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妊娠相关性黑色素瘤中雌激素和孕激素受体分析:免疫组化检测未发现激素受体。

Estrogen and progesterone receptor analysis in pregnancy-associated melanoma: absence of immunohistochemically detectable hormone receptors.

作者信息

Duncan L M, Travers R L, Koerner F C, Mihm M C, Sober A J

机构信息

Department of Pathology, Massachusetts General Hospital, Boston 02114.

出版信息

Hum Pathol. 1994 Jan;25(1):36-41. doi: 10.1016/0046-8177(94)90168-6.

Abstract

The role of estrogen in the initiation and progression of melanoma remains unclear. Some findings that suggest a hormonal role in melanoma initiation or progression include the following: (1) melanomas arising during pregnancy are thicker than those in nonpregnant women, (2) pregnant women with stage II (regional nodal metastases) melanoma have a worse prognosis than nonpregnant women of similar stage, and (3) melanoma is rare prior to puberty. Although biochemical assays have shown that estrogen-binding proteins are present in malignant melanoma, studies using a sensitive and more specific immunohistochemical technique have not found estrogen receptors (ERs) in melanoma. In our laboratory an immunohistochemical technique using monoclonal antibody H222 can detect ER in tumors with receptor levels lower than 9 fmol/mg protein and detects ER in a variety of tissues and species. In addition, monoclonal antibody KD68 is used to detect progesterone receptors immunohistochemically. We studied 14 cases of pregnancy-associated melanoma. None of our cases, ranging from melanoma in situ to metastatic melanoma, showed positive nuclear staining for ER, nor did any of these cases show positive immunohistochemical staining for progesterone receptor. Despite the wide tissue and species distribution of ER detected by the monoclonal antibody H222, this immunohistochemical technique does not appear to be useful in the study of possible hormonal effects on the progression of malignant melanoma. The estrogen-binding proteins in melanoma detected by biochemical techniques in previous studies probably are distinct from the well-defined human ER.

摘要

雌激素在黑色素瘤的发生和发展过程中所起的作用仍不明确。一些提示激素在黑色素瘤发生或发展中起作用的研究结果如下:(1)孕期出现的黑色素瘤比非孕期女性的黑色素瘤更厚;(2)患有II期(区域淋巴结转移)黑色素瘤的孕妇比处于相似分期的非孕期女性预后更差;(3)黑色素瘤在青春期前很罕见。尽管生化分析表明恶性黑色素瘤中存在雌激素结合蛋白,但使用敏感且更具特异性的免疫组化技术进行的研究并未在黑色素瘤中发现雌激素受体(ER)。在我们实验室,使用单克隆抗体H222的免疫组化技术能够检测受体水平低于9 fmol/mg蛋白的肿瘤中的ER,并能在多种组织和物种中检测到ER。此外,单克隆抗体KD68用于免疫组化检测孕激素受体。我们研究了14例妊娠相关黑色素瘤病例。从原位黑色素瘤到转移性黑色素瘤,我们的病例均未显示ER的细胞核染色阳性,这些病例也均未显示孕激素受体的免疫组化染色阳性。尽管单克隆抗体H222检测到的ER具有广泛的组织和物种分布,但这种免疫组化技术似乎对研究激素对恶性黑色素瘤进展可能产生的影响并无帮助。先前研究中通过生化技术在黑色素瘤中检测到的雌激素结合蛋白可能与明确的人类ER不同。

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