In order to perform the jak2 mutation test, blood sample is required, which is drawn using a syringe inserted into a superficial vein of the arm. Jak2 v617f mutation analysis 4617 diagnostic labs versiti. This mutation v617f, a change of valine to phenylalanine at the. Of the 14 v617f mutationnegative patients with pv, were male p. Detection of jak2 exon 12 mutations in 15 patients with jak2v617f. The molecular pathogenesis of most mpds is unknown. Although detection of jak2 v617f and mpl mutations in the appropriate. Rapid identification of heterozygous or homozygous jak2.
The ipsogen jak2 rgq pcr kit uses taqman polymerase chain reaction pcr probes and arms amplification refractory mutation system technology on the rotorgene q mdx us instrument for sensitive and specific jak2 v617f mutation analysis. Jak2 mutation v617f analysis regional medical lab test. Arms method the allelespecific pcr testing for the jak2 v617f mutation was performed as described previously. Genetic testing of the calr gene only found in et and pmf is medically necessary when the following criteria are met. The gain of function mutation v617f is found in majority of our pv patients, which supports the previous suggestions. Labcorp test details for jak2v617f mutation analysis, quantitative. Jak2 v617f mutational analysis by quantitative droplet digital pcr indication. This mutation was seen in pv by 65% to 97% and et 3057% and primary myelofibrosis 3595%. Jak2 v617f mutation detection, varies essentia health.
To create an inducible flipflop transgene, this construct was modified by inserting a lox66 site into intron 12 and a lox71 site after the polyadenylation signal and the segment between the loxp sites was. The abi7900 absolute quantitation software will compare the patient specimen values to the standard curves and generate percent values for wild type and mutant type. Jak2v617f in their granulocytes also expressed jak2v617f in their platelets. The v617f mutation in jak2 is a dominant gainof function mutation that contributes to the expansion of the myeloproliferative disorder clone. Jak2 gene fusions with the teletv6 and pcm1 genes have been found in patients suffering leukemia, particularly clonal eosinophilia forms of the disease. A gainoffunction mutation of jak2 in myeloproliferative disorders. Test details jak2 v617f quantitative mutation analysis. Jak2 v617f mutation analysis test detail quest diagnostics. Widespread occurrence of the jak2 v617f mutation in. Data for v617f only n 376 and for v617fr1063h doublemutation carriers n 14 were recorded at. Two amplification products per sample were monitored by realtime pcr using primersprobes specific to jak2 wild type wt and jak2 mutant v617f. Occurrence of the jak2 v617f mutation in patients with. Detection of exon 12 and 14 mutations in janus kinase 2.
Jak2 and mpl mutation analysis in myeloproliferative neoplasms. Apr 18, 2006 further jak2 v617f mutation analysis of individual hscderived colonies from two separate patients revealed differences in individual patient sensitivity to jak2 inhibition at the stem cell level, indicating that in some patients, hsc clones harboring the jak2 v617f mutation are less sensitive to inhibition with ag490 fig. About 90% of the patients with pv harbor jak2 v617f mutation, whereas approximately to 5060% of patients with et or pmf harbor jak2 v617f mutation 2,3,57. Jak2 mutations are acquired as opposed to inherited and result in the change of a single dna nucleotide base pair, called a point mutation. It is also infrequently present 3% to 5% in myelodysplastic syndrome, chronic myelomonocytic leukemia, and other atypical chronic myeloid disorders. Other testing, such as a bone marrow biopsy, may need to be performed to determine which mpn the person has and to evaluate its severity.
The mean age at diagnosis for the jak2 v617f mutation group was 60. Of the 83 patients who showed platelet expression of jak2v617f, 12 did not express the mutation in their granulocytes. The jak2 mutation test is typically ordered as a followup test if a person has a. Jak2 v617f mutation frequency in pad patients was significantly increased compared with healthy subjects from the kora f4 study or 5. Jan 20, 2014 the somatic gainoffunction mutation jak2v617f has been described in the vast.
Other important molecular markers in bcrabl1 negative mpn include calr exon 9 variant 20%30% of pmf and et and mpl exon 10 variant 5%10% of pmf and 3%5% of et. Dec 20, 2018 clinical characteristics, jak2 analysis, and nextgeneration sequencing ngs screening for mpn patients exhibiting jak2 v617f and jak2 r1063h mutations. The somatic gainoffunction mutation jak2v617f has been described in the vast. Jak2 v617f mutation analysis this dnabased assay tests leukocytes from blood or bone marrow aspirate for mutation at codon 617 of jak2, using an advanced dna sequencing method. The jak2 v617f mutation is associated with myeloproliferative neoplasms, including polycythemia vera, essential thrombocythemia and primary myelofibrosis. Widespread occurrence of the jak2 v617f mutation in chronic. Jak2v617f mutation analysis of granulocytes and platelets. Development of a high resolution melting analysis assay.
The v617f jak2 gene mutation results in the production of a jak2 protein that is constantly turned on constitutively activated, which, in essential thrombocythemia, leads to the overproduction of abnormal blood cells called megakaryocytes. A positive jak2 v617f mutation test, along with other supporting clinical signs, means it is likely that the person tested has an mpn. The jak2v617f exon 14 mutation analysis can be used in conjunction with bone marrow histology and cytogenetic analysis to assist in the diagnosis of myeloproliferative neoplasms mpn. Labcorp and its specialty testing group, a fully integrated portfolio of specialty and esoteric testing laboratories. Jak2 v617 mutation analysis qualitative neogenomics. For qualitative detection of the jak2 v617fg1849t mutation using realtime pcr. If the jak2 v617f mutation is detected and the person has other supporting clinical signs, then it is likely that the person has an mpn. Rapid identification of heterozygous or homozygous jak2 v617f. In the present study, we retrieved the results of all jak2v617f mutation analyses performed in the period 2006 2012. Clinical implications of quantitative jak2 v617f analysis.
Readytouse solutions and a qiagen pcr master mix are included in the kit for rapid qualitative analysis of the jak2 v617f g1849t mutation for up to 24 samples per run. All what does it mean when you test positive for jak 2. The jak2v617f mutation exon 14 is a valuable marker in bcrabl negative. Negative for jak2 v617f mutationpositive for jak2 v617f mutation. More than 95% of people with polycythemia vera pv and 5060% of people. Looking for calr mutations in familial myeloproliferative. Oct 27, 2014 frequency of the jak2 v617f mutation of included participants of the kora f4 study was 0. Confirms the diagnosis of myeloproliferative disorders polycythaemia vera, essential thombocythaemia, and primary myelofibrosis.
Zehnder from the molecular pathology laboratory, and departments of pathology and medicine hematology, stanford university school of medicine, stanford hospital and clinics and lucile. The jak2 v617f activating tyrosine kinase mutation is an infrequent event in both atypical myeloproliferative disorders and the myelodysplastic. In jak2, this kind of mutation, called a point mutation, replaces the normal amino acid valine abbreviated v with. Jak2 v617f mutation analysis, quantitative labcorp. This test looks for mutations in jak2 that are associated with bone marrow disorders caused by the production of too many blood cells. The absence of jak2v617f mutation in granulocytes was con. Somatic jak2 gene mutations are also associated with several related conditions. At diagnosis, mean hemoglobin levels were almost identical in the 2 groups, 19. For whole blood samples in which the jak2 v617f allele is detected and within the analytical measurement range amr, a quantitative value for the mutant allele burden will be reported. The jak2 mutation also called the v617f jak2 is found in about. Jak2 exon 12, 14, and 15, mpl and calr exon mutation testing is considered not medically necessary in all other circumstances including, but not limited to, the following situations.
Presently, the detection of jak2 v617f mutation is included into the who classification of myeloid neoplasms and acute leukemia 4. Jak2 v617f mutational analysis by quantitative droplet. However, a negative jak2 v617f result does not indicate absence of a mpn. Laboratory practice guidelines for detecting and reporting jak2. Jak2 v617f is named for a mutation at a specific location in the jak2 gene and is the primary genetic test for jak2 mutations that lead to mpns. The activating jak2 mutation with a gc to ta transversion at codon 617 jak2 v617f is associated with myeloproliferative neoplasms mpns, including polycythemia vera pv, essential thrombocythemia et, and myelofibrosis. Comparison of clinical characteristics between cases with and without jak2 v617f mutation was done by using mannwhitney u test wilcoxon rank sum test for wbc, platelet count, splenomegaly, and disease duration. Jak2 mutation analysis test, symptoms, treatment alexandria. Cooccurring jak2 v617f and r1063h mutations increase jak2. For the study, 43 samples 27 bone marrow aspirates. Detection of exon 12 and 14 mutations in janus kinase 2 gene. Lightcycler data were analyzed using the lightcycler 4. Testing is performed on plasma for increased sensitivity whenever possible.
Clinical characteristics, jak2 analysis, and nextgeneration sequencing ngs screening for mpn patients exhibiting jak2 v617f and jak2 r1063h mutations. The v617f mutation is occasionally found in people with cancer of bloodforming cells leukemia or other bone marrow disorders. The results were compared with clinical data from electronic. The jak2 v617f mutation results in the loss of a restriction site and will appear as a bluegreen peak at 267 bp. The finding of a single mutation in the jh2 autoinhibitory domain of the jak2 kinase v617f in a wide variety of myeloproliferative diseases mpd has revolutionized their definition. A jak2 mutational analysis is usually recommended when a physician suspects a myeloproliferative disorder. Mutations in jak2 have been implicated in polycythemia vera, essential thrombocythemia, and myelofibrosis as well as other myeloproliferative disorders. The primary jak2 mutation analysis determines a point mutation, called jak2 v617f. Jak2 v617f mutation is acquired as opposed to inherited and results in the change of a single dna nucleotide base pair. A point mutation in the jak2 gene, a member of the tyrosine kinase family, was recently identified and shown to be associated with several myeloproliferative disorders. Testing is performed on plasma for increased sensitivity whenever. Analysis of jak2v617f mutation in jordanian patients with. Here, we report a technical advance in the diagnosis of jak2 v617f in mpns by melting curve analysis mca. Performing a dilution series indicates the level of sensitivity of armspcr to be 12 %.
Oct 29, 2017 the primary jak2 test is jak2 v617f, named for a mutation at a specific location in the jak2 gene. Analysis of jak2v617f mutation in jordanian patients with myeloproliferative. About 34% of people with pv have an exon 12 mutation. Clinical utility of direct quantitative test for the v617f jak2 allele burden. The human bac, ctd2025a15, containing jak2 exons 112 was combined with a partial cdna encoding jak2 exons 25 containing the v617f mutation and a polyadenylation signal. The result is too many blood cells which clog the blood and make it sticky. This v617f mutation leads to constituitive tyrosine phosphorylation activity that promotes cytokine activity and induces erythrocytosis. Clinicalandhematologicalrelevanceof jak2 v617fand calr. The primary jak2 test is jak2 v617f, named for a mutation at a specific location in the jak2 gene. The v617f mutation, which causes the substitution of phenylalanine for valine at position 617 of the janus kinase jak 2 gene jak2, is often present in patients with polycythemia vera.
The quantitative realtime pcr assay detects v617f mutation c. Nine of ten individuals with polycythemia vera have jak2 mutation. A hematological data for jak2 v617f mpn patients n 390 subdivided according to the jak2 r1063h mutation status. Sep 15, 2005 of the 14 v617f mutationnegative patients with pv, were male p. Further jak2 v617f mutation analysis of individual hscderived colonies from two separate patients revealed differences in individual patient sensitivity to jak2 inhibition at the stem cell level, indicating that in some patients, hsc clones harboring the jak2 v617f mutation are less sensitive to inhibition with ag490 fig. Detection of jak2 v617f mutation increases the diagnosis of. V617f analysis is recommended before or concurrently with this test. Other testing, such as a bone marrow biopsy, may need to be performed to determine which mpn the person has and to evaluate its severity if the jak2 v617f test is negative but a jak2 exon 12 mutation is detected and the person has supporting clinical signs.
Positive mutation status is highly suggestive of a myeloid neoplasm, but must be correlated with clinical and other laboratory features for a definitive diagnosis. The abi7900 absolute quantitation software will compare the patient. Characterization of the double l611v v617f mutation of jak2. Jak2 and mpl mutation analysis in myeloproliferative. A negative jak2 v617f test but a positive jak2 exon 12 mutation or other non v617f mutation test along with supporting clinical signs means it is likely that the person has polycythemia vera.
Clinical performance of jak2 v617f mutation detection assays. Mutation analysis of jak2 exon 12 in v617fnegative cases did not reveal any additional sequence variants. An activating point mutation in codon 617 of jak2 v617f has been identified in three different chronic myeloproliferative disordersneoplasms, including polycythemia vera pv, essential thrombocythemia et and primary myelofibrosis pmf. The aim of this study was to evaluate performance of 3 screening and 1 quantitative method for jak2 v617f detection. Buddchiari syndrome, which results from a blocked vein in the liver, can also be associated with the v617f mutation when it is caused by an underlying bone marrow disorder. Jak2 v617f mutational status is an essential diagnostic index in myeloproliferative neoplasms mpns. Exon 1214 mutation analysis may be ordered separately, with concurrent v617f testing, by reflex after negative v617f testing, or as part of the mpn reflex panel.
Jak2 v617f mutation detection, blood sparrow laboratories. Finally, the rotorgene assaymanager software simplifies data analysis and management, and maximizes process safety for efficient and timely result reporting. However, among patients negative for this hallmark mutation, sequence analysis of jak2 exon 12 and 14 has revealed few underlying point mutations. Janus kinase 2 commonly called jak2 is a nonreceptor tyrosine kinase. Jul 09, 2019 the primary jak2 mutation analysis determines a point mutation, called jak2 v617f. The v617f mutation is in the pseudokinase jh2 domain of jak2, which is a negative regulatory region, and may interfere with inactivation of the kinase. Transformed essential thrombocytosis with a jak2 v617f. Since 2006, the laboratory for clinical biochemistry at haukeland university hospital has been performing analyses for the jak2v617f mutation in real time polymerase chain reactions pcr. Recently, emerging alternative technologies, like digital droplet pcr ddpcr, have been reported to overcome some of qpcr. The jak2 v617f mutation occurs in hematopoietic stem cells in.
This practice is a good tool for diagnosis of pv on genetic basis. Only half of the individuals diagnosed with essential thrombocythemia andor primary myelofibrosis are positive for jak2 mutation. Identification of a jak2 v617f mutation establishes the presence of a clonal disorder 14 and is an important diagnostic marker for these disorders. Characterization of the double l611vv617f mutation of jak2.
We developed a simple and sensitive method to detect this mutation via. Molecular test to detect mutations in myeloproliferative neoplasm mpn disorders. Definition of subtypes of essential thrombocythaemia and relation to polycythaemia vera based on jak2 v617f mutation status. Jak2 v617f mutation autoinhibitory domain activates the kinase. Abi prism 310 genetic analyzer, and sequencing analysis software applied biosystems. The jak2 v617f mutation occurs in hematopoietic stem cells. Jak2 mutation v617f detection by real time pcr clinical indication and relevance. Detection of the jak2 v617f variant is useful to help establish the diagnosis of mpn. Clinical performance of jak2 v617f mutation detection.
It is a member of the janus kinase family and has been implicated in signaling by members of the type ii cytokine receptor family e. Although widely used for detection of jak2 v617f mutation in peripheral blood pb, sensitive realtime quantitative pcr qpcr presents some methodological limitations. Gtr test id help each test is a specific, orderable test from a particular laboratory, and is assigned a unique gtr accession number. Pdf detection of v617f mutation of gene jak2 at patients. Detection of the jak2 v617f mutation by lightcycler pcr and. Negative for jak2 v617f mutation positive for jak2 v617f mutation. High percentage of jak2 exon 12 mutation in asian patients. Jak2 v617f mutation in healthy individuals a somatic gainoffunction mutation of the janus kinase 2 gene jak2 is present in most patients with polycythaemia vera, and in about half of those with essential thrombocythaemia and chronic idiopathic myelo. These disorders may include polycythemia vera pv, essential.
Detection of the jak2 v617f mutation by lightcycler pcr. Frequency of the jak2 v617f mutation of included participants of the kora f4 study was 0. Because platelets are formed from megakaryocytes, the overproduction of megakaryocytes results in an. Quantitative analysis of the jak2 v617f mutation using ddpcr was highly correlated with pyrosequencing data and may reflect the clinical response to treatment. Researchers believe that in mpd patients, the mutation in jak2 enhances messages asking for more cell production.