| Literature DB >> 32119686 |
Amber Dahlin1, Joanne E Sordillo2, Michael McGeachie1, Rachel S Kelly1, Kelan G Tantisira1,3, Sharon M Lutz2, Jessica Lasky-Su1, Ann Chen Wu1,2.
Abstract
While genome-wide association studies have identified genes involved in differential treatment responses to inhaled corticosteroids (ICS) in asthma, few studies have evaluated the potential effects of age in this context. A significant proportion of asthmatics experience exacerbations (hospitalizations and emergency department visits) during ICS treatment. We evaluated the interaction of genetic variation and age on ICS response (measured by the occurrence of exacerbations) through a genome-wide interaction study (GWIS) of 1,321 adult and child asthmatic patients of European ancestry. We identified 107 genome-wide suggestive (P<10-05) age-by-genotype interactions, two of which also met genome-wide significance (P<5x10-08) (rs34631960 [OR 2.3±1.6-3.3] in thrombospondin type 1 domain-containing protein 4 (THSD4) and rs2328386 [OR 0.5±0.3-0.7] in human immunodeficiency virus type I enhancer binding protein 2 (HIVEP2)) by joint analysis of GWIS results from discovery and replication populations. In addition to THSD4 and HIVEP2, age-by-genotype interactions also prioritized genes previously identified as asthma candidate genes, including DPP10, HDAC9, TBXAS1, FBXL7, and GSDMB/ORMDL3, as pharmacogenomic loci as well. This study is the first to link these genes to a pharmacogenetic trait for asthma.Entities:
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Year: 2020 PMID: 32119686 PMCID: PMC7051058 DOI: 10.1371/journal.pone.0229241
Source DB: PubMed Journal: PLoS One ISSN: 1932-6203 Impact factor: 3.240
Demographics of study populations.
| Discovery (N = 783) | Replication (N = 538) | ||||
|---|---|---|---|---|---|
| Sample size (N) | 113 | 24 | 270 | 58 | 229 |
| Sex (% male) | 58.4 | 29.2 | 27.4 | 69 | 29.7 |
| Age | 12.6 [9.2–17.2] | 35.8 [14.0–55.8] | 34.8 [20.0–68.5] | 7.3 [2.3–15.8] | 24.1 [5–46] |
| BMI (mean, [range]) | 20.9 [14.5–38] | 25.2 [18.8–35.7] | 31.2 [17.1–45.3] | 18.5 [14.2–28.5] | 26.9 [8.4–56.1] |
| Sample size (N) | 37 | 196 | 143 | 118 | 133 |
| Sex (% male) | 54.1 | 46.2 | 32.9 | 60.2 | 29.3 |
| Age | 13.4 [10.0–16.8] | 33.2 [14.4–65.2] | 31.4 [20.0–65.5] | 11.3 [6–17.8] | 25.6 [8–44] |
| BMI (mean, [range]) | 21.7 [16.3–41.1] | 25.2 [17.0–41.6] | 28.7 [16.5–43.3] | 20.7 [13.6–46.2] | 26.1 [15.4–49.5] |
*Age refers to age at event, for cases in PMRP and BioVu, or age at the final study visit, for all controls, and for the cases in CARE, ACRN and CAMP.
Summary of top 20 replicated age-by-genotype interactions obtained through GWIS of ICS response.
| Discovery | Replication | ||||||||
|---|---|---|---|---|---|---|---|---|---|
| SNP | Chr. | Major Allele | Minor Allele | Gene | Odds Ratio (95% CI) | P Value | Odds Ratio (95% CI) | P Value | Joint P Value |
| rs34631960 | 15 | CTT | C | 2.33(1.61–3.38); 0.12 (0.02–0.85) | 7.08X10-06 | 1.82(1.23–2.7); 7.35 (1.23–44.05) | 2.97X10-03 | 3.64X10-08 | |
| rs2328386 | 6 | C | T | 0.33(0.2–0.55); 0.19 (0.02–1.41) | 1.86X10-05 | 0.51(0.34–0.77); 0.55 (0.07–4.28) | 1.49X10-03 | 4.98X10-08 | |
| rs290119 | 5 | G | A | 2.38(1.6–3.53); 0.27 (0.03–2.51) | 1.76X10-05 | 1.96(1.28–3); 16.6(0.64–433.2) | 1.99X10-03 | 6.13X10-08 | |
| rs290122 | 5 | C | T | 2.38(1.6–3.53); 0.27 (0.03–2.51) | 1.76X10-05 | 1.96(1.28–3); 16.6(0.64–433.2) | 1.99X10-03 | 6.13X10-08 | |
| rs58836160 | 5 | T | TA | 2.38(1.6–3.53); 0.27 (0.03–2.51) | 1.76X10-05 | 1.96(1.28–3); 16.6(0.64–433.2) | 1.99X10-03 | 6.13X10-08 | |
| rs6892109 | 5 | C | T | 2.7(1.73–4.22); 0.01 (0–0.24) | 1.34X10-05 | 2.09(1.26–3.46); 6.2(0.38–101.5) | 4.39X10-03 | 9.90X10-08 | |
| chr12:121988899 | 12 | C | T | 2.38(1.62–3.48); 0.32 (0.05–2.2) | 8.52X10-06 | 1.69(1.14–2.51); 2.6(0.01–474.3) | 9.73X10-03 | 1.42X10-07 | |
| rs12658947 | 5 | A | G | 2.69(1.72–4.2); 0.02 (0–0.26) | 1.51X10-05 | 2.01(1.21–3.34); 4.84(0.3–79.23) | 6.71X10-03 | 1.69X10-07 | |
| rs12659412 | 5 | T | C | 2.69(1.72–4.2); 0.02 (0–0.26) | 1.51X10-05 | 2.01(1.21–3.34); 4.84(0.3–79.23) | 6.71X10-03 | 1.69X10-07 | |
| rs509061 | 1 | T | C | 2.08(1.5–2.89); 1.43 (0.33–6.26) | 1.28X10-05 | 1.72(1.15–2.59); 1.34(0.18–10.13) | 8.50X10-03 | 1.82X10-07 | |
| rs2052548 | 5 | A | C | 2.73(1.74–4.27); 0.01 (0–0.26) | 1.18X10-05 | 1.93(1.17–3.2); 3.64(0.25–52.65) | 1.02X10-02 | 2.03X10-07 | |
| rs72755734 | 5 | A | G | 2.72(1.74–4.26); 0.01 (0–0.25) | 1.22X10-05 | 1.93(1.17–3.2); 3.64(0.25–52.65) | 1.02X10-02 | 2.09X10-07 | |
| rs1477347 | 5 | G | A | 2.71(1.73–4.24); 0.01 (0–0.25) | 1.31X10-05 | 1.93(1.17–3.2); 3.68(0.25–53.25) | 1.02X10-02 | 2.24X10-07 | |
| chr12:121973317 | 12 | G | A | 2.30(1.58–3.35); 0.35 (0.05–2.33) | 1.45X10-05 | 1.67(1.13–2.49); 2.62(0.01–477.1) | 1.06X10-02 | 2.57X10-07 | |
| rs72755727 | 5 | A | T | 2.67(1.71–4.17); 0.01 (0–0.25) | 1.72X10-05 | 1.94(1.17–3.21); 7.09(0.54–93.35) | 1.00X10-02 | 2.84X10-07 | |
| rs77668680 | 1 | C | CAG | 2.23(1.58–3.14); 1.87 (0.4–8.72) | 4.23X10-06 | 1.54(1.02–2.33); 1.14(0.15–8.79) | 4.16X10-02 | 3.81X10-07 | |
| rs6500715 | 16 | G | C | 0.47(0.34–0.65); 0.59 (0.13–2.63) | 5.51X10-06 | 0.69(0.49–0.97); 1.38(0.16–11.97) | 3.54X10-02 | 3.96X10-07 | |
| rs34338452 | 8 | AT | A | 2.24(1.57–3.19); 1.02 (0.17–5.99) | 7.58X10-06 | 1.59(1.05–2.39); 1.04(0.13–8.19) | 2.78X10-02 | 3.99X10-07 | |
| rs10094604 | 8 | G | T | 2.28(1.6–3.24); 1.02 (0.17–6.02) | 4.73X10-06 | 1.53(1.02–2.29); 1.13(0.15–8.72) | 4.07X10-02 | 4.09X10-07 | |
| rs524887 | 1 | A | G | 2.23(1.58–3.14); 1.88 (0.4–8.75) | 4.57X10-06 | 1.53(1.01–2.31); 1.04(0.14–8) | 2.70X10-02 | 3.99X10-07 | |
Odds ratios and 95% confidence intervals are provided for age-by-genotype interactions.
∞Odds ratios with 95% confidence intervals for the main effect estimates. Minor allele frequencies for all variants are > 1%.
*P values were combined using a weighted Z-score method.
Fig 1Results of age-by-genotype interaction study for ICS response in asthma.
Manhattan plots show results for discovery (top panel) and replication (bottom panel) GWIS, by chromosome. Red line indicates threshold for genome-wide significance (P<5x10-08) while blue lines indicate suggestive threshold for genome-wide significance (P<10−05).