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333 results on '"Tasic, V."'

1. Two Brothers from Macedonia with Gitelman Syndrome

Author

Janchevska A, Tasic V, Jordanova O, Gucev Z, Jenkins L, Jovanovska N, Plaseska-Karanfilska D, Ashton E, and Bockenhauer D

Subjects
gitelman syndrome, hypokalemia, hypomagnesemia, hypocalciuria, slc12a3, Genetics, QH426-470
Abstract

Gitelman syndrome (GS) is a rare renal tubulopathy with an autosomal recessive mode of inheritance, caused by biallelic pathogenic variants in the SLC12A3 gene. The clinical features may overlap with other disorders, such as Bartter syndrome type 3, HNF1B nephropathy or even mitochondrial disease, but can be distinguished by molecular genetic analysis.

Published
2023
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2. TBX6 null variants and a common hypomorphic allele in congenital scoliosis.

Author

Shen, J, Chen, Y, Zhang, T, Zhang, J, Choy, K, Wang, J, Wang, Q, Li, S, Zhou, W, Guo, J, Wang, Y, Zhang, C, Zhao, Hong, An, Yu, Zhao, Yu, Liu, Z, Zuo, Y, Tian, Y, Weng, X, Sutton, V, Wang, H, Ming, Y, Kulkarni, S, Zhong, T, Giampietro, P, Dunwoodie, S, Cheung, S, Zhang, X, Jin, L, Lupski, J, Qiu, G, Zhang, F, Wu, N, Ming, X, Xiao, J, Wu, Z, Chen, X, Shinawi, M, Shen, Y, Yu, G, Liu, J, Xie, H, Gucev, Z, Liu, S, Yang, N, Al-Kateb, H, Chen, J, Hauser, N, Tasic, V, Liu, P, Su, X, Pan, X, Liu, C, Wang, L, and Shen, Joseph

Subjects
Adolescent, Asian People, Child, Child, Preschool, Chromosomes, Human, Pair 16, DNA Copy Number Variations, Female, Genetic Predisposition to Disease, Genotype, Humans, Male, Mutation, Pedigree, Phenotype, Radiography, Scoliosis, Sequence Deletion, Spine, T-Box Domain Proteins
Abstract

BACKGROUND: Congenital scoliosis is a common type of vertebral malformation. Genetic susceptibility has been implicated in congenital scoliosis. METHODS: We evaluated 161 Han Chinese persons with sporadic congenital scoliosis, 166 Han Chinese controls, and 2 pedigrees, family members of which had a 16p11.2 deletion, using comparative genomic hybridization, quantitative polymerase-chain-reaction analysis, and DNA sequencing. We carried out tests of replication using an additional series of 76 Han Chinese persons with congenital scoliosis and a multicenter series of 42 persons with 16p11.2 deletions. RESULTS: We identified a total of 17 heterozygous TBX6 null mutations in the 161 persons with sporadic congenital scoliosis (11%); we did not observe any null mutations in TBX6 in 166 controls (P

Published
2015

3. Duplication of the SOX3 gene in an sry-negative 46,XX male with associated congenital anomalies of kidneys and the urinary tract: Case report and review of the literature

Author

Tasic V, Mitrotti A, Riepe FG, Kulle AE, Laban N, Polenakovic M, Plaseska-Karanfilska D, Sanna-Cherchi S, Kostovski M, and Gucev Z

Subjects
congenital anomalies of kidneys and the urinary tract (cakut), copy number variations (cnvs), disorders of sex development (dsd), Genetics, QH426-470
Abstract

Disorders of sex development (DSD) are a group of rare conditions characterized by discrepancy between chromosomal sex, gonads and external genitalia. Congenital abnormalities of the kidney and urinary tract are often associated with DSD, mostly in multiple malformation syndromes. We describe the case of an 11-year-old Caucasian boy, with right kidney hypoplasia and hypospadias. Genome-wide copy number variation (CNV) analysis revealed a unique duplication of about 550 kb on chromosome Xq27, and a 46,XX karyotype, consistent with a sex reversal phenotype. This region includes multiple genes, and, among these, SOX3 emerged as the main phenotypic driver. This is the fifth case reporting a genomic imbalance involving the SOX3 gene in a 46,XX SRY-negative male, and the first with associated renal malformations. Our data provide plausible links between SOX3 gene dosage and kidney malformations. It is noteworthy that the current and reported SOX3 gene duplications are below the detection threshold of standard karyotypes and were found only by analyzing CNVs using DNA microarrays. Therefore, all 46,XX SRY-negative males should be screened for SOX3 gene duplications with DNA microarrays.

Published
2019
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4. Characteristic diagnostic clues of metatropic dysplasia: The lumbothoracic humpback with dumbbell appearance of the long bones

Author

Gucev Z, Kalcev G, Laban N, Bozinovski Z, Popovski N, Saveski A, Daskalov B, Plaseska-Karanfilska D, and Tasic V

Subjects
a dumbbell appearance, kyphosis, metatropic dysplasia, trpv4 gene mutation, Genetics, QH426-470
Abstract

Metatropic dysplasia (MD) is a rare skeletal dysplasia associated with heterozygous mutations in the TRPV4 gene. We describe a 28-month-old boy with knock-knees referred for metabolic investigation suspected of carrying vitamin D-resistant rickets. He has received regular vitamin D prophylaxis at the usual dose. Laboratory investigations revealed normal values for calcium, phosphorus and alkaline phosphatase. He was short (-3.5 SDS), his mental development was normal, and he started to walk at the age of 22 months. The diagnostic clue for the diagnosis of metatropic dysplasia was the presence of the hump back in the upper lumbar and lower thoracic vertebrae, in addition to a long and narrow chest. An X-ray survey of the skeleton revealed platyspondyly, dysplastic metaphyses with dumbbell appearance of the long bones, kyphoscoliosis, and narrow and elongated thorax with short ribs. This is the first patient with MD in the Republic of Macedonia. Knock-knees were the cause of his referral, as a peculiarity of his phenotype. The very presence of the hump back, and the dumbbell appearance of the long bones distinguished the MD from other bone dysplasias with similar characteristics. We believe that the presence of those two features can shorten the path to accurate diagnosis in the crowded field of overlapping skeletal dysplasias. The diagnosis of MD in this patient was further confirmed by the discovery of the mutation c.2396C>T; p.Pro799Leu (P799L) of the TRPV4 gene.

Published
2018
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5. Multi-population genome-wide association study implicates immune and non-immune factors in pediatric steroid-sensitive nephrotic syndrome.

Author

Barry, A., McNulty, M.T., Jia, X., Gupta, Y., Debiec, H., Luo, Y, Nagano, C., Horinouchi, T., Jung, S., Colucci, M., Ahram, D.F., Mitrotti, A., Sinha, A., Teeninga, N., Jin, G., Shril, S., Caridi, G., Bodria, M., Lim, T.Y., Westland, R., Zanoni, F., Marasa, M., Turudic, D., Giordano, M., Gesualdo, L., Magistroni, R., Pisani, I., Fiaccadori, E., Reiterova, J., Maringhini, S., Morello, W., Montini, G., Weng, P.L., Scolari, F., Saraga, M., Tasic, V., Santoro, D., Wijk, J.A. van, Milošević, D., Kawai, Y., Kiryluk, K., Pollak, M.R., Gharavi, A., Lin, F., Simœs E Silva, A.C., Loos, R.J., Kenny, E.E., Schreuder, M.F., Zurowska, A., Dossier, C., Ariceta, G., Drozynska-Duklas, M., Hogan, J., Jankauskiene, A., Hildebrandt, F., Prikhodina, L., Song, K., Bagga, A., Cheong H, 2.n.d., Ghiggeri, G.M., Vachvanichsanong, P., Nozu, K., Lee, D., Vivarelli, M., Raychaudhuri, S., Tokunaga, K., Sanna-Cherchi, S., Ronco, P., Iijima, K., Sampson, M.G., Barry, A., McNulty, M.T., Jia, X., Gupta, Y., Debiec, H., Luo, Y, Nagano, C., Horinouchi, T., Jung, S., Colucci, M., Ahram, D.F., Mitrotti, A., Sinha, A., Teeninga, N., Jin, G., Shril, S., Caridi, G., Bodria, M., Lim, T.Y., Westland, R., Zanoni, F., Marasa, M., Turudic, D., Giordano, M., Gesualdo, L., Magistroni, R., Pisani, I., Fiaccadori, E., Reiterova, J., Maringhini, S., Morello, W., Montini, G., Weng, P.L., Scolari, F., Saraga, M., Tasic, V., Santoro, D., Wijk, J.A. van, Milošević, D., Kawai, Y., Kiryluk, K., Pollak, M.R., Gharavi, A., Lin, F., Simœs E Silva, A.C., Loos, R.J., Kenny, E.E., Schreuder, M.F., Zurowska, A., Dossier, C., Ariceta, G., Drozynska-Duklas, M., Hogan, J., Jankauskiene, A., Hildebrandt, F., Prikhodina, L., Song, K., Bagga, A., Cheong H, 2.n.d., Ghiggeri, G.M., Vachvanichsanong, P., Nozu, K., Lee, D., Vivarelli, M., Raychaudhuri, S., Tokunaga, K., Sanna-Cherchi, S., Ronco, P., Iijima, K., and Sampson, M.G.

Abstract

Item does not contain fulltext, Pediatric steroid-sensitive nephrotic syndrome (pSSNS) is the most common childhood glomerular disease. Previous genome-wide association studies (GWAS) identified a risk locus in the HLA Class II region and three additional independent risk loci. But the genetic architecture of pSSNS, and its genetically driven pathobiology, is largely unknown. Here, we conduct a multi-population GWAS meta-analysis in 38,463 participants (2440 cases). We then conduct conditional analyses and population specific GWAS. We discover twelve significant associations-eight from the multi-population meta-analysis (four novel), two from the multi-population conditional analysis (one novel), and two additional novel loci from the European meta-analysis. Fine-mapping implicates specific amino acid haplotypes in HLA-DQA1 and HLA-DQB1 driving the HLA Class II risk locus. Non-HLA loci colocalize with eQTLs of monocytes and numerous T-cell subsets in independent datasets. Colocalization with kidney eQTLs is lacking but overlap with kidney cell open chromatin suggests an uncharacterized disease mechanism in kidney cells. A polygenic risk score (PRS) associates with earlier disease onset. Altogether, these discoveries expand our knowledge of pSSNS genetic architecture across populations and provide cell-specific insights into its molecular drivers. Evaluating these associations in additional cohorts will refine our understanding of population specificity, heterogeneity, and clinical and molecular associations.

Published
2023

6. X-Linked Recessive Form of Nephrogenic Diabetes Insipidus in A 7-Year-Old Boy

Author

Janchevska A., Tasic V., Gucev Z., Krstevska-Konstantinova M., and Cheong H. I.

Subjects
nephrogenic diabetes insipidus (ndi), arginine vasopressin (avp), antidiuretic hormone (adh), urine osmolality, Genetics, QH426-470
Abstract

Nephrogenic diabetes insipidus (NDI) is caused by the inability of renal collecting duct cells to respond to arginine vasopressin (AVP)/antidiuretic hormone (ADH). We present the case of a 7-year-old boy with a history of excretion of large amounts of dilute urine and polydipsia since infancy. The boy had several vomiting episodes with mild dehydration during the first 3 years of life. There was no evidence of headaches, dizziness or visual problems. He drinks between 2 and 3 L/day and has 24-hour diuresis of 2 liters, now. He has prepubertal appearance with appropriate weight [+0.85 standard deviation score (SDS)] and height (+0.15 SDS) for his age. His intelligence was also normal. The water deprivation test showed low urine osmolality after 8 hours of dehydration. After desmopressin administration, urine osmolality remained low. Serum osmolality was in the normal range for sex and age before and after desmopressin administration. This indicated a nephrogenic form of diabetes insipidus. Molecular analyses revealed a P286L [p.Pro(CCC)286Leu(CTC)] mutation in the AVPR2 gene, that was inherited from his mother. This patient is the first case with genetically confirmed X-linked inherited form of NDI in the Republic of Macedonia. Molecular analysis confirmed the clinical diagnosis and enabled genetic advice for this family.

Published
2014
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9. Characterization of SETD1A haploinsufficiency in humans and Drosophila defines a novel neurodevelopmental syndrome

Author

Kummeling, J., Stremmelaar, D.E., Raun, N., Reijnders, M.R., Willemsen, M.H., Ruiterkamp-Versteeg, M., Schepens, M.T.M., Man, C.C.O., Gilissen, C.F.H.A., Cho, M.T., McWalter, K., Sinnema, M., Wheless, J.W., Simon, M.E., Genetti, C.A., Casey, A.M., Terhal, P.A., Smagt, J.J. van der, Gassen, K.L.I. van, Joset, P., Bahr, A., Steindl, K., Rauch, A., Keller, E., Raas-Rothschild, A., Koolen, D.A., Agrawal, P.B., Hoffman, T.L., Powell-Hamilton, N.N., Thiffault, I., Engleman, K., Zhou, D., Bodamer, O., Hoefele, J., Riedhammer, K.M., Schwaibold, E.M.C., Tasic, V., Schubert, D., Top, D., Pfundt, R.P., Higgs, M.R., Kramer, J.M., Kleefstra, T., Kummeling, J., Stremmelaar, D.E., Raun, N., Reijnders, M.R., Willemsen, M.H., Ruiterkamp-Versteeg, M., Schepens, M.T.M., Man, C.C.O., Gilissen, C.F.H.A., Cho, M.T., McWalter, K., Sinnema, M., Wheless, J.W., Simon, M.E., Genetti, C.A., Casey, A.M., Terhal, P.A., Smagt, J.J. van der, Gassen, K.L.I. van, Joset, P., Bahr, A., Steindl, K., Rauch, A., Keller, E., Raas-Rothschild, A., Koolen, D.A., Agrawal, P.B., Hoffman, T.L., Powell-Hamilton, N.N., Thiffault, I., Engleman, K., Zhou, D., Bodamer, O., Hoefele, J., Riedhammer, K.M., Schwaibold, E.M.C., Tasic, V., Schubert, D., Top, D., Pfundt, R.P., Higgs, M.R., Kramer, J.M., and Kleefstra, T.

Abstract

Item does not contain fulltext, Defects in histone methyltransferases (HMTs) are major contributing factors in neurodevelopmental disorders (NDDs). Heterozygous variants of SETD1A involved in histone H3 lysine 4 (H3K4) methylation were previously identified in individuals with schizophrenia. Here, we define the clinical features of the Mendelian syndrome associated with haploinsufficiency of SETD1A by investigating 15 predominantly pediatric individuals who all have de novo SETD1A variants. These individuals present with a core set of symptoms comprising global developmental delay and/or intellectual disability, subtle facial dysmorphisms, behavioral and psychiatric problems. We examined cellular phenotypes in three patient-derived lymphoblastoid cell lines with three variants: p.Gly535Alafs*12, c.4582-2_4582delAG, and p.Tyr1499Asp. These patient cell lines displayed DNA damage repair defects that were comparable to previously observed RNAi-mediated depletion of SETD1A. This suggested that these variants, including the p.Tyr1499Asp in the catalytic SET domain, behave as loss-of-function (LoF) alleles. Previous studies demonstrated a role for SETD1A in cell cycle control and differentiation. However, individuals with SETD1A variants do not show major structural brain defects or severe microcephaly, suggesting that defective proliferation and differentiation of neural progenitors is unlikely the single underlying cause of the disorder. We show here that the Drosophila melanogaster SETD1A orthologue is required in postmitotic neurons of the fly brain for normal memory, suggesting a role in post development neuronal function. Together, this study defines a neurodevelopmental disorder caused by dominant de novo LoF variants in SETD1A and further supports a role for H3K4 methyltransferases in the regulation of neuronal processes underlying normal cognitive functioning.

Published
2021

10. Mutations in DSTYK and Dominant Urinary Tract Malformations

Author

Sanna-Cherchi, S., Sampogna, R. V., Papeta, N., Burgess, K. E., Nees, S. N., Perry, B. J., Choi, M., Bodria, M., Liu, Y., Weng, P. L., Lozanovski, V. J., Verbitsky, M., Lugani, F., Sterken, R., Paragas, N., Caridi, G., Carrea, A., Dagnino, M., Materna-Kiryluk, A., Santamaria, G., Murtas, C., Ristoska-Bojkovska, N., Izzi, C., Kacak, N., Bianco, B., Giberti, S., Gigante, M., Piaggio, G., Gesualdo, L., Kosuljandic Vukic, D., Vukojevic, K., Saraga-Babic, M., Saraga, M., Gucev, Z., Allegri, L., Latos-Bielenska, A., Casu, D., State, M., Scolari, F., Ravazzolo, R., Kiryluk, K., Al-Awqati, Q., DʼAgati, V. D., Drummond, I. A., Tasic, V., Lifton, R. P., Ghiggeri, G. M., and Gharavi, A. G.

Published
2013
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11. The European Society for Paediatric Nephrology study of pediatric renal care in Europe: comparative analysis 1998-2017

Author

Hoyer, P., Simao, C., Stefanidis, C. J., Tasic, V, Toots, U., Tur, N., Walle, J., Zurowska, A., Bjerre, A., Brandstrom, P., Chafai, R., Lotan, D., Davitaia, T., Dlin, V, Golubovic, E., Hadjipanayis, A., Shroff, Rukshana, Bakkaloglu, SEVCAN AZİME, Prikhodina, Larisa, Ehrich, Jochen, Shtiza, D., Hughes, D. A., Ivanov, D., Jankauskiene, A., Kamperis, K., Levart, Kersnik T., Laube, G., TOPALOĞLU, REZAN, Lungu, A., Milosevic, D., Levtchenko, Elena, Anton-Gamero, M., Arikoski, P., Aufricht, C., Awan, A., Baylarov, R., Murer, L., Nigmatullina, N., Podraska, L., Pokrajac, D., Reusz, G. S., Roussey, G., Roussinov, D., Conti, Said, Sarkissian, A., Schreuder, M., and Seeman, T.

Subjects
Nephrology, medicine.medical_specialty, Adolescent, 030232 urology & nephrology, Allied Health Personnel, 030204 cardiovascular system & hematology, Subspecialty, Pediatrics, Health Services Accessibility, Nephrologists, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Surveys and Questionnaires, medicine, Humans, Healthcare Disparities, Child, Health policy, Kidney transplantation, Societies, Medical, Kidney, business.industry, Acute kidney injury, medicine.disease, Europe, medicine.anatomical_structure, Family medicine, Pediatrics, Perinatology and Child Health, Kidney Diseases, business, Psychosocial, Kidney disease, Follow-Up Studies
Abstract

Background In 1998, a survey of the European Society for Paediatric Nephrology (ESPN) revealed substantial disparities in pediatric renal care among European countries. Therefore, ESPN aimed at harmonizing renal care in all European countries in the following 20 years. In 2017, we conducted a survey to evaluate the current status of renal health policies for children in Europe. Methods A 33-question web-based survey was designed and sent to presidents or representatives of national societies of pediatric nephrology in 44 European countries. Results Data was reported from 42 (95.5%) countries. The number of pediatric nephrologists per million child population increased from 1998 to 2017 in 70% of countries. Pediatric dialysis facilities for acute kidney injury and end-stage kidney disease were available in 95% of countries. The availability of pediatric kidney transplantation increased from 55 to 93% of countries. Considerable variation was found in the current availability of allied health professionals, including psychosocial and nutritional support, high-tech diagnostic methods, and treatment with expensive drugs for children with kidney diseases between different European countries. Conclusions The 20-year follow-up analysis of pediatric renal care services in European countries revealed that pediatric nephrology has become a well-established subspecialty in pediatrics and nephrology in 2017. The ESPN will continue its efforts to further improve pediatric renal care for European children by harmonizing remaining disparities of renal care services.

Published
2019

15. Novel ATP6V1B1 and ATP6V0A4 mutations in autosomal recessive distal renal tubular acidosis with new evidence for hearing loss

Author

Stover, E H, Borthwick, K J, Bavalia, C, Eady, N, Fritz, D M, Rungroj, N, Giersch, A B S, Morton, C C, Axon, P R, Akil, I, Al-Sabban, E A, Baguley, D M, Bianca, S, Bakkaloglu, A, Bircan, Z, Chauveau, D, Clermont, M-J, Guala, A, Hulton, S A, Kroes, H, Li Volti, G, Mir, S, Mocan, H, Nayir, A, Ozen, S, Rodriguez Soriano, J, Sanjad, S A, Tasic, V, Taylor, C M, Topaloglu, R, Smith, A N, and Karet, F E

Published
2002

16. Author Correction: The copy number variation landscape of congenital anomalies of the kidney and urinary tract (Nature Genetics, (2019), 51, 1, (117-127), 10.1038/s41588-018-0281-y)

Author

Verbitsky, M., Westland, R., Perez, A., Kiryluk, K., Liu, Q., Krithivasan, P., Mitrotti, A., Fasel, D. A., Batourina, E., Sampson, M. G., Bodria, M., Werth, M., Kao, C., Martino, J., Capone, V. P., Vivante, A., Shril, S., Kil, B. H., Marasa, M., Zhang, J. Y., Y. -J., Na, Lim, T. Y., Ahram, D., Weng, P. L., Heinzen, E. L., Carrea, A., Piaggio, G., Gesualdo, L., Manca, V., Masnata, G., Gigante, M., Cusi, D., Izzi, C., Scolari, F., van Wijk, J. A. E., Saraga, M., Santoro, D., Conti, G., Zamboli, P., White, H., Drozdz, D., Zachwieja, K., Miklaszewska, M., Tkaczyk, M., Tomczyk, D., Krakowska, A., Sikora, P., Jarmolinski, T., Borszewska-Kornacka, M. K., Pawluch, R., Szczepanska, M., Adamczyk, P., Mizerska-Wasiak, M., Krzemien, G., Szmigielska, A., Zaniew, M., Dobson, M. G., Darlow, J. M., Puri, P., Barton, D. E., Furth, S. L., Warady, B. A., Gucev, Z., Lozanovski, V. J., Tasic, V., Pisani, I., Allegri, L., Rodas, L. M., Campistol, J. M., Jeanpierre, C., Alam, S., Casale, P., Wong, C. S., Lin, F., Miranda, D. M., Oliveira, E. A., Simoes-e-Silva, A. C., Barasch, J. M., Levy, B., Wu, N., Hildebrandt, F., Ghiggeri, G. M., Latos-Bielenska, A., Materna-Kiryluk, A., Zhang, F., Hakonarson, H., Papaioannou, V. E., Mendelsohn, C. L., Gharavi, A. G., and Sanna-Cherchi, S.

Subjects
renal, genetics, cakut
Published
2019

17. Treatment and long-term outcome in primary distal renal tubular acidosis

Author

Lopez-Garcia SC, Emma F, Walsh SB, Fila M, Hooman N, Zaniew M, Bertholet-Thomas A, Colussi G, Burgmaier K, Levtchenko E, Sharma J, Singhal J, Soliman NA, Ariceta G, Basu B, Murer L, Tasic V, Tsygin A, Decramer S, Gil-Peña H, Koster-Kamphuis L, La Scola C, Gellermann J, Konrad M, Lilien M, Francisco T, Tramma D, Trnka P, Yüksel S, Caruso MR, Chromek M, Ekinci Z, Gambaro G, Kari JA, König J, Taroni F, Thumfart J, Trepiccione F, Winding L, Wühl E, Ağbaş A, Belkevich A, Vargas-Poussou R, and Blanchard A

Subjects
Acidosis, Renal Tubular/complications/genetics/*therapy, Adolescent, Adult, Aged, Bicarbonates/blood, Calcium/urine, Child, Child, Preschool, Cohort Studies, DNA Mutational Analysis, Deafness/complications/genetics/therapy, Female, Genetic Association Studies, Glomerular Filtration Rate, Hearing Loss, Sensorineural/complications/genetics/*therapy, Humans, Infant, Infant, Newborn, Male, Middle Aged, Mutation, Nephrocalcinosis/complications/genetics/therapy, Rare Diseases/complications, Vacuolar P
Abstract

BACKGROUND: Primary distal renal tubular acidosis (dRTA) is a rare disorder, and we aimed to gather data on treatment and long-term outcome. METHODS: We contacted paediatric and adult nephrologists through European professional organizations. Responding clinicians entered demographic, biochemical, genetic and clinical data in an online form. RESULTS: Adequate data were collected on 340 patients (29 countries, female 52%). Mutation testing had been performed on 206 patients (61%); pathogenic mutations were identified in 170 patients (83%). The median (range) presentation age was 0.5 (0-54) years and age at last follow-up was 11.0 (0-70.0) years. Adult height was slightly below average with a mean (SD score) of -0.57 (±1.16). There was an increased prevalence of chronic kidney disease (CKD) Stage ≥2 in children (35%) and adults (82%). Nephrocalcinosis was reported in 88%. Nephrolithiasis was more common with SLC4A1 mutations (42% versus 21%). Thirty-six percent had hearing loss, particularly in ATP6V1B1 (88%). The median (interquartile range) prescribed dose of alkali (mEq/kg/day) was 1.9 (1.2-3.3). Adequate metabolic control (normal plasma bicarbonate and normocalciuria) was achieved in 158 patients (51%), more commonly in countries with higher gross domestic product (67% versus 23%), and was associated with higher height and estimated glomerular filtration rate. CONCLUSION: Long-term follow-up from this large dRTA cohort shows an overall favourable outcome with normal adult height for most and no patient with CKD Stage 5. However, 82% of adult patients have CKD Stages 2-4. Importance of adequate metabolic control was highlighted by better growth and renal function but was achieved in only half of patients.

Published
2019

18. Treatment and long-term outcome in primary distal renal tubular acidosis

Author

Lopez-Garcia, S.C., Emma, F., Walsh, S.B., Fila, M., Hooman, N., Zaniew, M., Bertholet-Thomas, A., Colussi, G., Burgmaier, K., Levtchenko, E.N., Sharma, J., Singhal, J., Soliman, N.A., Ariceta, G., Basu, B., Murer, L., Tasic, V., Tsygin, A., Decramer, S., Gil-Pena, H., Koster-Kamphuis, L., La Scola, C., Gellermann, J., Konrad, M., Lilien, M., Francisco, T., Tramma, D., Trnka, P., Yuksel, S., Caruso, M.R., Chromek, M., Ekinci, Z., Gambaro, G., Kari, J.A., Konig, J., Taroni, F., Thumfart, J., Trepiccione, F., Winding, L., Wuhl, E., Agbas, A., Belkevich, A., Vargas-Poussou, R., Blanchard, A., Conti, G., Boyer, O., Dursun, I., Pinarbasi, A.S., Melek, E., Miglinas, M., Novo, R., Mallett, A., Milosevic, D., Szczepanska, M., Wente, S., Cheong, H.I., Sinha, R., Gucev, Z., Dufek, S., Iancu, D., Kleta, R., Schaefer, F., Bockenhauer, D., Lopez-Garcia, S.C., Emma, F., Walsh, S.B., Fila, M., Hooman, N., Zaniew, M., Bertholet-Thomas, A., Colussi, G., Burgmaier, K., Levtchenko, E.N., Sharma, J., Singhal, J., Soliman, N.A., Ariceta, G., Basu, B., Murer, L., Tasic, V., Tsygin, A., Decramer, S., Gil-Pena, H., Koster-Kamphuis, L., La Scola, C., Gellermann, J., Konrad, M., Lilien, M., Francisco, T., Tramma, D., Trnka, P., Yuksel, S., Caruso, M.R., Chromek, M., Ekinci, Z., Gambaro, G., Kari, J.A., Konig, J., Taroni, F., Thumfart, J., Trepiccione, F., Winding, L., Wuhl, E., Agbas, A., Belkevich, A., Vargas-Poussou, R., Blanchard, A., Conti, G., Boyer, O., Dursun, I., Pinarbasi, A.S., Melek, E., Miglinas, M., Novo, R., Mallett, A., Milosevic, D., Szczepanska, M., Wente, S., Cheong, H.I., Sinha, R., Gucev, Z., Dufek, S., Iancu, D., Kleta, R., Schaefer, F., and Bockenhauer, D.

Abstract

Contains fulltext : 204259.pdf (publisher's version ) (Closed access), BACKGROUND: Primary distal renal tubular acidosis (dRTA) is a rare disorder, and we aimed to gather data on treatment and long-term outcome. METHODS: We contacted paediatric and adult nephrologists through European professional organizations. Responding clinicians entered demographic, biochemical, genetic and clinical data in an online form. RESULTS: Adequate data were collected on 340 patients (29 countries, female 52%). Mutation testing had been performed on 206 patients (61%); pathogenic mutations were identified in 170 patients (83%). The median (range) presentation age was 0.5 (0-54) years and age at last follow-up was 11.0 (0-70.0) years. Adult height was slightly below average with a mean (SD score) of -0.57 (+/-1.16). There was an increased prevalence of chronic kidney disease (CKD) Stage >/=2 in children (35%) and adults (82%). Nephrocalcinosis was reported in 88%. Nephrolithiasis was more common with SLC4A1 mutations (42% versus 21%). Thirty-six percent had hearing loss, particularly in ATP6V1B1 (88%). The median (interquartile range) prescribed dose of alkali (mEq/kg/day) was 1.9 (1.2-3.3). Adequate metabolic control (normal plasma bicarbonate and normocalciuria) was achieved in 158 patients (51%), more commonly in countries with higher gross domestic product (67% versus 23%), and was associated with higher height and estimated glomerular filtration rate. CONCLUSION: Long-term follow-up from this large dRTA cohort shows an overall favourable outcome with normal adult height for most and no patient with CKD Stage 5. However, 82% of adult patients have CKD Stages 2-4. Importance of adequate metabolic control was highlighted by better growth and renal function but was achieved in only half of patients.

Published
2019

19. Functional rare and low frequency variants in BLK and BANK1 contribute to human lupus

Author

Jiang, SH, Athanasopoulos, V, Ellyard, J, Chuah, A, Cappello, J, Cook, A, Prabhu, SB, Cardenas, J, Gu, J, Stanley, M, Roco, JA, Papa, I, Yabas, M, Walters, GD, Burgio, G, McKeon, K, Byers, JM, Burrin, C, Enders, A, Miosge, LA, Canete, PF, Jelusic, M, Tasic, V, Lungu, AC, Alexander, S, Kitching, AR, Fulcher, DA, Shen, N, Arsov, T, Gatenby, PA, Babon, JJ, Mallon, DF, Collantes, CDL, Stone, EA, Wu, P, Field, MA, Andrews, TD, Cho, E, Pascual, V, Cook, MC, Vinuesa, CG, Jiang, SH, Athanasopoulos, V, Ellyard, J, Chuah, A, Cappello, J, Cook, A, Prabhu, SB, Cardenas, J, Gu, J, Stanley, M, Roco, JA, Papa, I, Yabas, M, Walters, GD, Burgio, G, McKeon, K, Byers, JM, Burrin, C, Enders, A, Miosge, LA, Canete, PF, Jelusic, M, Tasic, V, Lungu, AC, Alexander, S, Kitching, AR, Fulcher, DA, Shen, N, Arsov, T, Gatenby, PA, Babon, JJ, Mallon, DF, Collantes, CDL, Stone, EA, Wu, P, Field, MA, Andrews, TD, Cho, E, Pascual, V, Cook, MC, and Vinuesa, CG

Abstract

Systemic lupus erythematosus (SLE) is the prototypic systemic autoimmune disease. It is thought that many common variant gene loci of weak effect act additively to predispose to common autoimmune diseases, while the contribution of rare variants remains unclear. Here we describe that rare coding variants in lupus-risk genes are present in most SLE patients and healthy controls. We demonstrate the functional consequences of rare and low frequency missense variants in the interacting proteins BLK and BANK1, which are present alone, or in combination, in a substantial proportion of lupus patients. The rare variants found in patients, but not those found exclusively in controls, impair suppression of IRF5 and type-I IFN in human B cell lines and increase pathogenic lymphocytes in lupus-prone mice. Thus, rare gene variants are common in SLE and likely contribute to genetic risk.

Published
2019

20. Whole-Exome Sequencing Identifies Causative Mutations in Families with Congenital Anomalies of the Kidney and Urinary Tract.

Author

Ven, A.T. van der, Connaughton, D.M., Ityel, H., Mann, N., Nakayama, M., Chen, J., Vivante, A., Hwang, D.Y., Schulz, J, Braun, D.A., Schmidt, J.M., Schapiro, D., Schneider, R., Warejko, J.K., Daga, A., Majmundar, A.J., Tan, W., Jobst-Schwan, T., Hermle, T., Widmeier, E., Ashraf, S., Amar, A., Hoogstraten, C.A., Hugo, H., Kitzler, T.M., Kause, F., Kolvenbach, C.M., Dai, R., Spaneas, L., Amann, K., Stein, D.R., Baum, M.A., Somers, M.J.G., Rodig, N.M., Ferguson, M.A., Traum, A.Z., Daouk, G.H., Bogdanovic, R., Stajic, N., Soliman, N.A., Kari, J.A., Desoky, S. El, Fathy, H.M., Milosevic, D., Al-Saffar, M., Awad, H.S., Eid, L.A., Selvin, A., Senguttuvan, P., Sanna-Cherchi, S., Rehm, H.L., MacArthur, D.G., Lek, M., Laricchia, K.M., Wilson, M.W., Mane, S.M., Lifton, R.P., Lee, R.S., Bauer, S.B., Lu, W., Reutter, H.M., Tasic, V., Shril, S., Hildebrandt, F., Ven, A.T. van der, Connaughton, D.M., Ityel, H., Mann, N., Nakayama, M., Chen, J., Vivante, A., Hwang, D.Y., Schulz, J, Braun, D.A., Schmidt, J.M., Schapiro, D., Schneider, R., Warejko, J.K., Daga, A., Majmundar, A.J., Tan, W., Jobst-Schwan, T., Hermle, T., Widmeier, E., Ashraf, S., Amar, A., Hoogstraten, C.A., Hugo, H., Kitzler, T.M., Kause, F., Kolvenbach, C.M., Dai, R., Spaneas, L., Amann, K., Stein, D.R., Baum, M.A., Somers, M.J.G., Rodig, N.M., Ferguson, M.A., Traum, A.Z., Daouk, G.H., Bogdanovic, R., Stajic, N., Soliman, N.A., Kari, J.A., Desoky, S. El, Fathy, H.M., Milosevic, D., Al-Saffar, M., Awad, H.S., Eid, L.A., Selvin, A., Senguttuvan, P., Sanna-Cherchi, S., Rehm, H.L., MacArthur, D.G., Lek, M., Laricchia, K.M., Wilson, M.W., Mane, S.M., Lifton, R.P., Lee, R.S., Bauer, S.B., Lu, W., Reutter, H.M., Tasic, V., Shril, S., and Hildebrandt, F.

Abstract

1 september 2018, Item does not contain fulltext, BACKGROUND: Congenital anomalies of the kidney and urinary tract (CAKUT) are the most prevalent cause of kidney disease in the first three decades of life. Previous gene panel studies showed monogenic causation in up to 12% of patients with CAKUT. METHODS: We applied whole-exome sequencing to analyze the genotypes of individuals from 232 families with CAKUT, evaluating for mutations in single genes known to cause human CAKUT and genes known to cause CAKUT in mice. In consanguineous or multiplex families, we additionally performed a search for novel monogenic causes of CAKUT. RESULTS: In 29 families (13%), we detected a causative mutation in a known gene for isolated or syndromic CAKUT that sufficiently explained the patient's CAKUT phenotype. In three families (1%), we detected a mutation in a gene reported to cause a phenocopy of CAKUT. In 15 of 155 families with isolated CAKUT, we detected deleterious mutations in syndromic CAKUT genes. Our additional search for novel monogenic causes of CAKUT in consanguineous and multiplex families revealed a potential single, novel monogenic CAKUT gene in 19 of 232 families (8%). CONCLUSIONS: We identified monogenic mutations in a known human CAKUT gene or CAKUT phenocopy gene as the cause of disease in 14% of the CAKUT families in this study. Whole-exome sequencing provides an etiologic diagnosis in a high fraction of patients with CAKUT and will provide a new basis for the mechanistic understanding of CAKUT.

Published
2018

23. Mutations in DSTYK and dominant urinary tract malformations

Author

Sanna Cherchi, S, Sampogna, Rv, Papeta, N, Burgess, Ke, Nees, Sn, Perry, Bj, Choi, M, Bodria, M, Liu, Y, Weng, Pl, Lozanovski, Vj, Verbitsky, M, Lugani, F, Sterken, R, Paragas, N, Caridi, G, Carrea, A, Dagnino, M, Materna Kiryluk, A, Santamaria, G, Murtas, C, Ristoska Bojkovska, N, Izzi, C, Kacak, N, Bianco, B, Giberti, S, Gigante, M, Piaggio, G, Gesualdo, L, Kosuljandic Vukic, D, Vukojevic, K, Saraga Babic, M, Saraga, M, Gucev, Z, Allegri, L, Latos Bielenska, A, Casu, D, State, M, Scolari, F, Ravazzolo, Roberto, Kiryluk, K, Al Awqati, Q, D'Agati, Vd, Drummond, Ia, Tasic, V, Lifton, Rp, Ghiggeri, Gm, and Gharavi, Ag

Subjects
Male, Kidney Disease, Genetic Linkage, 030232 urology & nephrology, Genome-wide association study, Bioinformatics, medicine.disease_cause, Fibroblast growth factor, Kidney, Medical and Health Sciences, Mice, 0302 clinical medicine, 2.1 Biological and endogenous factors, Exome, RNA, Small Interfering, Aetiology, Urinary Tract, Child, Pediatric, 0303 health sciences, Mutation, General Medicine, 3. Good health, Pedigree, medicine.anatomical_structure, Receptor-Interacting Protein Serine-Threonine Kinases, Gene Knockdown Techniques, Female, Biotechnology, Adult, Urologic Diseases, Heterozygote, Urinary system, 1.1 Normal biological development and functioning, Molecular Sequence Data, Renal and urogenital, Small Interfering, 03 medical and health sciences, Young Adult, Clinical Research, Underpinning research, General & Internal Medicine, medicine, Genetics, Animals, Humans, 030304 developmental biology, Base Sequence, business.industry, Human Genome, Infant, Heterozygote advantage, Urogenital Abnormalities, Etiology, RNA, Congenital Structural Anomalies, business, Genome-Wide Association Study
Abstract

BackgroundCongenital abnormalities of the kidney and the urinary tract are the most common cause of pediatric kidney failure. These disorders are highly heterogeneous, and the etiologic factors are poorly understood.MethodsWe performed genomewide linkage analysis and whole-exome sequencing in a family with an autosomal dominant form of congenital abnormalities of the kidney or urinary tract (seven affected family members). We also performed a sequence analysis in 311 unrelated patients, as well as histologic and functional studies.ResultsLinkage analysis identified five regions of the genome that were shared among all affected family members. Exome sequencing identified a single, rare, deleterious variant within these linkage intervals, a heterozygous splice-site mutation in the dual serine-threonine and tyrosine protein kinase gene (DSTYK). This variant, which resulted in aberrant splicing of messenger RNA, was present in all affected family members. Additional, independent DSTYK mutations, including nonsense and splice-site mutations, were detected in 7 of 311 unrelated patients. DSTYK is highly expressed in the maturing epithelia of all major organs, localizing to cell membranes. Knockdown in zebrafish resulted in developmental defects in multiple organs, which suggested loss of fibroblast growth factor (FGF) signaling. Consistent with this finding is the observation that DSTYK colocalizes with FGF receptors in the ureteric bud and metanephric mesenchyme. DSTYK knockdown in human embryonic kidney cells inhibited FGF-stimulated phosphorylation of extracellular-signal-regulated kinase (ERK), the principal signal downstream of receptor tyrosine kinases.ConclusionsWe detected independent DSTYK mutations in 2.3% of patients with congenital abnormalities of the kidney or urinary tract, a finding that suggests that DSTYK is a major determinant of human urinary tract development, downstream of FGF signaling. (Funded by the National Institutes of Health and others.).

Published
2013

24. Duplication of the SOX3gene in an sry-negative 46,XX male with associated congenital anomalies of kidneys and the urinary tract: Case report and review of the literature

Author

Tasic, V, Mitrotti, A, Riepe, FG, Kulle, AE, Laban, N, Polenakovic, M, Plaseska-Karanfilska, D, Sanna-Cherchi, S, Kostovski, M, and Gucev, Z

Abstract

Disorders of sex development (DSD) are a group of rare conditions characterized by discrepancy between chromosomal sex, gonads and external genitalia. Congenital abnormalities of the kidney and urinary tract are often associated with DSD, mostly in multiple malformation syndromes. We describe the case of an 11-year-old Caucasian boy, with right kidney hypoplasia and hypospadias. Genome-wide copy number variation (CNV) analysis revealed a unique duplication of about 550 kb on chromosome Xq27, and a 46,XX karyotype, consistent with a sex reversal phenotype. This region includes multiple genes, and, among these, SOX3emerged as the main phenotypic driver. This is the fifth case reporting a genomic imbalance involving the SOX3gene in a 46,XX SRY-negative male, and the first with associated renal malformations. Our data provide plausible links between SOX3gene dosage and kidney malformations. It is noteworthy that the current and reported SOX3gene duplications are below the detection threshold of standard karyotypes and were found only by analyzing CNVs using DNA microarrays. Therefore, all 46,XX SRY-negative males should be screened for SOX3gene duplications with DNA microarrays.

Published
2019
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25. 2nd combined working group and management committee meeting of urine and kidney proteomics COST action 29-30 March 2009, Nafplio, Greece

Author

Vlahou, Antonia, Allmaier, G., Attwood, T., Bongcam-Rudloff, E., Charonis, Aristidis S., Frokiaer, J., Mischak, H., Schanstra, J., Spasovski, G., Aasberg, A., Allory, Y., Arthur, J., Banks, R., Baumann, M., Benigni, A., Bezerianos, Anastasios, Campistol, J. M., Candiano, G., Capasso, G., Carpentier, S., Dadlez, M., Constantinou-Deltas, Constantinos D., Dijilianov, D., De Zeeuw, D., Decramer, S., Dihazi, H., Domon, B., Endlich, N., d'Alche-Buc, F., D'Haese, P., Edelman, A., Egido, J., El Nahas, M., Farinazzo, A., Fernandez-Llama, P., Feldt-Rasmussen, B., Gansevoort, R., Garbis, S., Garin, J., Ghiggeri, G. M., Gimenez, I., Granier, C., Goumenos, Dimitrios S., Haylor, J. L., Hilario, M., Holthofer, H., Kalousis, Alexandros, Kaski, S., Knepper, M., Korneti, P., Kossida, Sophia A., Langham, R., Loftheim, H., Lopez-Novoa, J., Luider, T., Magni, F., Malats, N., Martin, J. L., Mayrhofer, C., Monsarrat, B., Mueller, G., Nielsen, S., Norling, M., O'Connell, S., Ortiz, A., Perunicic-Pekovic, G., Planelles, G., Polenakovic, M., Promponas, Vasilis J., Rasic-Milutinovic, Z., Rehulka, P., Peter, K., Righetti, P. G., Ronco, P., Ryan, M., Sánchez-Carbayo, M., Semmes, J., Sheehan, D., Stenman, U. -H, Stodkilde-Jorgensen, L., Tasic, V., Theodorescu, D., Thongboonkerd, V., Toncheva, D., Tsillibari, E., Tsiotis, Georgios, Unwin, R., Vanholder, R., Vassilev, D., Vickers, M. E., Verhulst, A., Vilasi, Annalisa, Vlahakos, D., Vonk, R., Wright, P. C., Yamamoto, Tadashi, Yutaka, Y., Zielenkiewicz, P., Promponas, Vasilis J. [0000-0003-3352-4831], and Constantinou-Deltas, Constantinos D. [0000-0001-5549-9169]

Subjects
tumor necrosis factor related apoptosis inducing ligand, medicine.medical_specialty, hypertension, microalbuminuria, urinalysis, heat shock protein 27, laser capture microdissection, Clinical Biochemistry, prevalence, capillary electrophoresis, Clinical proteomics, Urine, Proteomics, Bioinformatics, medical research, disease marker, proteomics, Medicine, Medical physics, Cost action, human, Biomarker discovery, conference paper, mass spectrometry, Kidney diseases, business.industry, lymphocyte antigen, Ontology, practice guideline, bioinformatics, chronic kidney failure, tumor necrosis factor like weak inducer of apoptosis, Laser capture, biological marker, molecular imaging, time of flight mass spectrometry, unclassified drug, Important research, priority journal, Tissue proteomics, Urine specimen, Imaging MS, atherosclerosis, business, Working group, CD74 antigen, monocyte chemotactic protein 1, chronic kidney disease
Abstract

EuroKUP (Urine and Kidney Proteomics www.eurokup.org) is a COST (European Cooperation in the field of Scientific and Technical research: www.cost.esf.org Action fostering amulti-disciplinary network of investigators from 25 countries and focusing on facilitating translational proteomic research in kidney diseases. Four Working Groups focusing respectively on defining clinically important research questions in kidney diseases, kidney tissue proteomics, urine proteomics and bioinformatics have been generated. The EuroKUP members had their second combined Working Group and Management Committee (MC) meeting in Nafplio, Greece from March 29 to 30, 2009. This report summarizes the main presentations, discussions and agreed action points during this meeting. These refer to the design of collaborative projects and clinical center networks for specific kidney diseases establishment of guidelines for kidney tissue proteomics analysis by laser-based imaging- and laser capture microdissection-MS development and characterization of a "standard" urine specimen to be used for assessment of platform capability and data comparability in clinical proteomics applications definition of statistical requirements in biomarker discovery studies and development of a specialized kidney and urine ontology. Various training activities are planned involving training schools on laser capture microdissection- and imaging-MS, workshops on ontologies as well as short-term travel grants for junior investigators. © 2009 Wiley-VCH Verlag GmbH & Co. KGaA, Weinheim. 3 1017 1022 Cited By :8

Published
2009
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26. Twenty-one additional cases of familial renal glucosuria: Absence of genetic heterogeneity, high prevalence of private mutations and further evidence of volume depletion

Author

Calado, J. Sznajer, Y. Metzger, D. Rita, A. Hogan, M.C. Kattamis, A. Scharf, M. Tasic, V. Greil, J. Brinkert, F. Kemper, M.J. Santer, R.

Abstract

Introduction. Familial renal glucosuria (FRG) is a rare renal tubular disorder caused by mutations within the SLC5A2 gene. It is characterized by persistent glucosuria in the absence of hyperglycaemia and any other signs of generalized tubular dysfunction. In small series of patients previously reported, the molecular and phenotypic findings in FRG families, including first hints of extracellular volume depletion and activation of the renin-angiotensin-aldosterone system induced by natriuresis, have been described. We have now extended this analysis to another 21 consecutive cases from 17 pedigrees, including 11 cases with severe glucose excretion. Methods. Mutation analysis was performed by direct sequencing of the genomic coding segments of the SLC5A2 gene. In two cases with severe glucosuria, basal plasma renin activity and serum aldosterone concentrations were determined. Results. Within the 17 pedigrees, we have identified a total of 20 different SLC5A2 mutations. Fifteen have not been previously reported. In all glucosuric individuals tested, at least one SLC5A2 mutation could be identified. Heterozygous individuals were found to have only mild glucose excretion whereas homozygous or compound heterozygous patients had severe glucosuria, ranging from 10 to 86.5 g/1.73 m2/24 h. In two patients of the latter group, basal plasma renin activity and serum aldosterone concentration were determined and found to be raised to an average of 4.6-fold and 3.1-fold of the upper limit of the normal range, respectively. Discussion. The identification of at least one mutated allele in every affected individual in this cohort of 17 consecutively investigated families strongly suggests that genetic heterogeneity is not prevalent in FRG. Although 5 of the detected alleles have been described previously, 15 are novel, confirming that most mutations in FRG are private. Our finding of an activation of compensatory mechanisms for salt loss may warrant more detailed studies of long-term hormonal and metabolic imbalances in patients with FRG. © The Author [2008]. Published by Oxford University Press on behalf of ERA-EDTA. All rights reserved.

Published
2008

28. Whole-exome resequencing reveals recessive mutations in TRAP1 in individuals with CAKUT and VACTERL association

Author

Saisawat, P., Kohl, S., Hilger, A.C., Hwang, D.Y., Yung Gee, H., Dworschak, G.C., Tasic, V., Pennimpede, T., Natarajan, S., Sperry, E., Matassa, D.S., Stajic, N., Bogdanovic, R., Blaauw, I. de, Marcelis, C.L.M., Wijers, C.H.W., Bartels, E., Schmiedeke, E., Schmidt, D., Marzheuser, S., Grasshoff-Derr, S., Holland-Cunz, S., Ludwig, M., Nothen, M.M., Draaken, M., Brosens, E., Heij, H., Tibboel, D., Herrmann, B.G., Solomon, B.D., Klein, A., Rooij, I.A.L.M. van, Esposito, F., Reutter, H.M., Hildebrandt, F., Saisawat, P., Kohl, S., Hilger, A.C., Hwang, D.Y., Yung Gee, H., Dworschak, G.C., Tasic, V., Pennimpede, T., Natarajan, S., Sperry, E., Matassa, D.S., Stajic, N., Bogdanovic, R., Blaauw, I. de, Marcelis, C.L.M., Wijers, C.H.W., Bartels, E., Schmiedeke, E., Schmidt, D., Marzheuser, S., Grasshoff-Derr, S., Holland-Cunz, S., Ludwig, M., Nothen, M.M., Draaken, M., Brosens, E., Heij, H., Tibboel, D., Herrmann, B.G., Solomon, B.D., Klein, A., Rooij, I.A.L.M. van, Esposito, F., Reutter, H.M., and Hildebrandt, F.

Abstract

Item does not contain fulltext, Congenital abnormalities of the kidney and urinary tract (CAKUT) account for approximately half of children with chronic kidney disease and they are the most frequent cause of end-stage renal disease in children in the US. However, its genetic etiology remains mostly elusive. VACTERL association is a rare disorder that involves congenital abnormalities in multiple organs including the kidney and urinary tract in up to 60% of the cases. By homozygosity mapping and whole-exome resequencing combined with high-throughput mutation analysis by array-based multiplex PCR and next-generation sequencing, we identified recessive mutations in the gene TNF receptor-associated protein 1 (TRAP1) in two families with isolated CAKUT and three families with VACTERL association. TRAP1 is a heat-shock protein 90-related mitochondrial chaperone possibly involved in antiapoptotic and endoplasmic reticulum stress signaling. Trap1 is expressed in renal epithelia of developing mouse kidney E13.5 and in the kidney of adult rats, most prominently in proximal tubules and in thick medullary ascending limbs of Henle's loop. Thus, we identified mutations in TRAP1 as highly likely causing CAKUT or VACTERL association with CAKUT.

Published
2014

30. Novel ARP6B1 and ATP6N1B mutations in autosomal recessive distal renal tubular acidosis with new evidence for mild hearing loss

Author

Stover, E. H., Bortwick, K. J., Bavalia, C, Eady, N, Fritz, D, Rungroj, N, Giersch, A. B. S., Morton, C. C., Axon, P. R., Akil, I, AL SABBAN, E, Baguley, D. M., Bianca, S, Bakkaloglu, A, Bircan, Z, Chauveau, D, Clermont, M. J., Guala, A, Hulton, S, Kroes, H, LI VOLTI, Giovanni, Mir, S, Mocan, H, Nayir, A, Ozen, S, RODRIGUEZ SORIANO, J, Sanjad, S, Tasic, V, Taylor, M, Topaloglu, R, Smith, A. N., and Karet, F.

Published
2002

31. Whole-exome resequencing reveals recessive mutations in TRAP1 in individuals with CAKUT and VACTERL association

Author

Saisawat, P. (Pawaree), Kohl, R.H.G., Hilger, A.C. (Alina C), Hwang, D.-Y. (Daw-Yang), Yung Gee, H. (Heon), Dworschak, G.C. (Gabriel C), Tasic, V. (Velibor), Pennimpede, T. (Tracie), Natarajan, S. (Sivakumar), Sperry, E. (Ethan), Matassa, D.S. (Danilo S), Stajic, N. (Natasa), Bogdanovic, R. (Radovan), Blaauw, I. (Ivo) de, Marcelis, C.L.M. (Carlo), Wijers, C.H.W. (Charlotte), Bartels, E. (Enrika), Schmiedeke, E. (Eberhard), Schmidt, D. (Dedan), Märzheuser, S. (Stefanie), Grasshoff-Derr, S. (Sabine), Holland-Cunz, S. (Stefan), Ludwig, M. (Michael), Nöthen, M.M. (Markus), Draaken, M. (Markus), Brosens, E. (Erwin), Heij, H.A. (Hugo Anne), Tibboel, D. (Dick), Herrmann, B.G. (Bernhard G), Solomon, B.D. (Benjamin D), Klein, J.E.M.M. (Annelies) de, Rooij, I.A.L.M. (Iris), Esposito, F. (Francesco), Reutter, H. (Heiko), Hildebrandt, F. (Friedhelm), Saisawat, P. (Pawaree), Kohl, R.H.G., Hilger, A.C. (Alina C), Hwang, D.-Y. (Daw-Yang), Yung Gee, H. (Heon), Dworschak, G.C. (Gabriel C), Tasic, V. (Velibor), Pennimpede, T. (Tracie), Natarajan, S. (Sivakumar), Sperry, E. (Ethan), Matassa, D.S. (Danilo S), Stajic, N. (Natasa), Bogdanovic, R. (Radovan), Blaauw, I. (Ivo) de, Marcelis, C.L.M. (Carlo), Wijers, C.H.W. (Charlotte), Bartels, E. (Enrika), Schmiedeke, E. (Eberhard), Schmidt, D. (Dedan), Märzheuser, S. (Stefanie), Grasshoff-Derr, S. (Sabine), Holland-Cunz, S. (Stefan), Ludwig, M. (Michael), Nöthen, M.M. (Markus), Draaken, M. (Markus), Brosens, E. (Erwin), Heij, H.A. (Hugo Anne), Tibboel, D. (Dick), Herrmann, B.G. (Bernhard G), Solomon, B.D. (Benjamin D), Klein, J.E.M.M. (Annelies) de, Rooij, I.A.L.M. (Iris), Esposito, F. (Francesco), Reutter, H. (Heiko), and Hildebrandt, F. (Friedhelm)

Published
2013
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32. The impact of CFNS-causing EFNB1 mutations on ephrin-B1 function

Author

Makarov, R, Steiner, B, Gucev, Z, Tasic, V, Wieacker, P, Wieland, I, Makarov, R, Steiner, B, Gucev, Z, Tasic, V, Wieacker, P, and Wieland, I

Abstract

BACKGROUND: Mutations of EFNB1 cause the X-linked malformation syndrome craniofrontonasal syndrome (CFNS). CFNS is characterized by an unusual phenotypic pattern of inheritance, because it affects heterozygous females more severely than hemizygous males. This sex-dependent inheritance has been explained by random X-inactivation in heterozygous females and the consequences of cellular interference of wild type and mutant EFNB1-expressing cell populations. EFNB1 encodes the transmembrane protein ephrin-B1, that forms bi-directional signalling complexes with Eph receptor tyrosine kinases expressed on complementary cells. Here, we studied the effects of patient-derived EFNB1 mutations predicted to give rise to truncated ephrin-B1 protein or to disturb Eph/ephrin-B1 reverse ephrin-B1 signalling. Five mutations are investigated in this work: nonsense mutation c.196C > T/p.R66X, frameshift mutation c.614_615delCT, splice-site mutation c.406 + 2T > C and two missense mutations p.P54L and p.T111I. Both missense mutations are located in the extracellular ephrin domain involved in Eph-ephrin-B1 recognition and higher order complex formation. METHODS: Nonsense mutation c.196C > T/p.R66X, frameshift mutation c.614_615delCT and splice-site mutation c.406+2T > C were detected in the primary patient fibroblasts by direct sequencing of the DNA and were further analysed by RT-PCR and Western blot analyses.The impact of missense mutations p.P54L and p.T111I on cell behaviour and reverse ephrin-B1 cell signalling was analysed in a cell culture model using NIH 3T3 fibroblasts. These cells were transfected with the constructs generated by in vitro site-directed mutagenesis. Investigation of missense mutations was performed using the Western blot analysis and time-lapse microscopy. RESULTS AND DISCUSSION: Nonsense mutation c.196C > T/p.R66X and frameshift mutation c.614_615delCT escape nonsense-mediated RNA decay (NMD), splice-site mutation c.406+2T > C results in either retention of intr

Published
2010

37. The importance of rare diseases: from the gene to society

Author

Dodge, J. A., primary, Chigladze, T., additional, Donadieu, J., additional, Grossman, Z., additional, Ramos, F., additional, Serlicorni, A., additional, Siderius, L., additional, Stefanidis, C. J., additional, Tasic, V., additional, Valiulis, A., additional, and Wierzba, J., additional

Published
2010
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40. Twenty-one additional cases of familial renal glucosuria: absence of genetic heterogeneity, high prevalence of private mutations and further evidence of volume depletion

Author

Calado, J., primary, Sznajer, Y., additional, Metzger, D., additional, Rita, A., additional, Hogan, M. C., additional, Kattamis, A., additional, Scharf, M., additional, Tasic, V., additional, Greil, J., additional, Brinkert, F., additional, Kemper, M. J., additional, and Santer, R., additional

Published
2008
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46. Comparison between initial skew rate and moment based method for the printed text skew estimation.

Author

Brodic, D., Milivojevic, D. R., Dokic, B., and Tasic, V.

Abstract

In this paper, the methods for the estimation of the printed text skew are explored. Initail skew rate and moment based method are presented. They are tested with single and multi line document image samples in different resolutions. Furthermore, the results are evaluated by common measures. Moment based method proved its advantage in the domain of accuracy and robustness over the initial skew rate method. [ABSTRACT FROM PUBLISHER]

Published
2012

47. Microcontroller based systems for peak load reduction.

Author

Tasic, V., Milivojevic, D.R., Pavlov, M., Despotovic, V., and Brodic, D.

Abstract

The peaks in energy consumption arise when a number of consumers start to run within a relatively short period of time. In the case of large consumers, this can lead to an overload of the electro-energetic system. In order to avoid such scenarios, the consumers have to pay peak load additionally. The share of this cost in overall costs for electricity can be significant, up to 50% for smaller production plants with discontinuous production. For large consumers, peak load costs usually do not exceed 30% of total costs for electricity. In order to reduce the peak load, it is necessary to provide consistent power consumption that is without major short-term peaks. The paper presents several examples of microcontroller based systems for peak load reduction. [ABSTRACT FROM PUBLISHER]

Published
2012

49. CHILDREN BORN SMALL FOR GESTATIONAL AGE (SGA).

Author

Jancevska A., Tasic V., Damcevski N., Danilovski D., Jovanovska V., and Gucev Z.

Subjects
*GESTATIONAL age, *STANDARD deviations, *NEWBORN infants, *METABOLIC syndrome, *HYPOGLYCEMIA, *HYPOTENSION
Abstract

SGA (small for gestational age) is a child born with birth weight and/or length (BW/BL) under two standard deviations (2 SDS) for the gestational age and sex of the population. ~5% of all newborn children are SGA. A broad spectrum of factors are found to be causative: maternal, placental, foetal, metabolic, and genetic. In the newborn period the SGA children are at greater risk of life-threatening conditions: hypoglycaemia, hypercoagulability, necrotic enterocolitis, direct hyperbilirubinemia, hypotension, etc. Approximately 10 percent of SGA children do not achieve catch-up growth and remain short (≤ -2 SDS) into adulthood. SGA people have an increased incidence of metabolic syndrome, coronary artery disease, stroke, low bone density and osteoporosis. SGA children aged more than 4 years with no evidence of spontaneous catch-up and with a height ≥ 2.5 SD are considered for growth hormone (GH) treatment. [ABSTRACT FROM AUTHOR]

Published
2012

50. GROWTH HORMONE DEFICIENCY (GHD) AND SMALL FOR GESTATIONAL AGE (SGA): GENETIC ALTERATIONS.

Author

Jancevska, A., Gucev, Z. S., Pop-Jordanova, N., and Tasic, V.

Subjects
PITUITARY dwarfism, GROWTH hormone releasing factor, GENOTYPE-environment interaction, PROTEINS, SOMATOMEDIN, CELL transformation
Abstract

Short stature associated with GH deficiency has been estimated to occur in about 1 in 4000 to 1 in 10,000 in various studies. In the last decade new genetic defects have been described in all the levels of the growth hormone-releasing hormone (GH-RH)-GH IGF (insulin-like growth factor) axis. Genetic defects in the GHRH and in various parts of the Insulin-like growth factor system have been demonstrated. Genetic defects causing isolated GH deficiency (GHD), as well as multiple pituitary hormonal deficiencies have been analysed in detail. Signalling molecules and transcription factors leading to the development of the pituitary gland have been discovered and their function recognized. In animal models and in humans the importance of the transcription factors HESX1, PROP1, POUIFI, LHX3, LHX4, TBXI9, SOX2 and SOX3 has been extensively studied. Genetic alterations of those transcription factors dictate the highly variable phenotype: from isolated hypopituitarism to multiple pituitary hormonal deficiencies with or without malformations (e.g. septu-optic dysplasia or holoprosencephaly). Small for gestational age (SGA) children are increasingly recognized to be a heterogeneous group in which new mechanisms of growth retardation and metabolic disturbances have been proposed. Since SGA is considered to be the main reason for the short stature in 10% of short adults this is a large group with a great potential for novel insights into mechanisms of growth and metabolic disturbances. A group of signalling proteins are involved in prenatal (SGA) growth retardation: IRS-1, PDK1, AKT1, and S6K1. In addition, an attractive modem theory supposes that a disturbed mother-placenta- foetus relation results in the activation of the so-called "thrifty phenotype" of which the IGF system is a vital part. The mechanisms assure short-term postnatal survival in conditions of deficient nutritional supply. However, as a consequence, the abundant postnatal nutritional supply and the "thrifty phenotype" result in increased adult risk of metabolic syndrome, diabetes mellitus type 2 (DM2) and cardiovascular disease. [ABSTRACT FROM AUTHOR]

Published
2009

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