t(14;18) Translocation: A Predictive Blood Biomarker for Follicular Lymphoma

Author:

Roulland Sandrine1,Kelly Rachel S.1,Morgado Ester1,Sungalee Stéphanie1,Solal-Celigny Philippe1,Colombat Philippe1,Jouve Nathalie1,Palli Domenico1,Pala Valeria1,Tumino Rosario1,Panico Salvatore1,Sacerdote Carlotta1,Quirós José R.1,Gonzáles Carlos A.1,Sánchez Maria-José1,Dorronsoro Miren1,Navarro Carmen1,Barricarte Aurelio1,Tjønneland Anne1,Olsen Anja1,Overvad Kim1,Canzian Federico1,Kaaks Rudolf1,Boeing Heiner1,Drogan Dagmar1,Nieters Alexandra1,Clavel-Chapelon Françoise1,Trichopoulou Antonia1,Trichopoulos Dimitrios1,Lagiou Pagona1,Bueno-de-Mesquita H. Bas1,Peeters Petra H.M.1,Vermeulen Roel1,Hallmans Göran1,Melin Beatrice1,Borgquist Signe1,Carlson Joyce1,Lund Eiliv1,Weiderpass Elisabete1,Khaw Kay-Tee1,Wareham Nick1,Key Timothy J.1,Travis Ruth C.1,Ferrari Pietro1,Romieu Isabelle1,Riboli Elio1,Salles Gilles1,Vineis Paolo1,Nadel Bertrand1

Affiliation:

1. Sandrine Roulland, Ester Morgado, Stéphanie Sungalee, Nathalie Jouve, and Bertrand Nadel, Aix-Marseille Université, Institut National de la Santé et de la Recherche Médicale (INSERM) U1104, and Centre National de la Recherche Scientifique (CNRS) Unités Mixtes de Recherche (UMR) 7280, Marseille; Philippe Solal-Celigny, Jean Bernard Center, Le Mans; Philippe Colombat, Bretonneau University Hospital, Tours; Françoise Clavel-Chapelon, INSERM U1018 Centre de Recherche en Epidémiologie et Santé des Populations...

Abstract

Purpose The (14;18) translocation constitutes both a genetic hallmark and critical early event in the natural history of follicular lymphoma (FL). However, t(14;18) is also detectable in the blood of otherwise healthy persons, and its relationship with progression to disease remains unclear. Here we sought to determine whether t(14;18)-positive cells in healthy individuals represent tumor precursors and whether their detection could be used as an early predictor for FL. Participants and Methods Among 520,000 healthy participants enrolled onto the EPIC (European Prospective Investigation Into Cancer and Nutrition) cohort, we identified 100 who developed FL 2 to 161 months after enrollment. Prediagnostic blood from these and 218 controls were screened for t(14;18) using sensitive polymerase chain reaction–based assays. Results were subsequently validated in an independent cohort (65 case participants; 128 controls). Clonal relationships between t(14;18) cells and FL were also assessed by molecular backtracking of paired prediagnostic blood and tumor samples. Results Clonal analysis of t(14;18) junctions in paired prediagnostic blood versus tumor samples demonstrated that progression to FL occurred from t(14;18)-positive committed precursors. Furthermore, healthy participants at enrollment who developed FL up to 15 years later showed a markedly higher t(14;18) prevalence and frequency than controls (P < .001). Altogether, we estimated a 23-fold higher risk of subsequent FL in blood samples associated with a frequency > 10−4 (odds ratio, 23.17; 95% CI, 9.98 to 67.31; P < .001). Remarkably, risk estimates remained high and significant up to 15 years before diagnosis. Conclusion High t(14;18) frequency in blood from healthy individuals defines the first predictive biomarker for FL, effective years before diagnosis.

Publisher

American Society of Clinical Oncology (ASCO)

Subject

Cancer Research,Oncology

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