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Improved molecular classification of serrated lesions of the colon by immunohistochemical detection of BRAF V600E

机译:通过免疫组织化学检测BRAF V600E改善结肠锯齿状病变的分子分类

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BRAF V600E mutation in serrated lesions of the colon has been implicated as an important mutation and as a specific marker for the serrated carcinogenic pathway. Recent findings point to microvesicular hyperplastic polyps that have similar histologic and molecular features to sessile serrated adenomas/polyps, as potential colorectal carcinoma precursors. The aim of this study was to evaluate BRAF V600E mutation status by immunohistochemistry in serrated lesions of the colon with regard to histomorphology. We investigated 194 serrated lesions of the colon, comprising 42 sessile serrated adenomas/polyps, 16 traditional serrated adenomas, 136 hyperplastic polyps and 20 tubular/tubulovillous adenomas (conventional adenomas) with the novel BRAF V600E mutation-specific antibody VE1. In addition, BRAF exon 15 and KRAS exon 2 status was investigated by capillary sequencing in selected cases. All sessile serrated adenomas/polyps (42/42, 100%), 15/16 (94%) traditional serrated adenomas and 84/136 (62%) hyperplastic polyps were VE1+. None of the VE1? serrated lesions showed BRAF V600E mutation. Forty out of 42 (95%) sessile serrated adenomas/polyps displayed areas with microvesicular hyperplastic polyp-like features. In microvesicular hyperplastic polyps, VE1 positivity was significantly associated with nuclear atypia (P=0.003); however, nuclear atypia was also present in VE1? cases. Immunostaining with VE1 allows not only the detection of BRAF V600E mutation but also the correlation with histomorphology on a cellular level in serrated lesions. VE1 enables a subclassification of microvesicular hyperplastic polyps according to the mutation status. This improved classification of serrated lesions including immunohistochemical evaluation of BRAF V600E mutation may be the key to identify lesions with higher potential to progression into sessile serrated adenoma/polyp, and further to BRAF V600E-mutated colorectal cancer.
机译:结肠锯齿状病变中的BRAF V600E突变被认为是重要的突变,并且是锯齿状致癌途径的特异性标记。最近的发现指出,微囊增生性息肉具有与无柄锯齿状腺瘤/息肉相似的组织学和分子特征,可作为潜在的结直肠癌前体。这项研究的目的是通过免疫组织化学评估结肠锯齿状病变的BRAF V600E突变状态的组织形态。我们用新的BRAF V600E突变特异性抗体VE1研究了194个结肠锯齿状病变,包括42个无柄锯齿状腺瘤/息肉,16个传统锯齿状腺瘤,136个增生性息肉和20个管状/微管腺瘤(常规腺瘤)。此外,在某些病例中,通过毛细管测序研究了BRAF外显子15和KRAS外显子2的状态。所有无柄锯齿状腺瘤/息肉(42/42,100%),15/16(94%)传统锯齿状腺瘤和84/136(62%)增生性息肉均为VE1 +。没有VE1?锯齿状病变显示BRAF V600E突变。 42个无梗锯齿状腺瘤/息肉中有40个(95%)表现出具有微泡状增生性息肉样特征的区域。在微泡增生性息肉中,VE1阳性与核型异型显着相关(P = 0.003)。但是,VE1中是否也存在核型异型?案件。 VE1免疫染色不仅可以检测BRAF V600E突变,而且还可以在锯齿状病变的细胞水平上与组织形态学相关。 VE1能够根据突变状态对微泡增生性息肉进行分类。锯齿状病变的改进分类包括对BRAF V600E突变的免疫组织化学评估,可能是鉴定具有发展为无柄锯齿状腺瘤/息肉以及进一步发展为BRAF V600E突变大肠癌的潜力的关键。

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