Incidence of T315I mutation in BCR/ABL-positive CML and ALL patients

Objectives Targeted therapy of Philadelphia-positive ALL and CML patients using imatinib (IM) has caused significant changes in treatment course and has increased the survival of patients. A small group of patients show resistance to IM. Acquired mutations in tyrosine kinase domain of BCR-ABL protei...

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Published in	Frontiers in biology Vol. 11; no. 5; pp. 404 - 411
Main Authors	Norozi, Fatemeh, Mohammadi-asl, Javad, Vosoughi, Tina, Far, Mohammad Ali Jalali, Malehi, Amal Saki, Saki, Najmaldin
Format	Journal Article
Language	English
Published	Beijing Higher Education Press 01.10.2016 Springer Nature B.V
Subjects	adenosine triphosphate binding sites Biochemistry Biomedical and Life Sciences blood composition Cell Biology complementary DNA Developmental Biology disease diagnosis Genetics and Population Dynamics hydrogen bonding Life Sciences Mutation neoplasm cells neoplasms Neurobiology patients Polymorphism Proteomics Research Article therapeutics tyrosine ALL imatinib T315I mutation CML BCR-ABL
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ISSN	1674-7984 1674-7992
DOI	10.1007/s11515-016-1423-1

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Abstract	Objectives Targeted therapy of Philadelphia-positive ALL and CML patients using imatinib (IM) has caused significant changes in treatment course and has increased the survival of patients. A small group of patients show resistance to IM. Acquired mutations in tyrosine kinase domain of BCR-ABL protein are a mechanism for development of resistance. T315I is one of the most common acquired mutations in this domain, which occurs in ATP binding site and inhibits the formation of hydrogen bond with IM. The aim of this study was to evaluate the prevalence of this mutation in BCR/ABL-positive CML and ALL patients. Methods To conduct this study, 60 BCR-ABL-positive patients (including 50 CML and 10 ALL patients) who were subject to treatment with IM were selected. After taking the samples, presence of T315I mutation was assessed using ARMS-PCR on cDNA and its polymorphism was evaluated by sequencing. Results The results showed that among 60 patients, only three patients had T315I mutation, which was detected using ARMS technique. The three patients bearing mutation were afflicted with CML and no significant association was found between blood parameters with duration of treatment in presence of mutation. Conclusions The mutation was found in three CML patients, which indicated lower likelihood and diagnostic value of this mutation in ALL patients. Given the negative direct sequencing results in T315I patients, it can be concluded that ARMS-PCR is a more sensitive technique when the number of cancer cells is low in patients during treatment.
AbstractList	Objectives Targeted therapy of Philadelphia-positive ALL and CML patients using imatinib (IM) has caused significant changes in treatment course and has increased the survival of patients. A small group of patients show resistance to IM. Acquired mutations in tyrosine kinase domain of BCR-ABL protein are a mechanism for development of resistance. T315I is one of the most common acquired mutations in this domain, which occurs in ATP binding site and inhibits the formation of hydrogen bond with IM. The aim of this study was to evaluate the prevalence of this mutation in BCR/ABL-positive CML and ALL patients. Methods To conduct this study, 60 BCR-ABL-positive patients (including 50 CML and 10 ALL patients) who were subject to treatment with IM were selected. After taking the samples, presence of T315I mutation was assessed using ARMS-PCR on cDNA and its polymorphism was evaluated by sequencing. Results The results showed that among 60 patients, only three patients had T315I mutation, which was detected using ARMS technique. The three patients bearing mutation were afflicted with CML and no significant association was found between blood parameters with duration of treatment in presence of mutation. Conclusions The mutation was found in three CML patients, which indicated lower likelihood and diagnostic value of this mutation in ALL patients. Given the negative direct sequencing results in T315I patients, it can be concluded that ARMS-PCR is a more sensitive technique when the number of cancer cells is low in patients during treatment. Objectives: Targeted therapy of Philadelphia-positive ALL and CML patients using imatinib (IM) has caused significant changes in treatment course and has increased the survival of patients. A small group of patients show resistance to IM. Acquired mutations in tyrosine kinase domain of BCR-ABL protein are a mechanism for development of resistance. T315I is one of the most common acquired mutations in this domain, which occurs in ATP binding site and inhibits the formation of hydrogen bond with IM. The aim of this study was to evaluate the prevalence of this mutation in BCR/ABL-positive CML and ALL patients. Methods: To conduct this study, 60 BCR-ABL-positive patients (including 50 CML and 10 ALL patients) who were subject to treatment with IM were selected. After taking the samples, presence of T315I mutation was assessed using ARMS-PCR on cDNA and its polymorphism was evaluated by sequencing. Results: The results showed that among 60 patients, only three patients had T315I mutation, which was detected using ARMS technique. The three patients bearing mutation were afflicted with CML and no significant association was found between blood parameters with duration of treatment in presence of mutation. Conclusions: The mutation was found in three CML patients, which indicated lower likelihood and diagnostic value of this mutation in ALL patients. Given the negative direct sequencing results in T315I patients, it can be concluded that ARMS-PCR is a more sensitive technique when the number of cancer cells is low in patients during treatment.
Author	Mohammadi-asl, Javad Saki, Najmaldin Norozi, Fatemeh Far, Mohammad Ali Jalali Vosoughi, Tina Malehi, Amal Saki
Author_xml	– sequence: 1 givenname: Fatemeh surname: Norozi fullname: Norozi, Fatemeh organization: Health Research Institute, Thalassemia and Hemoglobinopathy Research Center, Ahvaz Jundishapur University of Medical Sciences – sequence: 2 givenname: Javad surname: Mohammadi-asl fullname: Mohammadi-asl, Javad organization: Department of Medical Genetics, Ahvaz Jundishapur University of Medical Sciences – sequence: 3 givenname: Tina surname: Vosoughi fullname: Vosoughi, Tina organization: Health Research Institute, Thalassemia and Hemoglobinopathy Research Center, Ahvaz Jundishapur University of Medical Sciences – sequence: 4 givenname: Mohammad Ali Jalali surname: Far fullname: Far, Mohammad Ali Jalali organization: Health Research Institute, Thalassemia and Hemoglobinopathy Research Center, Ahvaz Jundishapur University of Medical Sciences – sequence: 5 givenname: Amal Saki surname: Malehi fullname: Malehi, Amal Saki organization: Health Research Institute, Thalassemia and Hemoglobinopathy Research Center, Ahvaz Jundishapur University of Medical Sciences – sequence: 6 givenname: Najmaldin surname: Saki fullname: Saki, Najmaldin email: najmaldinsaki@gmail.com organization: Health Research Institute, Thalassemia and Hemoglobinopathy Research Center, Ahvaz Jundishapur University of Medical Sciences
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Snippet	Objectives Targeted therapy of Philadelphia-positive ALL and CML patients using imatinib (IM) has caused significant changes in treatment course and has... Objectives Targeted therapy of Philadelphia-positive ALL and CML patients using imatinib (IM) has caused significant changes in treatment course and has... Objectives: Targeted therapy of Philadelphia-positive ALL and CML patients using imatinib (IM) has caused significant changes in treatment course and has... OBJECTIVES: Targeted therapy of Philadelphia-positive ALL and CML patients using imatinib (IM) has caused significant changes in treatment course and has...
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SubjectTerms	adenosine triphosphate binding sites Biochemistry Biomedical and Life Sciences blood composition Cell Biology complementary DNA Developmental Biology disease diagnosis Genetics and Population Dynamics hydrogen bonding Life Sciences Mutation neoplasm cells neoplasms Neurobiology patients Polymorphism Proteomics Research Article therapeutics tyrosine
Title	Incidence of T315I mutation in BCR/ABL-positive CML and ALL patients
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