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原发性皮肤γδ T细胞淋巴瘤的免疫表型转变提示抗原调制:对系列活检标本的研究

Immunophenotypic Shifts in Primary Cutaneous γδ T-Cell Lymphoma Suggest Antigenic Modulation: A Study of Sequential Biopsy Specimens.

作者信息

Agbay Rose Lou Marie C, Torres-Cabala Carlos A, Patel Keyur P, Merril Eric D, Duvic Madeleine, Quesada Andres, Prieto Victor G, Aung Phyu P, Loghavi Sanam, Young Ken H, Hu Shimin, Ferrufino-Schmidt Maria C, Tetzlaff Michael, Li Shaoying, Medeiros L Jeffrey, Miranda Roberto N

机构信息

Departments of *Hematopathology †Pathology ‡Dermatology ¶Translational and Molecular Pathology, The University of Texas MD Anderson Cancer Center, Houston, TX §University of Missouri, Kansas City, MO ∥Departamento de Patologia, Universidad Peruana Cayetano Heredia, Lima, Peru.

出版信息

Am J Surg Pathol. 2017 Apr;41(4):431-445. doi: 10.1097/PAS.0000000000000786.

Abstract

Primary cutaneous γδ T-cell lymphoma (PCGD TCL), an aggressive type of lymphoma, accounts for approximately 1% of all primary cutaneous lymphomas. We have occasionally observed changes in T-cell antigen expression (immunophenotypic [IP] shift) over time, a phenomenon that is considered rare in T-cell lymphoma including cutaneous T-cell lymphoma. Therefore, we assessed sequential biopsies of PCGD TCL for possible IP shifts of the lymphoma cells. We searched for cases of PCGD TCL with consecutive biopsies to perform a comprehensive immunohistochemical analysis of paired specimens. A median of 12 markers per case was tested. We evaluated the percentage of neoplastic lymphocytes and determined the differential expression of antigens (gain, loss, increase or decrease). We identified 9 patients with PCGD TCL with consecutive biopsies. All (100%) cases had IP shifts of at least 1 antigen, whereas overall 22 pairs of markers were shifted: gain of reactivity occurred in 7 (31.8%) and loss in 3 (13.6%); increased reactivity in 4 (18.2%) and decreased in 8 (36.4%). Molecular analysis of TCRγ showed identically sized monoclonal rearrangements between biopsy pairs in 4/4 (100%) patients. There was no correlation between IP shifts and the clinical appearance of lesions, histopathologic or cytologic features, or molecular rearrangements. IP shifts are common in PCGD TCL, occurring in all patients in this study and involving a variety of antigens. IP shifts do not seem to be linked to changes in the T-cell clone and are without obvious clinical or morphologic correlates. The occurrence of IP shifts in PCGD TCL suggests that antigen modulation may be involved in pathogenesis. IP shifts are somewhat frequent in T-cell lymphoma; however, it does not suggest a second neoplasm, and molecular studies can be used to determine clonal identity.

摘要

原发性皮肤γδ T细胞淋巴瘤(PCGD TCL)是一种侵袭性淋巴瘤,约占所有原发性皮肤淋巴瘤的1%。我们偶尔观察到T细胞抗原表达随时间变化(免疫表型[IP]转变),这种现象在包括皮肤T细胞淋巴瘤在内的T细胞淋巴瘤中被认为很罕见。因此,我们评估了PCGD TCL的连续活检标本,以寻找淋巴瘤细胞可能的IP转变。我们搜索了有连续活检标本的PCGD TCL病例,以便对配对标本进行全面的免疫组织化学分析。每个病例平均检测12种标志物。我们评估了肿瘤淋巴细胞的百分比,并确定了抗原的差异表达(获得、丧失、增加或减少)。我们确定了9例有连续活检标本的PCGD TCL患者。所有(100%)病例至少有1种抗原发生IP转变,而总体上有22对标志物发生转变:反应性增加的有7例(31.8%),丧失的有3例(13.6%);反应性增强的有4例(18.2%),减弱的有8例(36.4%)。对TCRγ的分子分析显示,4/4(100%)患者的活检标本对之间单克隆重排大小相同。IP转变与病变的临床表现、组织病理学或细胞学特征或分子重排之间没有相关性。IP转变在PCGD TCL中很常见,本研究中的所有患者均出现,且涉及多种抗原。IP转变似乎与T细胞克隆的变化无关,也没有明显的临床或形态学相关性。PCGD TCL中IP转变的发生提示抗原调节可能参与发病机制。IP转变在T细胞淋巴瘤中较为常见;然而,这并不提示存在第二种肿瘤,分子研究可用于确定克隆身份。

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