This result was in agreement with the previous study which showed an association between 46/1 haplotype and the risk of developing BCS with JAK2V617F mutation. Additionally, the current data demonstrated that no difference was found between patients with different rs12343867 genotypes, which implied
JAK2 46/1 haplotype seem not to be associated with distinct clinical and laboratory characteristics of BCS in China. Combined with the above two hypotheses, a possible explanation for the higher incidence of rs12343867 CC genotype in patients with JAK2V617F mutation is that the presence of CC genotype is GDC-0973 research buy not sufficient in itself for the disease but appears to be in linkage with JAK2V617F or other unidentified variations. Clearly, this explanation deserves further studies. Interestingly, the JAK2 46/1 haplotype was a risk factor for MPNs in China,[32, 33]
which were in line with previous reports conducted in Western countries.[17, 18, 21] According to researches, MPNs were only accounted for 4.1–5.0% in Chinese BCS patients.[34, 35] Taken with low prevalence of JAK2V617F CYC202 chemical structure mutation together, MPNs seemed not to be the etiological factor for Chinese BCS patients. Reviewed the researches about BCS in western countries, underlying inherited or acquired thrombotic risk factors were reported including MPNs, protein C deficiency, protein S deficiency, antithrombinIII deficiency, FVL mutation, prothrombin G20210A mutation, JAK2 exon12 mutation, MPLW515L/K mutation, paroxysmal nocturnal hemoglobinuria (PNH), antiphospholipid syndrome (APS), Behcet’s disease.[36-39]
medchemexpress However, in China, literatures indicated that FVL mutation, prothrombin G20210A mutation, and PNH were rarely found in BCS patients.[34, 39-41] Our research also showed a low prevalence of JAK2 exon12 mutation, while the other gene mutation showed negative. In addition, oral contraceptive use has been shown to increase the risk of BCS with odds ratios about 2.5 as compared to nonusers,[40] which was not demonstrated in our population. Combined with the results of our study, we could infer that the etiological distribution of BCS is geographically and ethnically different. A case-control study conducted in Nepal showed that IVC obstruction was associated with a very poor standard of living.[42] Our survey also displayed that majority of BCS patients presented with IVC obstruction (157/282, data not shown) and were engaged in manual work with family financial difficulties. In conclusion, our study suggested that the presence of 46/1 haplotype increased the risk of occurrence of JAK2V617F-positive BCS in China. In addition, BCS patients had a very low prevalence of the JAK2V617F mutation, which revealed that MPNs might not be the etiological factor of Chinese patients.