Genes (Feb 2022)

Loss of Heterozygosity in the Tumor DNA of De Novo Diagnosed Patients Is Associated with Poor Outcome for B-ALL but Not for T-ALL

  • Natalya Risinskaya,
  • Yana Kozhevnikova,
  • Olga Gavrilina,
  • Julia Chabaeva,
  • Ekaterina Kotova,
  • Anna Yushkova,
  • Galina Isinova,
  • Ksenija Zarubina,
  • Tatiana Obukhova,
  • Sergey Kulikov,
  • Hunan Julhakyan,
  • Andrey Sudarikov,
  • Elena Parovichnikova

DOI
https://doi.org/10.3390/genes13030398
Journal volume & issue
Vol. 13, no. 3
p. 398

Abstract

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Despite the introduction of new technologies in molecular diagnostics, one should not underestimate the traditional routine methods for studying tumor DNA. Here we present the evidence that short tandem repeat (STR) profiling of tumor DNA relative to DNA from healthy cells might identify chromosomal aberrations affecting therapy outcome. Tumor STR profiles of 87 adult patients with de novo Ph-negative ALL (40 B-ALL, 43 T-ALL, 4 mixed phenotype acute leukemia (MPAL)) treated according to the “RALL-2016” regimen were analyzed. DNA of tumor cells was isolated from patient bone marrow samples taken at diagnosis. Control DNA samples were taken from the buccal swab or the blood of patients in complete remission. Overall survival (OS) analysis was used to assess the independent impact of the LOH as a risk factor. Of the 87 patients, 21 were found with LOH in various STR loci (24%). For B-ALL patients, LOH (except 12p LOH) was an independent risk factor (OS hazard ratio 3.89, log-rank p-value 0.0395). In contrast, for T-ALL patients, the OS hazard ratio was 0.59 (log-rank p-value 0.62). LOH in particular STR loci measured at the onset of the disease could be used as a prognostic factor for poor outcome in B-ALL, but not in T-ALL.

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