Genomic Instability Is Defined by Specific Tumor Microenvironment in Ovarian Cancer: A Subgroup Analysis of AGO OVAR 12 Trial

被引:2
|
作者
Fumet, Jean-David [1 ,2 ,3 ,4 ]
Lardenois, Emilie [5 ,6 ]
Ray-Coquard, Isabelle [5 ,7 ,8 ]
Harter, Philipp [9 ,10 ]
Joly, Florence [11 ,12 ]
Canzler, Ulrich [13 ,14 ,15 ,16 ]
Truntzer, Caroline [3 ,17 ,18 ]
Tredan, Olivier [7 ,8 ]
Liebrich, Clemens [19 ,20 ]
Lortholary, Alain [21 ,22 ]
Pissaloux, Daniel [6 ,23 ]
Leary, Alexandra [24 ,25 ]
Pfisterer, Jacobus [26 ,27 ]
Eeckhoutte, Alexandre [28 ]
Hilpert, Felix [29 ,30 ]
Fabbro, Michel [31 ,32 ]
Caux, Christophe [5 ,33 ]
Alexandre, Jerome [34 ,35 ]
Houlier, Aurelie [6 ,23 ]
Sehouli, Jalid [36 ,37 ]
Sohier, Emilie [38 ]
Kimmig, Rainer [39 ,40 ]
Dubois, Bertrand [5 ,33 ]
Spaeth, Dominique [41 ,42 ]
Treilleux, Isabelle [6 ]
Frenel, Jean-Sebastien [43 ,44 ]
Herwig, Uwe [45 ,46 ]
Le Saux, Olivia [5 ,7 ,8 ]
Bendriss-Vermare, Nathalie [5 ,33 ]
du Bois, Andreas [47 ,48 ]
机构
[1] Ctr GF Leclerc, GINECO, 1 Rue Prof Mar, F-21000 Dijon, France
[2] Ctr GF Leclerc, Dept Med Oncol, 1 Rue Prof Mar, F-21000 Dijon, France
[3] Platform Transfer Canc Biol, F-21079 Dijon, France
[4] Univ Bourgogne Franche Comte, F-21000 Dijon, France
[5] Univ Claude Bernard Lyon 1, Univ Lyon, Canc Res Ctr Lyon, Ctr Leon Berard,INSERM 1052,CNRS 5286,Canc Immune, Lyon, France
[6] Leon Berard Ctr, Dept Pathol, F-69000 Lyon, France
[7] Univ Claude Bernard Lyon 1, GINECO, 28 Rue Laennec, F-69008 Lyon, France
[8] Univ Claude Bernard Lyon 1, Ctr Leon Berard, Dept Med Oncol, 28 Rue Laennec, F-69008 Lyon, France
[9] Evang Kliniken Essen Mitte, AGO, D-45136 Essen, Germany
[10] Evang Kliniken Essen Mitte, Dept Gynecol & Gynecol Oncol, D-45136 Essen, Germany
[11] Baclesse Canc Ctr, GINECO, F-14118 Caen, France
[12] Baclesse Canc Ctr, Dept Med Oncol, F-14118 Caen, France
[13] Tech Univ Dresden, AGO, Dresden, Germany
[14] Tech Univ Dresden, Dept Gynecol & Obstet, Fac Med, Dresden, Germany
[15] Tech Univ Dresden, Univ Hosp Carl Gustav Carus, Dresden, Germany
[16] Natl Ctr Tumor Dis NCT, Partner Site Dresden, D-01307 Dresden, Germany
[17] Genet & Immunol Med Inst GIMI, F-21000 Dijon, France
[18] INSERM, UMR 1231, F-21000 Dijon, France
[19] AGO, Sauerbruchstr 7, D-38840 Wolfsburg, Germany
[20] Klinikum Wolfsburg, AmO Interdisziplinares Ambulantes Onkol Zentrum K, Sauerbruchstr 7, D-38840 Wolfsburg, Germany
[21] GINECO, F-44200 Nantes, France
[22] Confluent Private Hosp, Inst Cancerol Catherine Sienne, F-44200 Nantes, France
[23] Univ Claude Bernard Lyon 1, Univ Lyon, INSERM 1052, CNRS 5286,Ctr Leon Berard,Canc Res Ctr Lyon,Equip, F-69000 Lyon, France
[24] Inst Gustave Roussy, GINECO, F-94805 Villejuif, France
[25] Inst Gustave Roussy, Dept Med Oncol, F-94805 Villejuif, France
[26] AGO, Herzog Friedrich Str 21, D-24103 Kiel, Germany
[27] Zentrum Gynakol Onkol, Herzog Friedrich Str 21, D-24103 Kiel, Germany
[28] PSL Res Univ, INSERM, U830, DNA Repair & Uveal Melanoma DRUm,Inst Curie, F-75005 Paris, France
[29] AGO, Moorkamp 2-6, D-20357 Hamburg, Germany
[30] Krankenhaus Jerusalem, Onkol Tagesklin, Moorkamp 2-6, D-20357 Hamburg, Germany
[31] GINECO, 208 Ave Apothicaires, F-34298 Montpellier, France
[32] ICM Val Aurelle, Oncol Med, 208 Ave Apothicaires, F-34298 Montpellier, France
[33] Ctr Leon Berard, Lab Immunotherapy Canc Lyon LICL, F-69000 Lyon, France
[34] Hop Cochin, GINECO, F-75014 Paris, France
[35] Hop Cochin, Dept Med Oncol, F-75014 Paris, France
[36] AGO, Augustenburger Pl 1, D-13353 Berlin, Germany
[37] Med Univ Berlin, Charite, Dept Gynecol, Ctr Oncol Surg, Augustenburger Pl 1, D-13353 Berlin, Germany
[38] Synergie Lyon Canc, Bioinformat Platform, F-69000 Lyon, France
[39] Univ Duisburg Essen Germany, AGO, D-45136 Essen, Germany
[40] Univ Duisburg Essen Germany, West German Canc Ctr, Dept Gynecol & Obstet, D-45136 Essen, Germany
[41] GINECO, F-54000 Nancy, France
[42] Ctr Oncol Gentilly, Dept Med Oncol, F-54000 Nancy, France
[43] GINECO, F-44800 St Herblain, France
[44] Inst Cancerol Ouest, Dept Med Oncol, Site Rene Gauducheau, F-44800 St Herblain, France
[45] AGO, Suntelstr 11a, D-22457 Hamburg, Germany
[46] Albertinen Krankenhaus, Dept Gynecol, Suntelstr 11a, D-22457 Hamburg, Germany
[47] AGO, D-45136 Essen, Germany
[48] Evangel Kliniken Essen Mitte KEM, D-45136 Essen, Germany
关键词
ovarian cancer; tumor immune microenvironment; HLA-E; copy number alterations; homologous recombination deficiency; HRD; HOMOLOGOUS RECOMBINATION REPAIR; HLA-E; BEVACIZUMAB; CHEMOTHERAPY; EXPRESSION; ASSOCIATION; BRCA1;
D O I
10.3390/cancers14051189
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Simple Summary Given the importance of genomic instability signatures in the management of ovarian cancer and the difficulties in defining the role of immunotherapy, our objective was to describe the tumor immune microenvironment in the light of genomic instability signatures. Intratumoral CD3(+) T lymphocytes confirmed its prognostic value. HLA-E appears to be a robust prognostic biomarker and preferentially overexpressed in homologous recombination deficiency (HRD) ovarian cancers. Our data provide a rationale for future immunotherapy strategies targeting the inhibitory CD94/NKG2A receptor of HLA-E in HRD tumors. Background: Following disappointing results with PD-1/PD-L1 inhibitors in ovarian cancer, it is essential to explore other immune targets. The aim of this study is to describe the tumor immune microenvironment (TME) according to genomic instability in high grade serous ovarian carcinoma (HGSOC) patients receiving primary debulking surgery followed by carboplatin-paclitaxel chemotherapy +/- nintedanib. Methods: 103 HGSOC patients' tumor samples from phase III AGO-OVAR-12 were analyzed. A comprehensive analysis of the TME was performed by immunohistochemistry on tissue microarray. Comparative genomic hybridization was carried out to evaluate genomic instability signatures through homologous recombination deficiency (HRD) score, genomic index, and somatic copy number alterations. The relationship between genomic instability and TME was explored. Results: Patients with high intratumoral CD3(+) T lymphocytes had longer progression-free survival (32 vs. 19.6 months, p = 0.009) and overall survival (OS) (median not reached). High HLA-E expression on tumor cells was associated with a longer OS (median OS not reached vs. 52.9 months, p = 0.002). HRD profile was associated with high HLA-E expression on tumor cells and an improved OS. In the multivariate analysis, residual tumor, intratumoral CD3, and HLA-E on tumor cells were more predictive than other parameters. Conclusions: Our results suggest HLA-E/CD94-NKG2A/2C is a potential immune target particularly in the HRD positive ovarian carcinoma subgroup.
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页数:16
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