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A new monoclonal antibody (CAL2) detects CALRETICULIN mutations in formalin-fixed and paraffin-embedded bone marrow biopsies

机译:一种新的单克隆抗体(CAL2)可检测福尔马林固定和石蜡包埋的骨髓活检组织中的CALRETICULIN突变

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摘要

Recent advances in the diagnostic of myeloproliferative neoplasms (MPNs) discovered CALRETICULIN (CALR) mutations as a major driver in these disorders. In contrast to JAK2 mutations being mainly associated with polycythaemia vera, CALR mutations are only associated with primary myelofibrosis (PMF) and essential thrombocythaemia (ET). CALR mutations are present in the majority of PMF and ET patients lacking JAK2 and MPL mutations. As these CALR mutations are absent from reactive bone marrow (BM) lesions their presence indicates ET or PMF. So far these mutations are detectable only by molecular assays. Their molecular detection is cumbersome because of the great CALR mutation heterogeneity. Therefore, the availability of a simple assay would be of great help. All CALR mutations reported lead to a frameshift generating a new 36 amino-acid C-terminus. We generated a monoclonal antibody (CAL2) to this C-neoterminus by immunizing mice with a representative peptide and compared its performance with Sanger sequencing data in 173 MPNs and other BM diseases. There was a 100% correlation between the molecular and the CAL2 immunohistochemical (IHC) assays. Thus, the detection of CALR mutations by the CAL2 IHC is a specific, sensitive, rapid, simple and low-cost method.
机译:骨髓增生性肿瘤(MPN)诊断的最新进展发现钙调蛋白(CALR)突变是这些疾病的主要驱动因素。与JAK2突变主要与真性红细胞增多症相关,CALR突变仅与原发性骨髓纤维化(PMF)和原发性血小板增多症(ET)相关。大多数缺少JAK2和MPL突变的PMF和ET患者中都存在CALR突变。由于反应性骨髓(BM)损伤中不存在这些CALR突变,因此它们的存在表明存在ET或PMF。到目前为止,这些突变只能通过分子测定法检测到。由于很大的CALR突变异质性,它们的分子检测很麻烦。因此,简单测定的可用性将有很大帮助。据报道,所有CALR突变都会导致移码,产生一个新的36个氨基酸的C末端。我们通过用代表性肽免疫小鼠来产生针对该C-新末端的单克隆抗体(CAL2),并将其性能与Sanger测序数据在173个MPN和其他BM疾病中的性能进行了比较。分子和CAL2免疫组织化学(IHC)分析之间存在100%的相关性。因此,通过CAL2 IHC检测CALR突变是一种特异性,灵敏,快速,简单且低成本的方法。

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