Autosomal recessive Alport syndrome caused by a novel COL4A4 splice site mutation: a case report

Šenjug, Petar; Nikuševa Martić, Tamara; Šenjug Perica, Marija; Oroz, Maja; Horaček, Matija; Ćuk, Martin; Abdović, Slaven; Galešić Ljubanović, Danica

doi:10.3325/cmj.2019.60.458

Pregled bibliografske jedinice broj: 1031697

Autosomal recessive Alport syndrome caused by a novel COL4A4 splice site mutation: a case report

Šenjug, Petar; Nikuševa Martić, Tamara; Šenjug Perica, Marija; Oroz, Maja; Horaček, Matija; Ćuk, Martin; Abdović, Slaven; Galešić Ljubanović, Danica

Autosomal recessive Alport syndrome caused by a novel COL4A4 splice site mutation: a case report // Croatian medical journal, 60 (2019), 5; 458-462 doi:10.3325/cmj.2019.60.458 (međunarodna recenzija, članak, znanstveni)

CROSBI ID: 1031697 Za ispravke kontaktirajte CROSBI podršku putem web obrasca

Naslov
Autosomal recessive Alport syndrome caused by a novel COL4A4 splice site mutation: a case report
(Autosomal recessive Alport syndrome caused by a novel COL4A4 splice site mutation: a case report)

Autori
Šenjug, Petar ; Nikuševa Martić, Tamara ; Šenjug Perica, Marija ; Oroz, Maja ; Horaček, Matija ; Ćuk, Martin ; Abdović, Slaven ; Galešić Ljubanović, Danica

Izvornik
Croatian medical journal (0353-9504) 60 (2019), 5; 458-462

Vrsta, podvrsta i kategorija rada
Radovi u časopisima, članak, znanstveni

Ključne riječi
Alport syndrome ; next generation sequencing

Sažetak
Alport syndrome (AS) is a genetically heterogenic, structural disorder of the glomerular basement membrane (GBM) due to the mutation of COL4A3, COL4A4, or COL4A5 genes, which clinically presents as progressive hematuric nephritis with ultrastructural changes of the GBM, high tone sensorineural hearing loss, and ocular lesions. About 15% of AS cases have autosomal mutations of COL4A3 and COL4A4 genes, including homozygous and compound heterozygous mutations. Here, we present a case of a two-year-old boy with autosomal recessive Alport syndrome (ARAS) caused by a novel c.193-2A>C COL4A4 mutation. The patient had a delayed motor and sensory development coupled with speech and language delay, megalencephaly, hematuria and proteinuria, and normal tonal audiogram and ophthalmology exam. Extensive genetic, metabolic, and neurologic workup performed at the age of 10 months was unremarkable and patient's megalencephaly was described as familial benign megalencephaly. Kidney biopsy analysis showed characteristic signs of AS. Mutations screening with use of Illumina MiSeq platform revealed that the patient was homozygous for a newly discovered splice acceptor pathogenic variant c.193-2A>C found in COL4A4 at the genomic position chr2:227985866 and both parents were heterozygous carriers. The genetic heterogeneity of AS makes the diagnostic process challenging. Although renal biopsy provides information about the characteristic GBM changes and the degree of renal parenchyma damage (interstitial fibrosis and tubular atrophy ratio), genetic testing is a more sensitive and specific method that also gives insight into potential disease severity and clinical course, and provides the basis for genetic counseling.

Izvorni jezik
Engleski

Znanstvena područja
Temeljne medicinske znanosti

POVEZANOST RADA

Ustanove:
Medicinski fakultet, Zagreb,
Klinika za infektivne bolesti "Dr Fran Mihaljević",
Klinička bolnica "Dubrava",
Dječja bolnica Srebrnjak,
Klinika za dječje bolesti

Profili:

Tamara Nikuševa Martić (autor)