Development and validation of a multigene variant profiling assay to guide targeted and immuno therapy selection in solid tumors

Author:

Akolkar DadasahebORCID,Patil Darshana,Srivastava NavinORCID,Patil Revati,Datta Vineet,Apurwa Sachin,Yashwante Nitin,Dhasarathan Raja,Gosavi Rahul,John Jinumary,Khan Shabishta,Jadhav Ninad,Mene Priti,Ahire Dhanashri,Pawar Sushant,Bodke Harshal,Sahoo Subhraline,Nile Arun,Saindane Dinesh,Darokar Harshal,Devhare Pradip,Srinivasan Ajay,Datar Rajan

Abstract

We present data on analytical validation of the multigene variant profiling assay (CellDx) to provide actionable indications for selection of targeted and immune checkpoint inhibitor (ICI) therapy in solid tumors. CellDx includes Next Generation Sequencing (NGS) profiling of gene variants in a targeted 452-gene panel as well as status of total Tumor Mutation Burden (TMB), Microsatellite instability (MSI), Mismatch Repair (MMR) and Programmed Cell Death—Ligand 1 (PD-L1) respectively. Validation parameters included accuracy, sensitivity, specificity and reproducibility for detection of Single Nucleotide Alterations (SNAs), Copy Number Alterations (CNAs), Insertions and Deletions (Indels), Gene fusions, MSI and PDL1. Cumulative analytical sensitivity and specificity of the assay were 99.03 (95% CI: 96.54–99.88) and 99.23% (95% CI: 98.54% - 99.65%) respectively with 99.20% overall Accuracy (95% CI: 98.57% - 99.60%) and 99.7% Precision based on evaluation of 116 reference samples. The clinical performance of CellDx was evaluated in a subsequent analysis of 299 clinical samples where 861 unique mutations were detected of which 791 were oncogenic and 47 were actionable. Indications in MMR, MSI and TMB for selection of ICI therapies were also detected in the clinical samples. The high specificity, sensitivity, accuracy and reproducibility of the CellDx assay is suitable for clinical application for guiding selection of targeted and immunotherapy agents in patients with solid organ tumors.

Funder

Datar Cancer Genetics

Publisher

Public Library of Science (PLoS)

Subject

Multidisciplinary

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