Digenic Alport Syndrome

Savige, Judy; Renieri, Alessandra; Ars, Elisabet; Daga, Sergio; Pinto, Anna Maria; Rothe, Hansjörg; Gale, Daniel P.; Aksenova, Marina; Čerkauskaitė, Agnė; Bielska, Olga; Lipska‐Ziętkiewicz, Beata S.; Gibson, Joel T

doi:10.2215/cjn.03120322

Cited by 32 publications

(23 citation statements)

References 43 publications

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“…Because there were two COL4A5 variants in one X chromosome in this family, the clinical phenotype of each victim was more severe than other families, the female patient developed ESRD at the age of 40, while the boy himself developed ESRD at the age of 11. In addition to the two COL4A5 variants in one X chromosome, the other X Chromosome also carried the two same COL4A5 variants, which contributed to a more severe renal phenotype in our boy, similar to the AS and FS case reported by Nishida et al 13 with homozygote COL4A5 variants or other digenic AS 20 . We suggest that the reason why AS patients combined with KS have a more severe renal phenotype might be homozygote or variants itself rather than X chromosome inactivation.…”

Section: Discussionsupporting

confidence: 85%

“…In addition to the two COL4A5 variants in one X chromosome, the other X Chromosome also carried the two same COL4A5 variants, which contributed to a more severe renal phenotype in our boy, similar to the AS and FS case reported by Nishida et al 13 with homozygote COL4A5 variants or other digenic AS. 20 We suggest that the reason why AS patients combined with KS have a more severe renal phenotype might be homozygote or variants itself rather than X chromosome inactivation. However, there are only four case reports of AS with KS in children, and among them two cases did not reach ESRD at the time when reported, see Table 2, the renal phenotypes need further observation with more samples in AS with KS.…”

Section: Discussionmentioning

confidence: 87%

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Combined Alport syndrome, Klinefelter syndrome and Fanconi syndrome in a Chinese boy

Zhang

Wang

2023

Nephrology

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Alport syndrome (AS) is a progressive renal disease characterized by hematuria and progressive renal failure. X‐linked dominant (XLAS) is the major inheritance form, accounting for almost 80% of the cases, caused by mutations in COL4A5 genes. Klinefelter syndrome (KS) is the most common genetic cause of human male gonadal dysgenesis. AS and KS are both rare disease, there are only three cases of combined AS and KS in the literatures. Fanconi syndrome (FS) caused by AS is also very rare. We report here the first case combined AS, KS and FS in a Chinese boy. We suggest that the severe renal phenotype and FS might be due to the two homozygous COL4A5 variants in our boy, and cases of AS combined KS will be good research objects for X chromosome inactivation.

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Section: Discussionsupporting

confidence: 85%

Section: Discussionmentioning

confidence: 87%

Combined Alport syndrome, Klinefelter syndrome and Fanconi syndrome in a Chinese boy

Zhang

Wang

2023

Nephrology

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“…Alport syndrome can also follow digenic inheritance, which is the presence of 2 pathogenic variants in different type IV collagen genes. 49 There have been several reports of digenic inheritance in Alport syndrome, which is another factor that likely contributes to variability in clinical presentation. 49 , 50 , 51 …”

Section: Geneticsmentioning

confidence: 99%

“… 49 There have been several reports of digenic inheritance in Alport syndrome, which is another factor that likely contributes to variability in clinical presentation. 49 , 50 , 51 …”

Section: Geneticsmentioning

confidence: 99%

Alport Syndrome: Clinical Spectrum and Therapeutic Advances

Gregorio¹,

Caparali²,

Shojaei³

et al. 2023

Kidney Medicine

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“…The diagnosis of thin membrane nephropathy was recommended to be abandoned [ 6 ]. Patients with pathogenic variants in more than one COL4 gene (digenic or trigenic inheritance), e.g., patients with digenic COL4A4 and COL4A3 mutations on different chromosomes (trans position) or on the same chromosome (cis position), demonstrate a clinical course similar to ARAS (trans position) or as ADAS (cis position) [ 7 ]. More studies evaluating the prognosis of patients’ digenic or trigenic mutations are necessary.…”

Section: Prevalence and Genetic Backgroundmentioning

confidence: 99%

Current and Future Therapeutical Options in Alport Syndrome

Reiterová

Tesař

2023

IJMS

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Alport syndrome (AS) is a hereditary kidney disease caused by pathogenic variants in COL4A3 and COL4A4 genes with autosomal recessive or autosomal dominant transmission or in the COL4A5 gene with X-linked inheritance. Digenic inheritance was also described. Clinically it is associated with microscopic hematuria, followed by proteinuria and chronic renal insufficiency with end-stage renal disease in young adults. Nowadays, there is no curative treatment available. The inhibitors of RAS (renin-angiotensin system) since childhood slow the progression of the disease. Sodium-glucose cotransporter-2 inhibitors seem to be promising drugs from DAPA-CKD (dapagliflozin–chronic kidney disease) study, but only a limited number of patients with Alport syndrome was included. Endothelin type A receptor and angiotensin II type 1 receptor combined inhibitors, and lipid-lowering agents are used in ongoing studies in patients with AS and focal segmental glomerulosclerosis (FSGS). Hydroxychloroquine in AS is studied in a clinical trial in China. Molecular genetic diagnosis of AS is crucial not only for prognosis prediction but also for future therapeutic options. Different types of mutations will require various types of gene, RNA, or protein therapy to improve the function, the of final protein product.

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Digenic Alport Syndrome

Cited by 32 publications

References 43 publications

Combined Alport syndrome, Klinefelter syndrome and Fanconi syndrome in a Chinese boy

Combined Alport syndrome, Klinefelter syndrome and Fanconi syndrome in a Chinese boy

Alport Syndrome: Clinical Spectrum and Therapeutic Advances

Current and Future Therapeutical Options in Alport Syndrome

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