Genetic architecture differences between pediatric and adult-onset inflammatory bowel diseases in the Polish population

نویسندگان

  • Jerzy Ostrowski
  • Agnieszka Paziewska
  • Izabella Lazowska
  • Filip Ambrozkiewicz
  • Krzysztof Goryca
  • Maria Kulecka
  • Tomasz Rawa
  • Jakub Karczmarski
  • Michalina Dabrowska
  • Natalia Zeber-Lubecka
  • Roman Tomecki
  • Anna Kluska
  • Aneta Balabas
  • Magdalena Piatkowska
  • Katarzyna Paczkowska
  • Jaroslaw Kierkus
  • Piotr Socha
  • Michal Lodyga
  • Grazyna Rydzewska
  • Maria Klopocka
  • Grazyna Mierzwa
  • Barbara Iwanczak
  • Elzbieta Krzesiek
  • Katarzyna Bak-Drabik
  • Jaroslaw Walkowiak
  • Beata Klincewicz
  • Piotr Radwan
  • Urszula Grzybowska-Chlebowczyk
  • Piotr Landowski
  • Agnieszka Jankowska
  • Bartosz Korczowski
  • Teresa Starzynska
  • Piotr Albrecht
  • Michal Mikula
چکیده

Most inflammatory bowel diseases (IBDs) are classic complex disorders represented by common alleles. Here we aimed to define the genetic architecture of pediatric and adult-onset IBDs for the Polish population. A total of 1495 patients were recruited, including 761 patients with Crohn's disease (CD; 424 pediatric), 734 patients with ulcerative colitis (UC; 390 pediatric), and 934 healthy controls. Allelotyping employed a pooled-DNA genome-wide association study (GWAS) and was validated by individual genotyping. Whole exome sequencing (WES) was performed on 44 IBD patients diagnosed before 6 years of age, 45 patients diagnosed after 40 years of age, and 18 healthy controls. Altogether, out of 88 selected SNPs, 31 SNPs were replicated for association with IBD. A novel BRD2 (rs1049526) association reached significance of P = 5.2 × 10-11 and odds ratio (OR) = 2.43. Twenty SNPs were shared between pediatric and adult patients; 1 and 7 were unique to adult-onset and pediatric-onset IBD, respectively. WES identified numerous rare and potentially deleterious variants in IBD-associated or innate immunity-associated genes. Deleterious alleles in both groups were over-represented among rare variants in affected children. Our GWAS revealed differences in the polygenic architecture of pediatric- and adult-onset IBD. A significant accumulation of rare and deleterious variants in affected children suggests a contribution by yet unexplained genetic components.

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عنوان ژورنال:

دوره 6  شماره 

صفحات  -

تاریخ انتشار 2016