of European RA patients assembled by the European Consortium on RA Families (ECRAF).HLA-DRB1 oligotyping was performed in families of European RA patients for whom both parents were alive. These families were consecutively recruited by the ECRAF between 1996 and 1998, for association studies. The frequencies of HLA-DR NIMA were compared with those of the noninherited paternal antigens (NIPA) after stratification for HLA-DR*04, *0401 and/or *0404, and SE status. NIMA or NIPA that coincided with inherited HLA-DR antigens were considered redundant and excluded from analysis. Calculations concerning the whole group and restricted to patients lacking parental RA were performed.One hundred seventy families from France (n = 81), Belgium (n = 23), Spain (n = 24), Italy (n = 19), Portugal (n = 14), and The Netherlands (n = 9) were oligotyped. The group of probands was predominantly female (88%), positive for rheumatoid factor, DR*04, and SE (71%, 58%, and 75%, respectively), and had erosive disease (75%). Parental RA was reported in 21 families. Using the NIPA as control, the frequency of HLA-DRB1*04, *0401 and/or *0404-, or SE-positive NIMA was not found to be increased in patients lacking these susceptibility alleles. The same was true when the 21 probands with parental RA were excluded from analysis. In DRB1*04-positive patients, we found no evidence of a relevant effect of HLA-DR3 or DR6 in the NIMA.Our results do not support the notion that noninherited maternal antigens have a role in susceptibility to RA in the offspring.

Published
2000

2. Autosomal dominant lateral temporal epilepsy: clinical and genetic study of a large Basque pedigree linked to chromosome 10q

Author

J J, Poza, A, Sáenz, A, Martínez-Gil, N, Cheron, A M, Cobo, M, Urtasun, J F, Martí-Massó, D, Grid, J S, Beckmann, J F, Prud'homme, and A, López de Munain

Subjects
Male, Epilepsy, Temporal Lobe, Genotype, Chromosomes, Human, Pair 10, Genetic Linkage, Humans, Female, Lod Score, Functional Laterality, Pedigree
Abstract

We report a large family with a temporal partial epilepsy syndrome inherited in an autosomal dominant mode, with a penetrance of about 80%. This epilepsy syndrome is benign, with age of onset in the second or third decade of life. It is characterized by rare partial seizures, usually secondarily generalized, arising mostly during sleep, without postictal confusion. There is a good response to the antiepileptic therapy but often a recurrence of seizures after drug withdrawal. The partial component, visual (lights, colors, and simple figures) or auditory (buzzing or "humming like a machine"), the existence of temporo-occipital interictal electroencephalographic epileptiform abnormalities, and the hypoperfusion in the temporal lobe detected by interictal hexamethylpropyleneamine oxime-technetium 99m (HMPAO-Tc99m) single-photon emission computed tomography, strongly suggest a lateral temporal lobe origin. The genetic analysis found linkage to chromosome 10q, and localized a gene in a 15-cM interval that overlaps a previously found localization for partial epilepsy in a large three-generation family. This syndrome could be called autosomal dominant lateral temporal epilepsy.

Published
1999

3. [Clinical and molecular genetic analysis of 4 Swiss families with the pure form of hereditary spastic spinal paralysis]

Author

J, von Fellenberg, C, Paternotte, J F, Prud'homme, J, Weissenbach, J, Hazan, and J M, Burgunder

Subjects
Adult, Aged, 80 and over, Chromosome Aberrations, Male, Spastic Paraplegia, Hereditary, Chromosome Disorders, Middle Aged, Spinal Cord Diseases, Pedigree, Haplotypes, Humans, Paralysis, Female, Molecular Biology, Switzerland, Aged
Abstract

Hereditary spastic paraplegia (HSP) is a rare neurodegenerative disease of the spinal cord with a progressive gait disorder, associated with other neurological abnormalities in the complicated form. A cluster of families with this disorder in the central part of the country has long been known to Swiss neurologists. In the present report, we describe our clinical and molecular findings in four large families originating from this region and suffering from a pure HSP form. Clinical presentation was similar in the four families. The age of onset varied widely from 2 to 70 years with the appearance of a gait disorder, which slowly progressed to wheelchair confinement after 30-70 years. No other neurological abnormality was found except for impairment of the vibration sense and sphincter abnormalities. In three families an association with markers of the SPG4 locus on chromosome 2 was found. In the fourth, the largest one, no linkage could be found with either SPG4, or with the other two known loci, SPG3 on chromosome 14 and SPG6 on chromosome 15. These data demonstrate the genetic heterogeneity in HSP, even in families from the same region. They also suggest the presence of at least one additional locus for the pure form.

Published
1998

4. Association of rheumatoid arthritis with an amino acid allelic variation of the T cell receptor

Author

François Cornelis, J F Prud'homme, Dominique Charron, A Nicod, K Pile, R.M. Flipo, D Kuntz, B P Wordsworth, M N Loste, S Walsh, T H Tran, P.M. Danzé, A Delaye, J Weissenbach, Thomas Bardin, S. Djoulah, L Hardwick, K Gibson, Maria Martinez, Virginia Lepage, Frédéric Lioté, and Sandra Lasbleiz

Subjects
Genotype, Receptors, Antigen, T-Cell, alpha-beta, Immunology, Biology, Arthritis, Rheumatoid, Rheumatology, Genetic variation, medicine, Immunology and Allergy, Humans, Pharmacology (medical), Genetic Predisposition to Disease, Allele, Alleles, Polymorphism, Single-Stranded Conformational, Case-control study, Genetic Variation, Single-strand conformation polymorphism, Odds ratio, medicine.disease, Rheumatoid arthritis, Case-Control Studies, Female, Restriction fragment length polymorphism
Abstract

Objective. To investigate allelic variations of T cell receptor residues for a contribution to rheumatoid arthritis (RA) susceptibility. Methods. We conducted an RA case-control study involving 1,579 northwest Europeans: 766 patients with erosive and rheumatoid factor-positive disease and 813 control subjects. Productive changes of segments TCRAV6S1, TCRAV7S1, TCRAV8S1, TCRAV10S2, and TCRBV6S1, TCRBV6S7 were investigated by single-strand conformation polymorphisms. The TCRAV8S1 association was confirmed by restriction fragment length polymorphism. Results. In the systematic study (77 patients and 119 controls), an increase in 1 TCRAV8S1 genotype was found in the RA patients (P = 0.0004). This finding was replicated in 2 further populations, one from France (212 patients and 254 controls) and the other from Britain (477 patients and 440 controls), with a similar odds ratio (OR), which allowed pooling of the data and confirmation of the association (OR 1.3 [95% confidence interval 1.1-1.7], P = 0.008). Conclusion. These findings show evidence that TCRA is an RA susceptibility locus.

Published
1997

5. Enzyme-linked immunosorbent assay of pS2 in breast cancers, benign tumors, and normal breast tissues. Correlation with prognosis and adjuvant hormone therapy

Author

J, Predine, F, Spyratos, J F, Prud'homme, C, Andrieu, K, Hacene, M, Brunet, C, Pallud, and E, Milgrom

Subjects
Adult, Aged, 80 and over, Ovariectomy, Tumor Suppressor Proteins, Proteins, Breast Neoplasms, Enzyme-Linked Immunosorbent Assay, Middle Aged, Prognosis, Combined Modality Therapy, Survival Analysis, Neoplasm Proteins, Breast Diseases, Tamoxifen, Antineoplastic Combined Chemotherapy Protocols, Multivariate Analysis, Humans, Female, Trefoil Factor-1, Breast, Aged
Abstract

An enzyme-linked immunosorbent assay using monoclonal and polyclonal antibodies against recombinant pS2 was devised. It was used to measure pS2 concentration in the cytosol of 339 breast cancer, 15 fibroadenomas, 16 cases of benign breast disease, and 6 normal breast tissues. The mean value of pS2 concentration was higher in cancer, but the protein could be detected readily in benign tumors and even in normal breast. The concentration of pS2 was significantly lower in postmenopausal women and tumors of differentiation Grade 3. The pS2 concentration was correlated strongly with the presence of estrogen receptors (ER) and progesterone receptors (PR). No correlation was observed with the size, histologic type of the tumor, and lymph node status. The prognostic value of pS2 appeared relatively limited. It was clear cut only for a relatively small group of patients (approximately 15%), who had low concentrations of pS2 (less than or equal to 0.32 ng/mg of protein). These patients had a shorter disease-free interval and overall survival time. The most striking correlation was observed with the outcome of adjuvant hormone therapy. pS2 concentration was shown to be the most potent prognostic factor, preceding even ER.

Published
1992

6. Modulation of proliferation, estradiol receptors and estrogen regulated protein PS2/BCEI in human breast cancer cell lines by gamma interferon

Author

E, Solary, J F, Prud'homme, C, Gauville, H, Magdelenat, and F, Calvo

Subjects
Tumor Suppressor Proteins, Proteins, Breast Neoplasms, Receptors, Estradiol, Recombinant Proteins, Cell Line, Neoplasm Proteins, Interferon-gamma, Serine, Tumor Cells, Cultured, Humans, Female, Trefoil Factor-1, RNA, Messenger, RNA, Neoplasm, Uridine, Cell Division
Abstract

The effects of recombinant gamma interferon (IFN gamma) on proliferation, estrogen-receptor (ER) content, mRNA level and protein secretion of a breast cancer estrogen-induced protein pS2/BCEI were investigated in two human breast cancer cell lines, ZR75-1 and T47D. Both cell lines have estrogen and progesterone receptors and previously showed HLA class I and class II responses to IFN gamma (Int J Cancer 1990; 45: 1169). An antiproliferative effect of IFN gamma (1000-5000 U/ml) was observed in serum containing medium on ZR75-1 but not on T47D cells. Noninhibitory concentration of IFN gamma (100 U/ml) had sensitising antiproliferative effect with antiestrogens on ZR75-1 cells whereas IFN gamma did not modify the growth inhibition observed in T47D cells with antiestrogens. In serum-free, estradiol-free, phenol-red-free chemically defined medium (Cancer Res 1984; 44: 4553), IFN gamma abolished in ZR75-1 but not in T47D the 30% growth stimulation induced by estradiol. In ZR75-1 cells, IFN gamma induced a transitory 30-50% increase of ER content, as measured by ER-enzymoimmunoassay, at day 2 of culture, and reduced mRNA level and secretion of pS2/BCEI. In T47D cells, a 30-50% decrease of ER content was observed but only when cells were long term cultured (30 weeks) with IFN gamma. In this cell line, no transcription of pS2/BCEI was observed. Antiproliferative action of IFN gamma on ZR75-1 cells is associated with an inhibition of estradiol effects and a reduction of pS2/BCEI mRNA level and protein secretion.

Published
1991

7. Monoclonal antibodies against native ant denatured forms of estrogen-induced breast cancer protein (BCEI/pS2) obtained by expression in Escherichia coli

Author

J F, Prud'homme, A, Jolivet, M F, Pichon, J F, Savouret, and E, Milgrom

Subjects
Protein Denaturation, Recombinant Fusion Proteins, Blotting, Western, Genetic Vectors, Antibodies, Monoclonal, Breast Neoplasms, DNA, Neoplasm, Immunohistochemistry, Antibodies, Chromatography, Affinity, Cell Line, Neoplasm Proteins, Escherichia coli, Humans, Female, Chromosome Deletion
Abstract

Several vectors were used to express the complementary DNA for breast cancer estrogen-induced protein BCEI (also called pS2) in Escherichia coli. The best results were obtained by using the pUR 290 expression vector after deletion of the sequence encoding the signal peptide of the protein. In these conditions, beta-galactosidase-BCEI/pS2 fusion protein accounted for approximately 20% of total proteins in bacterial extracts. It was purified by chromatography on DEAE-Trisacryl or by gel electrophoresis and electroelution. Polyclonal antibodies were obtained by immunization of rabbits and goats, and monoclonal antibodies were raised in mice. Two types of monoclonal antibodies were obtained: one class recognized the native protein and was very efficient for the immunoprecipitation and immunopurification of the protein from breast cancer cells; a second class recognized the denatured protein and was especially effective for immunoblot studies. BCEI/pS2 could be detected by immunocytochemistry in breast cancer biopsies using monoclonal antibodies on frozen or paraffin-embedded sections. One of the antibodies (mBCEI11) exhibited high affinity for the protein and could be used at 1.9 micrograms/ml concentration for immunolabeling of histological sections. The mBCEI11 antibody was used in immunoaffinity chromatography to purify the peptide in a single step from culture media of estrogen-treated MCF-7 cells.

Published
1990

8. Rheumatoid arthritis association with alleles of T-cell receptor α chain is influenced by HLA

Author

F. Liote, P.M. Danzé, R.M. Flippo, T H Tran, J F Prud'homme, K. Dzanouni, H. Zouali, I. Fajardy, Dominique Charron, D. Kuntz, M.N. Loste, Bardin T, J Weissenbach, P. Froguel, A Delaye, F. Cornélis, F. Didailler-Lambert, and Virginia Lepage

Subjects
Rheumatoid arthritis, Immunology, T-cell receptor, medicine, Immunology and Allergy, General Medicine, Human leukocyte antigen, Allele, Biology, medicine.disease
Published
1996
Full Text
View/download PDF

11. [Steroid hormone receptors in benign breast diseases]

Author

S, Fournier, J F, Prud'homme, P M, Martin, and F, Kuttenn

Subjects
Breast Diseases, Receptors, Steroid, Receptors, Estrogen, Humans, Breast Neoplasms, Female, Receptors, Estradiol, Adenofibroma, Receptors, Progesterone, Epithelium, Menstruation
Abstract

Benign breast diseases generally occur in women with progesterone insufficiency and an unopposed estrogen status. This hormonal imbalance is also a main risk factor for breast cancer in the long run. The presence of estradiol and progesterone receptors in benign breast disease are additional proof of their hormone dependence. The level of receptors is higher when the epithelial cellularity is high and also in more recent lesions, and younger women. The level and subcellular location of the receptors also depend on the endogenous secretion of steroids: their level varies throughout the menstrual cycle, and it is maximal at the end of the follicular phase, due to the high estradiol secretion. The cytosol and nuclear level and location of the receptors are also modified by hormonal therapy: estrogen-progestagens given as a contraceptive, or progestins given as a substitutive and antiestrogen therapy. These modifications constitute a biochemical basis for the hormonal progestagen treatment of benign breast diseases.

Published
1983

12. Spectrum of SPG4 mutations in autosomal dominant spastic paraplegia

Author

N, Fonknechten, D, Mavel, P, Byrne, C S, Davoine, C, Cruaud, D, Bönsch, D, Boentsch, D, Samson, P, Coutinho, M, Hutchinson, P, McMonagle, J M, Burgunder, A, Tartaglione, O, Heinzlef, I, Feki, T, Deufel, N, Parfrey, A, Brice, B, Fontaine, J F, Prud'homme, J, Weissenbach, A, Dürr, and J, Hazan

Subjects
Adult, Spastin, Adolescent, Genotype, Hereditary spastic paraplegia, RNA Splicing, Molecular Sequence Data, Mutation, Missense, Locus (genetics), Biology, medicine, Genetics, Missense mutation, Humans, Child, Gene, Molecular Biology, Genetics (clinical), Microtubule severing, Aged, Genes, Dominant, Adenosine Triphosphatases, Paraplegia, Polymorphism, Genetic, Genetic heterogeneity, General Medicine, Middle Aged, medicine.disease, Phenotype, Codon, Nonsense, Mutation, Asymptomatic carrier
Abstract

Autosomal dominant hereditary spastic paraplegia (AD-HSP) is a group of genetically heterogeneous neurodegenerative disorders characterized by pro- gressive spasticity of the lower limbs. Five AD-HSP loci have been mapped to chromosomes 14q, 2p, 15q, 8q and 12q. The SPG4 locus at 2p21-p22 has been shown to account for approximately 40% of all AD-HSP families. SPG4 encoding spastin, a putative nuclear AAA protein, has recently been identified. Here, sequence analysis of the 17 exons of SPG4 in 87 unrelated AD-HSP patients has resulted in the detection of 34 novel mutations. These SPG4 mutations are scattered along the coding region of the gene and include all types of DNA modification including missense (28%), nonsense (15%) and splice site point (26.5%) mutations as well as deletions (23%) and insertions (7.5%). The clinical analysis of the 238 mutation carriers revealed a high proportion of both asymptomatic carriers (14/238) and patients unaware of symptoms (45/238), and permitted the redefinition of this frequent form of AD-HSP.

Catalog

Books, media, physical & digital resources
See catalog results