Your search keyword '"Louiza Papazachariou"' showing total 5 results

1. Frequency of COL4A3/COL4A4 mutations amongst families segregating glomerular microscopic hematuria and evidence for activation of the unfolded protein response. Focal and segmental glomerulosclerosis is a frequent development during ageing.

Author

Louiza Papazachariou, Panayiota Demosthenous, Myrtani Pieri, Gregory Papagregoriou, Isavella Savva, Christoforos Stavrou, Michael Zavros, Yiannis Athanasiou, Kyriakos Ioannou, Charalambos Patsias, Alexia Panagides, Costas Potamitis, Kyproula Demetriou, Marios Prikis, Michael Hadjigavriel, Maria Kkolou, Panayiota Loukaidou, Androulla Pastelli, Aristos Michael, Akis Lazarou, Maria Arsali, Loukas Damianou, Ioanna Goutziamani, Andreas Soloukides, Lakis Yioukas, Avraam Elia, Ioanna Zouvani, Polycarpos Polycarpou, Alkis Pierides, Konstantinos Voskarides, and Constantinos Deltas

Subjects

Medicine, Science

Abstract

Familial glomerular hematuria(s) comprise a genetically heterogeneous group of conditions which include Alport Syndrome (AS) and thin basement membrane nephropathy (TBMN). Here we investigated 57 Greek-Cypriot families presenting glomerular microscopic hematuria (GMH), with or without proteinuria or chronic kidney function decline, but excluded classical AS. We specifically searched the COL4A3/A4 genes and identified 8 heterozygous mutations in 16 families (28,1%). Eight non-related families featured the founder mutation COL4A3-p.(G1334E). Renal biopsies from 8 patients showed TBMN and focal segmental glomerulosclerosis (FSGS). Ten patients (11.5%) reached end-stage kidney disease (ESKD) at ages ranging from 37-69-yo (mean 50,1-yo). Next generation sequencing of the patients who progressed to ESKD failed to reveal a second mutation in any of the COL4A3/A4/A5 genes, supporting that true heterozygosity for COL4A3/A4 mutations predisposes to CRF/ESKD. Although this could be viewed as a milder and late-onset form of autosomal dominant AS, we had no evidence of ultrastructural features or extrarenal manifestations that would justify this diagnosis. Functional studies in cultured podocytes transfected with wild type or mutant COL4A3 chains showed retention of mutant collagens and differential activation of the unfolded protein response (UPR) cascade. This signifies the potential role of the UPR cascade in modulating the final phenotype in patients with collagen IV nephropathies.

Published

2014

2. Epistatic role of the MYH9/APOL1 region on familial hematuria genes.

Author

Konstantinos Voskarides, Panayiota Demosthenous, Louiza Papazachariou, Maria Arsali, Yiannis Athanasiou, Michalis Zavros, Kostas Stylianou, Dimitris Xydakis, Eugenios Daphnis, Daniel P Gale, Patrick H Maxwell, Avraam Elia, Cristian Pattaro, Alkis Pierides, and Constantinos Deltas

Subjects

Medicine, Science

Abstract

Familial hematuria (FH) is explained by at least four different genes (see below). About 50% of patients develop late proteinuria and chronic kidney disease (CKD). We hypothesized that MYH9/APOL1, two closely linked genes associated with CKD, may be associated with adverse progression in FH. Our study included 102 thin basement membrane nephropathy (TBMN) patients with three known COL4A3/COL4A4 mutations (cohort A), 83 CFHR5/C3 glomerulopathy patients (cohort B) with a single CFHR5 mutation and 15 Alport syndrome patients (cohort C) with two known COL4A5 mild mutations, who were categorized as "Mild" (controls) or "Severe" (cases), based on renal manifestations. E1 and S1 MYH9 haplotypes and variant rs11089788 were analyzed for association with disease phenotype. Evidence for association with "Severe" progression in CFHR5 nephropathy was found with MYH9 variant rs11089788 and was confirmed in an independent FH cohort, D (cumulative p value = 0.001, odds ratio = 3.06, recessive model). No association was found with APOL1 gene. Quantitative Real time PCR did not reveal any functional significance for the rs11089788 risk allele. Our results derive additional evidence supporting previous reports according to which MYH9 is an important gene per se, predisposing to CKD, suggesting its usefulness as a prognostic marker for young hematuric patients.

Published

2013

3. The Power of Molecular Genetics in Establishing the Diagnosis and Offering Prenatal Testing: The Case for Alport Syndrome

Author

Alkis Pierides, Panagiota Demosthenous, Louiza Papazachariou, Panos Zirogiannis, Konstantinos Voskarides, and Constantinos Deltas

Subjects

Basement membrane, Genetics, medicine.medical_specialty, biology, business.industry, Glomerular basement membrane, medicine.disease, Molecular biology, Exon, Type IV collagen, medicine.anatomical_structure, Laminin, Molecular genetics, medicine, biology.protein, Alport syndrome, business, Gene

Abstract

Most Alport cases, 85%, are caused by mutations in the X-linked gene, COL4A5 that encodes the α5 chain of type IV collagen, the most abundant structural protein in the glomerular basement membrane (GBM). The remaining 15% of cases are caused by autosomal recessive mutations in the genes that encode the α3 and α4 chains of the type IV collagen, COL4A3/COL4A4 1,2. Thin basement membrane nephropathy (TBMN) is reportedly also a genetically heterogeneous condition, caused by heterozygous COL4A3/COL4A4 mutations in about 40-50% of the cases. No other responsible genes have been identified as yet. Collagen type IV, as all collagens, is a trimer formed by combinations of three of the six alpha chains, α1-α6. Genes COL4A1 and COL4A2 map to chromosome 13q34, COL4A3 and COL4A4 map to chromosome 2q36–q37 and COL4A5 and COL4A6 map to Xq22-23. All six genes are encoded in nearly 50 exons and close to 1600 aminoacids, and consist of an Nterminal 7S domain, a C-terminal non-collagenous (NC1) domain and a large collagenous domain in between, containing the characteristic Gly-X-Y repeat, common to all collagens. All six alpha chains contain 22-26 natural interruptions of the Gly-X-Y repeats, spread throughout their central collagenous domain. These are presumably regions of specific function and/or ligand binding sequences, of significance to its structural role in the basement membrane. Although there are many possible combinations among the six alpha chains, only three are biologically compatible and found in basement membranes. These are composed of α1α1α2, α3α4α5 and α5α5α6. Type IV collagen participates in forming networks interacting with additional important components of the basement membranes, such as laminin and nidogen 3,4. As a component of the glomerular filtration barrier, along

Published

2012

4. Investigation of Hellenic families with microscopic hematuria reveals the frequency of collagen IV mutations and evidence for activation of the unfolded protein response

Author

Constantinos Deltas, Louiza Papazachariou, Panagiota Demothenous, Myrtani Pieri, Konstantinos Voskarides, Alkis Pierides, Hellenic Nephrogenetics Research Consortium, Constantinos Deltas, Louiza Papazachariou, Panagiota Demothenous, Myrtani Pieri, Konstantinos Voskarides, Alkis Pierides, and Hellenic Nephrogenetics Research Consortium

Published

2014

5. The Power of Molecular Genetics in Establishing the Diagnosis and Offering Prenatal Testing: The Case for Alport Syndrome

Author

Constantinos Deltas, Konstantinos Voskarides, Panagiota Demosthenous, Louiza Papazachariou, Panos Zirogiannis, Alkis Pierides, Constantinos Deltas, Konstantinos Voskarides, Panagiota Demosthenous, Louiza Papazachariou, Panos Zirogiannis, and Alkis Pierides

Published

2012