Unbiased next generation sequencing analysis confirms the existence of autosomal dominant Alport syndrome in a relevant fraction of cases

Fallerini, Chiara; Dosa, Laura; Tita, Rossella; Prete, Dorella Del; Feriozzi, Sandro; Gai, Giorgia; Clementi, Maurizio; Manna, Angela La; Miglietti, Nunzia; Mancini, R. C.; Mandrile, Giorgia; Ghiggeri, Gian Marco; Piaggio, Giorgio; Brancati, Francesco; Diano, Laura; Frate, Elisabetta; Pinciaroli, Angela Rosa; Giani, Marisa; Castorina, Pierangela; Bresin, Elena; Giachino, Daniela; Marchi, Mario; Mari, Francesca; Bruttini, Mirella; Renieri, Alessandra; Ariani, Francesca

doi:10.1111/cge.12258

Cited by 122 publications

(128 citation statements)

References 16 publications

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“…Hearing loss was observed in 48% and ocular changes in 14% of the patients tested, while nearly all had ultrastructural GBM findings pathognomonic of AS. Interestingly, no FSGS was reported in this Italian cohort [31]. FSGS was not reported in additional cohorts of patients with heterozygous COL4A3/A4 mutations either, mainly from Italy.…”

Section: Tbmn and Accompanied Fsgs In The Molecular Genetics Eramentioning

confidence: 81%

“…Some authors have even reported that these patients with heterozygous mutations show autosomal dominant Alport syndrome (ADAS), since they described the ultrastructural pathognomonic features of the GBM, in addition to familial MH and proteinuria. Fallerini et al [31 ]reported on a cohort of heterozygous patients of whom 58% presented with proteinuria and 27.5% progressed to ESRD at a mean age of 56 years. Hearing loss was observed in 48% and ocular changes in 14% of the patients tested, while nearly all had ultrastructural GBM findings pathognomonic of AS.…”

Section: Tbmn and Accompanied Fsgs In The Molecular Genetics Eramentioning

confidence: 99%

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Carriers of Autosomal Recessive Alport Syndrome with Thin Basement Membrane Nephropathy Presenting as Focal Segmental Glomerulosclerosis in Later Life

Deltas

Savva²,

Voskarides³

et al. 2015

Nephron

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Collagen IV nephropathies (COL4Ns) comprise benign familial microscopic hematuria, thin basement membrane nephropathy (TBMN), X-linked Alport syndrome (AS) and also autosomal recessive and dominant AS. Apart from the X-linked form of AS, which is caused by hemizygous mutations in the COL4A5 gene, the other entities are caused by mutations in the COL4A3 or COL4A4 genes. The diagnosis of these conditions used to be based on clinical and/or histological findings of renal biopsies, but it is the new molecular genetics approach that revolutionised their investigation and proved particularly instrumental, especially, in many not so clear-cut cases. More recently, the spectrum of COL4N has expanded to include late onset focal segmental glomerulosclerosis (FSGS) that develops on top of TBMN in later life. Also, other reports showed that some patients with a primary diagnosis of familial FSGS proved to have variants in COL4 genes. In the presence of a renal biopsy picture of FSGS and in the absence of either electron microscopy studies or molecular genetic studies that point to TBMN and COL4N, the patient and his family may be mistakenly diagnosed with hereditary FSGS leading to unnecessary further investigations, erroneous family counselling and improper corticosteroid treatment. TBMN is a frequent finding in the general population, and according to several recent reports, it may be the underlying cause and the explanation for many familial and sporadic cases of late-onset FSGS with non-nephrotic proteinuria. This is an important new finding that needs widespread recognition. It is anticipated that the molecular genetic analysis with next generation sequencing will certainly offer timely correct diagnosis.

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Section: Tbmn and Accompanied Fsgs In The Molecular Genetics Eramentioning

confidence: 81%

Section: Tbmn and Accompanied Fsgs In The Molecular Genetics Eramentioning

confidence: 99%

Carriers of Autosomal Recessive Alport Syndrome with Thin Basement Membrane Nephropathy Presenting as Focal Segmental Glomerulosclerosis in Later Life

Deltas

Savva²,

Voskarides³

et al. 2015

Nephron

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“…Ten patients were considered as likely affected with BFH (however, in families 57 and 79, only women were affected), because individuals in at least two generations presented with isolated hematuria (without proteinuria or renal failure). One woman (40) presented with sporadic isolated hematuria without proteinuria. Supplemental Table 1 shows the clinical, biologic, and morphologic information, modified Flinter scoring (Concise Methods), and suspected mode of inheritance for each proband.…”

Section: Patients' Phenotypes and Mode Of Inheritancementioning

confidence: 99%

“…37 Analysis of our cohort for those criteria is shown Table 7, and the score of each patient is shown in Supplemental Table 1. Altogether, 4 index cases fulfilled four criteria, 14 index cases fulfilled three criteria, 38 index cases fulfilled two criteria, 43 index cases fulfilled one criterion (including 10 patients considered as BFH), and 2 index cases had zero criteria (one women [40] with sporadic hematuria and thin basement membrane and one man [42] with hematuria and proteinuria without hearing or eye defect and without known family history of renal disease). Surprisingly, two men had a discontinuous expression of the a5 (IV) in the skin BM.…”

Section: Patientsmentioning

confidence: 99%

Improving Mutation Screening in Familial Hematuric Nephropathies through Next Generation Sequencing

Morinière¹,

Dahan

Hilbert

et al. 2014

Journal of the American Society of Nephrology

135

131

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Alport syndrome is an inherited nephropathy associated with mutations in genes encoding type IV collagen chains present in the glomerular basement membrane. COL4A5 mutations are associated with the major X-linked form of the disease, and COL4A3 and COL4A4 mutations are associated with autosomal recessive and dominant forms (thought to be involved in 15% and 1%-5% of the families, respectively) and benign familial hematuria. Mutation screening of these three large genes is time-consuming and expensive. Here, we carried out a combination of multiplex PCR, amplicon quantification, and next generation sequencing (NGS) analysis of three genes in 101 unrelated patients. We identified 88 mutations and 6 variations of unknown significance on 116 alleles in 83 patients. Two additional indel mutations were found only by secondary Sanger sequencing, but they were easily identified retrospectively with the webbased sequence visualization tool Integrative Genomics Viewer. Altogether, 75 mutations were novel. Sequencing the three genes simultaneously was particularly advantageous as the mode of inheritance could not be determined with certainty in many instances. The proportion of mutations in COL4A3 and COL4A4 was notably high, and the autosomal dominant forms of Alport syndrome appear more frequently than reported previously. Finally, this approach allowed the identification of large COL4A3 and COL4A4 rearrangements not described previously. We conclude that NGS is efficient, reduces screening time and cost, and facilitates the provision of appropriate genetic counseling in Alport syndrome.

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“…One way to overcome these problems is to sequence all three genes simultaneously using NGS-targeted sequencing 14 . We present a new, efficient, amplicon based NGS protocol for simultaneous analysis of the coding regions (all the exons and flanking intronic sequences) of the COL4A3, A4 and A5 genes since a previously published NGS-based approach failed to detect mutations in 45% of their cases 11 . Both mutations and polymorphisms in the 3 investigated COL4A genes are thought to be highly population-specific due to the lack of selection pressure in case of the polymorphisms and low selection pressure in case of TBMN.…”

Section: Introductionmentioning

confidence: 99%

Application of next generation sequencing in the diagnosis of complex genetic disorders

Kovács¹

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Unbiased next generation sequencing analysis confirms the existence of autosomal dominant Alport syndrome in a relevant fraction of cases

Cited by 122 publications

References 16 publications

Carriers of Autosomal Recessive Alport Syndrome with Thin Basement Membrane Nephropathy Presenting as Focal Segmental Glomerulosclerosis in Later Life

Carriers of Autosomal Recessive Alport Syndrome with Thin Basement Membrane Nephropathy Presenting as Focal Segmental Glomerulosclerosis in Later Life

Improving Mutation Screening in Familial Hematuric Nephropathies through Next Generation Sequencing

Application of next generation sequencing in the diagnosis of complex genetic disorders

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