Department of Surgical and Molecular Pathology, Dokkyo Medical University School of Medicine, 880 Kitakobayashi, Mibu, Shimotsuga, Tochigi 321-0293, Japan; Department of Coloproctology, Social Health Insurance Hospital, 22-1 Hyakunincho, Shinjuku, Tokyo 169-0073, Japan; Department of Organ Regulatory Surgery, Fukushima Medical University School of Medicine, 1 Hikarigaoka, Fukushima 960-1295, Japan.
Hum Pathol. 2013 Nov;44(11):2393-9. doi: 10.1016/j.humpath.2013.06.008. Epub 2013 Sep 10.
Pancellular dysplasia involving neuroendocrine cells has been shown to be comparatively rare but crucially implicated in the development of neuroendocrine tumors in ulcerative colitis (UC). We attempted to clarify the prevalence of chromogranin A expression as a marker of neuroendocrine differentiation in UC-associated neoplasia by immunohistochemical analyses of 26 lesions of low-grade dysplasia (LGD), 32 high-grade dysplasias (HGDs) and 27 invasive cancers (INVs), along with p53 expression. We additionally assessed the utility of these proteins for differential diagnosis between LGD and HGD. Chromogranin A was considered positive when immunoreactive cells were more than 5% of neoplastic lesions, and the positivity tended to be higher in HGDs (57.7%) or INVs (46.7%) than LGDs (32.0%). Focal or diffuse nuclear staining for p53 was defined as positive. The positive rate for p53 was also higher in HGDs (59.4%; P = 0.037) or INVs (59.3%) than LGDs (30.8%). A similar trend was found in co-positivity for both proteins (HGDs, 30.7%/INVs, 26.7% versus LGDs, 12.0%). No positivity for both proteins was identified in the non-neoplastic mucosa. The combination of the two proteins improved the sensitivity (66.7%), specificity (80.0%), positive predictive value (72.7%) and negative predictive value (75.0%) for HGD as compared to p53 alone (sensitivity, 57.7%; specificity 68.0%; positive predictive value, 65.2%; negative predictive value, 60.7%). In conclusion, we show here that neuroendocrine differentiation is relatively common and represents an early event in the UC-neoplasia pathway in which p53 and chromogranin A are coordinately up-regulated. Immunohistochemical assessment of their expression might provide a useful adjunct tool for grading dysplasia in UC.
涉及神经内分泌细胞的全细胞发育不良已被证明相对罕见,但对溃疡性结肠炎(UC)中神经内分泌肿瘤的发展至关重要。我们试图通过免疫组织化学分析 26 例低级别发育不良(LGD)、32 例高级别发育不良(HGD)和 27 例浸润性癌(INV),以及 p53 表达,阐明嗜铬粒蛋白 A 表达作为 UC 相关肿瘤神经内分泌分化标志物的患病率。我们还评估了这些蛋白质在 LGD 和 HGD 之间的鉴别诊断中的效用。当免疫反应性细胞超过肿瘤病变的 5%时,认为嗜铬粒蛋白 A 为阳性,并且 HGD(57.7%)或 INV(46.7%)的阳性率高于 LGD(32.0%)。核 p53 染色阳性定义为阳性。HGD(59.4%;P=0.037)或 INV(59.3%)的 p53 阳性率也高于 LGD(30.8%)。在两种蛋白质的共阳性中也发现了类似的趋势(HGD,30.7%/INV,26.7%与 LGD,12.0%)。非肿瘤性黏膜中未发现两种蛋白质均为阳性。与单独使用 p53 相比,这两种蛋白质的组合提高了 HGD 的敏感性(66.7%)、特异性(80.0%)、阳性预测值(72.7%)和阴性预测值(75.0%)(敏感性,57.7%;特异性 68.0%;阳性预测值,65.2%;阴性预测值,60.7%)。总之,我们在这里表明,神经内分泌分化相对常见,是 UC 肿瘤发生途径中的早期事件,其中 p53 和嗜铬粒蛋白 A 协同上调。其表达的免疫组织化学评估可能为 UC 分级提供有用的辅助工具。
