A Collaborative Effort to Define Classification Criteria for ATM Variants in Hereditary Cancer Patients.

Lidia Feliubadaló,Anael López-Novo,Gabriel Capellá,Clara Ruiz-Ponte,Conxi Lázaro,Ignacio J Molina,Alysson T Sánchez,Daniel Rueda,Alejandro Moles-Fernández,Orland Diez,Luz-Marina Porras,Ana Osorio,Marta Pineda,Ana Blanco,Sara Gutiérrez-Enríquez,Marta Santamariña-Pena,Ana Vega,Xavier De La Cruz,Miguel De La Hoya

doi:10.1093/clinchem/hvaa250

Abstract

Gene panel testing by massive parallel sequencing has increased the diagnostic yield but also the number of variants of uncertain significance. Clinical interpretation of genomic data requires expertise for each gene and disease. Heterozygous ATM pathogenic variants increase the risk of cancer, particularly breast cancer. For this reason, ATM is included in most hereditary cancer panels. It is a large gene, showing a high number of variants, most of them of uncertain significance. Hence, we initiated a collaborative effort to improve and standardize variant classification for the ATM gene. Six independent laboratories collected information from 766 ATM variant carriers harboring 283 different variants. Data were submitted in a consensus template form, variant nomenclature and clinical information were curated, and monthly team conferences were established to review and adapt American College of Medical Genetics and Genomics/Association for Molecular Pathology (ACMG/AMP) criteria to ATM, which were used to classify 50 representative variants. Amid 283 different variants, 99 appeared more than once, 35 had differences in classification among laboratories. Refinement of ACMG/AMP criteria to ATM involved specification for twenty-one criteria and adjustment of strength for fourteen others. Afterwards, 50 variants carried by 254 index cases were classified with the established framework resulting in a consensus classification for all of them and a reduction in the number of variants of uncertain significance from 58% to 42%. Our results highlight the relevance of data sharing and data curation by multidisciplinary experts to achieve improved variant classification that will eventually improve clinical management.

Highlights

Genetic diagnosis for hereditary cancers (HC) has changed over the past decade thanks to the introduction of massive parallel sequencing (MPS) technologies which allow the screening of multiple genes outright
MPS diagnostic panels increase sensitivity and the number of variants of uncertain clinical significance (VUS) identified; application of MPS panels poses a significant challenge in the clinical management of patients and evidences the need for standardization in variant classification
We collected information from 769 individuals carrying 283 different ATM variants; 104 index cases carried more than one ATM variant

Summary

Introduction

Genetic diagnosis for hereditary cancers (HC) has changed over the past decade thanks to the introduction of massive parallel sequencing (MPS) technologies which allow the screening of multiple genes outright. The American College of Medical Genetics and Genomics (ACMG) and the Association for Molecular Pathology (AMP) have provided a general framework for classification of genetic variants [1]. These universal guidelines need to be tuned according to the disease and the specific gene by a consensus of experts. Heterozygous ATM pathogenic variants increase the risk of cancer, breast cancer For this reason, ATM is included in most hereditary cancer panels. ATM is included in most hereditary cancer panels It is a large gene, showing a high number of variants, most of them of uncertain significance. We initiated a collaborative effort to improve and standardize variant classification for the ATM gene

Methods

Results

Conclusion