MHC-restricted phosphopeptide antigens: preclinical validation and first-in-humans clinical trial in participants with high-risk melanoma

BACKGROUND: Phosphorylated peptides presented by MHC molecules represent a new class of neoantigens expressed on cancer cells and recognized by CD8 T-cells. These peptides are promising targets for cancer immunotherapy. Previous work identified an HLA-A*0201-restricted phosphopeptide from insulin re...

Descripción completa

Detalles Bibliográficos
Autores principales: Engelhard, Victor H, Obeng, Rebecca C, Cummings, Kara L, Petroni, Gina R, Ambakhutwala, Angela L, Chianese-Bullock, Kimberly A, Smith, Kelly T, Lulu, Amanda, Varhegyi, Nikole, Smolkin, Mark E, Myers, Paisley, Mahoney, Keira E, Shabanowitz, Jeffrey, Buettner, Nico, Hall, Emily H, Haden, Kathleen, Cobbold, Mark, Hunt, Donald F, Weiss, Geoffrey, Gaughan, Elizabeth, Slingluff, Jr, Craig L
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BMJ Publishing Group 2020
Materias:
Clinical/Translational Cancer Immunotherapy
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7228659/
https://www.ncbi.nlm.nih.gov/pubmed/32385144
http://dx.doi.org/10.1136/jitc-2019-000262
_version_ 1783534615176151040
author Engelhard, Victor H
Obeng, Rebecca C
Cummings, Kara L
Petroni, Gina R
Ambakhutwala, Angela L
Chianese-Bullock, Kimberly A
Smith, Kelly T
Lulu, Amanda
Varhegyi, Nikole
Smolkin, Mark E
Myers, Paisley
Mahoney, Keira E
Shabanowitz, Jeffrey
Buettner, Nico
Hall, Emily H
Haden, Kathleen
Cobbold, Mark
Hunt, Donald F
Weiss, Geoffrey
Gaughan, Elizabeth
Slingluff, Jr, Craig L
author_facet Engelhard, Victor H
Obeng, Rebecca C
Cummings, Kara L
Petroni, Gina R
Ambakhutwala, Angela L
Chianese-Bullock, Kimberly A
Smith, Kelly T
Lulu, Amanda
Varhegyi, Nikole
Smolkin, Mark E
Myers, Paisley
Mahoney, Keira E
Shabanowitz, Jeffrey
Buettner, Nico
Hall, Emily H
Haden, Kathleen
Cobbold, Mark
Hunt, Donald F
Weiss, Geoffrey
Gaughan, Elizabeth
Slingluff, Jr, Craig L
author_sort Engelhard, Victor H
collection PubMed
description BACKGROUND: Phosphorylated peptides presented by MHC molecules represent a new class of neoantigens expressed on cancer cells and recognized by CD8 T-cells. These peptides are promising targets for cancer immunotherapy. Previous work identified an HLA-A*0201-restricted phosphopeptide from insulin receptor substrate 2 (pIRS2) as one such target. The purpose of this study was to characterize a second phosphopeptide, from breast cancer antiestrogen resistance 3 (BCAR3), and to evaluate safety and immunogenicity of a novel immunotherapic vaccine comprising either or both of these phosphorylated peptides. METHODS: Phosphorylated BCAR3 protein was evaluated in melanoma and breast cancer cell lines by Western blot, and recognition by T-cells specific for HLA-A*0201-restricted phosphorylated BCAR3 peptide (pBCAR3(126-134)) was determined by (51)Cr release assay and intracellular cytokine staining. Human tumor explants were also evaluated by mass spectrometry for presentation of pIRS2 and pBCAR3 peptides. For the clinical trial, participants with resected stage IIA–IV melanoma were vaccinated 6 times over 12 weeks with one or both peptides in incomplete Freund’s adjuvant and Hiltonol (poly-ICLC). Adverse events (AEs) were coded based on National Cancer Institute (NCI) Common Terminology Criteria for Adverse Events (CTCAE) V.4.03, with provision for early study termination if dose-limiting toxicity (DLT) rates exceeded 33%. The enrollment target was 12 participants evaluable for immune response to each peptide. T-cell responses were assessed by interferon-γ ELISpot assay. RESULTS: pBCAR3 peptides were immunogenic in vivo in mice, and in vitro in normal human donors, and T-cells specific for pBCAR3(126-134) controlled outgrowth of a tumor xenograft. The pIRS2(1097-1105) peptide was identified by mass spectrometry from human hepatocellular carcinoma tumors. In the clinical trial, 15 participants were enrolled. All had grade 1 or 2 treatment-related AEs, but there were no grade 3–4 AEs, DLTs or deaths on study. T-cell responses were induced to the pIRS2(1097-1105) peptide in 5/12 patients (42%, 90% CI 18% to 68%) and to the pBCAR3(126-134) peptide in 2/12 patients (17%, 90% CI 3% to 44%). CONCLUSION: This study supports the safety and immunogenicity of vaccines containing the cancer-associated phosphopeptides pBCAR3(126-134) and pIRS2(1097-1105), and the data support continued development of immune therapy targeting phosphopeptides. Future studies will define ways to further enhance the magnitude and durability of phosphopeptide-specific immune responses. TRIAL REGISTRATION NUMBER: NCT01846143
format Online
Article
Text
id pubmed-7228659
institution National Center for Biotechnology Information
language English
publishDate 2020
publisher BMJ Publishing Group
record_format MEDLINE/PubMed
spelling pubmed-72286592020-05-18 MHC-restricted phosphopeptide antigens: preclinical validation and first-in-humans clinical trial in participants with high-risk melanoma Engelhard, Victor H Obeng, Rebecca C Cummings, Kara L Petroni, Gina R Ambakhutwala, Angela L Chianese-Bullock, Kimberly A Smith, Kelly T Lulu, Amanda Varhegyi, Nikole Smolkin, Mark E Myers, Paisley Mahoney, Keira E Shabanowitz, Jeffrey Buettner, Nico Hall, Emily H Haden, Kathleen Cobbold, Mark Hunt, Donald F Weiss, Geoffrey Gaughan, Elizabeth Slingluff, Jr, Craig L J Immunother Cancer Clinical/Translational Cancer Immunotherapy BACKGROUND: Phosphorylated peptides presented by MHC molecules represent a new class of neoantigens expressed on cancer cells and recognized by CD8 T-cells. These peptides are promising targets for cancer immunotherapy. Previous work identified an HLA-A*0201-restricted phosphopeptide from insulin receptor substrate 2 (pIRS2) as one such target. The purpose of this study was to characterize a second phosphopeptide, from breast cancer antiestrogen resistance 3 (BCAR3), and to evaluate safety and immunogenicity of a novel immunotherapic vaccine comprising either or both of these phosphorylated peptides. METHODS: Phosphorylated BCAR3 protein was evaluated in melanoma and breast cancer cell lines by Western blot, and recognition by T-cells specific for HLA-A*0201-restricted phosphorylated BCAR3 peptide (pBCAR3(126-134)) was determined by (51)Cr release assay and intracellular cytokine staining. Human tumor explants were also evaluated by mass spectrometry for presentation of pIRS2 and pBCAR3 peptides. For the clinical trial, participants with resected stage IIA–IV melanoma were vaccinated 6 times over 12 weeks with one or both peptides in incomplete Freund’s adjuvant and Hiltonol (poly-ICLC). Adverse events (AEs) were coded based on National Cancer Institute (NCI) Common Terminology Criteria for Adverse Events (CTCAE) V.4.03, with provision for early study termination if dose-limiting toxicity (DLT) rates exceeded 33%. The enrollment target was 12 participants evaluable for immune response to each peptide. T-cell responses were assessed by interferon-γ ELISpot assay. RESULTS: pBCAR3 peptides were immunogenic in vivo in mice, and in vitro in normal human donors, and T-cells specific for pBCAR3(126-134) controlled outgrowth of a tumor xenograft. The pIRS2(1097-1105) peptide was identified by mass spectrometry from human hepatocellular carcinoma tumors. In the clinical trial, 15 participants were enrolled. All had grade 1 or 2 treatment-related AEs, but there were no grade 3–4 AEs, DLTs or deaths on study. T-cell responses were induced to the pIRS2(1097-1105) peptide in 5/12 patients (42%, 90% CI 18% to 68%) and to the pBCAR3(126-134) peptide in 2/12 patients (17%, 90% CI 3% to 44%). CONCLUSION: This study supports the safety and immunogenicity of vaccines containing the cancer-associated phosphopeptides pBCAR3(126-134) and pIRS2(1097-1105), and the data support continued development of immune therapy targeting phosphopeptides. Future studies will define ways to further enhance the magnitude and durability of phosphopeptide-specific immune responses. TRIAL REGISTRATION NUMBER: NCT01846143 BMJ Publishing Group 2020-05-07 /pmc/articles/PMC7228659/ /pubmed/32385144 http://dx.doi.org/10.1136/jitc-2019-000262 Text en © Author(s) (or their employer(s)) 2020. Re-use permitted under CC BY-NC. No commercial re-use. See rights and permissions. Published by BMJ. http://creativecommons.org/licenses/by-nc/4.0/This is an open access article distributed in accordance with the Creative Commons Attribution Non Commercial (CC BY-NC 4.0) license, which permits others to distribute, remix, adapt, build upon this work non-commercially, and license their derivative works on different terms, provided the original work is properly cited, appropriate credit is given, any changes made indicated, and the use is non-commercial. See http://creativecommons.org/licenses/by-nc/4.0/.
spellingShingle Clinical/Translational Cancer Immunotherapy
Engelhard, Victor H
Obeng, Rebecca C
Cummings, Kara L
Petroni, Gina R
Ambakhutwala, Angela L
Chianese-Bullock, Kimberly A
Smith, Kelly T
Lulu, Amanda
Varhegyi, Nikole
Smolkin, Mark E
Myers, Paisley
Mahoney, Keira E
Shabanowitz, Jeffrey
Buettner, Nico
Hall, Emily H
Haden, Kathleen
Cobbold, Mark
Hunt, Donald F
Weiss, Geoffrey
Gaughan, Elizabeth
Slingluff, Jr, Craig L
MHC-restricted phosphopeptide antigens: preclinical validation and first-in-humans clinical trial in participants with high-risk melanoma
title MHC-restricted phosphopeptide antigens: preclinical validation and first-in-humans clinical trial in participants with high-risk melanoma
title_full MHC-restricted phosphopeptide antigens: preclinical validation and first-in-humans clinical trial in participants with high-risk melanoma
title_fullStr MHC-restricted phosphopeptide antigens: preclinical validation and first-in-humans clinical trial in participants with high-risk melanoma
title_full_unstemmed MHC-restricted phosphopeptide antigens: preclinical validation and first-in-humans clinical trial in participants with high-risk melanoma
title_short MHC-restricted phosphopeptide antigens: preclinical validation and first-in-humans clinical trial in participants with high-risk melanoma
title_sort mhc-restricted phosphopeptide antigens: preclinical validation and first-in-humans clinical trial in participants with high-risk melanoma
topic Clinical/Translational Cancer Immunotherapy
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7228659/
https://www.ncbi.nlm.nih.gov/pubmed/32385144
http://dx.doi.org/10.1136/jitc-2019-000262
work_keys_str_mv AT engelhardvictorh mhcrestrictedphosphopeptideantigenspreclinicalvalidationandfirstinhumansclinicaltrialinparticipantswithhighriskmelanoma
AT obengrebeccac mhcrestrictedphosphopeptideantigenspreclinicalvalidationandfirstinhumansclinicaltrialinparticipantswithhighriskmelanoma
AT cummingskaral mhcrestrictedphosphopeptideantigenspreclinicalvalidationandfirstinhumansclinicaltrialinparticipantswithhighriskmelanoma
AT petroniginar mhcrestrictedphosphopeptideantigenspreclinicalvalidationandfirstinhumansclinicaltrialinparticipantswithhighriskmelanoma
AT ambakhutwalaangelal mhcrestrictedphosphopeptideantigenspreclinicalvalidationandfirstinhumansclinicaltrialinparticipantswithhighriskmelanoma
AT chianesebullockkimberlya mhcrestrictedphosphopeptideantigenspreclinicalvalidationandfirstinhumansclinicaltrialinparticipantswithhighriskmelanoma
AT smithkellyt mhcrestrictedphosphopeptideantigenspreclinicalvalidationandfirstinhumansclinicaltrialinparticipantswithhighriskmelanoma
AT luluamanda mhcrestrictedphosphopeptideantigenspreclinicalvalidationandfirstinhumansclinicaltrialinparticipantswithhighriskmelanoma
AT varhegyinikole mhcrestrictedphosphopeptideantigenspreclinicalvalidationandfirstinhumansclinicaltrialinparticipantswithhighriskmelanoma
AT smolkinmarke mhcrestrictedphosphopeptideantigenspreclinicalvalidationandfirstinhumansclinicaltrialinparticipantswithhighriskmelanoma
AT myerspaisley mhcrestrictedphosphopeptideantigenspreclinicalvalidationandfirstinhumansclinicaltrialinparticipantswithhighriskmelanoma
AT mahoneykeirae mhcrestrictedphosphopeptideantigenspreclinicalvalidationandfirstinhumansclinicaltrialinparticipantswithhighriskmelanoma
AT shabanowitzjeffrey mhcrestrictedphosphopeptideantigenspreclinicalvalidationandfirstinhumansclinicaltrialinparticipantswithhighriskmelanoma
AT buettnernico mhcrestrictedphosphopeptideantigenspreclinicalvalidationandfirstinhumansclinicaltrialinparticipantswithhighriskmelanoma
AT hallemilyh mhcrestrictedphosphopeptideantigenspreclinicalvalidationandfirstinhumansclinicaltrialinparticipantswithhighriskmelanoma
AT hadenkathleen mhcrestrictedphosphopeptideantigenspreclinicalvalidationandfirstinhumansclinicaltrialinparticipantswithhighriskmelanoma
AT cobboldmark mhcrestrictedphosphopeptideantigenspreclinicalvalidationandfirstinhumansclinicaltrialinparticipantswithhighriskmelanoma
AT huntdonaldf mhcrestrictedphosphopeptideantigenspreclinicalvalidationandfirstinhumansclinicaltrialinparticipantswithhighriskmelanoma
AT weissgeoffrey mhcrestrictedphosphopeptideantigenspreclinicalvalidationandfirstinhumansclinicaltrialinparticipantswithhighriskmelanoma
AT gaughanelizabeth mhcrestrictedphosphopeptideantigenspreclinicalvalidationandfirstinhumansclinicaltrialinparticipantswithhighriskmelanoma
AT slingluffjrcraigl mhcrestrictedphosphopeptideantigenspreclinicalvalidationandfirstinhumansclinicaltrialinparticipantswithhighriskmelanoma

Ejemplares similares