Ultra-accurate Duplex Sequencing for the assessment of pretreatment ABL1 kinase domain mutations in Ph+ ALL

Author:

Short Nicholas J.,Kantarjian Hagop,Kanagal-Shamanna RashmiORCID,Sasaki Koji,Ravandi Farhad,Cortes Jorge,Konopleva Marina,Issa Ghayas C.ORCID,Kornblau Steven M.ORCID,Garcia-Manero Guillermo,Garris Rebecca,Higgins Jake,Pratt Gabriel,Williams Lindsey N.,Valentine Charles C.,Rivera Victor M.,Pritchard Justin,Salk Jesse J.,Radich Jerald,Jabbour Elias

Abstract

AbstractMutations of ABL1 are the dominant mechanism of relapse in Philadelphia chromosome-positive acute lymphoblastic leukemia (Ph + ALL). We performed highly accurate Duplex Sequencing of exons 4–10 of ABL1 on bone marrow or peripheral blood samples from 63 adult patients with previously untreated Ph + ALL who received induction with intensive chemotherapy plus a BCR-ABL1 TKI. We identified ABL1 mutations prior to BCR-ABL1 TKI exposure in 78% of patients. However, these mutations were generally present at extremely low levels (median variant allelic frequency 0.008% [range, 0.004%–3.71%] and did not clonally expand and lead to relapse in any patient, even when the pretreatment mutation was known to confer resistance to the TKI received. In relapse samples harboring a TKI-resistant ABL1 mutation, the corresponding mutation could not be detected pretreatment, despite validated sequencing sensitivity of Duplex Sequencing down to 0.005%. In samples under the selective pressure of ongoing TKI therapy, we detected low-level, emerging resistance mutations up to 5 months prior to relapse. These findings suggest that pretreatment ABL1 mutation assessment should not guide upfront TKI selection in Ph + ALL, although serial testing while on TKI therapy may allow for early detection of clinically actionable resistant clones.

Publisher

Springer Science and Business Media LLC

Subject

Oncology,Hematology

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