唾液腺肿瘤中转录抑制因子 GATA 结合 1 的频繁免疫组化表达：一种敏感但非特异性的标记物。

Archives of pathology & laboratory medicine Pub Date : 2024-05-27 DOI:10.5858/arpa.2023-0444-OA

Sanjay Sriram, Aanchal Kakkar, Chetna Sarma, Ria Mahendru, Rajeev Kumar, Kavneet Kaur, Alok Thakar, Svs Deo

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引用次数: 0

摘要

背景唾液腺（SG）肿瘤（SGNs）显示出相当大的免疫表型多样性。相当一部分唾液腺肿瘤会发生转移，从而增加了转移部位的诊断难度。转录抑制因子 GATA 结合 1（TRPS1）是一种新型的乳腺癌免疫组化标记物，已被发现可对某些 SGNs 产生染色作用：研究TRPS1和SRY相关HMG-box 10（SOX10）在各种SGN和非SG癌、头颈部副神经节瘤以及头颈部粘膜黑色素瘤中的免疫表达：TRPS1免疫反应评分（IRS）被确定为阴性或低、中、高阳性；SOX10被报告为阴性或阳性：对148例SGN、5例乳腺癌、105例非乳腺癌-非SG癌（包括33例头颈部鳞状细胞癌（HNSCC）、6例头颈部副神经节瘤和6例头颈部粘膜黑色素瘤）进行了TRPS1评估。所有 23 例良性 SGN 均显示 TRPS1 阳性，其中大多数具有高阳性 IRS（23 例中有 17 例，占 74%）。在 125 例 SG 癌中，有 115 例（92%）TRPS1 呈阳性，其中 94 例（75%）IRS 呈高阳性，15 例（12%）呈中等阳性，6 例（5%）呈低阳性。在非乳腺-非 SG 癌中，HNSCC、肺癌、甲状腺癌、肾癌和卵巢癌经常出现 TRPS1 染色。近一半的 HNSCC 具有高度（18 例中的 11 例；33%）或中度（18 例中的 4 例；12%）阳性 IRS。SG癌的平均IRS明显高于非乳腺非SG癌（P < .001）。TRPS1 阳性的非乳腺非 SG 癌中没有一个表达 SOX10：TRPS1在大多数良性和恶性SGN中均呈阳性。它在几种非乳腺癌-非 SG 癌中的表达表明，即使只考虑高阳性的 IRS，它对乳腺癌和 SG 癌也缺乏特异性。加入 SOX10 可提高 TRPS1 的鉴别作用。

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Frequent Immunohistochemical Expression of Transcriptional Repressor GATA Binding 1 in Salivary Gland Neoplasms: A Sensitive but Nonspecific Marker.

Context.—: Salivary gland (SG) neoplasms (SGNs) display considerable immunophenotypic diversity. A significant proportion of SG carcinomas develop metastases with increased diagnostic difficulty at metastatic sites. Transcriptional repressor GATA binding 1 (TRPS1), a novel immunohistochemical marker for breast cancer, has been found to stain certain SGNs.

Objective.—: To investigate TRPS1 and SRY-related HMG-box 10 (SOX10) immunoexpression in various SGNs and non-SG carcinomas, head and neck paragangliomas, and head and neck mucosal melanomas.

Design.—: TRPS1 immunoreactivity score (IRS) was determined as negative or low, intermediate, or high positive; SOX10 was reported as negative or positive.

Results.—: One hundred forty-eight SGNs, 5 breast carcinomas, 105 nonbreast-non-SG carcinomas, including 33 head and neck squamous cell carcinomas (HNSCCs), 6 head and neck paragangliomas, and 6 head and neck mucosal melanomas, were assessed for TRPS1. All 23 benign SGNs showed TRPS1 positivity, with the majority having high-positive IRS (17 of 23 cases; 74%). Among 125 SG carcinomas, 115 of 125 (92%) were TRPS1 positive, with high-positive IRS in 94 of 125 (75%), intermediate positive in 15 of 125 (12%), and low positive in 6 of 125 (5%). Among nonbreast-non-SG carcinomas, HNSCC, lung, thyroid, kidney, and ovarian carcinomas showed frequent TRPS1 staining. Nearly half of HNSCCs had high (11 of 18; 33%) or intermediate (4 of 18; 12%) positive IRS. Mean IRS in SG carcinomas was significantly higher than that in nonbreast-non-SG carcinomas (P < .001). None of the TRPS1-positive nonbreast-non-SG carcinomas expressed SOX10.

Conclusions.—: TRPS1 is positive in most benign and malignant SGNs. Its expression in several nonbreast-non-SG carcinomas indicates that it lacks specificity for breast and SG carcinomas, even if considering only high-positive IRS. Addition of SOX10 can increase discriminatory utility of TRPS1.

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Archives of pathology & laboratory medicine

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