Melanoma in situ and low risk pT1a melanoma: Need for new diagnostic terminology.

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS ACS Applied Bio Materials Pub Date : 2024-09-13 DOI:10.1016/j.clindermatol.2024.09.006
David E Elder, Raymond L Barnhill, Megan Eguchi, Joann G Elmore, Kathleen F Kerr, Stevan Knezevich
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Abstract

Melanoma incidence has risen rapidly, at least until recently, while mortality has changed only a little, a phenomenon suggestive of overdiagnosis, which can be defined as the diagnosis as "melanoma" of a lesion that would not have had the competence to cause death or symptoms even if it had not been excised. Overdiagnosis has been attributed to efforts at early diagnosis ("overdetection"), and to changes in criteria resulting in diagnosis as melanoma of lesions previously termed nevi ("overdefinition"). In terms of overdefinition, there is evidence that criteria for the histopathologic diagnosis of melanoma has changed over a period of approximately two decades. Specialization may play a role in overdefinition; research has shown that when pathologists interpret the same lesion, dermatopathologists are more likely to diagnose low stage (AJCC T1a) melanomas and general/surgical pathologists are more likely to diagnose atypical nevi. An important subset that contributes to overdiagnosis is those melanomas that lack the property of tumorigenic vertical growth phase, thus lacking metastatic competence, and perhaps not warranting diagnosis as overt melanomas. Studies have defined subsets of patients with very low stage lesions diagnosed as melanomas in which observed survival has been 100%. In the past, many of these lesions would have been diagnosed as nevi, constituting overdefinition. Other key characteristics for very low risk (or no risk) lesions that are currently termed invasive "melanomas" include low Breslow thickness, Clark's level II invasion, absence of mitoses, and clinically, lack of observed or experienced dynamic changes. We propose a provisional terminology for diagnosing extremely low risk subgroups as "Melanocytic neoplasms of low malignant potential", aimed at reducing the negative personal and social effects of a cancer diagnosis for patients whose health and wellbeing are in reality not affected by an overdiagnosed "melanoma". With additional confirmation and appropriate consensus, it is likely that some of these subgroups can be reclassified as atypical or dysplastic nevi.

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原位黑色素瘤和低危 pT1a 黑色素瘤:需要新的诊断术语。
至少直到最近,黑色素瘤的发病率一直在迅速上升,而死亡率却变化不大,这种现象表明存在过度诊断,过度诊断可以定义为将即使没有切除也不会导致死亡或症状的病变诊断为 "黑色素瘤"。过度诊断可归因于早期诊断的努力("过度检测"),也可归因于标准的改变导致以前称为痣的病变被诊断为黑色素瘤("过度定义")。就过度定义而言,有证据表明黑色素瘤的组织病理学诊断标准在大约二十年间发生了变化。研究表明,当病理学家对同一病变进行解释时,皮肤病理学家更倾向于诊断低分期(AJCC T1a)黑色素瘤,而普通/外科病理学家则更倾向于诊断非典型痣。造成过度诊断的一个重要亚群是那些缺乏垂直生长期致瘤特性的黑色素瘤,这些黑色素瘤缺乏转移能力,或许不值得诊断为明显的黑色素瘤。研究已经定义了被诊断为黑色素瘤的极低分期病变患者的子集,在这些患者中,观察到的存活率为 100%。在过去,这些病变很多都会被诊断为痣,这就构成了过度定义。目前被称为浸润性 "黑色素瘤 "的极低风险(或无风险)病变的其他关键特征包括布瑞斯洛厚度低、克拉克二级浸润、无有丝分裂,以及临床上缺乏观察到的或经历过的动态变化。我们建议将风险极低的亚组诊断为 "低恶性潜能黑色素细胞瘤"(Melanocytic neoplasms of low malignant potential),目的是减少癌症诊断对患者个人和社会的负面影响,因为事实上他们的健康和福祉并未受到过度诊断 "黑色素瘤 "的影响。在进一步确认和达成适当共识后,其中一些亚组很可能会被重新归类为非典型或发育不良痣。
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来源期刊
ACS Applied Bio Materials
ACS Applied Bio Materials Chemistry-Chemistry (all)
CiteScore
9.40
自引率
2.10%
发文量
464
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