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Calreticulin mutant myeloproliferative neoplasms induce MHC-I skewing, which can be overcome by an optimized peptide cancer vaccine
- Source :
- Gigoux , M , Holmström , M O , Zappasodi , R , Park , J J , Pourpe , S , Bozkus , C C , Mangarin , L M B , Redmond , D , Verma , S , Schad , S , George , M M , Venkatesh , D , Ghosh , A , Hoyos , D , Molvi , Z , Kamaz , B , Marneth , A E , Duke , W , Leventhal , M J , Jan , M , Ho , V T , Hobbs , G S , Knudsen , T A , Skov , V , Kjær , L , Larsen , T S , Hansen , D L , Lindsley , R C , Hasselbalch , H , Grauslund , J H , Lisle , T L , Met , Ö , Wilkinson , P , Greenbaum , B , Sepulveda , M A , Chan , T , Rampal , R , Andersen , M H , Abdel-Wahab , O , Bhardwaj , N , Wolchok , J D , Mullally , A & Merghoub , T 2022 , ' Calreticulin mutant myeloproliferative neoplasms induce MHC-I skewing, which can be overcome by an optimized peptide cancer vaccine ' , Science Translational Medicine , vol. 14 , no. 649 , eaba4380 .
- Publication Year :
- 2022
-
Abstract
- The majority of JAK2V617F-negative myeloproliferative neoplasms (MPNs) have disease-initiating frameshift mutations in calreticulin (CALR), resulting in a common carboxyl-terminal mutant fragment (CALRMUT), representing an attractive source of neoantigens for cancer vaccines. However, studies have shown that CALRMUT-specific T cells are rare in patients with CALRMUT MPN for unknown reasons. We examined class I major histocompatibility complex (MHC-I) allele frequencies in patients with CALRMUT MPN from two independent cohorts. We observed that MHC-I alleles that present CALRMUT neoepitopes with high affinity are underrepresented in patients with CALRMUT MPN. We speculated that this was due to an increased chance of immune-mediated tumor rejection by individuals expressing one of these MHC-I alleles such that the disease never clinically manifested. As a consequence of this MHC-I allele restriction, we reasoned that patients with CALRMUT MPN would not efficiently respond to a CALRMUT fragment cancer vaccine but would when immunized with a modified CALRMUT heteroclitic peptide vaccine approach. We found that heteroclitic CALRMUT peptides specifically designed for the MHC-I alleles of patients with CALRMUT MPN efficiently elicited a CALRMUT cross-reactive CD8+ T cell response in human peripheral blood samples but not to the matched weakly immunogenic CALRMUT native peptides. We corroborated this effect in vivo in mice and observed that C57BL/6J mice can mount a CD8+ T cell response to the CALRMUT fragment upon immunization with a CALRMUT heteroclitic, but not native, peptide. Together, our data emphasize the therapeutic potential of heteroclitic peptide–based cancer vaccines in patients with CALRMUT MPN.
Details
- Database :
- OAIster
- Journal :
- Gigoux , M , Holmström , M O , Zappasodi , R , Park , J J , Pourpe , S , Bozkus , C C , Mangarin , L M B , Redmond , D , Verma , S , Schad , S , George , M M , Venkatesh , D , Ghosh , A , Hoyos , D , Molvi , Z , Kamaz , B , Marneth , A E , Duke , W , Leventhal , M J , Jan , M , Ho , V T , Hobbs , G S , Knudsen , T A , Skov , V , Kjær , L , Larsen , T S , Hansen , D L , Lindsley , R C , Hasselbalch , H , Grauslund , J H , Lisle , T L , Met , Ö , Wilkinson , P , Greenbaum , B , Sepulveda , M A , Chan , T , Rampal , R , Andersen , M H , Abdel-Wahab , O , Bhardwaj , N , Wolchok , J D , Mullally , A & Merghoub , T 2022 , ' Calreticulin mutant myeloproliferative neoplasms induce MHC-I skewing, which can be overcome by an optimized peptide cancer vaccine ' , Science Translational Medicine , vol. 14 , no. 649 , eaba4380 .
- Notes :
- English
- Publication Type :
- Electronic Resource
- Accession number :
- edsoai.on1382512983
- Document Type :
- Electronic Resource