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转移性经治疗恶性生殖细胞肿瘤:SALL4 比胎盘碱性磷酸酶是更好的标志物吗?

Metastatic Treated Malignant Germ Cell Tumors: Is SALL4 a Better Marker Than Placental Alkaline Phosphatase?

作者信息

Andeen Nicole K, Tretiakova Maria S

机构信息

Department of Pathology, University of Washington, Seattle, WA.

出版信息

Appl Immunohistochem Mol Morphol. 2016 Mar;24(3):210-4. doi: 10.1097/PAI.0000000000000174.

DOI:10.1097/PAI.0000000000000174
PMID:25906119
Abstract

Studies have shown that in the metastatic setting and after treatment, expression of immunohistochemical markers may be diminished or lost. Transcription factor SALL4 (sal-like protein 4) has been recognized as a sensitive marker for both primary and metastatic malignant germ cell tumors (MGCTs), but has not been tested in the posttreatment setting. We sought to determine the level of SALL4 expression in treatment-resistant metastatic MGCT in comparison with pan-GCT marker placental alkaline phosphatase (PLAP). Thirty-six previously treated MGCTs, 16 untreated primary testicular MGCTs, and 4 cytology specimens were immunostained for SALL4 and PLAP, and staining characteristics were evaluated. In the treated MGCT group, there was diffuse SALL4 nuclear immunoreactivity in the majority of cases (27/36, 75%), labeling seminoma, yolk-sac tumor, embryonal carcinoma, and primitive neuroectodermal components. No treated metastatic MGCT lacked SALL4 immunoreactivity. In contrast, PLAP was diffusely expressed in only 14/36 (39%) cases of treated MGCTs, showed scattered focal weak to moderate positivity in 13/36 (36%), and was virtually absent in 9/36 (25%) cases. Both markers had scattered expression limited to the epithelial components of teratomatous regions. SALL4 also outperformed PLAP on a small sample of cytology blocks. Although SALL4 is not entirely specific, it is a highly sensitive marker with strong diffuse nuclear reactivity in the majority of MGCTs in the posttreatment setting, at significantly higher levels than PLAP (P<0.001). Persistent expression of SALL4 in metastatic MGCTs resistant to chemoradiation also raises the possibility for targeted systemic therapy as the anti-SALL4 peptide continues to be developed.

摘要

研究表明,在转移情况下以及治疗后,免疫组化标志物的表达可能会减弱或丧失。转录因子SALL4(类Sal蛋白4)已被公认为原发性和转移性恶性生殖细胞肿瘤(MGCT)的敏感标志物,但尚未在治疗后的情况下进行测试。我们试图确定与泛生殖细胞肿瘤标志物胎盘碱性磷酸酶(PLAP)相比,治疗抵抗性转移性MGCT中SALL4的表达水平。对36例先前接受治疗的MGCT、16例未经治疗的原发性睾丸MGCT和4例细胞学标本进行SALL4和PLAP免疫染色,并评估染色特征。在接受治疗的MGCT组中,大多数病例(27/36,75%)出现弥漫性SALL4核免疫反应,标记精原细胞瘤、卵黄囊瘤、胚胎癌和原始神经外胚层成分。没有治疗过的转移性MGCT缺乏SALL4免疫反应性。相比之下,PLAP仅在14/36(39%)的治疗后MGCT病例中弥漫性表达,在13/36(36%)的病例中表现为散在局灶性弱阳性至中度阳性,在9/36(25%)的病例中几乎不存在。两种标志物的散在表达均局限于畸胎瘤区域的上皮成分。在一小部分细胞学切片样本中,SALL4也优于PLAP。虽然SALL4并非完全特异,但它是一种高度敏感的标志物,在治疗后的大多数MGCT中具有强烈的弥漫性核反应性,水平明显高于PLAP(P<0.001)。在对放化疗耐药的转移性MGCT中持续表达SALL4也增加了靶向全身治疗的可能性,因为抗SALL4肽仍在研发中。

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