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Abstract Introduction: Digital PCR studies for clonal disease monitoring in B-ALL patients are currently limited due to the heterogeneous nature of mutations, which limitscost-effective assay designs. Materials and Methods: In the “DETECTOR study”, 70 samples (14 relapse and 56 sequential therapy samples) were tested for 13 mutations in the KRAS, NRAS, NT5C2, PMS2, UHRF1, KMT2D and TP53 genes via a novel triplex digital PCR assay. The results 37%) of our patients,driving 50% of very early-early relapses, thereby highlighting its utility for clonal monitoring in LMIC regions.
Bhatia et al. (Mon,) studied this question.