Abstract

Background : Chronic myeloid leukemia (CML) is a hematopoietic stem cell disease, associated with a reciprocal translocation between chromosomes 9 and chromosome 22, lead to the formation of the BCR-ABL fusion gene (Philadelphia chromosome). This fusion gene is believed to play golden role in the initial development of CML with constitutive tyrosine kinase activation.

Β Β  Successful use of tyrosine kinase inhibiters (TKIs) play a role in improve survival and increase prevalence of CML, but un fortunatelyΒ Β  mutations in the BCR-ABL kinase domain may cause, or contribute to increase, resistance to TKIs in CML patients.Β  .

Objective: This study was designed to assess the association of five most common BCR-ABL kinase domain mutations (T315I, M351T, E255K, M244V and E255V) with resistance state of CML patients on TKIs in Iraqi Middle Euphrates region.

Patients and methods: A retrospective case-control study in whichΒ  85Β  patients with chronic myeloid leukemia in chronic phase (45 patients as cases group and 40 patient as control group) were selected from three hemato-oncology centers in middle Euphrates in Iraq during the period from January 2016 till OctoberΒ  2016 out of a total ofΒ  240Β  CML patients ( 108 male and 132 female) who were registered during this period in these three centers Β and all patients on TKI (Imatinib and Nilotinib). Venous blood sampling done for BCR-ABL kinase domain mutations screening.

Results: Β four patients from cases group (4/45) were carriers of one of five selected ABL kinase domain mutations and no one of control group. T315I mutation was detected in 3/45 (6.6 %) of resistant patients, with a significant risk association to develop resistance to TKI therapy (odd ratio and C. I. ) (6.67, 0.3340Β -133.2255). E255V was detected in 1/45 ( 2.2 %) and also hadΒ  significant risk association to develop resistance to TKIs( odd ratio, C.I.) (2.73, 0.1081Β -68.9424). No one of these mutation had significance correlation with demographic or hematological features. M351T, E255K andΒ  M244V were not detected in any one of our study groups CML patients.

Conclusions: T315I and E255V among five ABL kinas domain mutations were detected in our CML patients with resistance to TKIs. All of them may play a role in development variable degree of resistance to first and second generation TKIs weather primary or secondary.T315I mutation is most common mutation withinΒ  BCR-ABL domain kinase gene.

Keywords

  • CML
  • TKIs
  • ABL domain kinase mutations