Clinical and molecular features of early onset pancreatic adenocarcinoma

Author:

Rémond Maxime1ORCID,Smolenschi Cristina12,Tarabay Anthony1,Gelli Maximiliano3,Fernandez‐de‐Sevilla Elena3,Mouawia Ali1,Cosconea Simona4,Tselikas Lambros5,Barbe Remy6,Fuerea Alina1,Bani Mohamed A.7,Deloger Marc8,Besse Benjamin19,Pudlarz Thomas1,Valéry Marine1,Boige Valérie1,Hollebecque Antoine12,Ducreux Michel19,Boilève Alice19

Affiliation:

1. Département de Médecine Gustave Roussy Villejuif France

2. Département d'Innovation Thérapeutique et d'Essais Précoces Gustave Roussy Villejuif France

3. Département de Chirurgie Gustave Roussy Villejuif France

4. Département d'Endoscopie Gustave Roussy Villejuif France

5. Département de Radiologie Interventionnelle Gustave Roussy Villejuif France

6. Département d'Imagerie Gustave Roussy Villejuif France

7. Département d'Anatomopathologie Gustave Roussy Villejuif France

8. Service de Bioinformatique Gustave Roussy Villejuif France

9. Université Paris Saclay Orsay France

Abstract

AbstractPancreatic adenocarcinoma (PDAC) is a major health burden and may become the second cause of death by cancer in developed countries. The incidence of early‐onset pancreatic cancer (EOPC, defined by an age at diagnosis <50 years old) is increasing. Here, we conducted a study of all PDAC patients followed at our institution. Patients were classified as EOPC or non‐early onset (nEOPC, >50). Eight hundred and seventy eight patients were included, of which 113 EOPC, exhibiting a comparable performance status. EOPC were more often diagnosed at the metastatic stage (70.0% vs 58.3%) and liver metastases were more prevalent at diagnosis (60.2% vs. 43.9%). The median overall survival (OS) from diagnosis was 18.1 months, similar between EOPC and nEOPC. Among patients who underwent surgery, recurrence‐free survival was similar between age groups. Among metastatic patients, first line progression free survival was similar but EOPC received more treatment lines (72.3% vs. 58.1% received ≥2 lines). Regarding molecular alterations, the mean tumor mutational burden (TMB) was lower in EOPC (1.42 vs. 2.95 mut/Mb). The prevalence of KRAS and BRCA1/2 mutations was similar, but EOPC displayed fewer alterations in CNKN2A/B. Fifty eight patients (18.6%) had actionable alterations (ESCAT I‐III) and 31 of them received molecularly matched treatments. On the transcriptomic level, despite its clinical aggressiveness, EOPC was less likely to display a basal‐like phenotype. To conclude, EOPC were diagnosed more frequently at the metastatic stage. OS and 1st line PFS were similar to nEOPC. EOPC displayed specific molecular features, such as a lower TMB and fewer alterations in CDKN2A/B.

Publisher

Wiley

Reference36 articles.

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