Increased expression of anion transporter SLC26A9 delays diabetes onset in cystic fibrosis
Anh-Thu N. Lam, … , Scott M. Blackman, Garry R. Cutting
Anh-Thu N. Lam, … , Scott M. Blackman, Garry R. Cutting
Published October 3, 2019
Citation Information: J Clin Invest. 2020;130(1):272-286. https://doi.org/10.1172/JCI129833.
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Research Article Endocrinology Genetics

Increased expression of anion transporter SLC26A9 delays diabetes onset in cystic fibrosis

Abstract

Diabetes is a common complication of cystic fibrosis (CF) that affects approximately 20% of adolescents and 40%–50% of adults with CF. The age at onset of CF-related diabetes (CFRD) (marked by clinical diagnosis and treatment initiation) is an important measure of the disease process. DNA variants associated with age at onset of CFRD reside in and near SLC26A9. Deep sequencing of the SLC26A9 gene in 762 individuals with CF revealed that 2 common DNA haplotypes formed by the risk variants account for the association with diabetes. Single-cell RNA sequencing (scRNA-Seq) indicated that SLC26A9 is predominantly expressed in pancreatic ductal cells and frequently coexpressed with CF transmembrane conductance regulator (CFTR) along with transcription factors that have binding sites 5′ of SLC26A9. These findings were replicated upon reanalysis of scRNA-Seq data from 4 independent studies. DNA fragments derived from the 5′ region of SLC26A9-bearing variants from the low-risk haplotype generated 12%–20% higher levels of expression in PANC-1 and CFPAC-1 cells compared with the high- risk haplotype. Taken together, our findings indicate that an increase in SLC26A9 expression in ductal cells of the pancreas delays the age at onset of diabetes, suggesting a CFTR-agnostic treatment for a major complication of CF.

Authors

Anh-Thu N. Lam, Melis A. Aksit, Briana Vecchio-Pagan, Celeste A. Shelton, Derek L. Osorio, Arianna F. Anzmann, Loyal A. Goff, David C. Whitcomb, Scott M. Blackman, Garry R. Cutting

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Figure 1

Association of SLC26A9 variants with age at onset of CFRD in 762 p.Phe508del (F508del) homozygous individuals.

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Association of SLC26A9 variants with age at onset of CFRD in 762 p.Phe50...
Variants within a 47.7 kb region encompassing SLC26A9 (shown to scale at bottom) were tested. (A) Manhattan plot for association with CFRD (points, left y axis) and recombination ratio plotted by genomic location (blue line, right y axis). (B) SKAT-O test for association of sets of common (upper panel) and rare (lower panel) variants with CFRD. All variants within each 5 kb window, moved across the entire region in increments of 1250 bp, were tested for a combined association with CFRD via the SKAT-O test. The x axis denotes position on chromosome 1 (hg19), y axis shows −log10 of the regional P value. Association values were plotted at the center of each 5 kb window. Common and rare variants were assigned based on a MAF cut-off of 1%. Red line indicates significance threshold Bonferroni’s corrected for the number of sliding windows (P = 0.01/36 = 2.7 × 10–4). No other RefSeq genes are present in this region other than SLC26A9.