Your search keyword '"Sanna-Cherchi S"' showing total 8 results

1. 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., M. Choi, Bodria, M., Y. Liu, P. L. Weng, Lozanovski, V. J., Verbitsky, M., Lugani, F., Sterken, R., Paragas, N., Caridi, G., Carrea, A., Dagnino, M., Matema-Kiryluk, A., and Santamaría, G.

Subjects

*KIDNEY failure, *PEDIATRIC research, *SERINE/THREONINE kinases, *FIBROBLAST growth factors, *KIDNEY abnormalities, *URINARY organ abnormalities

Abstract

The article discusses a study that analyzed pediatric kidney failure, which found that dual serine-threonine and tyrosine protein kinase (DSTYK) gene is a major determinant of human urinary tract development, downstream of fibroblast growth factor (FGF) signaling. Particular focus is given to a family with autosomal dominant form of congenital abnormalities of kidney and urinary tract who participated in the study. It also discusses the heterozygous mutations in the DSTYK.

Published

2013

2. Familial aggregation of primary glomerulonephritis in an Italian population isolate: Valtrompia study.

Author

Izzi, C., Sanna-Cherchi, S., Prati, E., Belleri, R., Remedio, A., Tardanico, R., Foramitti, M., Guerini, S., Viola, B. F., Movilli, E., Beerman, I., Lifton, R., Leone, L., Gharavi, A., and Scolari, F.

Subjects

*GLOMERULONEPHRITIS, *URINALYSIS, *IMMUNOGLOBULIN A, *KIDNEY diseases, *HETEROGENEITY, *PROTEINURIA

Abstract

Hereditary factors are suspected to contribute to the pathogenesis of sporadic primary glomerulonephritis, but their contribution is difficult to delineate in the general population. We studied the prevalence of primary glomerulonephritis in an isolated population from the extreme northern Valtrompia valley, Northern Italy. Investigation of medical records, community urinary screening program and molecular characterization of the population's ancestry were performed; genealogies of affected individuals were researched. Forty-three patients with primary glomerulonephritis were identified: 25 had biopsy-proven disease (11 immunoglobulin A (IgA) nephropathy; eight mesangial proliferative glomerulonephritis without IgA deposits; four focal segmental glomerular sclerosis; two membranous nephropathy), and 18 had clinical glomerulonephritis. All 43 patients originated from three mountain villages (Collio, San Colombano, and Bovegno). In contrast, we found only four cases of primary glomerulonephritis in two nearby villages (Pezzaze and Tavernole) that shared similar population histories and lifestyles, demonstrating heterogeneity of risk factors for glomerulonephritis (P=3 × 10−5). All 43 affected individuals could be traced back to common ancestors (XVI–XVII centuries), enabling the construction of three large pedigree including three parent–child affected pairs and five affected siblings pairs. Molecular data showed lower genetic diversity and increased inbreeding in the Valtrompia population compared to the control population. Molecular and genealogical evidence of limited set of founders and the absence of shared nephritogenic environmental factors suggest that our patients share a common genetic susceptibility to the development of primary glomerulonephritis. Further molecular study of our families will offer the possibility to shed light on the genetic background underlying these glomerular disorders.Kidney International (2006) 69, 1033–1040. doi:10.1038/sj.ki.5000185; published online 22 February 2006 [ABSTRACT FROM AUTHOR]

Published

2006

3. Quantifying collagen in mouse kidneys.

Author

Sanna-Cherchi, S.

Subjects

*GENES, *GENOMES, *GENETICS, *FIBROSIS, *KIDNEY diseases, *LABORATORY mice

Abstract

Identification of genes underlying quantitative trait loci (QTLs) represents a formidable task. Recent advances in the annotation of the mouse genome and the availability of newly developed mouse strains should boost gene discovery. Kato and colleagues report the localization of a QTL for collagen type I deposition in kidneys on mouse chromosome 2, representing the first step for the identification of a gene involved in interstitial fibrosis, an important pathway in progression to end-stage renal failure in many kidney disorders.Kidney International (2008) 73, 987–989. doi:10.1038/ki.2008.70 [ABSTRACT FROM AUTHOR]

Published

2008

4. Recurrent autosomal-dominant focal segmental glomerulosclerosis.

Author

Sanna-Cherchi, S., Somenzi, D., Carnevali, M. L., Pilato, F. P., Carraro, M., Ghiggeri, G. M., and Allegri, L.

Subjects

*LETTERS to the editor, *KIDNEY glomerulus

Abstract

A letter to the editor on recurrent autosomal-dominant focal segmental glomerulosclerosis in the 2006 issue, Vol. 70, of the journal is presented.

Published

2006

5. Podocin-Related Mechanisms in Posttransplantation Recurrence of Focal Segmental Glomerulsclerosis

Author

Caridi, G., Dagnino, M., Sanna-Cherchi, S., Perfumo, F., and Ghiggeri, G.M.

Subjects

*PREVENTIVE medicine, *URINALYSIS, *RESPIRATORY organs, *KIDNEY diseases

Abstract

Abstract: Posttransplantation recurrence of focal segmental glomerulosclerosis (FSGS) is one of the most disarming events in human pathology with important social and psychological consequences. It usually occurs in 30% to 50% of patients affected by the primary form of the disease with an abrupt onset in the majority of cases occurring within 1 month of the transplantation. Prediction of recurrent cases and early therapy with plasmapheresis are the main goals of the therapy. Although the mechanism of posttransplantation recurrence is still obscure, it has been proposed to be of a multifactorial origin, in which plasma factors determine the shedding of proteins of the slit-diaphragm, such as nephrin and podocin, with structural alterations of the ultra-filtering unit of the glomerulus. Low resynthesis of podocin and/or haplo-insufficiency due to heterozygous mutations should represent significant predisposing factors to proteinuria. In this review, the role of podocin in posttransplantation recurrence will be evaluated focusing on the possibility that resynthesis of the protein could represent a key step also for stable normalization of the renal filter. The recent characterization of the podocin promoter cis- and trans- acting elements and the possibility to characterize low- and high-podocin producer haplotypes offer opportunities to evaluate the capacity for podocin resynthesis in the donor kidney. A review of the literature on posttransplantation recurrence of FSGS in patients originally carrying homozygous and/or heterozygous NPHS2 mutations supports the general idea of a multifactorial origin of the primary disease that can be extended to the pathogenesis of posttransplantation recurrence. [Copyright &y& Elsevier]

Published

2006

6. Cis and trans regulatory elements in NPHS2 promoter: Implications in proteinuria and progression of renal diseases.

Author

Di Duca, M, Oleggini, R, Sanna-Cherchi, S, Pasquali, L, Di Donato, A, Parodi, S, Bertelli, R, Caridi, G, Frasca, G, Cerullo, G, Amoroso, A, Schena, F P, Scolari, F, and Ghiggeri, G M

Subjects

*PROMOTERS (Genetics), *PROTEINURIA, *KIDNEY diseases, *GENETIC polymorphisms, *GENE expression

Abstract

Podocin (NPHS2) expression in podocytes is associated with variable degrees of proteinuria and progression to renal failure in different glomerular diseases that suggests different expression profiles in NPHS2 promoter. Three functional polymorphisms in NPHS2 promoter (−51T, −116T, and −535 insCTTTTTT3) were found determining strong downregulation (−73, −59, and −82%, respectively) of the reporter gene expression when transfected in podocytes. Electrophoretic mobility shift assay experiments showed that all wild-type variants (−51G, −116C, and −535 insCTTTTTT2) formed specific DNA–protein complexes with podocyte nuclear extracts that were abolished by the presence of the rare forms (−51T, −116T, and −535 insCTTTTTT3). In the case of −51G, upstream stimulatory factor-1 (USF1) was identified as the specific trans element in accord to binding inhibition experiments and USF1 RNAi silencing. Haplotype analysis of 204 normal controls and 545 patients with renal diseases (308 immunoglobulin (Ig)A nephropathy and 237 focal segmental glomerulosclerosis) evidenced that −116/−51 and −535/P2OL formed two blocks in strong linkage disequilibrium in both normal and pathological cohorts. The high NPHS2 promoter profile −116C/−51G haplotype was more frequent in patients with IgA nephropathy (P-value=0.005) and was associated with a better clinical outcome in terms of proteinuria and creatinine levels. Overall our study describes functional variants of NPHS2 promoter and characterizes trans-acting elements that modulate podocin expression in the kidney. High producer NPHS2 promoter haplotypes seem protective in patients with chronic glomerular diseases.Kidney International (2006) 70, 1332–1341. doi:10.1038/sj.ki.5001767; published online 9 August 2006 [ABSTRACT FROM AUTHOR]

Published

2006

7. 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

*URINARY organs, *CHROMOSOME duplication, *DNA microarrays, *SEX differentiation disorders, *KIDNEYS, *KIDNEY pelvis, *PLANT chromosomes

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. [ABSTRACT FROM AUTHOR]

Published

2019

8. Circulating anti-actin and anti-ATP synthase antibodies identify a sub-set of patients with idiopathic nephrotic syndrome.

Author

Musante, L., Candiano, G., Bruschi, M., Santucci, L., Carnemolla, B., Orecchia, P., Giampuzzi, M., Zennaro, C., Sanna-Cherchi, S., Carraro, M., Oleggini, R., Camussi, G., Perfumo, F., and Ghiggeri, G. M.

Subjects

*IMMUNOGLOBULINS, *NEPHROTIC syndrome, *ELECTROPHORESIS, *IMMUNOGLOBULIN G, *URINALYSIS, *MURIDAE

Abstract

Idiopathic nephrotic syndrome (iNS) with resistance or dependence to steroids is a common disease in children but in spite of an increasing clinical impact its pathogenesis is unknown. We screened for the presence of circulating antibodies against glomerular (podocytes, mesangium) and tubular cells (tubular epithelia) a cohort of 60 children with iNS including 8 patients with a familial trait of iNS or with proven mutation of NPHS1-NPHS2 and 12 with good sensitivity to steroids. Positive sera were found in 8 cases, all belonging to the category without familial trait/molecular defects. The targets of antibodies were characterized with Western blot and MALDI-Mass utilizing β-hexyl cell extracts separated with two-dimensional electrophoresis. In all cases antibodies of the IgM class were directed against ATP synthase β chain alone (4 cases) or in combination with actin (3 cases); one child presented IgG against aldose reductase. The clinical picture was nephrotic syndrome with steroid resistance or dependence and variable cyclosporin sensitivity; 3 patients developed end stage renal failure. The basic pathology picture was focal segmental glomerulosclerosis (FSGS) in 4 cases and mesangial proliferative glomerulonephrites with deposition of IgM in 2. Overall, patients with circulating auto-antibodies could not be readely differentiated on clinical grounds with the exception of 3 children who developed positivity for antinuclear antibodies during the follow-up. Affinity-purified IgM from one patient who underwent plasmapheresis for therapeutical pourposes (but not from a normal pool) induced proteinuria in Sprague-Dawley rats and concomitant human IgM deposition within glomeruli. This is the first report of circulating anti-actin/ATP synthase β chain antibodies in a subset of patients with iNS. Both pathological significance and clinical impact given by the presence of these antibodies and the relationship with other conditions such as lupus-erythematosus, characterized by their presence, must be defined. [ABSTRACT FROM AUTHOR]

Published

2005