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Literature DB >> 19343480

Serial monitoring of T315I BCR-ABL mutation by Invader assay combined with RT-PCR.

Masahide Yamamoto¹, Kazuhiko Kakihana¹, Kazuteru Ohashi², Toshikazu Yamaguchi³, Kenichi Tadokoro³, Hideki Akiyama¹, Hisashi Sakamaki¹.

Abstract

We recently developed an Invader assay combined with reverse transcriptase polymerase-chain-reaction in order to quantify T315I bcr-abl transcripts. Using this assay, we serially monitored T315I bcr-abl transcripts in chronic myeloid leukemia (CML) patients whose bcr-abl transcripts were still detectable at 6 months after starting imatinib therapy. Although, we continued to monitor bcr-abl transcripts in 14 CML patients (13 chronic phases and 1 accelerated phase) for up to 12 months, there were no patients who were apparently resistant to imatinib due to the T315I mutation. In contrast, in a case of Philadelphia chromosome-positive acute lymphoid leukemia being treated with chemotherapy including imatinib, we monitored both wild-type and T315I bcr-abl transcripts, and found increased levels of T315I transcripts during relapse (0% at the time of diagnosis and 54.8% at relapse). Thus, our new approach could be a useful tool to study the kinetics of mutant clones and the pharmacokinetics of drug resistance with regard to the T315I mutation.

Entities: Chemical Disease Gene Mutation Species

Mesh：

Substances：
Fusion Proteins, bcr-abl

Year: 2009 PMID： 19343480 DOI： 10.1007/s12185-009-0290-9

Source DB: PubMed Journal: Int J Hematol ISSN： 0925-5710 Impact factor: 2.490

23 in total

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Authors: A Hochhaus; P La Rosée
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Authors: Matthew A Young; Neil P Shah; Luke H Chao; Markus Seeliger; Zdravko V Milanov; William H Biggs; Daniel K Treiber; Hitesh K Patel; Patrick P Zarrinkar; David J Lockhart; Charles L Sawyers; John Kuriyan
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4. Successful prior treatment with dasatinib followed by stem cell transplantation in a patient with CML in blastic crisis with a BCR-ABL mutation.

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6. Analysis of mitochondrial function in human induced pluripotent stem cells from patients with mitochondrial diabetes due to the A3243G mutation.

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6 in total