Utilizing PRAME Expression and a Meta-Analytic Framework for iSALT to Explore Atypical Late-Onset Nevi of the Elderly and Their Relationship With Lentiginous and Nested Nevoid Melanomas.

IF 1.1 4区 医学 Q4 DERMATOLOGY American Journal of Dermatopathology Pub Date : 2024-12-01 Epub Date: 2024-10-15 DOI:10.1097/DAD.0000000000002847
Steven Kossard, Shahin Sharifi, Linda Calvey
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Abstract

Background: In contrast to early-onset dysplastic nevi, late-onset atypical nevi of the elderly are more often precursors to distinctive nevoid melanomas. PReferentially expressed Antigen in MElanoma (PRAME) immunohistochemistry was applied to delineate the nevoid aspect of late-onset oncogenic nevoid pathway. Inducible Skin-Associated Lymphoid Tissue, regulatory T-cell mesenchymal hubs, has emerged as a translational tool and was used to define nevoid oncogenesis within a dynamic meta-analytic pathway.

Methods: PRAME immunohistochemistry was applied after designating a histopathologic diagnosis. Late-onset atypical nested lentiginous nevus, lentiginous nested melanoma, and hypercellular nested nevoid melanoma were the diagnostic categories. A positive PRAME for melanoma was set at 75% percentage labeling.A wide-ranging published evidence-based database was incorporated to develop a meta-analytic framework for oncogenic nevogenesis. This combined inducible Skin-Associated Lymphoid Tissue incorporating the pleiotropic functions of regulatory T cells regulating immunity and gene regulatory epigenetics as principal modulators.

Results: Concordant-negative PRAME expression was present in 64 of 81 (79%) atypical nested lentiginous nevi, concordant-positive PRAME expression occurred in 54 of 75 (72%) nevoid lentiginous and nested melanomas, and 18 of 23 (78%) nevoid hypercellular nested melanomas.

Conclusions: PRAME expression confirmed the existence of a late-onset oncogenic nevoid pathway that can be defined by histopathology. Subsequent meta-analysis data linked to the meta-analytic framework revealed that PRAME is an epigenetic surrogate antigen expressed because of repression of retinoic acid receptor signaling, preventing ligand-induced retinoic acid cellular differentiation, growth arrest, and apoptosis, and promoting melanoma growth and survival for melanomas. PRAME is only a single antigen within a highly complex dynamic framework that governs nevoid oncogenesis. Significantly, the retinoic acid/retinoic acid receptor complex has been shown to modulate the immunosuppressive arm of regulatory T cells underpinning immune tolerance and is pertinent to the broad framework but is not linked to PRAME expression in this arm.

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利用 PRAME 表达和 iSALT 的元分析框架探讨老年人的非典型晚发型痣及其与皮样痣和嵌套痣样黑色素瘤的关系。
背景:与早期发病的发育不良痣相比,晚期发病的老年非典型痣更常是独特痣型黑色素瘤的前兆。应用PReferentially expressed Antigen in MElanoma (PRAME)免疫组化技术,可确定晚发型致癌痣的痣样途径。诱导性皮肤相关淋巴组织是调节性T细胞间质枢纽,已成为一种转化工具,被用于在动态元分析途径中定义nevoid肿瘤发生:在确定组织病理学诊断后,应用 PRAME 免疫组化技术。晚期非典型巢状皮样痣、皮样巢状黑色素瘤和高细胞巢状痣样黑色素瘤是诊断类别。黑色素瘤的阳性 PRAME 定义为 75% 的标记百分比。我们将已发表的大量循证数据库纳入其中,建立了致癌痣生成的荟萃分析框架。该框架将诱导性皮肤相关淋巴组织与调节性 T 细胞调节免疫和基因调节表观遗传学的多重功能结合起来,作为主要的调节因子:81个非典型巢状黑痣中的64个(79%)存在PRAME一致阴性表达,75个黑痣中的54个(72%)和23个黑痣中的18个(78%)存在PRAME一致阳性表达:PRAME的表达证实了晚发型致癌痣通路的存在,这种通路可通过组织病理学加以定义。随后与荟萃分析框架相关联的荟萃分析数据显示,PRAME是一种表观遗传学替代抗原,其表达的原因是抑制视黄酸受体信号传导,阻止配体诱导的视黄酸细胞分化、生长停滞和凋亡,促进黑色素瘤的生长和存活。PRAME 只是控制痣癌发生的高度复杂动态框架中的一个抗原。值得注意的是,视黄酸/视黄酸受体复合物已被证明可调节调节性 T 细胞的免疫抑制臂,从而巩固免疫耐受,它与这一广泛的框架相关,但与 PRAME 在这一臂中的表达无关。
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来源期刊
CiteScore
1.80
自引率
9.10%
发文量
453
审稿时长
3 months
期刊介绍: The American Journal of Dermatopathology offers outstanding coverage of the latest diagnostic approaches and laboratory techniques, as well as insights into contemporary social, legal, and ethical concerns. Each issue features review articles on clinical, technical, and basic science advances and illuminating, detailed case reports. With the The American Journal of Dermatopathology you''ll be able to: -Incorporate step-by-step coverage of new or difficult-to-diagnose conditions from their earliest histopathologic signs to confirmatory immunohistochemical and molecular studies. -Apply the latest basic science findings and clinical approaches to your work right away. -Tap into the skills and expertise of your peers and colleagues the world over peer-reviewed original articles, "Extraordinary cases reports", coverage of practical guidelines, and graphic presentations. -Expand your horizons through the Journal''s idea-generating forum for debating controversial issues and learning from preeminent researchers and clinicians
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