A Novel Mutation in a Japanese Family with X-linked Alport Syndrome

Abe, Yoshifusa; Iyoda, Masayuki; Nozu, Kandai; Hibino, Satoshi; Hihara, Kei; Yamaguchi, Yutaka; Yamamura, Takehira; Minamikawa, Shogo; Iijima, Kazumoto; Shibata, Takanori; Itabashi, Kazuo

doi:10.2169/internalmedicine.55.6873

Cited by 4 publications

(5 citation statements)

References 18 publications

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“…Among 578 missense variants, 14 (2.4%) pathogenic variants caused by single-base substitutions at the last nucleotide positions in exons were included in this study (Figure 1 and Table 1). 5, [24][25][26][27][28][29][30][31][32][33][34][35][36] In addition, 6 novel variants in our cohort were included. Finally, 20 variants were included in this study.…”

Section: Analyzed Variantsmentioning

confidence: 99%

Last Nucleotide Substitutions of COL4A5 Exons Cause Aberrant Splicing

Aoto

Horinouchi

Yamamura

et al. 2022

Kidney International Reports

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Section: Analyzed Variantsmentioning

confidence: 99%

Last Nucleotide Substitutions of COL4A5 Exons Cause Aberrant Splicing

Aoto

Horinouchi

Yamamura

et al. 2022

Kidney International Reports

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“…15 However, studies of X-inactivation in humans are difficult to interpret, in part because X-inactivation patterns vary in affected tissues and the peripheral blood cells that are usually assayed. [16][17][18][19] The lack of genotype-phenotype correlation in women and girls with X-linked Alport syndrome manifests also as the large intrafamilial variability of the age at kidney failure, compared with male relatives. 9 Any genotype-phenotype correlation is considered less pronounced in females than in males, and that therefore larger cohorts are required to demonstrate a relationship.…”

Section: Introductionmentioning

confidence: 99%

“… 15 Nevertheless, studies in humans are difficult to interpret, in part because X-inactivation patterns vary in different affected tissues and the peripheral blood cells that are usually examined. 16 , 17 , 18 , 19 …”

mentioning

confidence: 99%

A Systematic Review of Pathogenic COL4A5 Variants and Proteinuria in Women and Girls With X-linked Alport Syndrome

Gibson¹,

Gooyer²,

Huang³

et al. 2022

Kidney International Reports

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“…Differences in X-chromosome inactivation may affect disease severity. Abe et al identified a novel variation in a Japanese family using X-chromosome inactivation assays [ 10 ]. Yamamura et al demonstrated that the phenotype of female XLAS patients is not always mild, and the mechanisms determining the severity of female XLAS are multifactorial [ 11 ].…”

Section: Discussionmentioning

confidence: 99%

A family case of X-linked Alport syndrome patients with a novel variant in COL4A5

et al. 2018

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We herein report 2 Japanese patients with X-linked Alport syndrome (XLAS), with a novel variant in COL4A5 . Patient 1 was a 16-year-old Japanese girl with a history of microscopic hematuria, without proteinuria, renal dysfunction, deafness, or ocular abnormalities. At 13 years of age, renal biopsy was performed; however, a diagnosis of AS was not considered. When her mother (patient 2) was 40 years of age (3 years after patient 1 underwent a renal biopsy), patient 2 was found to have asymptomatic hematuria, proteinuria, and an increased serum creatinine level, without deafness and ocular abnormalities. Subsequently, immunofluorescence staining for alpha 5 chains of type IV collagen was performed in patient 1. Pathological findings were consistent with AS, and genetic analysis demonstrated that both patients had a heterozygous mutation in COL4A5 (NM_000495.4: exon41:c.C3769T: p.Q1257X). To date, more than 900 different COL4A5 mutations have been identified; however, this variant has not been previously described. Physicians have to consider AS when they perform a renal biopsy in all patients with hematuria despite absent/present of family history, hearing loss, and ocular abnormality. Especially, when findings of light microscopy and immunofluorescence microscope are unclear, it should be considered carefully. Electron microscopy findings are very important.

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A Novel Mutation in a Japanese Family with X-linked Alport Syndrome

Cited by 4 publications

References 18 publications

Last Nucleotide Substitutions of COL4A5 Exons Cause Aberrant Splicing

Last Nucleotide Substitutions of COL4A5 Exons Cause Aberrant Splicing

A Systematic Review of Pathogenic COL4A5 Variants and Proteinuria in Women and Girls With X-linked Alport Syndrome

A family case of X-linked Alport syndrome patients with a novel variant in COL4A5

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