Clinical and genetic drivers of oligo-metastatic disease in colon cancer

Alessandro Ottaiano; Mariachiara Santorsola; Roberto Sirica; Annabella Di Mauro; Antonella Di Carlo; Monica Ianniello; Francesco Sabbatino; Rosa Castiello; Francesca Del Peschio; Marco Cascella; Francesco Perri; Maurizio Capuozzo; Nicola Martucci; Edoardo Mercadante; Valentina Borzillo; Rossella Di Franco; Francesco Izzo; Vincenza Granata; Carmine Picone; Antonella Petrillo; Massimiliano Berretta; Salvatore Stilo; Luca Tarotto; Anna Chiara Carratù; Gerardo Ferrara; Madhura Tathode; Alessia Maria Cossu; Marco Bocchetti; Michele Caraglia; Guglielmo Nasti; Giovanni Savarese

doi:10.1016/j.neo.2024.101111

Clinical and genetic drivers of oligo-metastatic disease in colon cancer

Neoplasia. 2024 Dec 21:60:101111. doi: 10.1016/j.neo.2024.101111. Online ahead of print.

Authors

Alessandro Ottaiano¹, Mariachiara Santorsola², Roberto Sirica³, Annabella Di Mauro⁴, Antonella Di Carlo³, Monica Ianniello³, Francesco Sabbatino⁵, Rosa Castiello³, Francesca Del Peschio³, Marco Cascella⁶, Francesco Perri⁷, Maurizio Capuozzo⁸, Nicola Martucci⁹, Edoardo Mercadante⁹, Valentina Borzillo¹⁰, Rossella Di Franco¹⁰, Francesco Izzo¹¹, Vincenza Granata¹², Carmine Picone¹², Antonella Petrillo¹², Massimiliano Berretta¹³, Salvatore Stilo¹⁴, Luca Tarotto¹⁴, Anna Chiara Carratù², Gerardo Ferrara⁴, Madhura Tathode¹⁵, Alessia Maria Cossu¹⁵, Marco Bocchetti¹⁵, Michele Caraglia¹⁵, Guglielmo Nasti², Giovanni Savarese³

Affiliations

¹ SSD-Innovative Therapies for Abdominal Metastases, IRCCS "G. Pascale", Istituto Nazionale Tumori di Napoli, Via M. Semmola, Naples 80131, Italy. Electronic address: [email protected].
² SSD-Innovative Therapies for Abdominal Metastases, IRCCS "G. Pascale", Istituto Nazionale Tumori di Napoli, Via M. Semmola, Naples 80131, Italy.
³ AMES, Centro Polidiagnostico Strumentale srl, Via Padre Carmine Fico 24, Casalnuovo Di Napoli 80013, Italy.
⁴ Unit of Pathology, IRCCS "G. Pascale", Istituto Nazionale Tumori di Napoli, Via M. Semmola, Naples 80131, Italy.
⁵ Medical Oncology, Department of Medicine, Surgery and Dentistry, University of Salerno, Baronissi 84081, Italy.
⁶ Unit of Anesthesia and Pain Medicine, Department of Medicine, Surgery and Dentistry, University of Salerno, Baronissi 84081, Italy.
⁷ Medical and Experimental Head and Neck Oncology Unit, IRCCS "G. Pascale", Istituto Nazionale Tumori di Napoli, Via M. Semmola, Naples 80131, Italy.
⁸ Coordinamento Farmaceutico, ASL-Naples-3, Ercolano 80056, Italy.
⁹ Unit of Thoracic Surgery, Istituto Nazionale Tumori di Napoli, IRCCS "G. Pascale", Via M. Semmola, Naples 80131, Italy.
¹⁰ Department of Radiation Oncology, IRCCS "G. Pascale", Istituto Nazionale Tumori di Napoli, Via M. Semmola, Naples 80131, Italy.
¹¹ Unit of Epato-Biliary Surgery, Istituto Nazionale Tumori di Napoli, IRCCS "G. Pascale", Via M. Semmola, Naples 80131, Italy.
¹² Unit of Radiology, Istituto Nazionale Tumori di Napoli, IRCCS "G. Pascale", Via M. Semmola, Naples 80131, Italy.
¹³ Department of Clinical and Experimental Medicine, University of Messina, Messina 98122, Italy.
¹⁴ Interventional Radiology Unit, Istituto Nazionale Tumori di Napoli, IRCCS "G. Pascale", Via M. Semmola, Naples 80131, Italy.
¹⁵ Department of Precision Medicine, University of Campania "L. Vanvitelli", Via Luigi De Crecchio 7, Naples 80138, Italy; Laboratory of Precision and Molecular Oncology, Biogem Scarl IRGS, Ariano Irpino, Italy.

PMID: 39709701
DOI: 10.1016/j.neo.2024.101111

Abstract

Background: Oligo-metastatic disease (OMD) in colon cancer patients exhibits distinct clinical behavior compared to poly-metastatic disease (PMD), with a more responsive and indolent course. This study aims to identify clinical and biological factors uniquely associated with oligo-metastatic behavior.

Methods: Metastatic colon cancer patients from an academic center underwent genetic characterization. OMD was defined as ≤3 lesions per organ, each with a total diameter <70 mm and none exceeding 25 mm. Tumor DNA sequencing by NGS utilized the TruSight Oncology 500 kit. Overall survival (OS) was determined from metastasis diagnosis until death using Kaplan-Meier analysis. Multivariate Cox regression examined prognostic links between clinicopathological and genetic factors. Associations with metastatic patterns were evaluated using Chi-square.

Results: The analysis involved 104 patients (44 with OMD, 60 with PMD). OMD was more prevalent in males (P = 0.0299) and with single organ involvement (P = 0.0226). Multivariate analysis adjusted for age (>70 vs. <70 years), gender (male vs. female), tumor side (right vs. left), metastatic involvement (more than one site vs. one site), response to first-line therapy (disease control vs. no disease control), and RAS/BRAF variants (wild-type vs. mutated) identified OMD vs. PMD as the strongest independent predictor of survival (HR: 0.14; 95 % CI: 0.06-0.33; P<0.0001). OMD patients exhibited distinct molecular characteristics, including lower frequencies of BRAF p.V600E (P=0.0315) and KRAS mutations (P=0.0456), as well as a higher frequency of high tumor mutational burden (P=0.0127). Additionally, by integrating data from public datasets and our case study, we hypothesize that some gene alterations (i.e.: BRAF, SMAD4, RAF1, and mTOR) may prevent OMD occurrence.

Conclusion: OMD, characterized by male predominance, single-site involvement, and distinct molecular features in colon cancer, suggests the need for tailored management strategies.

Keywords: BRAF; KRAS; Next generations sequencing; Oligo-metastatic disease; Prognosis; Tumor mutational burden.