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SALL4 是睾丸生殖细胞肿瘤的一种新型诊断标志物。

SALL4 is a novel diagnostic marker for testicular germ cell tumors.

机构信息

The Lauren V. Ackerman Laboratory of Surgical Pathology, Division of Anatomic and Molecular Pathology, Department of Pathology and Immunology, Washington University in Saint Louis, 660 S Euclid Avenue, Campus Box 8118, Saint Louis, MO 63110, USA.

出版信息

Am J Surg Pathol. 2009 Jul;33(7):1065-77. doi: 10.1097/PAS.0b013e3181a13eef.

Abstract

The diagnosis of testicular germ cell tumors (GCTs) sometimes can be challenging without ancillary markers. Here we performed an immunohistochemical study of a novel stem cell marker SALL4 in a large series of 110 primary testicular GCTs (65 pure and 45 mixed) containing the following types of tumors and/or tumor components: 50 intratubular germ cell neoplasias (ITGCNs), 62 classic seminomas, 2 spermatocytic seminomas, 39 embryonal carcinomas (EC), 5 pediatric and 26 postpubertal yolk sac tumors (YST), 7 pediatric and 25 postpubertal teratomas, and 5 choriocarcinomas. We compared SALL4 with OCT4 in all GCTs, and SALL4 to alpha-fetoprotein (AFP) and glypican-3 in all YSTs. To test SALL4 specificity, 23 testicular non-GCTs (10 Leydig cell tumors, 4 Sertoli cell tumors, 3 adenomatoid tumors, 3 paratesticular rhabdomyosarcomas, 2 diffuse large B-cell lymphomas, and 1 rete testis papillary cystadenoma) and 275 nontesticular tumors (158 metastatic carcinomas, 12 metastatic melanomas, 11 primary and 2 metastatic mesotheliomas, and 72 primary and 20 metastatic sarcomas) were also stained for SALL4. All ITGCNs, classic seminomas, and ECs demonstrated strong SALL4 and OCT4 staining in more than 90% tumor cells. All 31 YSTs (5 pediatric and 26 postpubertal) showed strong positive SALL4 staining in more than 90% tumor cells but had negative OCT4 staining. Both spermatocytic seminomas showed positive SALL4 staining in 80% to 95% tumor cells in all 3 types of tumor cells with weak-to-moderate staining intensity. Mononucleated trophoblastic cells were variably positive for SALL4 staining in all 5 choriocarcinomas. Focal SALL4 staining was seen in 4 of 7 pediatric and 23 of 27 postpubertal teratomas. OCT4 staining was not seen in any spermatocytic seminoma, choriocarcinoma, or teratoma. No SALL4 staining was seen in all 23 testicular non-GCTs. Of 275 nontesticular tumors, only 10 carcinomas and 1 sarcoma showed focal (<25% tumor cells) weak SALL4 staining. The only non-neoplastic cells within the testis stained with SALL4 were spermatogonia and few primary spermatocytes. AFP staining was seen in 29 of 31 YST but it was often focal and patchy. Although all 31 YSTs showed glypican-3 staining, 14 (45%) show staining in less than 30% tumor cells. Our findings indicate that SALL4 is a novel sensitive and relatively specific marker for testicular GCTs. SALL4 is a more sensitive marker than AFP and glypican-3 for YST.

摘要

睾丸生殖细胞肿瘤(GCTs)的诊断有时在没有辅助标志物的情况下具有挑战性。在这里,我们对一种新的干细胞标志物 SALL4 在 110 例原发性睾丸 GCT(65 例纯 GCT 和 45 例混合性 GCT)中进行了免疫组织化学研究,这些肿瘤包含以下类型的肿瘤和/或肿瘤成分:50 例管内生殖细胞肿瘤(ITGCNs)、62 例经典精原细胞瘤、2 例精原细胞瘤、39 例胚胎癌(EC)、5 例儿童和 26 例青春期后卵黄囊肿瘤(YST)、7 例儿童和 25 例青春期后畸胎瘤和 5 例绒毛膜癌。我们比较了 SALL4 在所有 GCT 中的 OCT4,以及 SALL4 在所有 YST 中的 AFP 和 Glypican-3。为了测试 SALL4 的特异性,对 23 例睾丸非 GCT(10 例 Leydig 细胞瘤、4 例 Sertoli 细胞瘤、3 例腺肌瘤、3 例睾丸旁横纹肌肉瘤、2 例弥漫性大 B 细胞淋巴瘤和 1 例 rete testis 乳头状囊腺瘤)和 275 例非睾丸肿瘤(158 例转移性癌、12 例转移性黑素瘤、11 例原发性和 2 例转移性间皮瘤以及 72 例原发性和 20 例转移性肉瘤)也进行了 SALL4 染色。所有 ITGCNs、经典精原细胞瘤和 EC 均在超过 90%的肿瘤细胞中显示出强烈的 SALL4 和 OCT4 染色。所有 31 例 YST(5 例儿童和 26 例青春期后)均在超过 90%的肿瘤细胞中显示出强烈的阳性 SALL4 染色,但 OCT4 染色为阴性。所有 3 种类型的肿瘤细胞中,2 例精原细胞瘤均显示出 80%至 95%的肿瘤细胞呈阳性 SALL4 染色,染色强度为弱至中等。所有 5 例绒毛膜癌中的单核滋养细胞均呈 SALL4 染色阳性。在 7 例儿童和 27 例青春期后畸胎瘤中,有 4 例观察到散在的 SALL4 染色。OCT4 染色在任何精原细胞瘤、绒毛膜癌或畸胎瘤中均未观察到。所有 23 例睾丸非 GCT 均未观察到 SALL4 染色。在 275 例非睾丸肿瘤中,仅 10 例癌和 1 例肉瘤显示出局灶性(<25%肿瘤细胞)弱阳性 SALL4 染色。睾丸内唯一染色的非肿瘤细胞是精原细胞和少数初级精母细胞。在 29 例 YST 中观察到 AFP 染色,但染色通常呈局灶性和斑片状。尽管所有 31 例 YST 均显示 Glypican-3 染色,但有 14 例(45%)在不到 30%的肿瘤细胞中显示染色。我们的研究结果表明,SALL4 是一种新的敏感且相对特异性的睾丸 GCT 标志物。SALL4 是一种比 AFP 和 Glypican-3 更敏感的 YST 标志物。

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