4.7 Article

Genetic Variation in the FAS Gene and Associations with Acute Lung Injury

Journal

Publisher

AMER THORACIC SOC
DOI: 10.1164/rccm.201003-0351OC

Keywords

adult respiratory distress syndrome; FAS receptor; genetic predisposition; apoptosis

Funding

  1. National Institutes of Health [P50-HL-73996, R01-HL-089807]
  2. National Heart, Lung, and Blood Institute
  3. Merck
  4. AHRQ
  5. Implicit Bioscience
  6. NHLBI
  7. NIAID
  8. CF Foundation
  9. Veterans Administration

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Rationale: Fas (CD95) modulates apoptosis and inflammation and is believed to play an important role in lung injury. Objectives: To determine if common genetic variation in FAS is associated with acute lung injury (ALI) susceptibility, risk of death, and FAS gene expression. Methods: We genotyped 14 single nucleotide polymorphisms (tagSNPS) in FAS in samples from healthy white volunteers (control subjects, n = 294) and patients with ALI (cases, n = 324) from the ARDSnet Fluid and Catheter Treatment Trial (FACTT). FAS genotypes associated with ALI in the discovery study were confirmed in a nested case-control validation study of critically ill patients at risk for ALI (n = 657). We also tested for associations between selected tagSNPS and FAS mRNA levels in whole blood from healthy control subjects exposed to media alone or LPS ex vivo. Measurements and Main Results: We identified associations between four tagSNPs in FAS (FAS(-11341A>T) [rs17447140], FAS(9325G>A) [rs2147420], FAS(21541C>T) [rs2234978], and FAS(24484A>T) [rs1051070]) and ALI case status. Haplotype-based analyses suggested that three of the tagSNPs (FAS(9325G>A), FAS(21541C>T), and FAS(244s4A>T)) function as a unit. The association with this haplotype and All was validated in a nested case-control study of at-risk subjects (P = 0.05). This haplotype was also associated with increased FAS mRNA levels in response to LPS stimulation. There was no association between FAS polymorphisms and risk of death among ALI cases. Conclusions: Common genetic variants in FAS are associated with ALI susceptibility. This is the first genetic evidence supporting a role for FAS in ALI.

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