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KMID : 0981820090290030243
Korean Journal of Laboratory Medicine
2009 Volume.29 No. 3 p.243 ~ p.248
Usefulness of Real-time Semi-quantitative PCR, JAK2 MutaScreenTM Kit for JAK2 V617F Screening
Chae Hyo-Jin

Lee Je-Hoon
Lim Ji-Hyang
Jung Seung-Won
Kim Myung-Shin
Kim Yong-Goo
Han Kyung-Ja
Cho Byung-Sik
Cho Seok-Goo
Lee Jong-Wook
Min Woo-Sung
Abstract
Background: Real-time PCR for quantification of JAK2 V617F has recently been introduced and used to evaluate the importance of mutant allele burden in both diagnosis and disease progression in myeloproliferative diseases (MPDs). We evaluated the usefulness of JAK2 MutaScreenTM kit that uses a real-time semiquantitative PCR method and has been designed to screen JAK2 V617F mutant allele burden.

Methods: Forty MPD patients were included in this study. We screened JAK2 V617F and determined the mutant allele burden using JAK2 MutaScreenTM kit. The mutant allele burden was estimated by six-scaled standards of JAK2 V617F mutant allele (2%, 5%, 12.5%, 31%, 50%, and 78%). For evaluation of test performance, an allele-specific PCR (AS-PCR) was carried out in all samples by using Seeplex JAK2 Genotyping kit. We assessed the clinical differences in distinct disease entities of MPDs according to JAK2 V617F mutant allele burden.

Results: JAK2 V617F mutation was detected in 30 cases, including 10 of 11 cases (91%) of polycythemia vera (PV), 13 of 20 cases (65%) of essential thrombocythemia (ET), and 2 of 3 cases (67%) of chronic idiopathic myelofibrosis (CIMF). The concordance rate between the two tests was 95% (38/40). JAK2 V617F mutant allele burden was greater than 50% in 17 cases, and 10 of them (59%) were PV. In contrast, mutant allele burden was less than 50% in 13 cases and 11 of them (85%) were ET.

Conclusion: JAK2 MutaScreenTM kit that utilizes a real-time semi-quantitative PCR method is a useful tool for diagnosing MPDs precisely. It can be used to assess the grade of mutant allele burden as well as to screen JAK2 V617F simultaneously.
KEYWORD
JAK2 V617F, Myeloproliferative disease, Real-time PCR, Allele burden
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