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387 results on '"Gershoni-Baruch R"'

4. EPG5-related Vici syndrome defines a new group of multisystem disorders due to defects in membrane trafficking and autophagy

Author

BYRNE, S, U-KING-IM, J M, BODI, I, DIONISI-VICI, C, AL-GAZALI, L, AL-OWAIN, M, BROWN, N J, EL-GARHI, R, GERSHONI-BARUCH, R, FILLOUX, F, KAMATH, A, KOELKER, S, MANCHESTER, D, MANZUR, A, MANDEL, H, MEIN, R, MIYATA, R, PILZ, D, ROGERS, C C, RYAN, M, SAID, E, SCHARA, U, STEIN, A, SEWRY, C A, TRAVAN, L, WIJBURG, F A, YAU, S, FANTO, M, GAUTEL, M, and JUNGBLUTH, H

Published
2015

5. Multicenter analysis of glucocerebrosidase mutations in Parkinson's disease

Author

Sidransky, E., Nalls, M.A., Aasly, J.O., Aharon-Peretz, J., Annesi, G., Barbosa, E.R., Bar-Shira, A., Berg, D., Bras, J., Brice, A., C.-M. Chen, Clark, L.N., Condroyer, C., De Marco, E.V., Eblan, M.J., Fahn, S., Farrer, M.J., Durr, A., H.-C. Fung, Gan-Or, Z., Gasser, T., Gershoni-Baruch R., Giladi, N., Griffith, A., Gurevich, T., Januario, C., Kropp, P., Lang, A.E., C.-J. Lee Chen, Lesage, S., Marder, K., Mata, I.F., Mirelman, A., Mutsui, J., Mizuta, I., Nicoletti, G., Oliveira, C., Ottman, R., Orr-Urteger, A., Pereira, L.V., Quattron, A., Spitz, M., E.-K. Tan, Tayebi, N., Toda, T., Troiano, S., Tsuji, S., Wittstock, M., Wolfsberg, T.G., Y.-R. Wu, Zabetian, C.P., Y. Zhao, and Ziegler, S.G.

Subjects
Parkinson's disease -- Risk factors, Hydrolases -- Health aspects, Enzymes -- Health aspects
Abstract

The study determines the frequency of glucocerebrosidase ("GBA") mutations in an ethnically diverse group of patients with Parkinson's disease. Findings indicate a strong relation between "GBA" mutations and Parkinson's disease.

Published
2009

18. Absence of alpha- and beta-dystroglycan is associated with Walker-Warburg syndrome

Author

Riemersma, M., Mandel, H., Beusekom, E. van, Gazzoli, I., Roscioli, T., Eran, A., Gershoni-Baruch, R., Gershoni, M., Pietrokovski, S., Vissers, L.E.L.M., Lefeber, D.J., Willemsen, M.A.A.P., Wevers, R.A., Bokhoven, H. van, Klinische Genetica, and RS: CARIM - R2 - Cardiac function and failure

Subjects
musculoskeletal diseases, congenital, hereditary, and neonatal diseases and abnormalities, Neurodevelopmental disorders Donders Center for Medical Neuroscience [Radboudumc 7], Disorders of movement Radboud Institute for Molecular Life Sciences [Radboudumc 3], Disorders of movement Donders Center for Medical Neuroscience [Radboudumc 3]
Abstract

Item does not contain fulltext OBJECTIVE: To identify the underlying genetic defect in 5 patients from a consanguineous family with a Walker-Warburg phenotype, together with intracranial calcifications. METHODS: Homozygosity mapping and exome sequencing, followed by Sanger sequencing of the obtained candidate gene, was performed. Expression of the candidate gene was tested by reverse transcription PCR. Patient fibroblasts were converted to myotubes, and the expression and function of dystroglycan was tested by Western blotting. RESULTS: We detected a homozygous loss-of-function frameshift mutation in the DAG1 gene and showed that this mutation results in a complete absence of both alpha- and beta-dystroglycan. CONCLUSIONS: A loss-of-function mutation in DAG1 can result in Walker-Warburg syndrome and is not embryonic lethal. 6 p.

Published
2015

19. EPG5-related Vici syndrome: a paradigm of neurodevelopmental disorders with defective autophagy

Author

Byrne, S, Jansen, L, U-King-Im, J-M, Siddiqui, A, Lidov, HGW, Bodi, I, Smith, L, Mein, R, Cullup, T, Dionisi-Vici, C, Al-Gazali, L, Al-Owain, M, Bruwer, Z, Al Thihli, K, El-Garhy, R, Flanigan, KM, Manickam, K, Zmuda, E, Banks, W, Gershoni-Baruch, R, Mandel, H, Dagan, E, Raas-Rothschild, A, Barash, H, Filloux, F, Creel, D, Harris, M, Hamosh, A, Koelker, S, Ebrahimi-Fakhari, D, Hoffmann, GF, Manchester, D, Boyer, PJ, Manzur, AY, Lourenco, CM, Pilz, DT, Kamath, A, Prabhakar, P, Rao, VK, Rogers, RC, Ryan, MM, Brown, NJ, McLean, CA, Said, E, Schara, U, Stein, A, Sewry, C, Travan, L, Wijburg, FA, Zenker, M, Mohammed, S, Fanto, M, Gautel, M, Jungbluth, H, Byrne, S, Jansen, L, U-King-Im, J-M, Siddiqui, A, Lidov, HGW, Bodi, I, Smith, L, Mein, R, Cullup, T, Dionisi-Vici, C, Al-Gazali, L, Al-Owain, M, Bruwer, Z, Al Thihli, K, El-Garhy, R, Flanigan, KM, Manickam, K, Zmuda, E, Banks, W, Gershoni-Baruch, R, Mandel, H, Dagan, E, Raas-Rothschild, A, Barash, H, Filloux, F, Creel, D, Harris, M, Hamosh, A, Koelker, S, Ebrahimi-Fakhari, D, Hoffmann, GF, Manchester, D, Boyer, PJ, Manzur, AY, Lourenco, CM, Pilz, DT, Kamath, A, Prabhakar, P, Rao, VK, Rogers, RC, Ryan, MM, Brown, NJ, McLean, CA, Said, E, Schara, U, Stein, A, Sewry, C, Travan, L, Wijburg, FA, Zenker, M, Mohammed, S, Fanto, M, Gautel, M, and Jungbluth, H

Abstract

Vici syndrome is a progressive neurodevelopmental multisystem disorder due to recessive mutations in the key autophagy gene EPG5. We report genetic, clinical, neuroradiological, and neuropathological features of 50 children from 30 families, as well as the neuronal phenotype of EPG5 knock-down in Drosophila melanogaster. We identified 39 different EPG5 mutations, most of them truncating and predicted to result in reduced EPG5 protein. Most mutations were private, but three recurrent mutations (p.Met2242Cysfs*5, p.Arg417*, and p.Gln336Arg) indicated possible founder effects. Presentation was mainly neonatal, with marked hypotonia and feeding difficulties. In addition to the five principal features (callosal agenesis, cataracts, hypopigmentation, cardiomyopathy, and immune dysfunction), we identified three equally consistent features (profound developmental delay, progressive microcephaly, and failure to thrive). The manifestation of all eight of these features has a specificity of 97%, and a sensitivity of 89% for the presence of an EPG5 mutation and will allow informed decisions about genetic testing. Clinical progression was relentless and many children died in infancy. Survival analysis demonstrated a median survival time of 24 months (95% confidence interval 0-49 months), with only a 10th of patients surviving to 5 years of age. Survival outcomes were significantly better in patients with compound heterozygous mutations (P = 0.046), as well as in patients with the recurrent p.Gln336Arg mutation. Acquired microcephaly and regression of skills in long-term survivors suggests a neurodegenerative component superimposed on the principal neurodevelopmental defect. Two-thirds of patients had a severe seizure disorder, placing EPG5 within the rapidly expanding group of genes associated with early-onset epileptic encephalopathies. Consistent neuroradiological features comprised structural abnormalities, in particular callosal agenesis and pontine hypoplasia, delayed myeli

Published
2016

23. A single nucleotide polymorphism in the RAD51 gene modifies cancer risk in BRCA2 but not BRCA 1 carriers

Author

Levy-Lahad, E., Lahad, A., Eisenberg, S., Dagan, E., Paperna, T., Kasinetz, L., Catane, R., Kaufman, B., Beller, U, Renbaum, P., and Gershoni-Baruch, R.

Subjects
Nucleotides -- Research, Genetic polymorphisms -- Research, Medical genetics -- Research, Cancer -- Genetic aspects, DNA repair -- Research, Disease susceptibility -- Genetic aspects, Science and technology
Abstract

BRCA 1 and BRCA2 carriers are at increased risk for both breast and ovarian cancer, but estimates of lifetime risk vary widely, suggesting their penetrance is modified by other genetic and/or environmental factors. The BRCA1 and BRCA2 proteins function in DNA repair in conjunction with RAD51. A preliminary report suggested that a single nucleotide polymorphism in the 5' untranslated region of RAD51 (135C/G) increases breast cancer risk in BRCA 1 and BRCA2 carriers. To investigate this effect we studied 257 female Ashkenazi Jewish carriers of one of the common BRCA 1 (185delAG, 5382insC) or BRCA2 (6174delT) mutations. Of this group, 164 were affected with breast and/or ovarian cancer and 93 were unaffected. RAD51 genotyping was performed on all subjects. Among BRCA 1 carriers, RAD51-135C frequency was similar in healthy and affected women [6.1% (3 of 49) and 9.9% (12 of 121), respectively], and RAD-135C did not influence age of cancer diagnosis [Hazard ratio (HR) = 1.18 for disease in RAD51-135C heterozygotes, not significant]. However, in BRCA2 carriers, RAD51-135C heterozygote frequency in affected women was 17.4% (8 of 46) compared with 4.9% (2 of 41) in unaffected women (P = 0.07). Survival analysis in BRCA2 carriers showed RAD51-135C increased risk of breast and/or ovarian cancer with an HR of 4.0 [95% confidence interval 1.6-9.8, P = 0.003]. This effect was largely due to increased breast cancer risk with an HR of 3.46 (95% confidence interval 1.3-9.2, P = 0.01) for breast cancer in BRCA2 carriers who were RAD51-135C heterozygotes. RAD51 status did not affect ovarian cancer risk. These results show RAD51-135C is a clinically significant modifier of BRCA2 penetrance, specifically in raising breast cancer risk at younger ages.

Published
2001

28. Anticipation in Familial Breast Cancer

Author

Dagan, E. and Gershoni-Baruch, R.

Subjects
Genetic research -- Analysis, Human genetics -- Research, Ashkenazim -- Diseases, Biological sciences
Published
2000

30. Timing of oral contraceptive use and the risk of breast cancer in BRCA1 mutation carriers

Author

Kotsopoulos, J, Lubinski, J, Gronwald, J, Cybulski, C, Demsky, R, Neuhausen, Sl, Kim Sing, C, Tung, N, Friedman, S, Senter, L, Weitzel, J, Karlan, B, Moller, P, Sun, P, Narod, Sa, Hereditary Breast Cancer Clinical Study Group: Lynch HT, Singer, C, Eng, C, Mitchell, G, Huzarski, T, Mccuaig, J, Hughes, K, Mills, G, Ghadirian, P, Eisen, A, Gilchrist, D, Blum, Jl, Zakalik, D, Pal, T, Daly, M, Weber, B, Snyder, C, Fallen, T, Chudley, A, Lunn, J, Donenberg, T, Kurz, Rn, Saal, H, Garber, J, Rennert, G, Sweet, K, Gershoni Baruch, R, Rappaport, C, Lemire, E, Stoppa Lyonnet, D, Olopade, Oi, Merajver, S, Bordeleau, L, Cullinane, Ca, Friedman, E, Mckinnon, W, Wood, M, Rayson, D, Meschino, W, Mclennan, J, Costalas, Jw, Reilly, Re, Vadaparampil, S, Offit, K, Kauff, N, Klijn, J, Euhus, D, Kwong, A, Isaacs, C, Couch, F, Manoukian, S, Byrski, T, Elser, C, Panchal, S, Armel, S, Nanda, S, Metcalfe, K, Poll, A, Rosen, B, Foulkes, Wd, Rebbeck, T, Ainsworth, P, Robidoux, A, Warner, E, Maehle, L, Osborne, M, Evans, G, Pasini, Barbara, Ginsburg, O, Cohen, S, Bohdan, G, Jakubowska, A, and Little, J.

Subjects
Adult, Heterozygote, Cancer Research, medicine.medical_specialty, Breast Neoplasms, Breast cancer, breast cancer, Risk Factors, medicine, Humans, Genetic Association Studies, Gynecology, Oral contraceptives, BRCA1 Protein, Obstetrics, business.industry, Age Factors, Case-control study, Cancer, Odds ratio, Middle Aged, medicine.disease, BRCA mutations, Oncology, Family planning, Case-Control Studies, Pill, Relative risk, Mutation, Female, Ovarian cancer, business, Contraceptives, Oral
Abstract

It is not clear if early oral contraceptive use increases the risk of breast cancer among young women with a breast cancer susceptibility gene 1 (BRCA1) mutation. Given the benefit of oral contraceptives for the prevention of ovarian cancer, estimating age-specific risk ratios for oral contraceptive use and breast cancer is important. We conducted a case-control study of 2,492 matched pairs of women with a deleterious BRCA1 mutation. Breast cancer cases and unaffected controls were matched on year of birth and country of residence. Detailed information about oral contraceptive use was collected from a routinely administered questionnaire. Conditional logistic regression was used to estimate the odds ratios (OR) and 95 % confidence intervals (CI) for the association between oral contraceptive and breast cancer, by age at first use and by age at diagnosis. Among BRCA1 mutation carriers, oral contraceptive use was significantly associated with an increased risk of breast cancer for women who started the pill prior to age 20 (OR 1.45; 95 % CI 1.20-1.75; P = 0.0001) and possibly between ages 20 and 25 as well (OR 1.19; 95 % CI 0.99-1.42; P = 0.06). The effect was limited to breast cancers diagnosed before age 40 (OR 1.40; 95 % CI 1.14-1.70; P = 0.001); the risk of early-onset breast cancer increased by 11 % with each additional year of pill use when initiated prior to age 20 (OR 1.11; 95 % CI 1.03-1.20; P = 0.008). There was no observed increase for women diagnosed at or after the age of 40 (OR 0.97; 95 % CI 0.79-1.20; P = 0.81). Oral contraceptive use before age 25 increases the risk of early-onset breast cancer among women with a BRCA1 mutation and the risk increases with duration of use. Caution should be taken when advising women with a BRCA1 mutation to take an oral contraceptive prior to age 25.

Published
2014

32. The impact of pregnancy on breast cancer survival in women who carry a BRCA1 or BRCA2 mutation

Author

Valentini, A, Lubinski, J, Byrski, T, Ghadirian, P, Moller, P, Lynch, Ht, Ainsworth, P, Neuhausen, Sl, Weitzel, J, Singer, Cf, Olopade, Oi, Saal, H, Lyonnet, Ds, Foulkes, Wd, Kim Sing, C, Manoukian, S, Zakalik, D, Armel, S, Senter, L, Eng, C, Grunfeld, E, Chiarelli, Am, Poll, A, Sun, P, Narod, Sa, Hereditary Breast Cancer Clinical Study Group: Gronwald, J, Cybulski, C, Huzarski, T, Robidoux, A, Offit, K, Gershoni Baruch, R, Isaacs, C, Tung, N, Rosen, B, Demsky, R, Mccuaig, J, Eisen, A, Bordeleau, L, Karlan, B, Garber, J, Gilchrist, D, Couch, F, Evans, G, Kwong, A, Maehle, L, Friedman, E, Mckinnon, W, Wood, M, Daly, M, Blum, Jl, Robson, M, Chudley, A, Panchal, S, Mclennan, J, Pasini, Barbara, Rennert, G, Lunn, J, Fallen, T, Rayson, D, Smith, M, Ginsburg, O, Lemire, E, Meschino, W, Vadaparampil, S, Euhus, D, Costalas, Jw, Donenberg, T, Kurz, Rn, Friedman, S, Sweet, K, Cullinane, Ca, Reilly, Re, Kotsopoulos, J, Nanda, S, and Metcalfe, K.

Subjects
Oncology, Cancer Research, medicine.medical_specialty, Heterozygote, Survival, Genes, BRCA2, Genes, BRCA1, Breast Neoplasms, Article, Cohort Studies, Breast cancer, Pregnancy, Risk Factors, Internal medicine, Medicine, Humans, skin and connective tissue diseases, Survival rate, business.industry, Proportional hazards model, Hazard ratio, BRCA mutation, BRCA mutations, Case-control study, medicine.disease, Case-Control Studies, Mutation, Female, business, Cohort study
Abstract

Physicians are often approached by young women with a BRCA mutation and a recent history of breast cancer who wish to have a baby. They wish to know if pregnancy impacts upon their future risks of cancer recurrence and survival. To date, there is little information on the survival experience of women who carry a mutation in one of the BRCA genes and who become pregnant. From an international multi-center cohort study of 12,084 women with a BRCA1 or BRCA2 mutation, we identified 128 case subjects who were diagnosed with breast cancer while pregnant or who became pregnant after a diagnosis of breast cancer. These women were age-matched to 269 mutation carriers with breast cancer who did not become pregnant (controls). Subjects were followed from the date of breast cancer diagnosis until the date of last follow-up or death from breast cancer. The Kaplan–Meier method was used to estimate 15-year survival rates. The hazard ratio for survival associated with pregnancy was calculated using a left-truncated Cox proportional hazard model, adjusting for other prognostic factors. Among women who were diagnosed with breast cancer when pregnant or who became pregnant thereafter, the 15-year survival rate was 91.5 %, compared to a survival of 88.6 % for women who did not become pregnant (adjusted hazard ratio = 0.76; 95 % CI 0.31–1.91; p = 0.56). Pregnancy concurrent with or after a diagnosis of breast cancer does not appear to adversely affect survival among BRCA1/2 mutation carriers.

Published
2013

33. Phenotypic spectrum and prevalence of INPP5E mutations in Joubert Syndrome and related disorders

Author

Lorena, Travaglini, Francesco, Brancati, Jennifer, Silhavy, Miriam, Iannicelli, Elizabeth, Nickerson, Nadia, Elkhartoufi, Eric, Scott, Emily, Spencer, Stacey, Gabriel, Sophie, Thomas, Bruria, Ben Zeev, Enrico, Bertini, Eugen, Boltshauser, Malika, Chaouch, Maria, Roberta Cilio, Mirjam, M. de Jong, Hulya, Kayserili, Gonul, Ogur, Andrea, Poretti, Sabrina, Signorini, Graziella, Uziel, Maha, S. Zaki, Ali Pacha, L, Zankl, A, Leventer, R, Grattan Smith, P, Janecke, A, Koch, J, Freilinger, M, D'Hooghe, M, Sznajer, Y, Vilain, C, Van Coster, R, Demerleir, L, Dias, K, Moco, C, Moreira, A, Ae Kim, C, Maegawa, G, Dakovic, I, Loncarevic, D, Mejaski Bosnjak, V, Petkovic, D, Abdel Salam GM, Abdel Aleem, A, Marti, I, Pinard, Jm, Quijano Roy, S, Sigaudy, S, de Lonlay, P, Romano, S, Verloes, A, Touraine, R, Koenig, M, Dollfus, H, Flori, E, Fradin, M, Lagier Tourenne, C, Messer, J, Collignon, P, Penzien, Jm, Bussmann, C, Merkenschlager, A, Philippi, H, Kurlemann, G, Grundmann, K, Dacou Voutetakis, C, Kitsiou Tzeli, S, Pons, R, Jerney, J, Halldorsson, S, Johannsdottir, J, Ludvigsson, P, Phadke, Sr, Girisha, Km, Doshi, H, Udani, V, Kaul, M, Stuart, B, Magee, A, Spiegel, R, Shalev, S, Mandel, H, Lev, D, Michelson, M, Idit, M, Ben Zeev, B, Gershoni Baruch, R, Ficcadenti, A, Fischetto, R, Gentile, M, Della Monica, M, Pezzani, M, Graziano, C, Seri, M, Benedicenti, F, Stanzial, F, Borgatti, R, Romaniello, R, Accorsi, P, Battaglia, S, Fazzi, E, Giordano, L, Pinelli, L, Boccone, L, Barone, R, Sorge, G, Briatore, E, Bigoni, S, Ferlini, A, Donati, Ma, Biancheri, R, Caridi, G, Divizia, Mt, Faravelli, F, Ghiggeri, G, Mirabelli, M, Pessagno, A, Rossi, A, Uliana, V, Amorini, M, Briguglio, M, Briuglia, S, Salpietro, Cd, Tortorella, G, Adami, A, Bonati, Mt, Castorina, P, D'Arrigo, S, Lalatta, F, Marra, G, Moroni, I, Pantaleoni, C, Riva, D, Scelsa, B, Spaccini, L, Del Giudice, E, Ludwig, K, Permunian, A, Suppiej, A, Macaluso, C, Pichiecchio, A, Battini, R, Di Giacomo, M, Priolo, M, Timpani, P, Pagani, G, Di Sabato ML, Emma, F, Leuzzi, V, Mancini, F, Majore, S, Micalizzi, A, Parisi, P, Romani, M, Stringini, G, Zanni, G, Ulgheri, L, Pollazzon, M, Renieri, Alessandra, Belligni, E, Grosso, E, Pieri, I, Silengo, M, Devescovi, R, Greco, D, Romano, C, Cazzagon, M, Simonati, A, Al Tawari AA, Bastaki, L, Mégarbané, A, Sabolic Avramovska, V, Said, E, Stromme, P, Koul, R, Rajab, A, Azam, M, Barbot, C, Salih, Ma, Tabarki, B, Jocic Jakubi, B, Martorell Sampol, L, Rodriguez, B, Pascual Castroviejo, I, Gener, B, Puschmann, A, Starck, L, Capone, A, Lemke, J, Fluss, J, Niedrist, D, Hennekam, Rc, Wolf, N, Gouider Khouja, N, Kraoua, I, Ceylaner, S, Teber, S, Akgul, M, Anlar, B, Comu, S, Kayserili, H, Yüksel, A, Akcakus, M, Caglayan, Ao, Aldemir, O, Al Gazali, L, Sztriha, L, Nicholl, D, Woods, Cg, Bennett, C, Hurst, J, Sheridan, E, Barnicoat, A, Hemingway, C, Lees, M, Wakeling, E, Blair, E, Bernes, S, Sanchez, H, Clark, Ae, Demarco, E, Donahue, C, Sherr, E, Hahn, J, Sanger, Td, Gallager, Te, Daugherty, C, Krishnamoorthy, Ks, Sarco, D, Walsh, Ca, Mckanna, T, Milisa, J, Chung, Wk, De Vivo DC, Raynes, H, Schubert, R, Seward, A, Brooks, Dg, Goldstein, A, Caldwell, J, Finsecke, E, Maria, Bl, Holden, K, Cruse, Rp, Karaca, E, Swoboda, Kj, Viskochil, D, Dobyns, Wb, Colin, Johnson, Tania, Attié Bitach, Joseph, G. Gleeson, Enza, Maria Valente, ANS - Amsterdam Neuroscience, APH - Amsterdam Public Health, Human Genetics, Paediatrics, OMÜ, University of Zurich, Valente, Enza Maria, Fluss, Joel Victor, Travaglini, L, Brancati, F, Silhavy, J, Iannicelli, M, Nickerson, E, Elkhartoufi, N, Scott, E, Spencer, E, Gabriel, S, Thomas, S, Ben Zeev, B, Bertini, E, Boltshauser, E, Chaouch, M, Cilio, Mr, de Jong, Mm, Kayserili, H, Ogur, G, Poretti, A, Signorini, S, Uziel, G, Zaki, M, Johnson, C, Atti? Bitach, T, Gleeson, Jg, Valente, Em, International JSRD Study, Group, and DEL GIUDICE, Ennio

Subjects
Male, Ciliata -- Anatomy, Proband, 10039 Institute of Medical Genetics, Meckel syndrome, RPGRIP1L, Syndromes, INPP5E, MODIFIER, Phosphoric Monoester Hydrolases/genetics, Ciliopathies, Polycystic Kidney Diseases/diagnosis/genetics, CILIUM, 0302 clinical medicine, Gene Frequency, Cerebellum, Prenatal Diagnosis, RETINAL DEGENERATION, Prevalence, MECKEL, ciliopathies, Joubert syndrome and related disorders, Eye Abnormalities, Child, Genetics (clinical), Encephalocele, Joubert syndrome, Genetics, Polycystic Kidney Diseases, 0303 health sciences, ddc:618, Cerebellar Diseases/diagnosis/genetics, Kidney Diseases, Cystic, Pedigree, 3. Good health, Phenotype, Child, Preschool, Medical genetics, Female, Retinitis Pigmentosa, FORM, Ciliary Motility Disorders, Heterozygote, medicine.medical_specialty, 2716 Genetics (clinical), Adolescent, Molecular Sequence Data, Encephalocele/diagnosis/genetics, AHI1, 610 Medicine & health, Biology, Retina, Article, Ciliopathies, INPP5E, Joubert syndrome and related disorders, Meckel syndrome, NO, Ciliary Motility Disorders/diagnosis/genetics, 03 medical and health sciences, 1311 Genetics, Cerebellar Diseases, REVEALS, medicine, Humans, Abnormalities, Multiple, Amino Acid Sequence, Kidney Diseases, Cystic/diagnosis/genetics, abnormalities, multiple, adolescent, amino acid sequence, cerebellar diseases, cerebellum, child, preschool, ciliary motility disorders, encephalocele, eye abnormalities, female, heterozygote, humans, infant, kidney diseases, cystic, male, molecular sequence data, pedigree, phosphoric monoester hydrolases, polycystic kidney diseases, prenatal diagnosis, prevalence, retina, gene frequency, mutation, phenotype, 030304 developmental biology, Eye Abnormalities/diagnosis/genetics, COACH SYNDROME, Retina/abnormalities, Genetic heterogeneity, Respiration disorders -- Therapy, Infant, medicine.disease, Phosphoric Monoester Hydrolases, INPP5E mutation, 10036 Medical Clinic, Mutation, 030217 neurology & neurosurgery
Abstract

Joubert syndrome and related disorders (JSRD) are clinically and genetically heterogeneous ciliopathies sharing a peculiar midbrain–hindbrain malformation known as the ‘molar tooth sign’. To date, 19 causative genes have been identified, all coding for proteins of the primary cilium. There is clinical and genetic overlap with other ciliopathies, in particular with Meckel syndrome (MKS), that is allelic to JSRD at nine distinct loci. We previously identified the INPP5E gene as causative of JSRD in seven families linked to the JBTS1 locus, yet the phenotypic spectrum and prevalence of INPP5E mutations in JSRD and MKS remain largely unknown. To address this issue, we performed INPP5E mutation analysis in 483 probands, including 408 JSRD patients representative of all clinical subgroups and 75 MKS fetuses. We identified 12 different mutations in 17 probands from 11 JSRD families, with an overall 2.7% mutation frequency among JSRD. The most common clinical presentation among mutated families (7/11, 64%) was Joubert syndrome with ocular involvement (either progressive retinopathy and/or colobomas), while the remaining cases had pure JS. Kidney, liver and skeletal involvement were not observed. None of the MKS foetuses carried INPP5E mutations, indicating that the two ciliopathies are not allelic at this locus., peer-reviewed

Published
2013

34. BRCA1 and BRCA2 families and the risk of skin cancer

Author

Ginsburg, Om, Kim Sing, C, Foulkes, Wd, Ghadirian, P, Lynch, Ht, Sun, P, Narod, Sa, Hereditary Breast Cancer Clinical Study Group: Olopade, Oi, Tung, N, Couch, F, Rosen, B, Friedman, E, Eisen, A, Domchek, S, Stoppa Lyonnet, D, Gershoni Baruch, R, Horsman, D, Wagner, T, Saal, H, Meschino, W, Offit, K, Trivedi, A, Robson, M, Osborne, M, Gilchrist, D, Eng, C, Weitzel, J, Mckinnon, W, Wood, M, Pasini, Barbara, Ainsworth, P, Daly, M, Garber, J, Sweet, K, Fallen, T, Karlan, B, Kurz, R, Isaacs, C, Neuhausen, S, Manoukian, S, Armel, S, Demsky, R, Lemire, E, Mclennan, J, and Evans, G.

Subjects
Oncology, Male, Cancer Research, medicine.medical_specialty, Heterozygote, Skin Neoplasms, endocrine system diseases, Risk Factors, Internal medicine, Epidemiology, Genetics, medicine, Carcinoma, Skin cancer, Humans, Basal cell carcinoma, Genetic Predisposition to Disease, Genetic Testing, skin and connective tissue diseases, Melanoma, Genetics (clinical), Genetic testing, BRCA2 Protein, medicine.diagnostic_test, business.industry, BRCA1 Protein, Cancer, Odds ratio, medicine.disease, BRCA1, BRCA2, Cohort study, Pedigree, Carcinoma, Basal Cell, Mutation, Female, business, Follow-Up Studies
Abstract

BRCA1 and BRCA2 mutation carriers have elevated risks of breast and ovarian cancers. The risks for cancers at other sites remain unclear. Melanoma has been associated with BRCA2 mutations in some studies, however, few surveys have included non-melanoma skin cancer. We followed 2729 women with a BRCA1 or BRCA2 mutation for an average of 5.0 years. These women were asked to report new cases of cancer diagnosed in themselves or in their family. The risks of skin cancer were compared for probands with BRCA1 and BRCA2 mutations. Of 1779 women with a BRCA1 mutation, 29 developed skin cancer in the follow-up period (1.6%). Of the 950 women with a BRCA2 mutation, 28 developed skin cancer (3.0%) (OR = 1.83 for BRCA2 versus BRCA1; 95% CI 1.08-3.10; P = 0.02). The odds ratio for basal cell carcinoma was higher (OR = 3.8; 95% CI 1.5-9.4; P = 0.002). BRCA2 mutation carriers are at increased risk for skin cancer, compared with BRCA1 carriers, in particular for basal cell carcinoma.

Published
2010

35. SMPD1 mutations and Parkinson disease

Author

Dagan, E., primary, Adir, V., additional, Schlesinger, I., additional, Borochowitz, Z., additional, Ayoub, M., additional, Mory, A., additional, Nassar, M., additional, Kurolap, A., additional, Aharon-Peretz, J., additional, and Gershoni-Baruch, R., additional

Published
2015
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36. Evaluation of a candidate breast cancer associated SNP in ERCC4 as a risk modifier in BRCA1 and BRCA2 mutation carriers. Results from the Consortium of Investigators of Modifiers of BRCA1/BRCA2 (CIMBA)

Author

Osorio, A, Milne, RL, Pita, G, Peterlongo, P, Heikkinen, T, Simard, J, Chenevix-Trench, G, Spurdle, AB, Beesley, J, Chen, X, Healey, S, KConFab, Neuhausen, SL, Ding, YC, Couch, FJ, Wang, X, Lindor, N, Manoukian, S, Barile, M, Viel, A, Tizzoni, L, Szabo, CI, Foretova, L, Zikan, M, Claes, K, Greene, MH, Mai, P, Rennert, G, Lejbkowicz, F, Barnett-Griness, O, Andrulis, IL, Ozcelik, H, Weerasooriya, N, OCGN, Gerdes, AM, Thomassen, M, Cruger, DG, Caligo, MA, Friedman, E, Kaufman, B, Laitman, Y, Cohen, S, Kontorovich, T, Gershoni-Baruch, R, Dagan, E, Jernström, H, Askmalm, MS, Arver, B, Malmer, B, SWE-BRCA, Domchek, SM, Nathanson, KL, Brunet, J, Ramón Y Cajal, T, Yannoukakos, D, Hamann, U, HEBON, Hogervorst, FB, Verhoef, S, Gómez García, EB, Wijnen, JT, van den Ouweland, A, EMBRACE, Easton, DF, Peock, S, Cook, M, Oliver, CT, Frost, D, Luccarini, C, Evans, DG, Lalloo, F, Eeles, R, Pichert, G, Cook, J, Hodgson, S, Morrison, PJ, Douglas, F, Godwin, AK, GEMO, Sinilnikova, OM, Barjhoux, L, Stoppa-Lyonnet, D, Moncoutier, V, Giraud, S, Cassini, C, Olivier-Faivre, L, Révillion, F, Peyrat, JP, Muller, D, Fricker, JP, Lynch, HT, John, EM, Buys, S, Daly, M, Hopper, JL, Terry, MB, Miron, A, Yassin, Y, Goldgar, D, Breast Cancer Family Registry, Singer, CF, Gschwantler-Kaulich, D, Pfeiler, G, Spiess, AC, Hansen, TV, Johannsson, OT, Kirchhoff, T, Offit, K, Kosarin, K, Piedmonte, M, Rodriguez, GC, Wakeley, K, Boggess, JF, Basil, J, Schwartz, PE, Blank, SV, Toland, AE, Montagna, M, Casella, C, Imyanitov, EN, Allavena, A, Schmutzler, RK, Versmold, B, Engel, C, Meindl, A, Ditsch, N, Arnold, N, Niederacher, D, Deissler, H, Fiebig, B, Varon-Mateeva, R, Schaefer, D, Froster, UG, Caldes, T, de la Hoya, M, McGuffog, L, Antoniou, AC, Nevanlinna, H, Radice, P, Benítez, J, and CMBA

Published
2009

37. Multicenter analysis of glucocerebrosidase mutations in Parkinson's disease

Author

Sidransky E, Nalls MA, Aasly JO, Aharon-Peretz J, Annesi G, Barbosa ER, Bar-Shira A, Berg D, Bras J, Brice A, Chen CM, Clark LN, Condroyer C, De Marco EV, Dürr A, Eblan MJ, Fahn S, Farrer MJ, Fung HC, Gan-Or Z, Gasser T, Gershoni-Baruch R, Giladi N, and Griff

Abstract

BACKGROUND: Recent studies indicate an increased frequency of mutations in the gene encoding glucocerebrosidase (GBA), a deficiency of which causes Gaucher's disease, among patients with Parkinson's disease. We aimed to ascertain the frequency of GBA mutations in an ethnically diverse group of patients with Parkinson's disease. METHODS: Sixteen centers participated in our international, collaborative study: five from the Americas, six from Europe, two from Israel, and three from Asia. Each center genotyped a standard DNA panel to permit comparison of the genotyping results across centers. Genotypes and phenotypic data from a total of 5691 patients with Parkinson's disease (780 Ashkenazi Jews) and 4898 controls (387 Ashkenazi Jews) were analyzed, with multivariate logistic-regression models and the Mantel-Haenszel procedure used to estimate odds ratios across centers. RESULTS: All 16 centers could detect two GBA mutations, L444P and N370S. Among Ashkenazi Jewish subjects, either mutation was found in 15% of patients and 3% of controls, and among non-Ashkenazi Jewish subjects, either mutation was found in 3% of patients and less than 1% of controls. GBA was fully sequenced for 1883 non-Ashkenazi Jewish patients, and mutations were identified in 7%, showing that limited mutation screening can miss half the mutant alleles. The odds ratio for any GBA mutation in patients versus controls was 5.43 across centers. As compared with patients who did not carry a GBA mutation, those with a GBA mutation presented earlier with the disease, were more likely to have affected relatives, and were more likely to have atypical clinical manifestations. CONCLUSIONS: Data collected from 16 centers demonstrate that there is a strong association between GBA mutations and Parkinson's disease

Published
2009

38. Hormone therapy and the risk of breast cancer in BRCA1 mutation carriers

Author

Eisen, A, Lubinski, J, Gronwald, J, Moller, P, Lynch, Ht, Klijn, J, Kim Sing, C, Neuhausen, Sl, Gilbert, L, Ghadirian, P, Manoukian, S, Rennert, G, Friedman, E, Isaacs, C, Rosen, E, Rosen, B, Daly, M, Sun, P, Narod, Sa, Hereditary, Breast Cancer Clinical Study Group, Collaborators: Olopade, O, Cummings, S, Tung, N, Couch, F, Foulkes, Wd, Domchek, S, Stoppa Lyonnet, D, Gershoni Baruch, R, Horsman, D, Wagner, T, Saal, H, Warner, E, Meschino, W, Offit, K, Trivedi, A, Robson, M, Osborne, M, Gilchrist, D, Eng, C, Weitzel, J, Mckinnon, W, Wood, M, Maugard, C, Pasini, Barbara, Ainsworth, P, Sweet, K, Pasche, B, Fallen, T, Karlan, B, Kurz, Rn, Armel, S, Tulman, A, Lemire, E, Mclennan, J, Evans, G, Byrski, T, Huzarski, T, Shulman, L., and Medical Oncology

Subjects
Oncology, Cancer Research, medicine.medical_treatment, BRCA, Genes, BRCA1, cancer risk, 0302 clinical medicine, Risk Factors, Surveys and Questionnaires, Odds Ratio, skin and connective tissue diseases, 030219 obstetrics & reproductive medicine, Estrogen Replacement Therapy, Hormone replacement therapy (menopause), Confounding Factors, Epidemiologic, Articles, Middle Aged, 3. Good health, Menopause, Postmenopause, 030220 oncology & carcinogenesis, Female, Breast disease, medicine.medical_specialty, Breast Neoplasms, Risk Assessment, 03 medical and health sciences, breast cancer, Breast cancer, SDG 3 - Good Health and Well-being, Internal medicine, medicine, Humans, Risk factor, Hormone therapy, Aged, Gynecology, business.industry, Oophorectomy, Cancer, Estrogens, Odds ratio, medicine.disease, Case-Control Studies, Sample Size, Multivariate Analysis, Mutation, Progestins, business
Abstract

Background: Hormone therapy (HT) is commonly given to women to alleviate the climacteric symptoms associated with menopause. There is concern that this treatment may increase the risk of breast cancer. The potential association of HT and breast cancer risk is of particular interest to women who carry a mutation in BRCA1 because they face a high lifetime risk of breast cancer and because many of these women take HT after undergoing prophylactic surgical oophorectomy at a young age. Methods: We conducted a matched case-control study of 472 postmenopausal women with a BRCA1 mutation to examine whether or not the use of HT is associated with subsequent risk of breast cancer. Breast cancer case patients and control subjects were matched with respect to age, age at menopause, and type of menopause (surgical or natural). Odds ratios (ORs) and 95% confidence intervals (CIs) were estimated with conditional logistic regression. Statistical tests were two-sided. Results: In this group of BRCA1 mutation carriers, the adjusted OR for breast cancer associated with ever use of HT compared with never use was 0.58 (95% CI = 0.35 to 0.96; P =. 03). In analyses by type of HT, an inverse association with breast cancer risk was observed with use of estrogen only (OR = 0.51, 95% CI = 0.27 to 0.98; P =. 04); the association with use of estrogen plus progesterone was not statistically significant (OR = 0.66, 95% CI = 0.34 to 1.27; P =. 21). Conclusion: Among postmenopausal women with a BRCA1 mutation, HT use was not associated with increased risk of breast cancer; indeed, in this population, it was associated with a decreased risk.

Published
2008
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39. Smoking and the risk of breast cancer in BRCA1 and BRCA2 carriers: an update

Author

Ginsburg, O, Ghadirian, P, Lubinski, J, Cybulski, C, Lynch, H, Neuhausen, S, Kim Sing, C, Robson, M, Domchek, S, Isaacs, C, Klijn, J, Armel, S, Foulkes, Wd, Tung, N, Moller, P, Sun, P, Narod, Sa, Olopade, O, Cummings, S, Couch, F, Rosen, B, Stoppa Lyonnet, D, Gershoni Baruch, R, Horsman, D, Wagner, T, Saal, H, Warner, E, Meschino, W, Offit, K, Trivedi, A, Osborne, M, Gilchrist, D, Eng, C, Weitzel, J, Mckinnon, W, Wood, M, Maugard, C, Pasini, Barbara, Ainsworth, P, Sweet, K, Pasche, B, Karlan, B, Kurz, Rn, Tulman, A, Lemire, E, Mclennan, J, Evans, G, Byrski, T, Huzarski, T, Gronwald, J, Gorski, B, Friedman, E, Eisen, A, Daly, M, Garber, J, and Merajver, S.

Subjects
Adult, Cancer Research, medicine.medical_specialty, Heterozygote, endocrine system diseases, Adolescent, Epidemiology, Genes, BRCA2, Genes, BRCA1, Breast Neoplasms, Biochemistry, Article, Young Adult, Breast cancer, breast cancer, Mutation Carrier, Risk Factors, 80 and over, medicine, Humans, Young adult, skin and connective tissue diseases, risk, Aged, Gynecology, Aged, 80 and over, Obstetrics, business.industry, BRCA mutation, Smoking, Case-control study, Cancer, Odds ratio, Middle Aged, medicine.disease, BRCA1, BRCA2, smoking, Genes, Oncology, Case-Control Studies, Mutation, Female, Breast disease, business
Abstract

Among women with a mutation in BRCA1 or BRCA2, the risk of breast cancer is high, but it may be modified by exogenous and endogenous factors. There is concern that exposure to carcinogens in cigarette smoke may increase the risk of cancer in mutation carriers. We conducted a matched case-control study of 2,538 cases of breast cancer among women with a BRCA1 (n = 1,920) or a BRCA2 (n = 618) mutation. One non-affected mutation carrier control was selected for each case, matched on mutation, country of birth, and year of birth. Odds ratios were calculated using conditional logistic regression, adjusted for oral contraceptive use and parity. Ever-smoking was not associated with an increased breast cancer risk among BRCA1 carriers (OR = 1.09; 95% CI 0.95-1.24) or among BRCA2 carriers (OR = 0.81; 95% CI 0.63-1.05). The result did not differ when cases were restricted to women who completed the questionnaire within two years of diagnosis. A modest, but significant increase in risk was seen among BRCA1 carriers with a past history of smoking (OR = 1.27; 95% CI 1.06-1.50), but not among current smokers (OR = 0.95; 0.81-1.12). There appears to be no increase in the risk of breast cancer associated with current smoking in BRCA1 or BRCA2 carriers. There is a possibility of an increased risk of breast cancer among BRCA1 carriers associated with past smoking. There may be different effects of carcinogens in BRCA mutation carriers, depending upon the timing of exposure.

Published
2008

42. Evaluation of a candidate breast cancer associated SNP in ERCC4 as a risk modifier in BRCA1 and BRCA2 mutation carriers. Results from the Consortium of Investigators of Modifiers of BRCA1/BRCA2 (CIMBA)

Author

Osorio, A., Milne, R L, Pita, G., Peterlongo, P., Heikkinen, T., Simard, J., Chenevix-Trench, G., Spurdle, A B, Beesley, J., Chen, X., Healey, S., Neuhausen, S L, Ding, Y C, Couch, F J, Wang, X., Lindor, N., Manoukian, S., Barile, M., Viel, A., Tizzoni, L., Szabo, C I, Foretova, L., Zikan, M., Claes, K., Greene, M H, Mai, P., Rennert, G., Lejbkowicz, F., Barnett-Griness, O., Andrulis, I L, Ozcelik, H., Weerasooriya, N., Gerdes, A-M, Thomassen, M., Cruger, D G, Caligo, M A, Friedman, E., Kaufman, B., Laitman, Y., Cohen, S., Kontorovich, T., Gershoni-Baruch, R., Dagan, E., Jernstrom, H., Stenmark Askmalm, Marie, Arver, B., Malmer, B., Domchek, S M, Nathanson, K L, Brunet, J., Cajal, T. Ramon y, Yannoukakos, D., Hamann, U., Hogervorst, F B L, Verhoef, S., Gomez Garcia, E B, Wijnen, J T, van den Ouweland, A., Easton, D F, Peock, S., Cook, M., Oliver, C T, Frost, D., Luccarini, C., Evans, D G, Lalloo, F., Eeles, R., Pichert, G., Cook, J., Hodgson, S., Morrison, P J, Douglas, F., Godwin, A K, Sinilnikova, O M, Barjhoux, L., Stoppa-Lyonnet, D., Moncoutier, V., Giraud, S., Cassini, C., Olivier-Faivre, L., Revillion, F., Peyrat, J-P, Muller, D., Fricker, J-P, Lynch, H T, John, E M, Buys, S., Daly, M., Hopper, J L, Terry, M B, Miron, A., Yassin, Y., Goldgar, D., Singer, C F, Gschwantler-Kaulich, D., Pfeiler, G., Spiess, A-C, v. O. Hansen, Thomas, T. Johannsson, O., Kirchhoff, T., Offit, K., Kosarin, K., Piedmonte, M., C. Rodriguez, G., Wakeley, K., F. Boggess, J., Basil, J., E. Schwartz, P., V. Blank, S., E. Toland, A., Montagna, M., Casella, C., N. Imyanitov, E., Allavena, A., K. Schmutzler, R., Versmold, B., Engel, C., Meindl, A., Ditsch, N., Arnold, N., Niederacher, D., Deissler, H., Fiebig, B., Varon-Mateeva, R., Schaefer, D., G. Froster, U., Caldes, T., de la Hoya, M., McGuffog, L., C. Antoniou, A., Nevanlinna, H., Radice, P., Benitez, J., Osorio, A., Milne, R L, Pita, G., Peterlongo, P., Heikkinen, T., Simard, J., Chenevix-Trench, G., Spurdle, A B, Beesley, J., Chen, X., Healey, S., Neuhausen, S L, Ding, Y C, Couch, F J, Wang, X., Lindor, N., Manoukian, S., Barile, M., Viel, A., Tizzoni, L., Szabo, C I, Foretova, L., Zikan, M., Claes, K., Greene, M H, Mai, P., Rennert, G., Lejbkowicz, F., Barnett-Griness, O., Andrulis, I L, Ozcelik, H., Weerasooriya, N., Gerdes, A-M, Thomassen, M., Cruger, D G, Caligo, M A, Friedman, E., Kaufman, B., Laitman, Y., Cohen, S., Kontorovich, T., Gershoni-Baruch, R., Dagan, E., Jernstrom, H., Stenmark Askmalm, Marie, Arver, B., Malmer, B., Domchek, S M, Nathanson, K L, Brunet, J., Cajal, T. Ramon y, Yannoukakos, D., Hamann, U., Hogervorst, F B L, Verhoef, S., Gomez Garcia, E B, Wijnen, J T, van den Ouweland, A., Easton, D F, Peock, S., Cook, M., Oliver, C T, Frost, D., Luccarini, C., Evans, D G, Lalloo, F., Eeles, R., Pichert, G., Cook, J., Hodgson, S., Morrison, P J, Douglas, F., Godwin, A K, Sinilnikova, O M, Barjhoux, L., Stoppa-Lyonnet, D., Moncoutier, V., Giraud, S., Cassini, C., Olivier-Faivre, L., Revillion, F., Peyrat, J-P, Muller, D., Fricker, J-P, Lynch, H T, John, E M, Buys, S., Daly, M., Hopper, J L, Terry, M B, Miron, A., Yassin, Y., Goldgar, D., Singer, C F, Gschwantler-Kaulich, D., Pfeiler, G., Spiess, A-C, v. O. Hansen, Thomas, T. Johannsson, O., Kirchhoff, T., Offit, K., Kosarin, K., Piedmonte, M., C. Rodriguez, G., Wakeley, K., F. Boggess, J., Basil, J., E. Schwartz, P., V. Blank, S., E. Toland, A., Montagna, M., Casella, C., N. Imyanitov, E., Allavena, A., K. Schmutzler, R., Versmold, B., Engel, C., Meindl, A., Ditsch, N., Arnold, N., Niederacher, D., Deissler, H., Fiebig, B., Varon-Mateeva, R., Schaefer, D., G. Froster, U., Caldes, T., de la Hoya, M., McGuffog, L., C. Antoniou, A., Nevanlinna, H., Radice, P., and Benitez, J.

Abstract

BACKGROUND: In this study we aimed to evaluate the role of a SNP in intron I of the ERCC4 gene (rs744154), previously reported to be associated with a reduced risk of breast cancer in the general population, as a breast cancer risk modifier in BRCA1 and BRCA2 mutation carriers. METHODS: We have genotyped rs744154 in 9408 BRCA1 and 5632 BRCA2 mutation carriers from the Consortium of Investigators of Modifiers of BRCA1/2 (CIMBA) and assessed its association with breast cancer risk using a retrospective weighted cohort approach. RESULTS: We found no evidence of association with breast cancer risk for BRCA1 (per-allele HR: 0.98, 95% CI: 0.93-1.04, P = 0.5) or BRCA2 (per-allele HR: 0.97, 95% CI: 0.89-1.06, P = 0.5) mutation carriers. CONCLUSION: This SNP is not a significant modifier of breast cancer risk for mutation carriers, though weak associations cannot be ruled out.

Published
2009
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43. Hormone therapy and the risk of breast cancer in BRCA1 mutation carriers

Author

Eisen, A. (Andrea), Lubinski, J. (Jan), Gronwald, J. (Jacek), Moller, P. (Pal), Lynch, H. (Henry), Klijn, J.G.M. (Jan), Kim-Sing, C. (Charmaine), Neuhausen, S.L. (Susan), Gilbert, L. (Lucy), Ghadirian, P. (Parviz), Manoukian, S. (Siranoush), Rennert, G. (Gad), Friedman, E. (Eitan), Isaacs, C. (Claudine), Rosen, B. (Barry), Daly, M.J. (Mark), Sun, P. (Ping), Narod, S. (Steven), Olopade, O.I. (Olofunmilayo), Cummings, S. (Shelly), Tung, N. (Nadine), Couch, F.J. (Fergus), Foulkes, W.D. (William), Domchek, S.M. (Susan), Stoppa-Lyonnet, D. (Dominique), Gershoni-Baruch, R. (Ruth), Horsman, D. (David), Saal, H. (Howard), Warner, E. (Ellen), Meschino, W. (Wendy), Offit, K. (Kenneth), Trivedi, A. (Amber), Robson, M. (Mark), Osborne, M. (Michael), Gilchrist, D. (Dawna), Weitzel, J.N. (Jeffrey), McKinnon, W. (Wendy), Wood, M. (Marie), Maugard, C. (Christine), Pasini, B. (Barbara), Wagner, T. (Teresa), Sweet, K., Pasche, B. (Boris), Fallen, T. (Taya), Karlan, B.Y. (Beth), Eng, C. (Charis), Kurz, R.N., Armel, S. (Susan), Tulman, A. (Anna), Ainsworth, P.J. (Peter), Lemire, E. (Edmond), McLennan, J., Evans, G. (Gareth), Byrski, T. (Tomas), Huzarski, T. (Tomas), Shulman, L. (Lee), Eisen, A. (Andrea), Lubinski, J. (Jan), Gronwald, J. (Jacek), Moller, P. (Pal), Lynch, H. (Henry), Klijn, J.G.M. (Jan), Kim-Sing, C. (Charmaine), Neuhausen, S.L. (Susan), Gilbert, L. (Lucy), Ghadirian, P. (Parviz), Manoukian, S. (Siranoush), Rennert, G. (Gad), Friedman, E. (Eitan), Isaacs, C. (Claudine), Rosen, B. (Barry), Daly, M.J. (Mark), Sun, P. (Ping), Narod, S. (Steven), Olopade, O.I. (Olofunmilayo), Cummings, S. (Shelly), Tung, N. (Nadine), Couch, F.J. (Fergus), Foulkes, W.D. (William), Domchek, S.M. (Susan), Stoppa-Lyonnet, D. (Dominique), Gershoni-Baruch, R. (Ruth), Horsman, D. (David), Saal, H. (Howard), Warner, E. (Ellen), Meschino, W. (Wendy), Offit, K. (Kenneth), Trivedi, A. (Amber), Robson, M. (Mark), Osborne, M. (Michael), Gilchrist, D. (Dawna), Weitzel, J.N. (Jeffrey), McKinnon, W. (Wendy), Wood, M. (Marie), Maugard, C. (Christine), Pasini, B. (Barbara), Wagner, T. (Teresa), Sweet, K., Pasche, B. (Boris), Fallen, T. (Taya), Karlan, B.Y. (Beth), Eng, C. (Charis), Kurz, R.N., Armel, S. (Susan), Tulman, A. (Anna), Ainsworth, P.J. (Peter), Lemire, E. (Edmond), McLennan, J., Evans, G. (Gareth), Byrski, T. (Tomas), Huzarski, T. (Tomas), and Shulman, L. (Lee)

Abstract

Background: Hormone therapy (HT) is commonly given to women to alleviate the climacteric symptoms associated with menopause. There is concern that this treatment may increase the risk of breast cancer. The potential association of HT and breast cancer risk is of particular interest to women who carry a mutation in BRCA1 because they face a high lifetime risk of breast cancer and because many of these women take HT after undergoing prophylactic surgical oophorectomy at a young age. Methods: We conducted a matched case-control study of 472 postmenopausal women with a BRCA1 mutation to examine whether or not the use of HT is associated with subsequent risk of breast cancer. Breast cancer case patients and control subjects were matched with respect to age, age at menopause, and type of menopause (surgical or natural). Odds ratios (ORs) and 95% confidence intervals (CIs) were estimated with conditional logistic regression. Statistical tests were two-sided. Results: In this group of BRCA1 mutation carriers, the adjusted OR for breast cancer associated with ever use of HT compared with never use was 0.58 (95% CI = 0.35 to 0.96; P =. 03). In analyses by type of HT, an inverse association with breast cancer risk was observed with use of estrogen only (OR = 0.51, 95% CI = 0.27 to 0.98; P =. 04); the association with use of estrogen plus progesterone was not statistically significant (OR = 0.66, 95% CI = 0.34 to 1.27; P =. 21). Conclusion: Among postmenopausal women with a BRCA1 mutation, HT use was not associated with increased risk of breast cancer; indeed, in this population, it was associated with a decreased risk.

Published
2008
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44. International variation in rates of uptake of preventive options in BRCA1 and BRCA2 mutation carriers

Author

Metcalfe, K.A. (Kelly), Birenbaum-Carmeli, D. (Daphna), Lubinski, J. (Jan), Gronwald, J. (Jacek), Lynch, H. (Henry), Moller, P. (Pal), Ghadirian, P. (Parviz), Foulkes, W.D. (William), Klijn, J.G.M. (Jan), Friedman, E. (Eitan), Kim-Sing, C. (Charmaine), Ainsworth, P.J. (Peter), Rosen, B. (Barry), Domchek, S.M. (Susan), Wagner, T. (Teresa), Tung, N. (Nadine), Manoukian, S. (Siranoush), Couch, F.J. (Fergus), Sun, P. (Ping), Narod, S. (Steven), Daly, M.J. (Mark), Eisen, A. (Andrea), Saal, H.M., Sweet, K., Lyonnet, D. (Dominique), Rennen, G., McLennan, J., Gershoni-Baruch, R., Garber, J., Cummings, S., Weitzel, J.N. (Jeffrey), Karlan, B.Y. (Beth), Kurz, R.N., McKinnon, W., Wood, M., Osborne, M. (Michael), Gilchrist, D., Chudley, A., Fishman, D. (David), Meschino, W.S., Lemire, E., Maugard, C., Mills, G., Merajver, S.D. (Sofia), Rayson, D., Collée, J.M. (Margriet), Metcalfe, K.A. (Kelly), Birenbaum-Carmeli, D. (Daphna), Lubinski, J. (Jan), Gronwald, J. (Jacek), Lynch, H. (Henry), Moller, P. (Pal), Ghadirian, P. (Parviz), Foulkes, W.D. (William), Klijn, J.G.M. (Jan), Friedman, E. (Eitan), Kim-Sing, C. (Charmaine), Ainsworth, P.J. (Peter), Rosen, B. (Barry), Domchek, S.M. (Susan), Wagner, T. (Teresa), Tung, N. (Nadine), Manoukian, S. (Siranoush), Couch, F.J. (Fergus), Sun, P. (Ping), Narod, S. (Steven), Daly, M.J. (Mark), Eisen, A. (Andrea), Saal, H.M., Sweet, K., Lyonnet, D. (Dominique), Rennen, G., McLennan, J., Gershoni-Baruch, R., Garber, J., Cummings, S., Weitzel, J.N. (Jeffrey), Karlan, B.Y. (Beth), Kurz, R.N., McKinnon, W., Wood, M., Osborne, M. (Michael), Gilchrist, D., Chudley, A., Fishman, D. (David), Meschino, W.S., Lemire, E., Maugard, C., Mills, G., Merajver, S.D. (Sofia), Rayson, D., and Collée, J.M. (Margriet)

Abstract

Several options for cancer prevention are available for women with a BRCA1 or BRCA2 mutation, including prophylactic surgery, chemoprevention and

Published
2008
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46. Deficiency of UBR1, a ubiquitin ligase of the N-end rule pathway, causes pancreatic dysfunction, malformations and mental retardation (Johanson-Blizzard syndrome).

Author

Zenker, M., Mayerle, J., Lerch, M.M., Tagariello, A., Zerres, K., Durie, P.R., Beier, M., Hulskamp, G., Guzman, C., Rehder, H., Beemer, F.A., Hamel, B.C.J., Vanlieferinghen, P., Gershoni-Baruch, R., Vieira, M.W., Dumic, M., Auslender, R., Gil-da-Silva-Lopes, V.L., Steinlicht, S., Rauh, M., Shalev, S.A., Thiel, C., Winterpacht, A., Kwon, Y.T., Varshavsky, A., Reis, A., Zenker, M., Mayerle, J., Lerch, M.M., Tagariello, A., Zerres, K., Durie, P.R., Beier, M., Hulskamp, G., Guzman, C., Rehder, H., Beemer, F.A., Hamel, B.C.J., Vanlieferinghen, P., Gershoni-Baruch, R., Vieira, M.W., Dumic, M., Auslender, R., Gil-da-Silva-Lopes, V.L., Steinlicht, S., Rauh, M., Shalev, S.A., Thiel, C., Winterpacht, A., Kwon, Y.T., Varshavsky, A., and Reis, A.

Abstract

Contains fulltext : 48537.pdf (publisher's version ) (Closed access), Johanson-Blizzard syndrome (OMIM 243800) is an autosomal recessive disorder that includes congenital exocrine pancreatic insufficiency, multiple malformations such as nasal wing aplasia, and frequent mental retardation. We mapped the disease-associated locus to chromosome 15q14-21.1 and identified mutations, mostly truncating ones, in the gene UBR1 in 12 unrelated families with Johanson-Blizzard syndrome. UBR1 encodes one of at least four functionally overlapping E3 ubiquitin ligases of the N-end rule pathway, a conserved proteolytic system whose substrates include proteins with destabilizing N-terminal residues. Pancreas of individuals with Johanson-Blizzard syndrome did not express UBR1 and had intrauterine-onset destructive pancreatitis. In addition, we found that Ubr1(-/-) mice, whose previously reported phenotypes include reduced weight and behavioral abnormalities, had an exocrine pancreatic insufficiency, with impaired stimulus-secretion coupling and increased susceptibility to pancreatic injury. Our findings indicate that deficiency of UBR1 perturbs the pancreas' acinar cells and other organs, presumably owing to metabolic stabilization of specific substrates of the N-end rule pathway.

Published
2005

48. The LRRK2 G2019S mutation is associated with Parkinson disease and concomitant non-skin cancers

Author

Inzelberg, R., primary, Cohen, O. S., additional, Aharon-Peretz, J., additional, Schlesinger, I., additional, Gershoni-Baruch, R., additional, Djaldetti, R., additional, Nitsan, Z., additional, Ephraty, L., additional, Tunkel, O., additional, Kozlova, E., additional, Inzelberg, L., additional, Kaplan, N., additional, Fixler Mehr, T., additional, Mory, A., additional, Dagan, E., additional, Schechtman, E., additional, Friedman, E., additional, and Hassin-Baer, S., additional

Published
2012
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50. Clinical and genetic distinction between Walker-Warburg syndrome and muscle-eye-brain disease.

Author

Cormand, B., Pihko, H., Bayes, M., Valanne, L., Santavuori, P., Talim, B., Gershoni-Baruch, R., Ahmad, A., Bokhoven, J.H.L.M. van, Brunner, H.G., Voit, T., Topaloglu, H., Dobyns, W.B., Lehesjoki, A.E., Cormand, B., Pihko, H., Bayes, M., Valanne, L., Santavuori, P., Talim, B., Gershoni-Baruch, R., Ahmad, A., Bokhoven, J.H.L.M. van, Brunner, H.G., Voit, T., Topaloglu, H., Dobyns, W.B., and Lehesjoki, A.E.

Abstract

Item does not contain fulltext, BACKGROUND: Three rare autosomal recessive disorders share the combination of congenital muscular dystrophy and brain malformations including a neuronal migration defect: muscle-eye-brain disease (MEB), Walker-Warburg syndrome (WWS), and Fukuyama congenital muscular dystrophy (FCMD). In addition, ocular abnormalities are a constant feature in MEB and WWS. Lack of consistent ocular abnormalities in FCMD has allowed a clear clinical demarcation of this syndrome, whereas the phenotypic distinction between MEB and WWS has remained controversial. The MEB gene is located on chromosome 1p32-p34. OBJECTIVES: To establish distinguishing diagnostic criteria for MEB and WWS and to determine whether MEB and WWS are allelic disorders. METHODS: The authors undertook clinical characterization followed by linkage analysis in 19 MEB/WWS families with 29 affected individuals. With use of clinical diagnostic criteria based on Finnish patients with MEB, each patient was categorized as having either MEB or WWS. A linkage and haplotype analysis using 10 markers spanning the MEB locus was performed on the entire family resource. RESULTS: Patients in 11 families were classified as having MEB and in 8 families as WWS. Strong evidence in favor of genetic heterogeneity was obtained in the 19 families. There was evidence for linkage to 1p32-p34 in all but 1 of the 11 pedigrees segregating the MEB phenotype. In contrast, linkage to the MEB locus was excluded in seven of eight of the WWS families. CONCLUSION: These results allow the classification of MEB and WWS as distinct disorders on both clinical and genetic grounds and provide a basis for the mapping of the WWS gene(s).

Published
2001

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