SLC7A9 mutations in all three cystinuria subtypes

Daniel Leclerc; Marylise Boutros; Daniel Suh; Qing Wu; Manuel Palacin; James R Ellis; Paul Goodyer; Rima Rozen

doi:10.1046/j.1523-1755.2002.00602.x

SLC7A9 mutations in all three cystinuria subtypes

Kidney Int. 2002 Nov;62(5):1550-9. doi: 10.1046/j.1523-1755.2002.00602.x.

Authors

Daniel Leclerc¹, Marylise Boutros, Daniel Suh, Qing Wu, Manuel Palacin, James R Ellis, Paul Goodyer, Rima Rozen

Affiliation

¹ Department of Human Genetics, McGill University-Montreal Children's Hospital, Montreal, Quebec,Canada.

PMID: 12371955
DOI: 10.1046/j.1523-1755.2002.00602.x

Abstract

Background: Cystinuria is an inherited disorder of cystine and dibasic amino acid transport in kidney. Subtypes are defined by the urinary cystine excretion patterns of the obligate heterozygous parents: Type I/N (fully recessive or silent); Type II/N (high excretor); Type III/N (moderate excretor). The first gene implicated in cystinuria (SLC3A1) is associated with the Type I urinary phenotype. A second cystinuria gene (SLC7A9) was recently isolated, and mutations of this gene were associated with dominant (non-Type I) cystinuria alleles. Here we report genotype-phenotype studies of SLC7A9 mutations in a cohort of well-characterized cystinuria probands and their family members.

Methods: Individual exons of the SLC7A9 gene were screened by single strand conformation polymorphism (SSCP) analysis and sequencing of abnormally migrating fragments.

Results: Seven mutations were identified. A single bp insertion (799insA) was present in four patients: on Type III alleles in two patients and on Type II alleles in two patients. These results suggest that Type II and Type III may be caused by the same mutation and, therefore, other factors must influence urinary cystine excretion. A 4bp deletion in intron 12 (IVS12+4delAGTA) and a missense mutation (1245G-->A, A354T) were identified on Type III alleles. A nonsense codon (1491G-->T, E436X) and a possible splicing mutation (IVS9-17G-->A) were seen in a Type I/III patient, but the mutations could not be assigned to particular alleles. Of additional interest were two missense mutations (316T-->C, I44T and 967C-->T, P261L) linked to Type I alleles.

Conclusion: Our results provide evidence that some SLC7A9 mutations may be associated with fully recessive (Type I) forms of cystinuria. We also demonstrate SLC7A9 mutations in dominant Types II and III cystinuria. The finding of SLC7A9 mutations in all three subtypes underscores the complex interactions between specific cystinuria genes and other factors influencing cystine excretion. A simpler phenotypic classification scheme (recessive and dominant) for cystinuria is warranted.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Adult
Alternative Splicing
Amino Acid Transport Systems, Basic*
Base Sequence
Carrier Proteins / genetics*
Carrier Proteins / metabolism*
Child
Codon, Nonsense
Cystinuria / classification
Cystinuria / genetics*
Cystinuria / metabolism*
Female
Gene Deletion
Genotype
Humans
Male
Membrane Glycoproteins / genetics*
Membrane Glycoproteins / metabolism*
Molecular Sequence Data
Mutation, Missense*
Phenotype

Substances

Amino Acid Transport Systems, Basic
Carrier Proteins
Codon, Nonsense
Membrane Glycoproteins
SLC7A9 protein, human