CALR, JAK2 and MPL Genes Mutations in Myeloproliferative Neoplasms, Single Center Experience

INTRODUCTION: Genetic tests are very important for the diagnosis of Philedelphia negative myeloproliferative neoplasms (MPN), in addition to clinical findings and laboratory results. JAK2 V617F mutation is the most common genomic variaton among these group of diseases. Otherwise, analysis of W515L/K mutation in MPL gene and CALR gene mutations is crucial. In this study, prevalence of JAK2 V617F, MPL W515L/K mutations and, spectrum and prevalence of CALR gene mutations were investigated in MPN patients.
METHODS: Genetic test results of JAK2 V617 mutation, MPL W515L/K mutation and CALR gene mutations of 41 MPN patients were analysed, retrospectively. Genetic parameters were performed with real-time PCR.
RESULTS: While the frequency of JAK2 V617F mutation was 36% and CALR mutation was 17% in all patients, MPL W515L/K mutation was not detected in any patient. In terms of subgroups of MPN; in polycythemia vera, essential thrombocytosis and primary myelofibrosis groups, the incidence of JAK2 V617F mutation was 67%, 33% and 25%, respectively; and the incidence of CALR mutation was 8%, 29% and 8%, respectively. MPL W515L/K was absent in all groups.
DISCUSSION AND CONCLUSION: Previous studies have reported that the frequency of JAK2 V617F, MPL W515L/K and CALR mutations in Ph (-) MPN group diseases is very variable. As conclusion, it is thought that environmental factors such as smoking and altitude have an effect besides epigenetic factors such as ethnicity in distribution of mutations.

Myeloproliferatif Neoplazilerde CALR, JAK2 ve MPL Gen Mutasyonlarýnýn Sýklýðýnýn ve Birlikteliðinin Deðerlendirilmesi; Tek Merkez Deneyimi

GÝRÝÞ ve AMAÇ: Philedelphia negatif Ph(-) myeloproliferatif neoplazilerin (MPN) tanýsýnda klinik ve laboratuvar bulgularýnýn yanýnda genetik testler çok önemlidir. Bunlar arasýnda JAK2 genindeki V617F mutasyonu en sýk görülen genomik varyasyondur. Bunlara ek olarak MPL geninde W515L/K mutasyonunun ve CALR genindeki mutasyonlarýn araþtýrýlmasý da önem taþýmaktadýr. Çalýþmamýzda, MPN tanýsý almýþ olan hastalarda retrospektif olarak JAK2 V617F, MPL W515L/K ve CALR mutasyon daðýlýmý ve sýklýðý araþtýrýldý.
YÖNTEM ve GEREÇLER: MPN grubu hastalýk tanýsý ile baþvuran 41 hastanýn JAK2 V617 mutasyonu, MPL W515L/K mutasyonu ve CALR gen mutasyonlarýna yönelik test sonuçlarý retrospektif olarak incelendi. Genetik parametreler real-time PCR cihazý ile analiz edildi.
BULGULAR: Tüm hastalarda JAK2 V617F mutasyon sýklýðý %36, CALR mutasyon sýklýðý %17 olarak bulunurken, MPL W515L/K mutasyonu hiçbir hastada gözlenmedi. MPN’nin alt gruplarýný oluþturan; polisitemi vera, esansiyel trombositoz ve primer myelofibrozis gruplarýnda JAK2 V617F mutasyon sýklýðý sýrasýyla %67, %33 ve %25 olarak bulunurken; CALR mutasyon sýklýðý ise %8, %29 ve %8 olarak bulundu. MPL W515L/K ise hiçbir grupta gözlenmedi.
TARTIÞMA ve SONUÇ: Daha önce yapýlan çalýþmalarda Ph(-) MPN grubu hastalýklarda JAK2 V617F, MPL W515L/K ve CALR mutasyon sýklýðýnýn çok geniþ aralýklarda olduðu bildirilmiþtir. Sonuç olarak, mutasyonlarýn daðýlýmýnda etnisite ve epigenetik faktörlerin yaný sýra sigara, rakým gibi çevresel faktörlerin de etkisinin olduðunu düþünülmektedir.