Your search keyword '"Abdullah, Julia"' showing total 2 results

1. Mutation analysis of BCR-ABL1 kinase domain in chronic myeloid leukemia patients with tyrosine kinase inhibitors resistance: a Malaysian cohort study.

Author

Seman, Zahidah Abu, Ahid, Fadly, Kamaluddin, Nor Rizan, Sahid, Ermi Neiza Mohd, Esa, Ezalia, Said, Siti Shahrum Muhamed, Azman, Norazlina, Mat, Wan Khairull Dhalila Wan, Abdullah, Julia, Ali, Nurul Aqilah, Khalid, Mohd Khairul Nizam Mohd, and Yusoff, Yuslina Mat

Subjects

CHRONIC myeloid leukemia, NUCLEOTIDE sequencing, PROTEIN-tyrosine kinase inhibitors, GENETIC mutation, DASATINIB, COHORT analysis, MEDICAL protocols

Abstract

Objective: Mutational analysis of BCR::ABL1 kinase domain (KD) is a crucial component of clinical decision algorithms for chronic myeloid leukemia (CML) patients with failure or warning responses to tyrosine kinase inhibitor (TKI) therapy. This study aimed to detect BCR::ABL1 KD mutations in CML patients with treatment resistance and assess the concordance between NGS (next generation sequencing) and Sanger sequencing (SS) in detecting these mutations. Results: In total, 12 different BCR::ABL1 KD mutations were identified by SS in 22.6% (19/84) of patients who were resistant to TKI treatment. Interestingly, NGS analysis of the same patient group revealed an additional four different BCR::ABL1 KD mutations in 27.4% (23/84) of patients. These mutations are M244V, A344V, E355A, and E459K with variant read frequency below 15%. No mutation was detected in 18 patients with optimal response to TKI therapy. Resistance to TKIs is associated with the acquisition of additional mutations in BCR::ABL1 KD after treatment with TKIs. Additionally, the use of NGS is advised for accurately determining the mutation status of BCR::ABL1 KD, particularly in cases where the allele frequency is low, and for identifying mutations across multiple exons simultaneously. Therefore, the utilization of NGS as a diagnostic platform for this test is very promising to guide therapeutic decision-making. [ABSTRACT FROM AUTHOR]

Published

2024

2. Comprehensive analysis of mutations and clonal evolution patterns in a cohort of patients with cytogenetically normal acute myeloid leukemia.

Author

Mat Yusoff, Yuslina, Ahid, Fadly, Abu Seman, Zahidah, Abdullah, Julia, Kamaluddin, Nor Rizan, Esa, Ezalia, and Zakaria, Zubaidah

Subjects

ACUTE myeloid leukemia, GENETIC mutation, SYMPTOMS, SOMATIC mutation, PHENOTYPIC plasticity, DISEASE relapse

Abstract

Background: Relapsed acute myeloid leukemia (AML) is associated with the acquisition of additional somatic mutations which are thought to drive phenotypic adaptability, clonal selection and evolution of leukemic clones during treatment. We performed high throughput exome sequencing of matched presentation and relapsed samples from 6 cytogenetically normal AML (CN-AML) patients treated with standard remission induction chemotherapy in order to contribute with the investigation of the mutational landscape of CN-AML and clonal evolution during AML treatment. Result: A total of 24 and 32 somatic variants were identified in presentation and relapse samples respectively with an average of 4.0 variants per patient at presentation and 5.3 variants per patient at relapse, with SNVs being more frequent than indels at both disease stages. All patients have somatic variants in at least one gene that is frequently mutated in AML at both disease presentation and relapse, with most of these variants are classic AML and recurrent hotspot mutations including NPM1 p.W288fs, FLT3-ITD, NRAS p.G12D and IDH2 p.R140Q. In addition, we found two distinct clonal evolution patterns of relapse: (1) a leukemic clone at disease presentation acquires additional mutations and evolves into the relapse clone after the chemotherapy; (2) a leukemic clone at disease presentation persists at relapse without the addition of novel somatic mutations. Conclusions: The findings of this study suggest that the relapse-initiating clones may pre-exist prior to therapy, which harbor or acquire mutations that confer selective advantage during chemotherapy, resulting in clonal expansion and eventually leading to relapse. [ABSTRACT FROM AUTHOR]

Published

2021