KEAP1-driven co-mutations in lung adenocarcinoma unresponsive to immunotherapy despite high tumor mutational burden

D. Marinelli; M. Mazzotta; S. Scalera; I. Terrenato; F. Sperati; L. D'Ambrosio; M. Pallocca; G. Corleone; E. Krasniqi; L. Pizzuti; M. Barba; S. Carpano; P. Vici; M. Filetti; R. Giusti; A. Vecchione; M. Occhipinti; A. Gelibter; A. Botticelli; Nicola F. De; L. Ciuffreda; F. Goeman; E. Gallo; P. Visca; E. Pescarmona; M. Fanciulli; Ruggero De Maria Marchiano; P. Marchetti; G. Ciliberto; M. Maugeri-Sacca

doi:10.1016/j.annonc.2020.08.2105

KEAP1-driven co-mutations in lung adenocarcinoma unresponsive to immunotherapy despite high tumor mutational burden

D. Marinelli
, M. Mazzotta
, S. Scalera
, I. Terrenato
, F. Sperati
, L. D'Ambrosio
, M. Pallocca
, G. Corleone
, E. Krasniqi
, L. Pizzuti
, M. Barba
, S. Carpano
, P. Vici
, M. Filetti
, R. Giusti
, A. Vecchione
, M. Occhipinti
, A. Gelibter
, A. Botticelli
, Nicola F. De

L. Ciuffreda, F. Goeman, E. Gallo, P. Visca, E. Pescarmona, M. Fanciulli, Ruggero De Maria Marchiano, P. Marchetti, G. Ciliberto, M. Maugeri-Sacca^*

^*Autore corrispondente per questo lavoro

Sant'Andrea Hospital
IRCCS Istituti fisioterapici ospitalieri - Istituto Regina Elena
IRCCS Istituto Dermatologico Santa Maria e San Gallicano – Roma
University of Rome La Sapienza

Risultato della ricerca: Contributo in rivista › Articolo

17 Citazioni (Scopus)

Abstract

Background: Immune checkpoint inhibitors (ICIs) have demonstrated significant overall survival (OS) benefit in lung adenocarcinoma (LUAD). Nevertheless, a remarkable interpatient heterogeneity characterizes immunotherapy efficacy, regardless of programmed death-ligand 1 (PD-L1) expression and tumor mutational burden (TMB). KEAP1 mutations are associated with shorter survival in LUAD patients receiving chemotherapy. We hypothesized that the pattern of KEAP1 co-mutations and mutual exclusivity may identify LUAD patients unresponsive to immunotherapy. Patients and methods: KEAP1 mutational co-occurrences and somatic interactions were studied in the whole MSKCC LUAD dataset. The impact of coexisting alterations on survival outcomes in ICI-treated LUAD patients was verified in the randomized phase II/III POPLAR/OAK trials (blood-based sequencing, bNGS cohort, N = 253). Three tissue-based sequencing studies (Rome, MSKCC and DFCI) were used for independent validation (tNGS cohort, N = 289). Immunogenomic features were analyzed using The Cancer Genome Atlas (TCGA) LUAD study. Results: On the basis of KEAP1 mutational co-occurrences, we identified four genes potentially associated with reduced efficacy of immunotherapy (KEAP1, PBRM1, SMARCA4 and STK11). Independent of the nature of co-occurring alterations, tumors with coexisting mutations (CoMut) had inferior survival as compared with single-mutant (SM) and wild-type (WT) tumors (bNGS cohort: CoMut versus SM log-rank P = 0.048, CoMut versus WT log-rank P < 0.001; tNGS cohort: CoMut versus SM log-rank P = 0.037, CoMut versus WT log-rank P = 0.006). The CoMut subset harbored higher TMB than the WT disease and the adverse significance of coexisting alterations was maintained in LUAD with high TMB. Significant immunogenomic differences were observed between the CoMut and WT groups in terms of core immune signatures, T-cell receptor repertoire, T helper cell signatures and immunomodulatory genes. Conclusions: This study indicates that coexisting alterations in a limited set of genes characterize a subset of LUAD unresponsive to immunotherapy and with high TMB. An immune-cold microenvironment may account for the clinical course of the disease.

Lingua originale	Inglese
pagine (da-a)	1746-1754
Numero di pagine	9
Rivista	Annals of Oncology
Volume	31
Numero di pubblicazione	12
DOI	https://doi.org/10.1016/j.annonc.2020.08.2105
Stato di pubblicazione	Pubblicato - 2020

OSS delle Nazioni Unite

Questo processo contribuisce al raggiungimento dei seguenti obiettivi di sviluppo sostenibile

SDG 3 Salute e benessere

All Science Journal Classification (ASJC) codes

Ematologia
Oncologia

Keywords

KEAP1 co-mutations
immunogenomic
immunotherapy
lung adenocarcinoma
tumor mutational burden

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10.1016/j.annonc.2020.08.2105

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Marinelli, D., Mazzotta, M., Scalera, S., Terrenato, I., Sperati, F., D'Ambrosio, L., Pallocca, M., Corleone, G., Krasniqi, E., Pizzuti, L., Barba, M., Carpano, S., Vici, P., Filetti, M., Giusti, R., Vecchione, A., Occhipinti, M., Gelibter, A., Botticelli, A., ... Maugeri-Sacca, M. (2020). KEAP1-driven co-mutations in lung adenocarcinoma unresponsive to immunotherapy despite high tumor mutational burden. Annals of Oncology, 31(12), 1746-1754. https://doi.org/10.1016/j.annonc.2020.08.2105

@article{440348aac8c04cedb17422226266b9ff,

title = "KEAP1-driven co-mutations in lung adenocarcinoma unresponsive to immunotherapy despite high tumor mutational burden",

abstract = "Background: Immune checkpoint inhibitors (ICIs) have demonstrated significant overall survival (OS) benefit in lung adenocarcinoma (LUAD). Nevertheless, a remarkable interpatient heterogeneity characterizes immunotherapy efficacy, regardless of programmed death-ligand 1 (PD-L1) expression and tumor mutational burden (TMB). KEAP1 mutations are associated with shorter survival in LUAD patients receiving chemotherapy. We hypothesized that the pattern of KEAP1 co-mutations and mutual exclusivity may identify LUAD patients unresponsive to immunotherapy. Patients and methods: KEAP1 mutational co-occurrences and somatic interactions were studied in the whole MSKCC LUAD dataset. The impact of coexisting alterations on survival outcomes in ICI-treated LUAD patients was verified in the randomized phase II/III POPLAR/OAK trials (blood-based sequencing, bNGS cohort, N = 253). Three tissue-based sequencing studies (Rome, MSKCC and DFCI) were used for independent validation (tNGS cohort, N = 289). Immunogenomic features were analyzed using The Cancer Genome Atlas (TCGA) LUAD study. Results: On the basis of KEAP1 mutational co-occurrences, we identified four genes potentially associated with reduced efficacy of immunotherapy (KEAP1, PBRM1, SMARCA4 and STK11). Independent of the nature of co-occurring alterations, tumors with coexisting mutations (CoMut) had inferior survival as compared with single-mutant (SM) and wild-type (WT) tumors (bNGS cohort: CoMut versus SM log-rank P = 0.048, CoMut versus WT log-rank P < 0.001; tNGS cohort: CoMut versus SM log-rank P = 0.037, CoMut versus WT log-rank P = 0.006). The CoMut subset harbored higher TMB than the WT disease and the adverse significance of coexisting alterations was maintained in LUAD with high TMB. Significant immunogenomic differences were observed between the CoMut and WT groups in terms of core immune signatures, T-cell receptor repertoire, T helper cell signatures and immunomodulatory genes. Conclusions: This study indicates that coexisting alterations in a limited set of genes characterize a subset of LUAD unresponsive to immunotherapy and with high TMB. An immune-cold microenvironment may account for the clinical course of the disease.",

keywords = "KEAP1 co-mutations, immunogenomic, immunotherapy, lung adenocarcinoma, tumor mutational burden, KEAP1 co-mutations, immunogenomic, immunotherapy, lung adenocarcinoma, tumor mutational burden",

author = "D. Marinelli and M. Mazzotta and S. Scalera and I. Terrenato and F. Sperati and L. D'Ambrosio and M. Pallocca and G. Corleone and E. Krasniqi and L. Pizzuti and M. Barba and S. Carpano and P. Vici and M. Filetti and R. Giusti and A. Vecchione and M. Occhipinti and A. Gelibter and A. Botticelli and De, \{Nicola F.\} and L. Ciuffreda and F. Goeman and E. Gallo and P. Visca and E. Pescarmona and M. Fanciulli and \{De Maria Marchiano\}, Ruggero and P. Marchetti and G. Ciliberto and M. Maugeri-Sacca",

year = "2020",

doi = "10.1016/j.annonc.2020.08.2105",

language = "English",

volume = "31",

pages = "1746--1754",

journal = "Annals of Oncology",

issn = "0923-7534",

publisher = "Elsevier Ltd",

number = "12",

}

Marinelli, D, Mazzotta, M, Scalera, S, Terrenato, I, Sperati, F, D'Ambrosio, L, Pallocca, M, Corleone, G, Krasniqi, E, Pizzuti, L, Barba, M, Carpano, S, Vici, P, Filetti, M, Giusti, R, Vecchione, A, Occhipinti, M, Gelibter, A, Botticelli, A, De, NF, Ciuffreda, L, Goeman, F, Gallo, E, Visca, P, Pescarmona, E, Fanciulli, M, De Maria Marchiano, R, Marchetti, P, Ciliberto, G & Maugeri-Sacca, M 2020, 'KEAP1-driven co-mutations in lung adenocarcinoma unresponsive to immunotherapy despite high tumor mutational burden', Annals of Oncology, vol. 31, n. 12, pagg. 1746-1754. https://doi.org/10.1016/j.annonc.2020.08.2105

TY - JOUR

T1 - KEAP1-driven co-mutations in lung adenocarcinoma unresponsive to immunotherapy despite high tumor mutational burden

AU - Marinelli, D.

AU - Mazzotta, M.

AU - Scalera, S.

AU - Terrenato, I.

AU - Sperati, F.

AU - D'Ambrosio, L.

AU - Pallocca, M.

AU - Corleone, G.

AU - Krasniqi, E.

AU - Pizzuti, L.

AU - Barba, M.

AU - Carpano, S.

AU - Vici, P.

AU - Filetti, M.

AU - Giusti, R.

AU - Vecchione, A.

AU - Occhipinti, M.

AU - Gelibter, A.

AU - Botticelli, A.

AU - De, Nicola F.

AU - Ciuffreda, L.

AU - Goeman, F.

AU - Gallo, E.

AU - Visca, P.

AU - Pescarmona, E.

AU - Fanciulli, M.

AU - De Maria Marchiano, Ruggero

AU - Marchetti, P.

AU - Ciliberto, G.

AU - Maugeri-Sacca, M.

PY - 2020

Y1 - 2020

N2 - Background: Immune checkpoint inhibitors (ICIs) have demonstrated significant overall survival (OS) benefit in lung adenocarcinoma (LUAD). Nevertheless, a remarkable interpatient heterogeneity characterizes immunotherapy efficacy, regardless of programmed death-ligand 1 (PD-L1) expression and tumor mutational burden (TMB). KEAP1 mutations are associated with shorter survival in LUAD patients receiving chemotherapy. We hypothesized that the pattern of KEAP1 co-mutations and mutual exclusivity may identify LUAD patients unresponsive to immunotherapy. Patients and methods: KEAP1 mutational co-occurrences and somatic interactions were studied in the whole MSKCC LUAD dataset. The impact of coexisting alterations on survival outcomes in ICI-treated LUAD patients was verified in the randomized phase II/III POPLAR/OAK trials (blood-based sequencing, bNGS cohort, N = 253). Three tissue-based sequencing studies (Rome, MSKCC and DFCI) were used for independent validation (tNGS cohort, N = 289). Immunogenomic features were analyzed using The Cancer Genome Atlas (TCGA) LUAD study. Results: On the basis of KEAP1 mutational co-occurrences, we identified four genes potentially associated with reduced efficacy of immunotherapy (KEAP1, PBRM1, SMARCA4 and STK11). Independent of the nature of co-occurring alterations, tumors with coexisting mutations (CoMut) had inferior survival as compared with single-mutant (SM) and wild-type (WT) tumors (bNGS cohort: CoMut versus SM log-rank P = 0.048, CoMut versus WT log-rank P < 0.001; tNGS cohort: CoMut versus SM log-rank P = 0.037, CoMut versus WT log-rank P = 0.006). The CoMut subset harbored higher TMB than the WT disease and the adverse significance of coexisting alterations was maintained in LUAD with high TMB. Significant immunogenomic differences were observed between the CoMut and WT groups in terms of core immune signatures, T-cell receptor repertoire, T helper cell signatures and immunomodulatory genes. Conclusions: This study indicates that coexisting alterations in a limited set of genes characterize a subset of LUAD unresponsive to immunotherapy and with high TMB. An immune-cold microenvironment may account for the clinical course of the disease.

AB - Background: Immune checkpoint inhibitors (ICIs) have demonstrated significant overall survival (OS) benefit in lung adenocarcinoma (LUAD). Nevertheless, a remarkable interpatient heterogeneity characterizes immunotherapy efficacy, regardless of programmed death-ligand 1 (PD-L1) expression and tumor mutational burden (TMB). KEAP1 mutations are associated with shorter survival in LUAD patients receiving chemotherapy. We hypothesized that the pattern of KEAP1 co-mutations and mutual exclusivity may identify LUAD patients unresponsive to immunotherapy. Patients and methods: KEAP1 mutational co-occurrences and somatic interactions were studied in the whole MSKCC LUAD dataset. The impact of coexisting alterations on survival outcomes in ICI-treated LUAD patients was verified in the randomized phase II/III POPLAR/OAK trials (blood-based sequencing, bNGS cohort, N = 253). Three tissue-based sequencing studies (Rome, MSKCC and DFCI) were used for independent validation (tNGS cohort, N = 289). Immunogenomic features were analyzed using The Cancer Genome Atlas (TCGA) LUAD study. Results: On the basis of KEAP1 mutational co-occurrences, we identified four genes potentially associated with reduced efficacy of immunotherapy (KEAP1, PBRM1, SMARCA4 and STK11). Independent of the nature of co-occurring alterations, tumors with coexisting mutations (CoMut) had inferior survival as compared with single-mutant (SM) and wild-type (WT) tumors (bNGS cohort: CoMut versus SM log-rank P = 0.048, CoMut versus WT log-rank P < 0.001; tNGS cohort: CoMut versus SM log-rank P = 0.037, CoMut versus WT log-rank P = 0.006). The CoMut subset harbored higher TMB than the WT disease and the adverse significance of coexisting alterations was maintained in LUAD with high TMB. Significant immunogenomic differences were observed between the CoMut and WT groups in terms of core immune signatures, T-cell receptor repertoire, T helper cell signatures and immunomodulatory genes. Conclusions: This study indicates that coexisting alterations in a limited set of genes characterize a subset of LUAD unresponsive to immunotherapy and with high TMB. An immune-cold microenvironment may account for the clinical course of the disease.

KW - KEAP1 co-mutations

KW - immunogenomic

KW - immunotherapy

KW - lung adenocarcinoma

KW - tumor mutational burden

KW - KEAP1 co-mutations

KW - immunogenomic

KW - immunotherapy

KW - lung adenocarcinoma

KW - tumor mutational burden

UR - https://publicatt.unicatt.it/handle/10807/167053

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UR - https://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=85091848994&origin=inward

U2 - 10.1016/j.annonc.2020.08.2105

DO - 10.1016/j.annonc.2020.08.2105

M3 - Article

SN - 0923-7534

VL - 31

SP - 1746

EP - 1754

JO - Annals of Oncology

JF - Annals of Oncology

IS - 12

ER -

KEAP1-driven co-mutations in lung adenocarcinoma unresponsive to immunotherapy despite high tumor mutational burden

Abstract

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Keywords

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