Cancer Science & Therapy

Biography

Biography: Yan Zhao

Abstract

Statement of the Problem: The nucleophosmin (NPM1) is the most mutated gene (~30%) in Acute Myeloid Leukemia (AML)¹. Three NPM1 mutations (type A, B, and D) represent ~84% in NPM1-mutated AML cases while other uncommon subtypes occupy ~16%². Xpert^® NPM1 mutation, an automated cartridge-based test for measuring NPM1 mutation transcript levels (type A, B and D), is standardized to quantify the amount of mutated NPM1 relative to ABL1 control gene based on delta Ct in peripheral blood³. Since mutated NPM1 level is crucial for risk assessment, medication selection, and ongoing therapeutic monitoring in AML^4,5, it is important to obtain the NPM1 mutation copy number (CN). The aim of this work is to develop NPM1 mutation CN estimator and to compare %NPM1 mutation/ABL1 reporting between delta Ct-based and CN-based methods. Methodology & Theoretical Orientation: Five levels of NPM1 mutations (A, B, D) and ABL1 IVT-RNA panels as well as two lots of Xpert^® NPM1 mutation tests were used to generate standard curves for CN and %CN reporting. The cell lysates from cell lines carrying either NPM1 mutation A, B, or D and AML clinical samples containing NPM1 mutations were examined to evaluate the CN and %CN between two lots of the Xpert^® NPM1 mutation tests and to compare the delta Ct-based and CN-based methods for reporting %NPM1 mutation/ABL.  Findings: Linearity was demonstrated in Ct vs CN input for NPM1 mutation and ABL1 with R2 above 0.96 for Lot1 and Lo2. Less than 3-fold difference was exhibited for CN and %CN across two lots of Xpert^® NPM1 mutation test. Less than 3-fold difference was observed in %NPM1 mutation/ABL1 reporting between delta Ct-based and CN-based approaches. Conclusion & Significance: An NPM1 mutation copy number estimator for Xpert^® NPM1 mutation test was established, which will provide diagnostic and prognostic values for NPM1-mutated AML patients.