Abstract 2240P
Background
Immune checkpoint inhibitors (ICI) are highly efficacious but ∼ 50% of cancer patients on combination and ∼10% on ICI monotherapy experience ≥ grade 3 immune-related adverse events (irAE). Managing irAEs is challenging and there is a lack of predictive biomarkers. We conducted genome-wide association analyses (GWAS) to identify markers associated with irAEs.
Methods
599 cancer patients on ICIs were genotyped and genome-wide imputation was performed. Association testing with CTCAE graded irAEs was conducted (0=grade 0-2, 1=grade ≥3 irAE). Markers with P<5x10-6 were tested in a validation cohort. A transcriptome-wide association study (TWAS) was also performed.
Results
72% of the discovery cohort had melanoma, 37% received combination therapy and 31% developed ≥ grade 3 irAE. 8 SNPs were associated with any ≥ grade 3 irAE at P<5x10-6 but none replicated at P<0.05 (Table 2240P). Of note one, rs35429660, is significantly associated with ZNF701 expression in monocytes and ZNF701 was also significant in the TWAS (P=5.1x10-7). In an analysis of individual organ irAEs, we identified markers at P<5x10-6 in the discovery phase. One, rs77941834, was associated with hepatitis in the validation phase (P=0.04) and expression of LINC02021 in T cells (4.6 x10-8). 11 other SNPs had suggestive evidence of validation. One maps to MAST3, linked to inflammatory bowel disease and another maps to IFI44, linked to multisystem inflammatory syndrome, viral hepatitis and immune cell infiltration. The IL7 SNP previously reported as associated with any grade irAE at GWAS significance was nominally significant (P=0.05) in our data.
Table: 2240P
Markers associated with any ≥ grade 3 irAE at P<5x10-6 in discovery phase
rsID | Toxicity associated allele | Discovery OR (95% CI) | Discovery P-value | Validation OR (95% CI) | Validation P-value | Meta P-value |
rs1310844785 | TTG | 2.5(1.8-3.6) | 8.91 x 10-8 | 0.8(0.6-1.2) | 0.26 | 0.0038 |
rs7197466 | T | 2.1(1.5-2.9) | 2.19 x 10-6 | 1(0.8-1.4) | 0.81 | 0.00077 |
rs35429660 | C | 2.2(1.6-3) | 5.13 x 10-7 | 1.2(0.8-1.6) | 0.36 | 7.32 x 10-5 |
rs1389216733 | CA | 6.3(2.6-15.7) | 3.07 x 10-6 | 1.6(0.8-3.5) | 0.18 | 0.0004 |
rs6864863 | A | 2.1(1.5-2.9) | 3.73 x 10-6 | 0.8(0.6-1) | 0.07 | 0.11 |
rs4527728 | T | 2.2(1.6-3.1) | 2.68 x 10-6 | 1.2(0.9-1.6) | 0.26 | 0.00012 |
rs1208547611 | CTT | 2.5(1.7-3.7) | 3.59 x 10-6 | 1.1(0.7-1.5) | 0.79 | 0.0015 |
rs2472135 | A | 2.1(1.6-2.8) | 5.83 x 10-7 | 1.1(0.8-1.5) | 0.43 | 7.98 x 10-5 |
Conclusions
We identified novel variants, including an immune eQTL for ZNF701, associated with serious ICI induced irAE. None reached genome-wide significance (P<5x10-8). Meta-analysis with other cohorts is required to confirm our results and identify further markers predictive of irAE risk.
Clinical trial identification
IRAS 237779.
Editorial acknowledgement
Legal entity responsible for the study
University of Birmingham.
Funding
University of Birmingham, Cancer Research UK Birmingham.
Disclosure
I.S. Chin: Non-Financial Interests, Personal and Institutional, Research Grant: Cancer Research UK Birmingham Centre. All other authors have declared no conflicts of interest.
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