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薄型黑色素瘤:一个包含四种皮肤黑色素瘤组织学亚型的通用术语。

Thin Melanoma: A Generic Term Including Four Histological Subtypes of Cutaneous Melanoma.

作者信息

Roncati Luca, Pusiol Teresa, Piscioli Francesco

机构信息

Luca Roncati MD, PhD, Department of Diagnostic and Clinical Medicine and of Public Health Section of Pathology, University of Modena and Reggio Emilia, Policlinico Hospital, I-41124 Modena (MO), Italy;

出版信息

Acta Dermatovenerol Croat. 2016 Dec;24(4):169-174.

Abstract

Today, the scientific community is focusing on the prognostic significance of different histological subtypes of thin melanoma (1). The current staging system for melanoma of the American Joint Committee on Cancer (AJCC) uses Breslow thickness as the primary attribute: melanomas with up to 1 mm thickness is defined as thin, because they present a good prognosis after surgical excision, with a 10-year survival rate of 85-90% in case of a tumor-free margin ≥1 cm (2). There is a significant interaction between mitotic rate and Breslow depth, so the predictive value of the mitotic rate on sentinel lymph node (SLN) positivity can be dependent on Breslow thickness (3). Cutaneous melanoma generally evolves through three clearly discernible progression stages. At first, transformed melanocytes proliferate above the epidermal basement membrane (the in situ or epidermal radial growth phase); they then invade the papillary dermis (the micro-invasive radial growth phase); and subsequently acquire the capacity to grow as a well-known malignant tumor (the invasive vertical growth phase). More specifically, micro-invasive melanoma is a non-tumorigenic radial growth phase of cutaneous melanoma, which invades the superficial dermis without forming a tumor nodule or papule, in absence of regression (3). In contrast, the micro-invasive radial growth phase of cutaneous melanoma with regression will rarely metastasize and, for this reason, the lesion should be recognized and could also be categorized as a 'micro-invasive radial growth phase of uncertain tumorigenic potential' (4). The early vertical growth phase of tumorigenic melanoma is characterized by the presence of a cell cluster in the dermis that is larger than the largest cluster in the epidermis (5). This feature is typical of tumorigenicity, while the mitogenicity is documented by the observation of mitotic figures in dermal melanoma cells (5,6). The early vertical growth phase and the radial growth phase with regression have a statistical chance of distant metastases (7). Therefore, thin melanoma includes four main histological subtypes, which reflect a specific biological behavior: the in situ epidermal radial growth phase, the non-tumorigenic micro-invasive radial growth phase, the micro-invasive radial growth phase with regression of uncertain tumorigenic potential, and the tumorigenic early vertical growth phase. In conclusion, thin melanoma can be considered a generic term and its subtypes should be histologically distinguished beyond its site of origin (acral versus non-acral) because they have different prognostic relevance.

摘要

如今,科学界正聚焦于薄型黑色素瘤不同组织学亚型的预后意义(1)。美国癌症联合委员会(AJCC)目前的黑色素瘤分期系统以 Breslow 厚度作为主要指标:厚度达 1 mm 及以下的黑色素瘤被定义为薄型,因为手术切除后它们预后良好,若切缘无瘤距≥1 cm,10 年生存率为 85 - 90%(2)。有丝分裂率与 Breslow 深度之间存在显著相互作用,因此有丝分裂率对前哨淋巴结(SLN)阳性的预测价值可能取决于 Breslow 厚度(3)。皮肤黑色素瘤通常经历三个清晰可辨的进展阶段。起初,转化的黑素细胞在表皮基底膜上方增殖(原位或表皮径向生长阶段);接着它们侵入乳头真皮(微侵袭径向生长阶段);随后获得作为一种广为人知的恶性肿瘤生长的能力(侵袭性垂直生长阶段)。更具体地说,微侵袭性黑色素瘤是皮肤黑色素瘤的非致瘤性径向生长阶段,它在无消退的情况下侵入浅表真皮,不形成肿瘤结节或丘疹(3)。相比之下,有消退的皮肤黑色素瘤微侵袭径向生长阶段很少发生转移,因此,该病变应被识别,也可归类为“肿瘤发生潜能不确定的微侵袭径向生长阶段”(4)。致瘤性黑色素瘤的早期垂直生长阶段的特征是真皮中存在一个细胞簇,其大于表皮中最大的细胞簇(5)。这一特征是致瘤性的典型表现,而有丝分裂活性则通过真皮黑色素瘤细胞中有丝分裂象的观察得以证实(5,6)。早期垂直生长阶段和有消退的径向生长阶段有发生远处转移的统计学可能性(7)。因此,薄型黑色素瘤包括四种主要组织学亚型,它们反映了特定的生物学行为:原位表皮径向生长阶段、非致瘤性微侵袭径向生长阶段、肿瘤发生潜能不确定的有消退的微侵袭径向生长阶段以及致瘤性早期垂直生长阶段。总之,薄型黑色素瘤可被视为一个通用术语,其亚型应在组织学上加以区分,而不仅仅依据其起源部位(肢端与非肢端),因为它们具有不同的预后相关性。

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