Abstract
BackgroundClear cell renal cell carcinoma (ccRCC) is the dominant subtype of renal cancer. With currently available therapies, cure of advanced and metastatic ccRCC is achieved only in rare cases. Here, we developed a workflow integrating different -omics technologies to identify ccRCC-specific HLA-presented peptides as potential drug targets for ccRCC immunotherapy.MethodsWe analyzed HLA-presented peptides by MS-based ligandomics of 55 ccRCC tumors (cohort 1), paired non-tumor renal tissues, and 158 benign tissues from other organs. Pathways enriched in ccRCC compared to its cell type of origin were identified by transcriptome and gene set enrichment analyses in 51 tumor tissues of the same cohort. To retrieve a list of candidate targets with involvement in ccRCC pathogenesis, ccRCC-specific pathway genes were intersected with the source genes of tumor-exclusive peptides. The candidates were validated in an independent cohort from The Cancer Genome Atlas (TCGA KIRC, n = 452). DNA methylation (TCGA KIRC, n = 273), somatic mutations (TCGA KIRC, n = 392), and gene ontology (GO) and correlations with tumor metabolites (cohort 1, n = 30) and immune-oncological markers (cohort 1, n = 37) were analyzed to characterize regulatory and functional involvements. CD8+ T cell priming assays were used to identify immunogenic peptides. The candidate gene EGLN3 was functionally investigated in cell culture.ResultsA total of 34,226 HLA class I- and 19,325 class II-presented peptides were identified in ccRCC tissue, of which 443 class I and 203 class II peptides were ccRCC-specific and presented in ≥ 3 tumors. One hundred eighty-five of the 499 corresponding source genes were involved in pathways activated by ccRCC tumors. After validation in the independent cohort from TCGA, 113 final candidate genes remained. Candidates were involved in extracellular matrix organization, hypoxic signaling, immune processes, and others. Nine of the 12 peptides assessed by immunogenicity analysis were able to activate naïve CD8+ T cells, including peptides derived from EGLN3. Functional analysis of EGLN3 revealed possible tumor-promoting functions.ConclusionsIntegration of HLA ligandomics, transcriptomics, genetic, and epigenetic data leads to the identification of novel functionally relevant therapeutic targets for ccRCC immunotherapy. Validation of the identified targets is recommended to expand the treatment landscape of ccRCC.
Highlights
Clear cell renal cell carcinoma is the dominant subtype of renal cancer
Integration of human leukocyte antigen (HLA) ligandomics, transcriptomics, genetic, and epigenetic data leads to the identification of novel functionally relevant therapeutic targets for Clear cell renal cell carcinoma (ccRCC) immunotherapy
Over-represented self-peptides in ccRCC determined by HLA ligandomics Since ccRCC is known as a cancer entity with low mutational load [21], we aimed to identify tumor overrepresented non-mutated peptides
Summary
Cure of advanced and metastatic ccRCC is achieved only in rare cases. For patients with advanced and metastatic disease, the prognosis is poor, with only 12% alive 5 years after diagnosis [2]. The limited number of targeted pathways in ccRCC therapy leaves non-responding patients with almost no therapeutic options and very poor prognosis. Combination regimens of immune checkpoint inhibitors and other agents are clinically investigated [4] and first studies support for instance the combination of atezolizumab and bevacizumab as a first-line treatment option for patients with advanced RCC [10]. Alone or in combination, is able to achieve long-term responses in advanced and metastatic ccRCC, similar to the responses observed in malignant melanoma, will emerge in the future
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