The SPINK gene family and celiac disease susceptibility
Publication date
2007
Authors
Wapenaar, M.C.
Monsuur, A.J.
Poell, J.
Slot, R. van 't
Meijer, J.W.R.
Meijer, G.A.
Mulder, C.J.
Mearin, M.L.
Wijmenga, C.
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Supervisors
DOI
Document Type
Article
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Abstract
The gene family of serine protease inhibitors of
the Kazal type (SPINK) are functional and positional
candidate genes for celiac disease (CD). Our aim was to
assess the gut mucosal gene expression and genetic
association of SPINK1, -2, -4, and -5 in the Dutch CD
population. Gene expression was determined for all four
SPINK genes by quantitative reverse-transcription polymerase
chain reaction in duodenal biopsy samples from
untreated (n=15) and diet-treated patients (n=31) and
controls (n=16). Genetic association of the four SPINK
genes was tested within a total of 18 haplotype tagging
SNPs, one coding SNP, 310 patients, and 180 controls. The
SPINK4 study cohort was further expanded to include 479
CD cases and 540 controls. SPINK4 DNA sequence
analysis was performed on six members of a multigeneration
CD family to detect possible point mutations or
deletions. SPINK4 showed differential gene expression,
which was at its highest in untreated patients and dropped
sharply upon commencement of a gluten-free diet. Genetic
association tests for all four SPINK genes were negative,
including SPINK4 in the extended case/control cohort. No
SPINK4 mutations or deletions were observed in the
multigeneration CD family with linkage to chromosome
9p21-13 nor was the coding SNP disease-specific. SPINK4
exhibits CD pathology-related differential gene expression,
likely derived from altered goblet cell activity. All of the
four SPINK genes tested do not contribute to the genetic
risk for CD in the Dutch population.
Keywords
SPINK genes, Celiac disease, Quantitative reverse-transcription polymerase chain reaction, Genetic association