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Poster session 18

1505P - Exploratory biomarker analysis of the NEONAX trial for response prediction to perioperative (PO) and adjuvant (A) Gem-nabPac chemotherapy (CTX) in resectable PDAC patients (rPDAC Pts)

Date

14 Sep 2024

Session

Poster session 18

Topics

Clinical Research; Cancer Biology; Cytotoxic Therapy; Tumour Immunology; Pathology/Molecular Biology; Translational Research; Targeted Therapy; Molecular Oncology

Tumour Site

Pancreatic Adenocarcinoma

Presenters

Anton Lahusen

Citation

Annals of Oncology (2024) 35 (suppl_2): S923-S936. 10.1016/annonc/annonc1605

Authors

A. Lahusen¹, T.J. Ettrich¹, M. Kirchner², K. Kluck², S. Wisser³, W. Uhl⁴, M. Kornmann⁵, H. Algül⁶, H. Friess⁷, A.O. Koenig⁸, A. Kleger¹, J. Schuhbaur¹, L. Perkhofer¹, J. Budczies², M.A. Tempero⁹, A. Reinacher-Schick¹⁰, A. Stenzinger², A. Tannapfel³, T. Eiseler¹, T. Seufferlein¹

Author affiliations

¹ Internal Medicine I, University Hospital, 89081 - Ulm/DE
² Institute Of Pathology, University Hospital, 69120 - Heidelberg/DE
³ Institute Of Pathology, Georgius Agricola Stiftung Ruhr-Universität, 44789 - Bochum/DE
⁴ General And Visceral Surgery, Katholisches Klinikum St. Josef-Hospital, 44791 - Bochum/DE
⁵ General And Visceral Surgery, Universitätsklinikum Ulm, 89075 - Ulm/DE
⁶ Comprehensive Cancer Center, TUM Technical University, 80333 - Munich/DE
⁷ General And Visceral Surgery, Klinikum Rechts der Isar TUM, 81675 - Munich/DE
⁸ Gastroenterology, Universitätsmedizin, 37075 - Goettingen/DE
⁹ Hematology And Oncology, UCSF Helen Diller Family Comprehensive Cancer Center, 94115 - San Francisco/US
¹⁰ Oncology And Palliative Care, Katholisches Klinikum St. Josef-Hospital, 44791 - Bochum/DE

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Abstract 1505P

Background

The recent phase II NEONAX trial examined PO and A Gem-nabPac CTX for rPDAC Pts. The objective of this study was to identify underlying alterations in the tumor immune microenvironment (TiME) associated with shortest (S) or longest (L) disease-free survival (DFS) and to identify corresponding biomarkers predicting CTX success.

Methods

Pts from both study arms were stratified into groups based on S- or L-DFS (n = 32, n = 8 Pts/group). PDAC tissues (surgical resection) were subjected to RNA (NanoString^TM, PanCancer IO360^TM) profiling. CTX-naïve blood samples were analyzed via multiplexed ELISA (mELISA, 80-Plex ProcartaPlex^TM). For feature selection via machine learning (ML), the Weka-based algorithms WrapperSubsetEval (WSE) with Naïve Bayes, J48, or a multilayer perceptron neuronal network (MLP) were used. Pts were divided into training (80%) and validation (20%) datasets and categorized by using either MLP or J48 classifiers.

Results

Comparisons of L- vs. S-DFS transcriptomics data revealed significantly increased inflammation (upregulated genes: CXCL9, SELP, CDH5), immune cell activation (enriched: NK cell cytotoxicity, activated CD8 T cells), and immune cell infiltration (CD8 T cells, NK cells) for treated (PO group) but not treatment-naïve (A group) L-TTF tumors. Screening of CTX-naïve blood samples (mELISA) detected 80 immune-related factors. Feature selection for S- vs. L-DFS prediction (n = 80 Pts; PO: n = 42, A: n = 38) revealed a panel of 8 proteins for the PO group (Naïve Bayes; CSF3, LGALS3, GZMA, CCL1, IL20, IL3, CCL7, PTX3), 6 proteins for the A group (J48; IL1A, IL1B, IL3, IL34, MIF, CCL19), and 7 proteins for the combined (c)rPDAC group (MLP; CCL21, CX3CL1, IL16, IL20, IL7, PTX3, TSLP). ML successfully predicted S-/L-DFS for the PO (via MLP), crPDAC (via MLP), and A (via J48) group (ROC-AUC (training) > 0.9, ROC-AUC (validation) > 0.9, respectively).

Conclusions

In our study, we have identified a favorable TiME for L-DFS rPDAC Pts under PO Gem-nabPac CTX. We further present minimal immune-related liquid biomarker signatures based on mELISA and ML for early prediction of Gem-nabPac CTX success in PO and A treatment settings, or for rPDAC Pts in general.

Clinical trial identification

NCT02047513; AIO Studie: AIO-PAK-0313.

Editorial acknowledgement

Legal entity responsible for the study

T. Seufferlein.

Funding

Celgene/Bristol Myers Squibb.

Disclosure

All authors have declared no conflicts of interest.