Immunoproteasome expression is associated with better prognosis and response to checkpoint therapies in melanoma

Shelly Kalaora; Joo Sang Lee; Eilon Barnea; Ronen Levy; Polina Greenberg; Michal Alon; Gal Yagel; Gitit Bar Eli; Roni Oren; Aviyah Peri; Sushant Patkar; Lital Bitton; Steven A. Rosenberg; Michal Lotem; Yishai Levin; Arie Admon; Eytan Ruppin; Yardena Samuels

doi:10.1038/s41467-020-14639-9

Immunoproteasome expression is associated with better prognosis and response to checkpoint therapies in melanoma

Shelly Kalaora
, Joo Sang Lee
, Eilon Barnea
, Ronen Levy
, Polina Greenberg
, Michal Alon
, Gal Yagel
, Gitit Bar Eli
, Roni Oren
, Aviyah Peri
, Sushant Patkar
, Lital Bitton
, Steven A. Rosenberg
, Michal Lotem
, Yishai Levin
, Arie Admon
, Eytan Ruppin
, Yardena Samuels

Weizmann Institute of Science
National Institutes of Health
Sungkyunkwan University
Technion-Israel Institute of Technology
Hebrew University Medical School

Research output: Contribution to journal › Article › peer-review

132 Scopus citations

Abstract

Predicting the outcome of immunotherapy treatment in melanoma patients is challenging. Alterations in genes involved in antigen presentation and the interferon gamma (IFNγ) pathway play an important role in the immune response to tumors. We describe here that the overexpression of PSMB8 and PSMB9, two major components of the immunoproteasome, is predictive of better survival and improved response to immune-checkpoint inhibitors of melanoma patients. We study the mechanism underlying this connection by analyzing the antigenic peptide repertoire of cells that overexpress these subunits using HLA peptidomics. We find a higher response of patient-matched tumor infiltrating lymphocytes against antigens diferentially presented after immunoproteasome overexpression. Importantly, we find that PSMB8 and PSMB9 expression levels are much stronger predictors of melanoma patientsʼ immune response to checkpoint inhibitors than the tumors’ mutational burden. These results suggest that PSMB8 and PSMB9 expression levels can serve as important biomarkers for stratifying melanoma patients for immune-checkpoint treatment.

Original language	English
Article number	896
Journal	Nature Communications
Volume	11
Issue number	1
DOIs	https://doi.org/10.1038/s41467-020-14639-9
State	Published - 1 Dec 2020
Externally published	Yes

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SDG 3 Good Health and Well-being

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10.1038/s41467-020-14639-9

Cite this

Kalaora, S., Lee, J. S., Barnea, E., Levy, R., Greenberg, P., Alon, M., Yagel, G., Bar Eli, G., Oren, R., Peri, A., Patkar, S., Bitton, L., Rosenberg, S. A., Lotem, M., Levin, Y., Admon, A., Ruppin, E., & Samuels, Y. (2020). Immunoproteasome expression is associated with better prognosis and response to checkpoint therapies in melanoma. Nature Communications, 11(1), Article 896. https://doi.org/10.1038/s41467-020-14639-9

@article{ad31cb6738cc4f4280dfc1462074171e,

title = "Immunoproteasome expression is associated with better prognosis and response to checkpoint therapies in melanoma",

abstract = "Predicting the outcome of immunotherapy treatment in melanoma patients is challenging. Alterations in genes involved in antigen presentation and the interferon gamma (IFNγ) pathway play an important role in the immune response to tumors. We describe here that the overexpression of PSMB8 and PSMB9, two major components of the immunoproteasome, is predictive of better survival and improved response to immune-checkpoint inhibitors of melanoma patients. We study the mechanism underlying this connection by analyzing the antigenic peptide repertoire of cells that overexpress these subunits using HLA peptidomics. We find a higher response of patient-matched tumor infiltrating lymphocytes against antigens diferentially presented after immunoproteasome overexpression. Importantly, we find that PSMB8 and PSMB9 expression levels are much stronger predictors of melanoma patientsʼ immune response to checkpoint inhibitors than the tumors{\textquoteright} mutational burden. These results suggest that PSMB8 and PSMB9 expression levels can serve as important biomarkers for stratifying melanoma patients for immune-checkpoint treatment.",

author = "Shelly Kalaora and Lee, \{Joo Sang\} and Eilon Barnea and Ronen Levy and Polina Greenberg and Michal Alon and Gal Yagel and \{Bar Eli\}, Gitit and Roni Oren and Aviyah Peri and Sushant Patkar and Lital Bitton and Rosenberg, \{Steven A.\} and Michal Lotem and Yishai Levin and Arie Admon and Eytan Ruppin and Yardena Samuels",

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doi = "10.1038/s41467-020-14639-9",

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Kalaora, S, Lee, JS, Barnea, E, Levy, R, Greenberg, P, Alon, M, Yagel, G, Bar Eli, G, Oren, R, Peri, A, Patkar, S, Bitton, L, Rosenberg, SA, Lotem, M, Levin, Y, Admon, A, Ruppin, E & Samuels, Y 2020, 'Immunoproteasome expression is associated with better prognosis and response to checkpoint therapies in melanoma', Nature Communications, vol. 11, no. 1, 896. https://doi.org/10.1038/s41467-020-14639-9

TY - JOUR

T1 - Immunoproteasome expression is associated with better prognosis and response to checkpoint therapies in melanoma

AU - Kalaora, Shelly

AU - Lee, Joo Sang

AU - Barnea, Eilon

AU - Levy, Ronen

AU - Greenberg, Polina

AU - Alon, Michal

AU - Yagel, Gal

AU - Bar Eli, Gitit

AU - Oren, Roni

AU - Peri, Aviyah

AU - Patkar, Sushant

AU - Bitton, Lital

AU - Rosenberg, Steven A.

AU - Lotem, Michal

AU - Levin, Yishai

AU - Admon, Arie

AU - Ruppin, Eytan

AU - Samuels, Yardena

PY - 2020/12/1

Y1 - 2020/12/1

N2 - Predicting the outcome of immunotherapy treatment in melanoma patients is challenging. Alterations in genes involved in antigen presentation and the interferon gamma (IFNγ) pathway play an important role in the immune response to tumors. We describe here that the overexpression of PSMB8 and PSMB9, two major components of the immunoproteasome, is predictive of better survival and improved response to immune-checkpoint inhibitors of melanoma patients. We study the mechanism underlying this connection by analyzing the antigenic peptide repertoire of cells that overexpress these subunits using HLA peptidomics. We find a higher response of patient-matched tumor infiltrating lymphocytes against antigens diferentially presented after immunoproteasome overexpression. Importantly, we find that PSMB8 and PSMB9 expression levels are much stronger predictors of melanoma patientsʼ immune response to checkpoint inhibitors than the tumors’ mutational burden. These results suggest that PSMB8 and PSMB9 expression levels can serve as important biomarkers for stratifying melanoma patients for immune-checkpoint treatment.

AB - Predicting the outcome of immunotherapy treatment in melanoma patients is challenging. Alterations in genes involved in antigen presentation and the interferon gamma (IFNγ) pathway play an important role in the immune response to tumors. We describe here that the overexpression of PSMB8 and PSMB9, two major components of the immunoproteasome, is predictive of better survival and improved response to immune-checkpoint inhibitors of melanoma patients. We study the mechanism underlying this connection by analyzing the antigenic peptide repertoire of cells that overexpress these subunits using HLA peptidomics. We find a higher response of patient-matched tumor infiltrating lymphocytes against antigens diferentially presented after immunoproteasome overexpression. Importantly, we find that PSMB8 and PSMB9 expression levels are much stronger predictors of melanoma patientsʼ immune response to checkpoint inhibitors than the tumors’ mutational burden. These results suggest that PSMB8 and PSMB9 expression levels can serve as important biomarkers for stratifying melanoma patients for immune-checkpoint treatment.

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SN - 2041-1723

VL - 11

JO - Nature Communications

JF - Nature Communications

IS - 1

M1 - 896

ER -

Immunoproteasome expression is associated with better prognosis and response to checkpoint therapies in melanoma

Abstract

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