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Enhanced immunohistochemical detection of neural infiltration in primary melanoma: Is there a clinical value?

机译:增强免疫组化检测原发性黑色素瘤中神经浸润的临床价值?

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Neural infiltration in primary melanoma is a histopathologic feature that has been associated with desmoplastic histopathologic subtype and local recurrence in the literature. We tested the hypothesis that improved detection and characterization of neural infiltration into peritumoral or intratumoral location and perineural or intraneural involvement could have a prognostic relevance. We studied 128 primary melanoma cases prospectively accrued and followed at New York University using immunohistochemical detection with antihuman neurofilament protein and routine histology with hematoxylin and eosin. Neural infiltration, defined as the presence of tumor cells involving or immediately surrounding nerve foci, was identified and characterized using both detection methods. Neural infiltration rate of detection was enhanced by immunohistochemistry for neurofilament in matched-pair design (47% by immunohistochemistry versus 25% by routine histology). Immunohistochemical detection of neural infiltration was significantly associated with ulceration (P =.021), desmoplastic and acral lentiginous histologic subtype (P =.008), and headeck/hands/feet tumor location (P =.037). Routinely detected neural infiltration was significantly associated with local recurrence (P =.010). Immunohistochemistry detected more intratumoral neural infiltration cases compared with routine histology (30% versus 3%, respectively). Peritumoral and intratumoral nerve location had no impact on clinical outcomes. Using a multivariate model controlling for stage, neither routinely detected neural infiltration nor enhanced immunohistochemical characterization of neural infiltration was significantly associated with disease-free or overall survival. Our data demonstrate that routinely detected neural infiltration is associated with local recurrence in all histologic subtypes but that improved detection and characterization of neural infiltration with immunohistochemistry in primary melanoma does not add to prognostic relevance.
机译:原发性黑色素瘤中的神经浸润是一种组织病理学特征,在文献中与增生性组织病理学亚型和局部复发有关。我们检验了以下假设,即改善对肿瘤浸润周围或肿瘤内位置以及神经周或神经内受累的神经浸润的检测和表征可能与预后相关。我们研究了128位原发性原发性黑色素瘤病例,并在纽约大学进行了抗人神经丝蛋白免疫组化检测以及苏木精和曙红的常规组织学检查。使用两种检测方法都可以识别和表征神经浸润,神经浸润是指涉及或紧邻神经病灶的肿瘤细胞的存在。配对设计中神经丝的免疫组织化学提高了神经浸润的检出率(免疫组织化学检测为47%,常规组织学检测为25%)。免疫组化检测神经浸润与溃疡(P = .021),增生和手足轻度组织学亚型(P = .008)以及头/颈部/手/脚肿瘤位置(P = .037)显着相关。常规检测到的神经浸润与局部复发显着相关(P = .010)。与常规组织学相比,免疫组织化学检测到更多的肿瘤内神经浸润病例(分别为30%和3%)。瘤周和瘤内神经的位置对临床结果没有影响。使用控制阶段的多元模型,常规检测的神经浸润和增强的神经浸润免疫组织化学特征均与无病或总体生存率显着相关。我们的数据表明,在所有组织学亚型中,常规检测到的神经浸润均与局部复发相关,但在原发性黑色素瘤中用免疫组织化学方法改善神经浸润的检测和表征不会增加预后的相关性。

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