Detection of BCR-ABL gene mutations in chronic myeloid leukemia using biochips


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A biochip-based method was developed to identify the BCR-ABL mutations that affect the thyrosine kinase domain and determine resistance to targeted therapy with thyrosine kinase inhibitors. The method is based on RT–PCR followed by allele-specific hybridization on a biochip with immobilized oligonucleotide probes. The biochip addresses 11 mutations, which are responsible for up to 85% of imatinib resistance cases. A method to decect the clinically significant mutation T315I was designed on the basis of LNA-clamped PCR and proved highly sensitive, detecting the mutation in clinical samples with a leukemic cell content of 5% or higher. The method was validated using clinical samples from chronic myeloid leukemia (CML) patients with acquired resistance to imatinib. The results of hybridization on biochip were verified by Sanger sequencing.

作者简介

A. Ikonnikova

Engelhardt Institute of Molecular Biology

Email: nased@biochip.ru
俄罗斯联邦, Moscow, 119991

Yu. Yatsenko

Engelhardt Institute of Molecular Biology

Email: nased@biochip.ru
俄罗斯联邦, Moscow, 119991

O. Kremenetskaya

Center for Theoretical Problems of Physicochemical Pharmacology

Email: nased@biochip.ru
俄罗斯联邦, Moscow, 119991

O. Vinogradova

Rogachev Federal Research Clinical Center of Pediatric Hematology, Oncology and Immunology

Email: nased@biochip.ru
俄罗斯联邦, Moscow, 117997

D. Fesenko

Engelhardt Institute of Molecular Biology

Email: nased@biochip.ru
俄罗斯联邦, Moscow, 119991

I. Abramov

Engelhardt Institute of Molecular Biology

Email: nased@biochip.ru
俄罗斯联邦, Moscow, 119991

V. Ovsepyan

Kirov Research Institute of Hematology and Blood Transfusion

Email: nased@biochip.ru
俄罗斯联邦, Kirov, 610027

T. Nasedkina

Engelhardt Institute of Molecular Biology

编辑信件的主要联系方式.
Email: nased@biochip.ru
俄罗斯联邦, Moscow, 119991

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