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The KIT D816V allele burden predicts survival in patients with mastocytosis and correlates with the WHO type of the disease

机译:KIT D816V等位基因负荷预测肥大细胞增多症患者的生存并与WHO疾病类型相关

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摘要

KIT D816V is present in a majority of patients with systemic mastocytosis (SM). We determined the KIT D816V allele burden by quantitative real-time PCR in bone marrow and peripheral blood of 105 patients with mastocytosis. KIT D816V was detected in 92/105 patients (88%). Significant differences in the median allele burden were observed between disease subgroups: cutaneous mastocytosis (0.042%), indolent SM (0.285%), smoldering SM (5.991%), aggressive SM (9.346%), and SM with associated hematologic non-mast cell lineage disease (3.761%) (P < 0.001). The KIT D816V burden also correlated with serum tryptase (R = 0.5, P < 0.005) but not with mast cell infiltration in bone marrow or mediator symptoms. Moreover, the allele burden was of prognostic significance regarding survival (P < 0.01). Patients responding to cytoreductive therapy showed a significant decrease in KIT D816V (P < 0.05). To conclude, the KIT D816V burden correlates with the variant of mastocytosis, predicts survival, and is a valuable follow-up parameter in SM.
机译:KIT D816V存在于大多数系统性肥大细胞增多症(SM)患者中。我们通过定量实时PCR检测105例肥大细胞增多症患者的骨髓和外周血中的KIT D816V等位基因负担。在92/105位患者中检出了KIT D816V(88%)。在疾病亚组之间观察到中位等位基因负荷的显着差异:皮肤肥大细胞增多症(0.042%),惰性SM(0.285%),闷热SM(5.991%),侵袭性SM(9.346%)和伴有血液学非肥大细胞的SM宗谱疾病(3.761%)(P <0.001)。 KIT D816V负担也与血清类胰蛋白酶有关(R = 0.5,P <0.005),但与骨髓中肥大细胞浸润或介导的症状无关。此外,等位基因负荷对生存具有预后意义(P <0.01)。对细胞减少疗法有反应的患者显示KIT D816V显着降低(P <0.05)。总而言之,KIT D816V负担与肥大细胞增多症的变体相关,可以预测存活率,并且是SM中有价值的随访参数。

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