Mutations in DSTYK and dominant urinary tract malformations

Sanna-Cherchi, S.; ...; Kosuljandić Vukić, Djurdjica; Vukojević, Katarina; Saraga-Babić, Mirna; Saraga, Marijan; ...; Tasić, V.; ...; ...; Gharavi, A.G.

Pregled bibliografske jedinice broj: 641635

Mutations in DSTYK and dominant urinary tract malformations

Sanna-Cherchi, S.; ...; Kosuljandić Vukić, Djurdjica; Vukojević, Katarina; Saraga-Babić, Mirna; Saraga, Marijan; ...; Tasić, V.; ...; ...; Gharavi, A.G.

Mutations in DSTYK and dominant urinary tract malformations // The New England journal of medicine, 369 (2013), 7; 621-629 (međunarodna recenzija, članak, znanstveni)

CROSBI ID: 641635 Za ispravke kontaktirajte CROSBI podršku putem web obrasca

Naslov
Mutations in DSTYK and dominant urinary tract malformations

Autori
Sanna-Cherchi, S. ; ... ; Kosuljandić Vukić, Djurdjica ; Vukojević, Katarina ; Saraga-Babić, Mirna ; Saraga, Marijan ; ... ; Tasić, V. ; ... ; ... ; Gharavi, A.G.

Izvornik
The New England journal of medicine (0028-4793) 369 (2013), 7; 621-629

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

Ključne riječi
DSTYK mutation; urinary tract malformations

Sažetak
Congenital abnormalities of the kidney and the urinary tract are the most common cause of pediatric kidney failure. These disorders are highly heterogeneous, and the etiologic factors are poorly understood. We performed genomewide linkage analysis and whole-exome sequencing in a family with an autosomal dominant form of congenital abnormalities of the kidney or urinary tract (seven affected family members). We also performed a sequence analysis in 311 unrelated patients, as well as histologic and functional studies. Linkage analysis identified five regions of the genome that were shared among all affected family members. Exome sequencing identified a single, rare, deleterious variant within these linkage intervals, a heterozygous splice-site mutation in the dual serine–threonine and tyrosine protein kinase gene (DSTYK). This variant, which resulted in aberrant splicing of messenger RNA, was present in all affected family members. Additional, independent DSTYK mutations, including nonsense and splice-site mutations, were detected in 7 of 311 unrelated patients. DSTYK is highly expressed in the maturing epithelia of all major organs, localizing to cell membranes. Knockdown in zebrafish resulted in developmental defects in multiple organs, which suggested loss of fibroblast growth factor (FGF) signaling. Consistent with this finding is the observation that DSTYK colocalizes with FGF receptors in the ureteric bud and metanephric mesenchyme. DSTYK knockdown in human embryonic kidney cells inhibited FGF-stimulated phosphorylation of extracellular-signal-regulated kinase (ERK), the principal signal downstream of receptor tyrosine kinases. We detected independent DSTYK mutations in 2.3% of patients with congenital abnormalities of the kidney or urinary tract, a finding that suggests that DSTYK is a major determinant of human urinary tract development, downstream of FGF signaling.

Izvorni jezik
Engleski

Znanstvena područja
Kliničke medicinske znanosti

POVEZANOST RADA

Projekti:
216-2160528-0507 - Genski izražaj u ranom razvoju čovjeka (Saraga-Babić, Mirna) ( CroRIS)

Ustanove:
Medicinski fakultet, Split

Profili:

Mirna Saraga-Babić (autor)