Published January 13, 2023 | Version v1
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Genomic characteristics and clinical significance of CD56+ Circulating Tumor Cells in SCLC

Creators

  • 1. Univ Rennes 1, INSERM, OSS (Oncogenesis Stress Signaling), UMR_S 1242, CLCC Eugene Marquis, F-35000, Rennes, France; Service de Pneumologie, CHU Rennes, Rennes, France
  • 2. Univ Rennes 1, INSERM, OSS (Oncogenesis Stress Signaling), UMR_S 1242, CLCC Eugene Marquis, F-35000, Rennes, France
  • 3. Division of Molecular Genome Analysis (B050), German Cancer Research Center (DKFZ), Im Neuenheimer Feld 280, 69120 Heidelberg, Germany; e-NIOS PC, Kallithea-Athens, Greece
  • 4. e-NIOS PC, Kallithea-Athens, Greece
  • 5. Univ Rennes, CNRS, INSERM, BIOSIT UAR 3480, US_S 018, Oncotrial, F-35000 Rennes, France; Biotrial Pharmacology, Unité De Pharmacologie Préclinique, Rennes, France
  • 6. Centre of Systems Biology, Biomedical Research Foundation of the Academy of Athens, 4 Soranou Ephessiou Street, 11527, Athens, Greece
  • 7. Service de Pneumologie, CHU Rennes, Rennes, France
  • 8. Univ Rennes, CNRS, INSERM, BIOSIT UAR 3480, US_S 018, Oncotrial, F-35000 Rennes, France
  • 9. e-NIOS PC, Kallithea-Athens, Greece; Centre of Systems Biology, Biomedical Research Foundation of the Academy of Athens, 4 Soranou Ephessiou Street, 11527, Athens, Greece
  • 10. Univ Rennes 1, INSERM, OSS (Oncogenesis Stress Signaling), UMR_S 1242, CLCC Eugene Marquis, F-35000, Rennes, France; Univ Rennes, CNRS, INSERM, BIOSIT UAR 3480, US_S 018, Oncotrial, F-35000 Rennes, France

Description

Introduction: Circulating Tumor Cells (CTC) have been studied in various solid tumors but clinical utility of CTC in Small Cell Lung Cancer (SCLC) remains unclear. The aim of the CTC-CPC study was to develop an EpCAM-independent CTC isolation method allowing isolation of a broader range of living CTC from SCLC and decipher their genomic and biological characteristics.

Patients and methods: CTC-CPC is a monocentric prospective non-interventional study including treatment-naïve newly diagnosed SCLC. CD56+CTC were isolated from whole blood samples, at diagnosis and relapse after first-line treatment and submitted to  Whole-exome-sequencing (WES).

Results: Phenotypic study confirms tumor lineage and tumorigenic properties of isolated cells for the 4 patients analyzed with WES. WES of CD56+CTC and matched tumor biopsy reveal genomic alteration frequently impaired in SCLC. At diagnosis CD56+CTC were characterized by a high mutation load, a distinct mutational profile and a unique genomic, compared to match tumors biopsies. In addition to classical pathways altered in SCLC, we found new biological processes specifically affected in CD56+CTC at diagnosis. High numeration of CD56+CTC (>7/ml) at diagnosis was associated with ES-SCLC. Comparing CD56+CTC isolated at diagnosis and relapse, we identify differentially altered oncogenic pathways (e.g. DLL3 or MAPK pathway).

Conclusions: We report a versatile method of CD56+CTC detection in SCLC. Numeration of CD56+CTC at diagnosis is correlated with disease extension. Isolated CD56+CTC are tumorigenic and a distinct mutational profile. We report a minimal gene set as a unique signature of CD56+CTC and identify new affected biological pathways enriched in EpCAM-independent isolated CTC in SCLC.

Notes

Supplementary material for the publication, including important components: 1) Command line code example used for the identification of somatic variants from raw data (SCLC.ReproducibleExample.CommandLine.12012022.txt) 2) Rscript to create specific figures and parts of the computational workflow with R/Rstudio (SCLC.Paper.AnalysisFigures.12012022.R) & relative R session information (RSessionInfo.SCLC.OriginalAnalysis) 3) Additional important files to support the reproducibility of the bioinformatics analysis (i.e. VCF files for mutational patterns)

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