HLA-B*07:02 and HLA-C*07:02 are associated with trimethoprim-sulfamethoxazole respiratory failure.
Jennifer L GoldmanJenna O MillerNeil A MillerRobert EveleighAndrew GibsonElizabeth J PhillipsTomi PastinenPublished in: The pharmacogenomics journal (2022)
We have identified an underrecognized severe adverse drug reaction (ADR) of trimethoprim-sulfamethoxazole (TMP-SMX) associated respiratory failure in previously healthy children and young adults. We investigated potential genetic risk factors associated with TMP-SMX induced respiratory failure in a cohort of seven patients. We explored whole genome sequence among seven patients representing nearly half of all reported cases worldwide and 63 unrelated control individuals in two stages: (1) human leukocyte antigen (HLA) locus variation as several other ADRs have been associated HLA genetic variants and (2) coding variation to catalog and explore potential rare variants contributing to this devastating reaction. All cases were either heterozygous (carriers) or homozygous for the common HLA-B*07:02-HLA-C*07:02 haplotype. Despite the small sample size, this observation is statistically significant both in conservative comparison to maximum reported population frequencies (binomial P = 0.00017 for HLA-B and P = 0.00028 for HLA-C) and to our control population assessed by same HLA genotyping approach (binomial P = 0.000001 for HLA-B and P = 0.000018 for HLA-C). No gene elsewhere in the genome harnessed shared rare case enriched coding variation. Our results suggests that HLA-B*07:02 and HLA-C*07:02 are necessary for a patient to develop respiratory failure due to TMP-SMX.
Keyphrases
- respiratory failure
- extracorporeal membrane oxygenation
- mechanical ventilation
- young adults
- end stage renal disease
- adverse drug
- genome wide
- newly diagnosed
- acute respiratory distress syndrome
- ejection fraction
- chronic kidney disease
- copy number
- prognostic factors
- rare case
- peritoneal dialysis
- endothelial cells
- emergency department
- drug induced
- early onset
- risk assessment
- gene expression
- microbial community
- dna methylation
- climate change
- wastewater treatment
- peripheral blood
- antibiotic resistance genes
- single molecule
- stress induced
- high glucose
- atomic force microscopy
- electronic health record
- electron transfer