Clinical and genetic analysis of patients with cystinuria in the United Kingdom

Clinical and genetic analysis of patients with cystinuria in the United Kingdom

Cystinuria is a rare inherited renal stone disease. Mutations in the amino acid exchanger System b(0,+), the two subunits of which are encoded by SLC3A1 and SLC7A9, predominantly underlie this disease. The work analyzed the epidemiology of cystinuria and the influence of mutations in these two genes...

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Veröffentlicht in:Clinical journal of the American Society of Nephrology 2015-07, Vol.10 (7), p.1235-1245
Hauptverfasser: Rhodes, Hannah L, Yarram-Smith, Laura, Rice, Sarah J, Tabaksert, Ayla, Edwards, Noel, Hartley, Alice, Woodward, Mark N, Smithson, Sarah L, Tomson, Charles, Welsh, Gavin I, Williams, Margaret, Thwaites, David T, Sayer, John A, Coward, Richard J M
Format: Artikel
Sprache:eng
Schlagworte:
Adolescent
Adult
Age of Onset
Amino Acid Transport Systems, Basic - genetics
Amino Acid Transport Systems, Neutral - genetics
Child
Child, Preschool
Cystinuria - diagnosis
Cystinuria - epidemiology
Cystinuria - genetics
Cystinuria - therapy
Disease Progression
DNA Mutational Analysis - methods
Female
Gene Frequency
Genetic Predisposition to Disease
Humans
Kidney Calculi - diagnosis
Kidney Calculi - epidemiology
Kidney Calculi - genetics
Kidney Failure, Chronic - diagnosis
Kidney Failure, Chronic - epidemiology
Kidney Failure, Chronic - genetics
Male
Middle Aged
Multiplex Polymerase Chain Reaction
Mutation
Original
Phenotype
Prevalence
Registries
Renal Insufficiency, Chronic - diagnosis
Renal Insufficiency, Chronic - epidemiology
Renal Insufficiency, Chronic - genetics
Retrospective Studies
Severity of Illness Index
United Kingdom - epidemiology
Young Adult
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Zusammenfassung:Cystinuria is a rare inherited renal stone disease. Mutations in the amino acid exchanger System b(0,+), the two subunits of which are encoded by SLC3A1 and SLC7A9, predominantly underlie this disease. The work analyzed the epidemiology of cystinuria and the influence of mutations in these two genes on disease severity in a United Kingdom cohort. Prevalent patients were studied from 2012 to 2014 in the northeast and southwest of the United Kingdom. Clinical phenotypes were defined, and genetic analysis of SLC3A1 and SLC7A9 combining Sanger sequencing and multiplex ligation probe-dependent amplification was performed. In total, 76 patients (42 men and 34 women) were studied. All subjects had proven cystine stones. Median age of presentation (first stone episode) was 24 years old, but 21% of patients presented after 40 years old. Patients had varied clinical courses, with 37% of patients having ≥10 stone episodes; 70% had evidence of CKD, and 9% had reached ESRD as a result of cystinuria and its complications. Patients with cystinuria received a variety of different therapies, with no obvious treatment consensus. Notably, 20% of patients had staghorn calculi, with associated impaired renal function in 80% of these patients. Genetic analysis revealed that biallelic mutations were present in either SLC3A1 (n=27) or SLC7A9 (n=20); 22 patients had only one mutated allele detected (SLC3A1 in five patients and SLC7A9 in 17 patients). In total, 37 different mutant variant alleles were identified, including 12 novel mutations; 22% of mutations were caused by large gene rearrangements. No genotype-phenotype association was detected in this cohort. Patients with cystinuria in the United Kingdom often present atypically with staghorn calculi at ≥40 years old and commonly develop significant renal impairment. There is no association of clinical course with genotype. Treatments directed toward reducing stone burden need to be rationalized and developed to optimize patient care.
ISSN:1555-9041
1555-905X
DOI:10.2215/CJN.10981114