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2. Rampant introgressive hybridization in Pogoniulus tinkerbirds (Piciformes: Lybiidae) despite millions of years of divergence

Author

Nwankwo, Emmanuel C, Mortega, Kim G, Karageorgos, Athanasios, Ogolowa, Bridget O, Papagregoriou, Gregory, Grether, Gregory F, Monadjem, Ara, and Kirschel, Alexander NG

Subjects
asymmetry, barbets, contact zones, convergence, interbreeding, introgression, phylogenetics, plumage coloration, speciation, species interactions, Biological Sciences, Evolutionary Biology
Published
2019

4. An international cohort study of autosomal dominant tubulointerstitial kidney disease due to REN mutations identifies distinct clinical subtypes

Author

Živná, Martina, Kidd, Kendrah, Zaidan, Mohamad, Vyleťal, Petr, Barešová, Veronika, Hodaňová, Kateřina, Sovová, Jana, Hartmannová, Hana, Votruba, Miroslav, Trešlová, Helena, Jedličková, Ivana, Sikora, Jakub, Hůlková, Helena, Robins, Victoria, Hnízda, Aleš, Živný, Jan, Papagregoriou, Gregory, Mesnard, Laurent, Beck, Bodo B., Wenzel, Andrea, Tory, Kálmán, Häeffner, Karsten, Wolf, Matthias T.F., Bleyer, Michael E., Sayer, John A., Ong, Albert C.M., Balogh, Lídia, Jakubowska, Anna, Łaszkiewicz, Agnieszka, Clissold, Rhian, Shaw-Smith, Charles, Munshi, Raj, Haws, Robert M., Izzi, Claudia, Capelli, Irene, Santostefano, Marisa, Graziano, Claudio, Scolari, Francesco, Sussman, Amy, Trachtman, Howard, Decramer, Stephane, Matignon, Marie, Grimbert, Philippe, Shoemaker, Lawrence R., Stavrou, Christoforos, Abdelwahed, Mayssa, Belghith, Neila, Sinclair, Matthew, Claes, Kathleen, Kopel, Tal, Moe, Sharon, Deltas, Constantinos, Knebelmann, Bertrand, Rampoldi, Luca, Kmoch, Stanislav, and Bleyer, Anthony J.

Published
2020
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5. Risk mapping for better governance in biobanking: the case of biobank.cy.

Author

Akyüz, Kaya, Goisauf, Melanie, Martin, Gillian M., Mayrhofer, Michaela Th., Antoniou, Stella, Charalambidou, Georgia, Deltas, Constantinos, Malatras, Apostolos, Papagregoriou, Gregory, Stefanou, Charalambos, and Voutounou, Mariel

Subjects
NETWORK governance, QUALITATIVE research, STAKEHOLDER analysis
Abstract

Introduction: Risk governance is central for the successful and ethical operation of biobanks and the continued social license for being custodians of samples and data. Risks in biobanking are often framed as risks for participants, whereas the biobank's risks are often considered as technical ones. Risk governance relies on identifying, assessing, mitigating and communicating all risks based on technical and standardized procedures. However, within such processes, biobank staff are often involved tangentially. In this study, the aim has been to conduct a risk mapping exercise bringing biobank staff as key actors into the process, making better sense of emerging structure of biobanks. Methods: Based on the qualitative research method of situational analysis as well as the card-based discussion and stakeholder engagement processes, risk mapping was conducted at the biobank setting as an interactive engagement exercise. The analyzed material comprises mainly of moderated group discussions. Results: The findings from the risk mapping activity are framed through an organismic metaphor: the biobank as a growing, living organism in a changing environment, where trust and sustainability are cross-cutting elements in making sense of the risks. Focusing on the situatedness of the dynamics within biobanking activity highlights the importance of prioritizing relations at the core of risk governance and promoting ethicality in the biobanking process by expanding the repertoire of considered risks. Conclusion: With the organismic metaphor, the research brings the diverse group of biobank staff to the central stage for risk governance, highlighting how accounting for such diversity and interdependencies at the biobank setting is a prerequisite for an adaptive risk governance. [ABSTRACT FROM AUTHOR]

Published
2024
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6. Clinical and genetic spectra of autosomal dominant tubulointerstitial kidney disease due to mutations in UMOD and MUC1

Author

Olinger, Eric, Hofmann, Patrick, Kidd, Kendrah, Dufour, Inès, Belge, Hendrica, Schaeffer, Céline, Kipp, Anne, Bonny, Olivier, Deltas, Constantinos, Demoulin, Nathalie, Fehr, Thomas, Fuster, Daniel G., Gale, Daniel P., Goffin, Eric, Hodaňová, Kateřina, Huynh-Do, Uyen, Kistler, Andreas, Morelle, Johann, Papagregoriou, Gregory, Pirson, Yves, Sandford, Richard, Sayer, John A., Torra, Roser, Venzin, Christina, Venzin, Reto, Vogt, Bruno, Živná, Martina, Greka, Anna, Dahan, Karin, Rampoldi, Luca, Kmoch, Stanislav, Bleyer, Anthony J., Sr., and Devuyst, Olivier

Published
2020
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7. Massive Parallel DNA Sequencing of Patients with Inherited Cardiomyopathies in Cyprus and Suggestion of Digenic or Oligogenic Inheritance

Author

Koutsofti, Constantina, primary, Ioannides, Marios, additional, Polydorou, Christiana, additional, Papagregoriou, Gregory, additional, Malatras, Apostolos, additional, Michael, George, additional, Hadjiioannou, Irene, additional, Pieri, Stylianos, additional, Loizidou, Eleni M., additional, Eftychiou, Christos, additional, Papasavvas, Elias, additional, Christophides, Theodoros, additional, Alkelai, Anna, additional, Kapoor, Manav, additional, Shuldiner, Alan R., additional, Avraamides, Panayiotis, additional, and Deltas, Constantinos, additional

Published
2024
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8. Autosomal dominant kidney disease phenocopying hypertensive nephropathy in Turkish Cypriot Families

Author

Ozdemir, Fezile, primary, Oygar, D. Deren, additional, Behlul, Ahmet, additional, Ataç, Salahi, additional, Bardak, Simge, additional, Yükseliş, Meral, additional, Papagregoriou, Gregory, additional, Malatras, Apostolos, additional, Gale, Daniel P., additional, Neild, Guy H., additional, Deltas, Constantinos, additional, and Gurkan, Cemal, additional

Published
2024
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9. biobank.cy: The Biobank of Cyprus past, present and future

Author

Loizidou, Eleni M., primary, Kyratzi, Maria, additional, Tsiarli, Maria A., additional, Kakouri, Andrea C., additional, Charalambidou, Georgia, additional, Antoniou, Stella, additional, Pieri, Stylianos, additional, Veloudi, Panagiota, additional, Mayrhofer, Michaela Th., additional, Wutte, Andrea, additional, Kozera, Lukasz, additional, Habermann, Jens, additional, Muller, Heimo, additional, Zatloukal, Kurt, additional, Sargsyan, Karine, additional, Michaelides, Alexandros, additional, Papaioannou, Maria, additional, Schizas, Christos, additional, Malatras, Apostolos, additional, Papagregoriou, Gregory, additional, and Deltas, Constantinos, additional

Published
2024
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12. Genetic Modifiers of Mendelian Monogenic Collagen IV Nephropathies in Humans and Mice

Author

Deltas, Constantinos, primary, Papagregoriou, Gregory, additional, Louka, Stavroula F., additional, Malatras, Apostolos, additional, Flinter, Frances, additional, Gale, Daniel P., additional, Gear, Susie, additional, Gross, Oliver, additional, Hoefele, Julia, additional, Lennon, Rachel, additional, Miner, Jeffrey H., additional, Renieri, Alessandra, additional, Savige, Judy, additional, and Turner, A. Neil, additional

Published
2023
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13. #5441 EVIDENCE THAT CHAPERONE 4-PBA TREATMENT ALLEVIATES THE RENAL PHENOTYPE IN ALPORT SYNDROME MOUSE MODELS

Author

Ioannou, Pavlos, primary, Odiatis, Christoforos, additional, Antoniadou, Kyriaki, additional, Pieri, Myrtani, additional, Papagregoriou, Gregory, additional, Malatras, Apostolos, additional, Samiotaki, Martina, additional, Horaček, Matija, additional, Ljubanovic, Danica Galesic, additional, Stylianou, Kostas, additional, and Deltas, Constantinos, additional

Published
2023
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15. Autosomal dominant tubulointerstitial kidney disease cosegregating with COL4A4:p.G545A in Turkish Cypriot families with kidney failure

Author

Ozdemir, Fezile, primary, Oygar, D Deren, additional, Behlul, Ahmet, additional, Ataç, Salahi, additional, Bardak, Simge, additional, Yükseliş, Meral, additional, Deltas, Constantinos, additional, Papagregoriou, Gregory, additional, Malatras, Apostolos, additional, Gale, Daniel P, additional, Gurkan, Cemal, additional, and Neild, Guy H, additional

Published
2023
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16. Novel and Founder Pathogenic Variants in X-Linked Alport Syndrome Families in Greece

Author

Hadjipanagi, Despina, primary, Papagregoriou, Gregory, additional, Koutsofti, Constantina, additional, Polydorou, Christiana, additional, Alivanis, Polichronis, additional, Andrikos, Aimilios, additional, Christodoulidou, Stalo, additional, Dardamanis, Manthos, additional, Diamantopoulos, Athanasios A., additional, Fountoglou, Anastasios, additional, Frangou, Eleni, additional, Georgaki, Eleni, additional, Giannikouris, Ioannis, additional, Gkinis, Velissarios, additional, Goudas, Pavlos C., additional, Kalaitzidis, Rigas G., additional, Kaperonis, Nikolaos, additional, Koutroumpas, Georgios, additional, Makrydimas, George, additional, Myserlis, Grigorios, additional, Mitsioni, Andromachi, additional, Paliouras, Christos, additional, Papachristou, Fotios, additional, Papadopoulou, Dorothea, additional, Papagalanis, Nikolaos, additional, Papagianni, Aikaterini, additional, Perysinaki, Garyfalia, additional, Siomou, Ekaterini, additional, Sombolos, Konstantinos, additional, Tzanakis, Ioannis, additional, Vergoulas, Georgios V., additional, Printza, Nicoletta, additional, and Deltas, Constantinos, additional

Published
2022
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18. A bovine miRNA, bta‐miR‐154c, withstands in vitro human digestion but does not affect cell viability of colorectal human cell lines after transfection

Author

Pieri, Myrtani, primary, Theori, Elena, additional, Dweep, Harsh, additional, Flourentzou, Myrofora, additional, Kalampalika, Foteini, additional, Maniori, Maria‐Arsenia, additional, Papagregoriou, Gregory, additional, Papaneophytou, Christos, additional, and Felekkis, Kyriacos, additional

Published
2022
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20. Circulating IgG Levels in SARS-CoV-2 Convalescent Individuals in Cyprus

Author

Mamais, Ioannis, primary, Malatras, Apostolos, additional, Papagregoriou, Gregory, additional, Giallourou, Natasa, additional, Kakouri, Andrea C., additional, Karayiannis, Peter, additional, Koliou, Maria, additional, Christaki, Eirini, additional, Nikolopoulos, Georgios K., additional, and Deltas, Constantinos, additional

Published
2021
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22. An international cohort study of autosomal dominant tubulointerstitial kidney disease due to mutations identifies distinct clinical subtypes

Author

Živná, Martina, primary, Kidd, Kendrah, additional, Zaidan, Mohamad, additional, Vyleťal, Petr, additional, Barešová, Veronika, additional, Hodaňová, Kateřina, additional, Sovová, Jana, additional, Hartmannová, Hana, additional, Votruba, Miroslav, additional, Trešlová, Helena, additional, Jedličková, Ivana, additional, Sikora, Jakub, additional, Hůlková, Helena, additional, Robins, Victoria, additional, Hnízda, Aleš, additional, Živný, Jan, additional, Papagregoriou, Gregory, additional, Mesnard, Laurent, additional, Beck, Bodo B., additional, Wenzel, Andrea, additional, Tory, Kálmán, additional, Häeffner, Karsten, additional, Wolf, Matthias T.F., additional, Bleyer, Michael E., additional, Sayer, John A., additional, Ong, Albert C.M., additional, Balogh, Lídia, additional, Jakubowska, Anna, additional, Łaszkiewicz, Agnieszka, additional, Clissold, Rhian, additional, Shaw-Smith, Charles, additional, Munshi, Raj, additional, Haws, Robert M., additional, Izzi, Claudia, additional, Capelli, Irene, additional, Santostefano, Marisa, additional, Graziano, Claudio, additional, Scolari, Francesco, additional, Sussman, Amy, additional, Trachtman, Howard, additional, Decramer, Stephane, additional, Matignon, Marie, additional, Grimbert, Philippe, additional, Shoemaker, Lawrence R., additional, Stavrou, Christoforos, additional, Abdelwahed, Mayssa, additional, Belghith, Neila, additional, Sinclair, Matthew, additional, Claes, Kathleen, additional, Kopel, Tal, additional, Moe, Sharon, additional, Deltas, Constantinos, additional, Knebelmann, Bertrand, additional, Rampoldi, Luca, additional, Kmoch, Stanislav, additional, and Bleyer, Anthony J., additional

Published
2020
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25. COL4A5 and LAMA5 variants co-inherited in familial hematuria: Digenic inheritance or genetic modifier effect?

Author

Voskarides, Konstantinos, Papagregoriou, Gregory, Hadjipanagi, Despina, Petrou, Ioanelli, Savva, Isavella, Elia, Avraam, Athanasiou, Yiannis, Pastelli, Androulla, Kkolou, Maria, Hadjigavriel, Michalis, Stavrou, Christoforos, Pierides, Alkis, Deltas, Constantinos, and Deltas, Constantinos [0000-0001-5549-9169]

Subjects
0301 basic medicine, Male, Pathology, 030232 urology & nephrology, Renal cysts, lcsh:RC870-923, urologic and male genital diseases, Glomerulonephritis, Membranous, 0302 clinical medicine, Focal segmental glomerulosclerosis, Medicine, Exome sequencing, Metalloproteinase, Collagen IV, Glomerular basement membrane, Middle Aged, Kidney disease, female genital diseases and pregnancy complications, Pedigree, medicine.anatomical_structure, Nephrology, Laminin alpha 5, Female, medicine.symptom, Research Article, Adult, Collagen Type IV, medicine.medical_specialty, Kidney cysts, Nephropathy, 03 medical and health sciences, Internal medicine, Exome Sequencing, Humans, Digenic inheritance, Genetic Testing, Alport syndrome, Hematuria, Modifier gene, business.industry, Genetic Variation, Familial hematuria, medicine.disease, lcsh:Diseases of the genitourinary system. Urology, FSGS, 030104 developmental biology, Thin Basement Membrane Nephropathy (TBMN), Synaptopodin, Laminin, business
Abstract

Background: About 40-50% of patients with familial microscopic hematuria (FMH) caused by thin basement membrane nephropathy (TBMN) inherit heterozygous mutations in collagen IV genes (COL4A3, COL4A4). On long follow-up, the full phenotypic spectrum of these patients varies a lot, ranging from isolated MH or MH plus low-grade proteinuria to chronic renal failure of variable degree, including end-stage renal disease (ESRD). Methods: Here, we performed Whole Exome Sequencing (WES) in patients of six families, presenting with autosomal dominant FMH, with or without progression to proteinuria and loss of renal function, all previously found negative for severe collagen IV mutations. Hierarchical filtering of the WES data was performed, followed by mutation prediction analysis, Sanger sequencing and genetic segregation analysis. Results: In one family with four patients, we found evidence for the contribution of two co-inherited variants in two crucial genes expressed in the glomerular basement membrane (GBM); LAMA5-p.Pro1243Leu and COL4A5-p.Asp654Tyr. Mutations in COL4A5 cause classical X-linked Alport Syndrome, while rare mutations in the LAMA5 have been reported in patients with focal segmental glomerulosclerosis. The phenotypic spectrum of the patients includes hematuria, proteinuria, focal segmental glomerulosclerosis, loss of kidney function and renal cortical cysts. Conclusions: A modifier role of LAMA5 on the background of a hypomorphic Alport syndrome causing mutation is a possible explanation of our findings. Digenic inheritance is another scenario, following the concept that mutations at both loci more accurately explain the spectrum of symptoms, but further investigation is needed under this concept. This is the third report linking a LAMA5 variant with human renal disease and expanding the spectrum of genes involved in glomerular pathologies accompanied by familial hematurias. The cystic phenotype overlaps with that of a mouse model, which carried a Lama5 hypomorphic mutation that caused severely reduced Lama5 protein levels and produced kidney cysts. 2018 The Author(s). The work was supported from the Cyprus Research Promotion Foundation through the grant NEW INFRASTRUCTURE/STRATEGIC/0308/24 to CD (co-funded by the European Regional Development Fund and the Republic of Cyprus). The funding body did not contribute to the design of study, collection, analysis and interpretation of data, or in manuscript writing. Scopus

Published
2018

26. Noninvasive Immunohistochemical Diagnosis and Novel MUC1 Mutations Causing Autosomal Dominant Tubulointerstitial Kidney Disease

Author

Živná, Martina, Kidd, Kendrah, Přistoupilová, Anna, Barešová, Veronika, DeFelice, Mathew, Blumenstiel, Brendan, Harden, Maegan, Conlon, Peter, Lavin, Peter, Connaughton, Dervla M., Hartmannová, Hana, Hodaňová, Kateřina, Stránecký, Viktor, Vrbacká, Alena, Živný, Jan, Votruba, Miroslav, Sovová, Jana, Hůlková, Helena, Robins, Victoria, Perry, Rebecca, Wenzel, Andrea, Beck, Bodo B., Seeman, Tomáš, Viklický, Ondřej, Rajnochová-Bloudíčková, Sylvie, Papagregoriou, Gregory, Deltas, Constantinos C., Alper, Seth L., Greka, Anna, Bleyer, Anthony J., Kmoch, Stanislav, Vyleťal, Petr, and Deltas, Constantinos [0000-0001-5549-9169]

Subjects
0301 basic medicine, Pathology, medicine.medical_specialty, medicine.diagnostic_test, 030232 urology & nephrology, General Medicine, Biology, medicine.disease, Frameshift mutation, Pathogenesis, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Nephrology, Gene duplication, medicine, Immunohistochemistry, Gene, Immunostaining, Kidney disease, Genetic testing
Abstract

Visual Overview Download figureOpen in new tabDownload powerpoint Background Autosomal dominant tubulointerstitial kidney disease caused by mucin-1 gene (MUC1) mutations (ADTKD-MUC1) is characterized by progressive kidney failure. Genetic evaluation for ADTKD-MUC1 specifically tests for a cytosine duplication that creates a unique frameshift protein (MUC1fs). Our goal was to develop immunohistochemical methods to detect the MUC1fs created by the cytosine duplication and, possibly, by other similar frameshift mutations and to identify novel MUC1 mutations in individuals with positive immunohistochemical staining for the MUC1fs protein. Methods We performed MUC1fs immunostaining on urinary cell smears and various tissues from ADTKD-MUC1–positive and –negative controls as well as in individuals from 37 ADTKD families that were negative for mutations in known ADTKD genes. We used novel analytic methods to identify MUC1 frameshift mutations. Results After technique refinement, the sensitivity and specificity for MUC1fs immunostaining of urinary cell smears were 94.2% and 88.6%, respectively. Further genetic testing on 17 families with positive MUC1fs immunostaining revealed six families with five novel MUC1 frameshift mutations that all predict production of the identical MUC1fs protein. Conclusions We developed a noninvasive immunohistochemical method to detect MUC1fs that, after further validation, may be useful in the future for diagnostic testing. Production of the MUC1fs protein may be central to the pathogenesis of ADTKD-MUC1. 29 9 2418 2431

Published
2018

27. Additional file 1: of COL4A5 and LAMA5 variants co-inherited in familial hematuria: digenic inheritance or genetic modifier effect?

Author

Voskarides, Konstantinos, Papagregoriou, Gregory, Hadjipanagi, Despina, Ioanelli Petrou, Savva, Isavella, Avraam Elia, Yiannis Athanasiou, Androulla Pastelli, Kkolou, Maria, Hadjigavriel, Michalis, Stavrou, Christoforos, Pierides, Alkis, and Constantinos Deltas

Abstract

WES statistics. Number of genetic variants called after the WES analysis. (DOCX 15 kb)

Published
2018
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29. Small Molecule Targets TMED9 and Promotes Lysosomal Degradation to Reverse Proteinopathy

Author

Dvela-Levitt, Moran, primary, Kost-Alimova, Maria, additional, Emani, Maheswarareddy, additional, Kohnert, Eva, additional, Thompson, Rebecca, additional, Sidhom, Eriene-Heidi, additional, Rivadeneira, Ana, additional, Sahakian, Nareh, additional, Roignot, Julie, additional, Papagregoriou, Gregory, additional, Montesinos, Monica S., additional, Clark, Abbe R., additional, McKinney, David, additional, Gutierrez, Juan, additional, Roth, Mark, additional, Ronco, Lucienne, additional, Elonga, Esther, additional, Carter, Todd A., additional, Gnirke, Andreas, additional, Melanson, Michelle, additional, Hartland, Kate, additional, Wieder, Nicolas, additional, Hsu, Jane C.-H., additional, Deltas, Constantinos, additional, Hughey, Rebecca, additional, Bleyer, Anthony J., additional, Kmoch, Stanislav, additional, Živná, Martina, additional, Barešova, Veronika, additional, Kota, Savithri, additional, Schlondorff, Johannes, additional, Heiman, Myriam, additional, Alper, Seth L., additional, Wagner, Florence, additional, Weins, Astrid, additional, Golub, Todd R., additional, Lander, Eric S., additional, and Greka, Anna, additional

Published
2019
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31. FO067ADTKD-MUC1 IN THE CYPRIOT POPULATION: GENOTYPING, DEEP-PHENOTYPING, BIOMARKER DISCOVERY AND THE SEARCH FOR A ROBUST TREATMENT

Author

Papagregoriou, Gregory, primary, Stavrou, Christoforos, additional, Christofides, Andrea, additional, Koutsofti, Constantina, additional, Zivna, Martina, additional, Kuhn, Eric, additional, Roignot, Julie, additional, Kmoch, Stanislav, additional, Bleyer, Anthony J, additional, Greka, Anna, additional, and Deltas, Constantinos, additional

Published
2019
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32. Distal renal tubular acidosis in a Libyan patient: Evidence for digenic inheritance

Author

Nagara, Majdi, Papagregoriou, Gregory, Ben Abdallah, Rim, Landoulsi, Zied, Bouyacoub, Yosra, Elouej, Sahar, Kefi, Rym, Pippucci, Tommaso, Voskarides, Konstantinos, Bashamboo, Anu, McElreavey, Kenneth, Hachicha, Mongia, Romeo, Giovanni, Seri, Marco, Deltas, Constantinos, Abdelhak, Sonia, Marseille medical genetics - Centre de génétique médicale de Marseille (MMG), Aix Marseille Université (AMU)-Institut National de la Santé et de la Recherche Médicale (INSERM), Laboratoire de Génomique Biomédicale et Oncogénétique - Biomedical Genomics and Oncogenetics Laboratory (LR11IPT05), Université de Tunis El Manar (UTM)-Institut Pasteur de Tunis, Réseau International des Instituts Pasteur (RIIP)-Réseau International des Instituts Pasteur (RIIP), University of Cyprus [Nicosia] (UCY), Department of Pediatrics, Hedi Chaker Hospital [Sfax], Alma Mater Studiorum Università di Bologna [Bologna] (UNIBO), Molecular Medicine Research Center, Laboratory of Molecular and Medical Genetics, University of Cyprus, Molecular Medicine Research Center and Laboratory of Molecular and Medical Genetics, Department of Biological Sciences, University of Cyprus, Génétique du Développement humain - Human developmental genetics, Institut Pasteur [Paris] (IP)-Centre National de la Recherche Scientifique (CNRS), Université de Tunis El Manar (UTM), University of Cyprus [Nicosia], Centre National de la Recherche Scientifique (CNRS)-Institut Pasteur [Paris], Nagara, Majdi, Papagregoriou, Gregory, Ben Abdallah, Rim, Landoulsi, Zied, Bouyacoub, Yosra, Elouej, Sahar, Kefi, Rym, Pippucci, Tommaso, Voskarides, Konstantino, Bashamboo, Anu, McElreavey, Kenneth, Hachicha, Mongia, Romeo, Giovanni, Seri, Marco, Deltas, Constantino, Abdelhak, Sonia, Institut Pasteur [Paris]-Centre National de la Recherche Scientifique (CNRS), and Deltas, Constantinos [0000-0001-5549-9169]

Subjects
0301 basic medicine, Male, Heterozygote, Multifactorial Inheritance, Vacuolar Proton-Translocating ATPases, Genetic counseling, Libya, Biology, medicine.disease_cause, Early-onset sensorineural hearing lo, Early-onset sensorineural hearing loss, 03 medical and health sciences, 0302 clinical medicine, Genetic, Distal renal tubular acidosis, Genetics, medicine, Humans, Digenic inheritance, dRTA Childhood, Genetics (clinical), Exome sequencing, Mutation, Heterozygote advantage, General Medicine, Acidosis, Renal Tubular, medicine.disease, Disease gene identification, 3. Good health, 030104 developmental biology, 030220 oncology & carcinogenesis, Child, Preschool, WES, [SDV.MHEP]Life Sciences [q-bio]/Human health and pathology
Abstract

International audience; AIM OF THE STUDY Recent advances in understanding the underlying molecular mechanism for distal renal tubular acidosis (dRTA), led to an increased attention towards the primary and the familial forms of the disease. Mutations in ATP6V1B1 and ATP6V0A4 are usually responsible for the recessive form of the disease. Mutations in gene AE1 encoding the Cl-/HCO3- exchanger, usually present as dominant dRTA, but a recessive pattern has been recently described. Our objective is to identify the mutational spectrum responsible of dRTA in a consanguineous Libyan family. MATERIALS AND METHODS Both ATP6V0A4 and ATP6V1B1 genes were preferentially screened in our patient. Additional whole exome sequencing (WES) in the same patient, offered a wider view on potential chromosomal rearrangements as well as the mutational spectrum of other genes involved in this disease. RESULTS The patient is a heterozygote for two different mutations, one in each of the genes ATP6V0A4 and ATP6V1B1, while no deleterious variation was detected in the remaining genes responsible for the recessive form of dRTA. Homozygosity mapping and WES confirmed our findings and supported the hypothesis of a digenic inheritance model existing as an explanation for dRTA. CONCLUSIONS To our knowledge, this is the first report describing a Libyan patient with dRTA who suffered from early-onset sensorineural hearing loss, with a digenic mode of inheritance, supported by the identification of two novel mutations. This study increases the understanding of how dRTA is genetically transmitted, while offers a good outline towards the molecular diagnostics and genetic counseling for dRTA in Lybians.

Published
2016

33. Noninvasive Immunohistochemical Diagnosis and Novel MUC1 Mutations Causing Autosomal Dominant Tubulointerstitial Kidney Disease

Author

Živná, Martina, primary, Kidd, Kendrah, additional, Přistoupilová, Anna, additional, Barešová, Veronika, additional, DeFelice, Mathew, additional, Blumenstiel, Brendan, additional, Harden, Maegan, additional, Conlon, Peter, additional, Lavin, Peter, additional, Connaughton, Dervla M., additional, Hartmannová, Hana, additional, Hodaňová, Kateřina, additional, Stránecký, Viktor, additional, Vrbacká, Alena, additional, Vyleťal, Petr, additional, Živný, Jan, additional, Votruba, Miroslav, additional, Sovová, Jana, additional, Hůlková, Helena, additional, Robins, Victoria, additional, Perry, Rebecca, additional, Wenzel, Andrea, additional, Beck, Bodo B., additional, Seeman, Tomáš, additional, Viklický, Ondřej, additional, Rajnochová-Bloudíčková, Sylvie, additional, Papagregoriou, Gregory, additional, Deltas, Constantinos C., additional, Alper, Seth L., additional, Greka, Anna, additional, Bleyer, Anthony J., additional, and Kmoch, Stanislav, additional

Published
2018
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34. COL4A5 and LAMA5 variants co-inherited in familial hematuria: digenic inheritance or genetic modifier effect?

Author

Voskarides, Konstantinos, primary, Papagregoriou, Gregory, additional, Hadjipanagi, Despina, additional, Petrou, Ioanelli, additional, Savva, Isavella, additional, Elia, Avraam, additional, Athanasiou, Yiannis, additional, Pastelli, Androulla, additional, Kkolou, Maria, additional, Hadjigavriel, Michalis, additional, Stavrou, Christoforos, additional, Pierides, Alkis, additional, and Deltas, Constantinos, additional

Published
2018
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35. Cystic diseases of the kidney: molecular biology and genetics

Author

Deltas, Constantinos and Papagregoriou, Gregory

Subjects
Cysts -- Genetic aspects -- Diagnosis, Kidney diseases -- Genetic aspects -- Diagnosis -- Care and treatment, Genetic screening -- Usage, Health
Abstract

* Context.--Cystic diseases of the kidney are a very heterogeneous group of renal inherited conditions, with more than 33 genes involved and encompassing Xlinked, autosomal dominant, and autosomal recessive inheritance. Although mostly monogenic with mendelian inheritance, there are clearly examples of oligogenic inheritance, such as 3 mutations in 2 genes, while the existence of genetic modifiers is perhaps the norm, based on the extent of variable expressivity and the broad spectrum of symptoms. Objectives.--To present in the form of a mini review the major known cystic diseases of the kidney for which genes have been mapped or cloned and characterized, with some information on their cellular and molecular biology and genetics, and to pay special attention to commenting on the issues of molecular diagnostics, in view of the genetic and allelic heterogeneity. Data Sources.--We used major reviews that make excellent detailed presentation of the various diseases, as well as original publications. Conclusions.--There is already extensive genetic heterogeneity in the group of cystic diseases of the kidney; however, there are still many more genes awaiting to be discovered that are implicated or mutated in these diseases. In addition, the synergism and interaction among this repertoire of gene products is largely unknown, while a common unifying aspect is the expression of nearly all of them at the primary cilium or the basal body. A major interplay of functions is anticipated, while mutations in all converge in the unifying phenotype of cyst formation. (Arch Pathol Lab Med. 2010;134:569-582), Geneticists have been searching for new genes to explain the inheritance patterns of many genetic diseases, including the cystic diseases of the kidney (CDKs), during the past 3 to 4 [...]

Published
2010

36. An international cohort study of autosomal dominant tubulointerstitial kidney disease due to RENmutations identifies distinct clinical subtypes

Author

Živná, Martina, Kidd, Kendrah, Zaidan, Mohamad, Vyleťal, Petr, Barešová, Veronika, Hodaňová, Kateřina, Sovová, Jana, Hartmannová, Hana, Votruba, Miroslav, Trešlová, Helena, Jedličková, Ivana, Sikora, Jakub, Hůlková, Helena, Robins, Victoria, Hnízda, Aleš, Živný, Jan, Papagregoriou, Gregory, Mesnard, Laurent, Beck, Bodo B., Wenzel, Andrea, Tory, Kálmán, Häeffner, Karsten, Wolf, Matthias T.F., Bleyer, Michael E., Sayer, John A., Ong, Albert C.M., Balogh, Lídia, Jakubowska, Anna, Łaszkiewicz, Agnieszka, Clissold, Rhian, Shaw-Smith, Charles, Munshi, Raj, Haws, Robert M., Izzi, Claudia, Capelli, Irene, Santostefano, Marisa, Graziano, Claudio, Scolari, Francesco, Sussman, Amy, Trachtman, Howard, Decramer, Stephane, Matignon, Marie, Grimbert, Philippe, Shoemaker, Lawrence R., Stavrou, Christoforos, Abdelwahed, Mayssa, Belghith, Neila, Sinclair, Matthew, Claes, Kathleen, Kopel, Tal, Moe, Sharon, Deltas, Constantinos, Knebelmann, Bertrand, Rampoldi, Luca, Kmoch, Stanislav, and Bleyer, Anthony J.

Abstract

There have been few clinical or scientific reports of autosomal dominant tubulointerstitial kidney disease due to RENmutations (ADTKD-REN), limiting characterization. To further study this, we formed an international cohort characterizing 111 individuals from 30 families with both clinical and laboratory findings. Sixty-nine individuals had a RENmutation in the signal peptide region (signal group), 27 in the prosegment (prosegment group), and 15 in the mature renin peptide (mature group). Signal group patients were most severely affected, presenting at a mean age of 19.7 years, with the prosegment group presenting at 22.4 years, and the mature group at 37 years. Anemia was present in childhood in 91% in the signal group, 69% prosegment, and none of the mature group. RENsignal peptide mutations reduced hydrophobicity of the signal peptide, which is necessary for recognition and translocation across the endoplasmic reticulum, leading to aberrant delivery of preprorenin into the cytoplasm. RENmutations in the prosegment led to deposition of prorenin and renin in the endoplasmic reticulum-Golgi intermediate compartment and decreased prorenin secretion. Mutations in mature renin led to deposition of the mutant prorenin in the endoplasmic reticulum, similar to patients with ADTKD-UMOD, with a rate of progression to end stage kidney disease (63.6 years) that was significantly slower vs. the signal (53.1 years) and prosegment groups (50.8 years) (significant hazard ratio 0.367). Thus, clinical and laboratory studies revealed subtypes of ADTKD-RENthat are pathophysiologically, diagnostically, and clinically distinct.

Published
2020
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38. A novel splice-site mutation in ATP6V0A4 gene in two brothers with distal renal tubular acidosis from a consanguineous Tunisian family

Author

Nagara, Majdi, Voskarides, Konstantinos, Elouej, S., Zaravinos, Apostolos, Riahi, Zied, Papagregoriou, Gregory N., Kefi Ben Atig, Rym, Boussetta, Khadija, Constantinou-Deltas, Constantinos D., Abdelhak, S., Tinsa, Faten, and Constantinou-Deltas, Constantinos D. [0000-0001-5549-9169]

Subjects
Male, child, Vacuolar Proton-Translocating ATPases, Tunisia, Novel mutation, ATP6V0A4, Distal renal tubular acidosis (dRTA), Tunisian population, adult, Siblings, Donor splice site, High-Throughput Nucleotide Sequencing, acidosis, renal tubular, ATP6V0A4 protein, human, consanguinity, Mutation, Humans, genetics, RNA Splice Sites, physiopathology, dna mutational analysis
Abstract

93 859 863 Cited By :1

Published
2015

39. Clinical and genetic spectra of autosomal dominant tubulointerstitial kidney disease due to mutations in UMODand MUC1

Author

Olinger, Eric, Hofmann, Patrick, Kidd, Kendrah, Dufour, Inès, Belge, Hendrica, Schaeffer, Céline, Kipp, Anne, Bonny, Olivier, Deltas, Constantinos, Demoulin, Nathalie, Fehr, Thomas, Fuster, Daniel G., Gale, Daniel P., Goffin, Eric, Hodaňová, Kateřina, Huynh-Do, Uyen, Kistler, Andreas, Morelle, Johann, Papagregoriou, Gregory, Pirson, Yves, Sandford, Richard, Sayer, John A., Torra, Roser, Venzin, Christina, Venzin, Reto, Vogt, Bruno, Živná, Martina, Greka, Anna, Dahan, Karin, Rampoldi, Luca, Kmoch, Stanislav, Bleyer, Anthony J., and Devuyst, Olivier

Abstract

Autosomal dominant tubulointerstitial kidney disease (ADTKD) is an increasingly recognized cause of end-stage kidney disease, primarily due to mutations in UMODand MUC1. The lack of clinical recognition and the small size of cohorts have slowed the understanding of disease ontology and development of diagnostic algorithms. We analyzed two registries from Europe and the United States to define genetic and clinical characteristics of ADTKD-UMODand ADTKD-MUC1and develop a practical score to guide genetic testing. Our study encompassed 726 patients from 585 families with a presumptive diagnosis of ADTKD along with clinical, biochemical, genetic and radiologic data. Collectively, 106 different UMODmutations were detected in 216/562 (38.4%) of families with ADTKD (303 patients), and 4 different MUC1mutations in 72/205 (35.1%) of the families that are UMOD-negative (83 patients). The median kidney survival was significantly shorter in patients with ADTKD-MUC1compared to ADTKD-UMOD(46 vs. 54 years, respectively), whereas the median gout-free survival was dramatically reduced in patients with ADTKD-UMODcompared to ADTKD-MUC1(30 vs. 67 years, respectively). In contrast to patients with ADTKD-UMOD, patients with ADTKD-MUC1had normal urinary excretion of uromodulin and distribution of uromodulin in tubular cells. A diagnostic algorithm based on a simple score coupled with urinary uromodulin measurements separated patients with ADTKD-UMODfrom those with ADTKD-MUC1with a sensitivity of 94.1%, a specificity of 74.3% and a positive predictive value of 84.2% for a UMODmutation. Thus, ADTKD-UMODis more frequently diagnosed than ADTKD-MUC1, ADTKD subtypes present with distinct clinical features, and a simple score coupled with urine uromodulin measurements may help prioritizing genetic testing.

Published
2020
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40. 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

Papazachariou, Louiza, Demosthenous, Panayiota, Pieri, Myrtani, Papagregoriou, Gregory N., Savva, Isavella, Stavrou, Christoforos V., Zavros, Michalis, Athanasiou, Yiannis, Ioannou, Kyriakos, Patsias, Charalambos, Panagides, Alexia, Potamitis, Costas, Demetriou, Kyproula, Prikis, Marios, Hadjigavriel, Michalis, Kkolou, Maria, Loukaidou, Panayiota, Pastelli, Androulla, Michael, Aristos, Lazarou, Akis, Arsali, Maria, Damianou, Loukas, Goutziamani, Ioanna, Soloukides, Andreas P., Yioukas, Lakis, Elia, Avraam, Zouvani, Ioanna, Polycarpou, Polycarpos, Pierides, Alkis M., Voskarides, Konstantinos, Constantinou-Deltas, Constantinos D., Demosthenous, Panayiota M., Voskarides, Konstantinos A., and Constantinou-Deltas, Constantinos D. [0000-0001-5549-9169]

Subjects
Male, Aging, Pathology, sequence analysis, kidney dysfunction, kidney disease, polymerase chain reaction, Nephritis, Hereditary, urologic and male genital diseases, Autoantigens, nephritis, middle aged, Renal Failure, genetics, Greece, Glomerulosclerosis, Focal Segmental, Glomerular basement membrane, adult, thin basement membrane nephropathy, High-Throughput Nucleotide Sequencing, tumstatin, Endoplasmic Reticula, aged, Nephrology, Medicine, Cellular Structures and Organelles, focal glomerulosclerosis, Collagen Type IV, medicine.medical_specialty, phenotype, Science, kidney biopsy, DNA sequence, Article, Nephropathy, Genetics, Renal Diseases, Point Mutation, Humans, human, end stage renal disease, COL4A3 gene, Aged, Hematuria, human cell, Biology and Life Sciences, DNA, medicine.disease, major clinical study, Endocrinology, Mutation, glomerulus basement membrane, Kidney Failure, Chronic, genetic transfection, proteinuria, mutation, podocyte, preschool child, Basement Membrane, Glomerulonephritis, Focal segmental glomerulosclerosis, Chronic Kidney Disease, Glomerular Basement Membrane, Medicine and Health Sciences, gene mutation, Microscopic hematuria, child, Secretory Pathway, Multidisciplinary, Podocytes, COL4A4 gene, cell line, unfolded protein response, Middle Aged, chronic kidney failure, autoantigen, Extracellular Matrix, medicine.anatomical_structure, female, Cell Processes, Female, COL4A4 protein, human, Research Article, Adult, Cell Line, Frameshift mutation, high throughput sequencing, male, collagen type 4, Internal medicine, medicine, heterozygosity, controlled study, family study, Alport syndrome, Cypriot, cell culture, Base Sequence, business.industry, aging, Glomerulosclerosis, Human Genetics, nucleotide sequence, Cell Biology, Sequence Analysis, DNA, type IV collagen alpha3 chain, hematuria, Unfolded Protein Response, pathology, business, metabolism, genetic predisposition, Kidney disease
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. © 2014 Papazachariou et al. 9 12 Cited By :13

Published
2014

41. A miR-1207-5p Binding Site Polymorphism Abolishes Regulation of HBEGF and Is Associated with Disease Severity in CFHR5 Nephropathy

Author

Papagregoriou, Gregory N., Erguler, K., Dweep, H., Voskarides, Konstantinos, Koupepidou, P., Athanasiou, Yiannis, Pierides, Alkis M., Gretz, N., Felekkis, Kyriacos N., Constantinou-Deltas, Constantinos D., and Constantinou-Deltas, Constantinos D. [0000-0001-5549-9169]

Subjects
molecular cloning, podocyte, Anatomy and Physiology, genetic association, genotype, kidney disease, Glomerulonephritis, Membranous, Severity of Illness Index, Western blotting, single nucleotide polymorphism, Immune Physiology, Nucleic Acids, Molecular Cell Biology, genetic algorithm, genetic polymorphism, genetics, complement, Regulation of gene expression, microRNA 1207 5p, Multidisciplinary, medicine.diagnostic_test, microRNA, predictive value, disease course, article, allele, Transfection, gene expression regulation, bioinformatics, chronic kidney failure, luciferase, reporter gene, gene therapy, HBEGF gene, unclassified drug, CFHR5 gene, Disease Progression, Medicine, Intercellular Signaling Peptides and Proteins, disease severity, down regulation, hospitalization, Research Article, Heparin-binding EGF-like Growth Factor, marker gene, Science, heparin binding epidermal growth factor, DNA sequence, Single-nucleotide polymorphism, Biology, glomerulopathy, heparin-binding EGF-like growth factor, Nephropathy, Molecular Genetics, Western blot, medicine, Genetics, follow up, Humans, controlled study, signal peptide, human, Allele, gene, gene identification, Binding Sites, Polymorphism, Genetic, binding site, human cell, DNA fragment, MIRN1207 microRNA, human, Human Genetics, Complement System Proteins, Genetic Therapy, medicine.disease, 3' untranslated region, Molecular biology, MicroRNAs, FHR5 protein, human, Gene Expression Regulation, RNA, Kidney Failure, Chronic, CFHR5 nephropathy, genetic transfection, membranous glomerulonephritis, Population Genetics
Abstract

Heparin binding epidermal growth factor (HBEGF) is expressed in podocytes and was shown to play a role in glomerular physiology. MicroRNA binding sites on the 3′UTR of HBEGF were predicted using miRWalk algorithm and followed by DNA sequencing in 103 patients diagnosed with mild or severe glomerulopathy. A single nucleotide polymorphism, miRSNP C1936T (rs13385), was identified at the 3′UTR of HBEGF that corresponds to the second base of the hsa-miR-1207-5p seed region. When AB8/13 undifferentiated podocytes were transfected with miRNA mimics of hsa-miR-1207-5p, the HBEGF protein levels were reduced by about 50%. A DNA fragment containing the miRSNP allele-1936C was cloned into the pMIR-Report Luciferase vector and co-transfected with miRNA mimics of hsa-miR-1207-5p into AB8/13 podocytes. In agreement with western blot data, this resulted in reduced luciferase expression demonstrating the ability of hsa-miR-1207-5p to directly regulate HBEGF expression. On the contrary, in the presence of the miRSNP 1936T allele, this regulation was abolished. Collectively, these results demonstrate that variant 1936T of this miRSNP prevents hsa-miR-1207-5p from down-regulating HBEGF in podocytes. We hypothesized that this variant has a functional role as a genetic modifier. To this end, we showed that in a cohort of 78 patients diagnosed with CFHR5 nephropathy (also known as C3-glomerulopathy), inheritance of miRSNP 1936T allele was significantly increased in the group demonstrating progression to chronic renal failure on long follow-up. No similar association was detected in a cohort of patients with thin basement membrane nephropathy. This is the first report associating a miRSNP as genetic modifier to a monogenic renal disorder. © 2012 Papagregoriou et al. 7 Cited By :30

Published
2012

42. 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

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

Published
2014
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44. Evidence for miR-548c-5p regulation of FOXC2 transcription through a distal genomic target site in human podocytes

Author

Christofides, Andrea, Papagregoriou, Gregory, Dweep, Harsh, Makrides, Neoklis, Gretz, Norbert, Felekkis, Kyriacos, Deltas, Constantinos, and Deltas, Constantinos [0000-0001-5549-9169]

Subjects
Transcription, Genetic, Down-Regulation, Cell Line, Podocyte, 03 medical and health sciences, Cellular and Molecular Neuroscience, Transcription (biology), medicine, Humans, Luciferase, RNA, Messenger, Enhancer, Molecular Biology, Transcription factor, Pharmacology, 0303 health sciences, Base Sequence, biology, Podocytes, 030302 biochemistry & molecular biology, Cell Differentiation, Forkhead Transcription Factors, Promoter, Genomics, Cell Biology, Transfection, Cell biology, MicroRNAs, HEK293 Cells, medicine.anatomical_structure, Gene Expression Regulation, biology.protein, Molecular Medicine, FOXC2
Abstract

Podocytes are highly differentiated epithelial cells outlining the glomerular vessels. FOXC2 is a transcription factor essential for inducing podocyte differentiation, development and maturation, and is considered to be the earliest podocyte marker. miRNA prediction analysis revealed a full-length target site for the primate-specific miR-548c-5p at a genomic region > 8 kb upstream of FOXC2. We hypothesised that the transcription rates of FOXC2 during podocyte differentiation might be tuned by miR-548c-5p through this target site. Experiments were performed with cultured human podocytes, transfected with luciferase reporter constructs bearing this target site region within an enhancer element of the native plasmid. The results confirmed a seed region-driven targeting potential by the miRNA, with mimics downregulating and inhibitors enhancing luciferase activity. Introducing mutations into the miRNA target seed region abolished the expected response. In cultured podocytes, FOXC2 mRNA and protein levels responded to miR-548c-5p abundance in a coordinated manner before and after induction of differentiation, with high statistical significance. Ago-ChIP experiments revealed occupancy of the miRNA target site by miRNA/RISC in undifferentiated cells and its release when differentiation is initiated, allowing its interaction with the gene’s promoter region to amplify FOXC2 expression, as shown by chromosome conformation capture and qRT-PCR. Moreover, the expression pattern of FOXC2 during podocyte differentiation seems to be affected by miR-548c-5p, as removal of either endogenous or mimic miR-548c-5p results in increased FOXC2 protein levels and cells resembling those undergoing differentiation. Collectively, results indicate a well-orchestrated regulatory model of FOXC2 expression by a remote upstream target site for miR-548c-5p. 77 12 2441 2459

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45. Haploinsufficiency of the miR-873/miR-876 microRNA cluster is associated with craniofacial abnormalities

Author

Koufaris, Costas, Papagregoriou, Gregory N., Kousoulidou, Ludmila, Moutafi, Maria, Tauber, Maïthé Thérèse, Jouret, Béatrice, Kieffer, Isabelle, Constantinou-Deltas, Constantinos D., Tanteles, George A., Anastasiadou, Violetta C., Patsalis, Philippos C., Sismani, Carolina, and Constantinou-Deltas, Constantinos D. [0000-0001-5549-9169]

Subjects
genetic association, Craniofacial abnormality, Sequence Homology, nerve protein, Haploinsufficiency, gene cluster, sonic hedgehog protein, Craniofacial, Alexander disease, Learning Disorders, genetics, membrane protein, chromosome 9p, Developmental defect, gene mutation, Hypertelorism, Sequence Deletion, Genetics, MiR-876, microRNA, MiR-873, Learning Disabilities, hypertelorism, chromosome deletion, General Medicine, bioinformatics, cell line, Hedgehog signaling pathway, neuroblastoma cell line, unclassified drug, priority journal, LINGO2 protein, Multigene Family, sequence alignment, Mammalia, medicine.symptom, signal transduction, Signal Transduction, skull, microRNA 876, Molecular Sequence Data, DNA sequence, morphogenesis, comparative genomic hybridization, Nerve Tissue Proteins, Biology, Article, Cell Line, learning disorder, craniofacial malformation, medicine, embryology, Humans, controlled study, Hedgehog Proteins, human, Hedgehog, multigene family, Body Patterning, growth, development and aging, MIRN876 microRNA, human, Base Sequence, gene deletion, MIRN873 microRNA, human, human cell, Skull, Macrocephaly, nucleotide sequence, Erinaceidae, sequence homology, Sequence Analysis, DNA, medicine.disease, Megalencephaly, MicroRNAs, molecular genetics, microRNA 873, Sequence Alignment, metabolism
Abstract

MicroRNA haploinsufficiency has been associated with developmental defects in only a limited number of cases. Here we report a de novo genomic microdeletion that includes the LINGO2 gene as well as two microRNA genes, MIR873 and MIR876, in a patient with craniofacial abnormalities - in particular macrocephaly and hypertelorism - and learning difficulties. Subsequent analysis revealed that the microRNAs affected by this de novo microdeletion form a mammalian-lineage, neuronal tissue-enriched cluster. In addition, bioinformatic analysis and experimental data indicate that miR-873 is involved in the regulation of the Hedgehog signaling, an essential pathway involved in craniofacial patterning and differentiation. Collectively these observations are consistent with a role of the miR-873/miR-876 microRNA cluster in physiological cranial bone development and indicate that mutations affecting these microRNAs could be a rare cause of developmental defect in humans. © 2015 Elsevier B.V. 561 95 100 Cited By :5

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46. Omega-3 fatty acids protect retinal neurons in the DBA/2J hereditary glaucoma mouse model

Author

Kalogerou, Maria, Kolovos, Panagiotis, Prokopiou, Ekatherine, Papagregoriou, Gregory, Deltas, Constantinos, Malas, Stavros, Georgiou, Tassos, and Deltas, Constantinos [0000-0001-5549-9169]

Subjects
Male, Retinal Ganglion Cells, genetic structures, Nitric Oxide Synthase Type II, Timolol, Administration, Ophthalmic, Mice, chemistry.chemical_compound, 0302 clinical medicine, Optic Nerve Diseases, chemistry.chemical_classification, Arachidonic Acid, biology, Interleukin-18, food and beverages, Eicosapentaenoic acid, Sensory Systems, Nitric oxide synthase, Drug Combinations, Eicosapentaenoic Acid, Mice, Inbred DBA, Docosahexaenoic acid, Female, lipids (amino acids, peptides, and proteins), Arachidonic acid, Glaucoma, Open-Angle, medicine.drug, Polyunsaturated fatty acid, medicine.medical_specialty, Cell Survival, Adrenergic beta-Antagonists, Blotting, Western, Real-Time Polymerase Chain Reaction, Neuroprotection, Tonometry, Ocular, 03 medical and health sciences, Cellular and Molecular Neuroscience, Internal medicine, Fatty Acids, Omega-3, medicine, Animals, Intraocular Pressure, Arginase, Tumor Necrosis Factor-alpha, business.industry, Retinal, eye diseases, Mice, Inbred C57BL, Disease Models, Animal, Ophthalmology, Endocrinology, chemistry, 030221 ophthalmology & optometry, biology.protein, sense organs, Ophthalmic Solutions, business, 030217 neurology & neurosurgery
Abstract

The purpose of this study was to evaluate the neuroprotective effects of omega-3 polyunsaturated fatty acid (ω3-PUFA) supplementation, alone or in combination with timolol eye drops, in a mouse model of hereditary glaucoma. DBA/2J mice (8.5-month-old) were assigned to an ω3-PUFAs + timolol, ω3-PUFAs only, timolol only, or an untreated group. Treated mice received a daily gavage administration of eicosapentaenoic acid (EPA) and docosahexaenoic acid and/or topical instillation of timolol (0.5%) once a day for 3 months. Blood was analysed regularly to determine ω3-PUFA levels and retinas were histologically analysed. Real-time PCR and Western blot were performed for retinal pro-inflammatory cytokines and macrophages. Blood arachidonic acid/EPA ratio gradually decreased and reached the desired therapeutic range (1–1.5) after 4 weeks of daily gavage with ω3-PUFAs in the ω3-PUFAs + timolol and ω3-PUFAs only groups. Retinal ganglion cell densities were significantly higher in the ω3-PUFAs + timolol (1303.77 ± 139.62/mm2), ω3-PUFAs only (768.40 ± 52.44/mm2) and timolol only (910.57 ± 57.28/mm2) groups than in the untreated group (323.39 ± 95.18/mm2). ω3-PUFA supplementation alone or timolol alone, significantly increased protein expression levels of M1 macrophage-secreted inducible nitric oxide synthase and M2 macrophage-secreted arginase-1 in the retina, which led to significant decreases in the expression levels of tumour necrosis factor-α (TNF-α). ω3-PUFA supplementation alone also resulted in significantly reduced expression of interleukin-18 (IL-18). ω3-PUFA + timolol treatment had no effect on the expression level of any of the aforementioned mediators in the retina. Supplementation with ω3-PUFAs has neuroprotective effect in the retinas of DBA/2J mice that is enhanced when combined with timolol eye drops. The continued inflammation following ω3-PUFAs + timolol treatment suggests that downregulation of IL-18 and TNF-α may not be the only factors involved in ω3-PUFA-mediated neuroprotection in the retina. 167 128 139

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49. Eight-Fold Increased COVID-19 Mortality in Autosomal Dominant Tubulointerstitial Kidney Disease due to MUC1 Mutations: An Observational Study.

Author

Kidd KO, Williams AH, Taylor A, Martin L, Robins V, Sayer JA, Olinger E, Mabillard HR, Papagregoriou G, Deltas C, Stavrou C, Conlon PJ, Hogan RE, Elhassan EAE, Springer D, Zima T, Izzi C, Vrbacká A, Piherová L, Pohludka M, Radina M, Vylet'al P, Hodanova K, Zivna M, Kmoch S, and Bleyer AJ

Abstract

Background: MUC1 and UMOD pathogenic variants cause autosomal dominant tubulointerstitial kidney disease (ADTKD). MUC1 is expressed in kidney, nasal mucosa and respiratory tract, while UMOD is expressed only in kidney. Due to haplo-insufficiency ADTKD- MUC1 patients produce approximately 50% of normal mucin-1., Methods: To determine whether decreased mucin-1 production was associated with an increased COVID-19 risk, we sent a survey to members of an ADTKD registry in September 2021, after the initial, severe wave of COVID-19. We linked results to previously obtained ADTKD genotype and plasma CA15-3 (mucin-1) levels and created a longitudinal registry of COVID-19 related deaths., Results: Surveys were emailed to 637 individuals, with responses from 89 ADTKD- MUC1 and 132 ADTKD- UMOD individuals. 19/83 (23%) ADTKD- MUC1 survey respondents reported a prior COVID-19 infection vs. 14/125 (11%) ADTKD- UMOD respondents (odds ratio (OR) 2.35 (95%CI 1.60-3.11, P = 0.0260). Including additional familial cases reported from survey respondents, 10/41 (24%) ADTKD- MUC1 individuals died of COVID-19 vs. 1/30 (3%) with ADTKD- UMOD , with OR 9.21 (95%CI 1.22-69.32), P = 0.03. The mean plasma mucin-1 level prior to infection in 14 infected and 27 uninfected ADTKD- MUC1 individuals was 7.06±4.12 vs. 10.21±4.02 U/mL ( P = 0.035). Over three years duration, our longitudinal registry identified 19 COVID-19 deaths in 360 ADTKD- MUC1 individuals (5%) vs. 3 deaths in 478 ADTKD- UMOD individuals (0.6%) ( P = 0.0007). Multivariate logistic regression revealed the following odds ratios (95% confidence interval) for COVID-19 deaths: ADTKD- MUC1 8.4 (2.9-29.5), kidney transplant 5.5 (1.6-9.1), body mass index (kg/m 2 ) 1.1 (1.0-1.2), age (y) 1.04 (1.0-1.1)., Conclusions: Individuals with ADTKD- MUC1 are at an eight-fold increased risk of COVID-19 mortality vs. ADTKD- UMOD individuals. Haplo-insufficient production of mucin-1 may be responsible.

Published
2024
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50. A glycine substitution in the collagenous domain of Col4a3 in mice recapitulates late onset Alport syndrome.

Author

Odiatis C, Savva I, Pieri M, Ioannou P, Petrou P, Papagregoriou G, Antoniadou K, Makrides N, Stefanou C, Ljubanović DG, Nikolaou G, Borza DB, Stylianou K, Gross O, and Deltas C

Abstract

Alport syndrome (AS) is a severe inherited glomerulopathy caused by mutations in the genes encoding the α-chains of type-IV collagen, the most abundant component of the extracellular glomerular basement membrane (GBM). Currently most AS mouse models are knockout models for one of the collagen-IV genes. In contrast, about half of AS patients have missense mutations, with single aminoacid substitutions of glycine being the most common. The only mouse model for AS with a homozygous knockin missense mutation, Col4a3-p.Gly1332Glu, was partly described before by our group. Here, a detailed in-depth description of the same mouse is presented, along with another compound heterozygous mouse that carries the glycine substitution in trans with a knockout allele. Both mice recapitulate essential features of AS, including shorten lifespan by 30-35%, increased proteinuria, increased serum urea and creatinine, pathognomonic alternate GBM thinning and thickening, and podocyte foot process effacement. Notably, glomeruli and tubuli respond differently to mutant collagen-IV protomers, with reduced expression in tubules but apparently normal in glomeruli. However, equally important is the fact that in the glomeruli the mutant α3-chain as well as the normal α4/α5 chains seem to undergo a cleavage at, or near the point of the mutation, possibly by the metalloproteinase MMP-9, producing a 35 kDa C-terminal fragment. These mouse models represent a good tool for better understanding the spectrum of molecular mechanisms governing collagen-IV nephropathies and could be used for pre-clinical studies aimed at better treatments for AS., (© 2021 The Authors.)

Published
2020
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