CTNS molecular genetics profile in a Persian nephropathic cystinosis population

CTNS molecular genetics profile in a Persian nephropathic cystinosis population

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Purpose: In this report, we document the CTNS gene mutations of 28 Iranian patients with nephropathic cystinosis age 1–17 years. All presented initially with severe failure to thrive, polyuria, and polydipsia. Methods: Cystinosis was primarily diagnosed by a pediatric nephrologist and then referred...

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Main Authors: Farideh Ghazi, Rozita Hosseini, Mansoureh Akouchekian, Shahram Teimourian, Zohreh Ataei Kachoei, Hassan Otukesh, William A. Gahl, Babak Behnam
Format: Article
Language:English
Published: Elsevier 2017-05-01
Series:Nefrología (English Edition)
Subjects:
Cystinosis
CTNS
Novel
Mutation
Iran
Online Access:http://www.sciencedirect.com/science/article/pii/S2013251417300494
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spelling doaj-08a43fe9c6784106a7ca0c41ef4ff6332020-11-25T01:22:20ZengElsevierNefrología (English Edition)2013-25142017-05-0137330131010.1016/j.nefroe.2017.02.007CTNS molecular genetics profile in a Persian nephropathic cystinosis populationFarideh Ghazi0Rozita Hosseini1Mansoureh Akouchekian2Shahram Teimourian3Zohreh Ataei Kachoei4Hassan Otukesh5William A. Gahl6Babak Behnam7Department of Medical Genetics and Molecular Biology, Faculty of Medicine, Iran University of Medical Sciences (IUMS), Tehran, IranDepartment of Pediatrics, Faculty of Medicine, Ali Asghar Children Hospital, Iran University of Medical Sciences (IUMS), Tehran, IranDepartment of Medical Genetics and Molecular Biology, Faculty of Medicine, Iran University of Medical Sciences (IUMS), Tehran, IranDepartment of Medical Genetics and Molecular Biology, Faculty of Medicine, Iran University of Medical Sciences (IUMS), Tehran, IranDepartment of Medical Genetics and Molecular Biology, Faculty of Medicine, Iran University of Medical Sciences (IUMS), Tehran, IranDepartment of Pediatrics, Faculty of Medicine, Ali Asghar Children Hospital, Iran University of Medical Sciences (IUMS), Tehran, IranSection on Human Biochemical Genetics, Medical Genetics Branch, National Human Genome Research Institute, NIH, Bethesda, MD, USADepartment of Medical Genetics and Molecular Biology, Faculty of Medicine, Iran University of Medical Sciences (IUMS), Tehran, IranPurpose: In this report, we document the CTNS gene mutations of 28 Iranian patients with nephropathic cystinosis age 1–17 years. All presented initially with severe failure to thrive, polyuria, and polydipsia. Methods: Cystinosis was primarily diagnosed by a pediatric nephrologist and then referred to the Iran University of Medical Sciences genetics clinic for consultation and molecular analysis, which involved polymerase chain reaction (PCR) amplification to determine the presence or absence of the 57-kb founder deletion in CTNS, followed by direct sequencing of the coding exons of CTNS. Results: The common 57-kb deletion was not observed in any of the 28 Iranian patients. In 14 of 28 patients (50%), mutations were observed in exons 6 and 7. No mutation was detected in exon 5, and only one (3.6%) patient with cystinosis showed a previously reported 4-bp deletion in exon 3 of CTNS. Four patients (14.3%) had a previously reported mutation (c.969C>A; p.N323K) in exon 11, and five (18%) had novel homozygous deletions in exon 6 leading to premature truncation of the protein. These deletions included c.323delA; p.Q108RfsX10 in three individuals and c.257-258delCT; p.S86FfsX37 in two cases. Other frame-shift mutations were all novel homozygous single base pair deletion/insertions including one in CTNS exon 9 (c.661insT; p.V221CfsX6), and four (14.3%) in exon 4, i.e., c.92insG; p.V31GfsX28 in two and c.120delC; p.T40TfsX10 in two. In total, we identified eight previously reported mutations and eight novel mutations in our patients. The only detected splice site mutation (IVS3-2A>C) was associated with the insertion mutation in the exon 9. Conclusion: This study, the first molecular genetic analysis of non-ethnic-specific Iranian nephropathic cystinosis patients, may provide guidance for molecular diagnostics of cystinosis in Iran.http://www.sciencedirect.com/science/article/pii/S2013251417300494CystinosisCTNSNovelMutationIran
collection DOAJ
language English
format Article
sources DOAJ
author Farideh Ghazi
Rozita Hosseini
Mansoureh Akouchekian
Shahram Teimourian
Zohreh Ataei Kachoei
Hassan Otukesh
William A. Gahl
Babak Behnam
spellingShingle Farideh Ghazi
Rozita Hosseini
Mansoureh Akouchekian
Shahram Teimourian
Zohreh Ataei Kachoei
Hassan Otukesh
William A. Gahl
Babak Behnam
CTNS molecular genetics profile in a Persian nephropathic cystinosis population
Nefrología (English Edition)
Cystinosis
CTNS
Novel
Mutation
Iran
author_facet Farideh Ghazi
Rozita Hosseini
Mansoureh Akouchekian
Shahram Teimourian
Zohreh Ataei Kachoei
Hassan Otukesh
William A. Gahl
Babak Behnam
author_sort Farideh Ghazi
title CTNS molecular genetics profile in a Persian nephropathic cystinosis population
title_short CTNS molecular genetics profile in a Persian nephropathic cystinosis population
title_full CTNS molecular genetics profile in a Persian nephropathic cystinosis population
title_fullStr CTNS molecular genetics profile in a Persian nephropathic cystinosis population
title_full_unstemmed CTNS molecular genetics profile in a Persian nephropathic cystinosis population
title_sort ctns molecular genetics profile in a persian nephropathic cystinosis population
publisher Elsevier
series Nefrología (English Edition)
issn 2013-2514
publishDate 2017-05-01
description Purpose: In this report, we document the CTNS gene mutations of 28 Iranian patients with nephropathic cystinosis age 1–17 years. All presented initially with severe failure to thrive, polyuria, and polydipsia. Methods: Cystinosis was primarily diagnosed by a pediatric nephrologist and then referred to the Iran University of Medical Sciences genetics clinic for consultation and molecular analysis, which involved polymerase chain reaction (PCR) amplification to determine the presence or absence of the 57-kb founder deletion in CTNS, followed by direct sequencing of the coding exons of CTNS. Results: The common 57-kb deletion was not observed in any of the 28 Iranian patients. In 14 of 28 patients (50%), mutations were observed in exons 6 and 7. No mutation was detected in exon 5, and only one (3.6%) patient with cystinosis showed a previously reported 4-bp deletion in exon 3 of CTNS. Four patients (14.3%) had a previously reported mutation (c.969C>A; p.N323K) in exon 11, and five (18%) had novel homozygous deletions in exon 6 leading to premature truncation of the protein. These deletions included c.323delA; p.Q108RfsX10 in three individuals and c.257-258delCT; p.S86FfsX37 in two cases. Other frame-shift mutations were all novel homozygous single base pair deletion/insertions including one in CTNS exon 9 (c.661insT; p.V221CfsX6), and four (14.3%) in exon 4, i.e., c.92insG; p.V31GfsX28 in two and c.120delC; p.T40TfsX10 in two. In total, we identified eight previously reported mutations and eight novel mutations in our patients. The only detected splice site mutation (IVS3-2A>C) was associated with the insertion mutation in the exon 9. Conclusion: This study, the first molecular genetic analysis of non-ethnic-specific Iranian nephropathic cystinosis patients, may provide guidance for molecular diagnostics of cystinosis in Iran.
topic Cystinosis
CTNS
Novel
Mutation
Iran
url http://www.sciencedirect.com/science/article/pii/S2013251417300494
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AT mansourehakouchekian ctnsmoleculargeneticsprofileinapersiannephropathiccystinosispopulation
AT shahramteimourian ctnsmoleculargeneticsprofileinapersiannephropathiccystinosispopulation
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