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人垂体腺瘤中选择性剪接的雌激素受体信使核糖核酸变体的肿瘤特异性表达。

Tumor-specific expression of alternatively spliced estrogen receptor messenger ribonucleic acid variants in human pituitary adenomas.

作者信息

Chaidarun S S, Klibanski A, Alexander J M

机构信息

Department of Medicine, Massachusetts General Hospital, Boston 02114, USA.

出版信息

J Clin Endocrinol Metab. 1997 Apr;82(4):1058-65. doi: 10.1210/jcem.82.4.3864.

Abstract

The well documented mitogenic and hormone regulatory effects of estrogen (E2) on pituitary cells are mediated via its nuclear receptor (ER), a cellular homolog of v-erbA oncogene. ER isoforms generated by alternative exon splicing, termed ER variants delta 2ER to delta 7ER, have been identified in breast cancer and have been postulated to have important pathogenetic and clinical implications in tumorigenesis and/or development of hormone resistance. Because pituitary tumors, particularly prolactinomas, are known to be E2-dependent, we investigated alternatively spliced ER variant messenger ribonucleic acid expression in 40 human pituitary tumors of various phenotypes and normal pituitary tissues, using reverse transcription-PCR and Southern blot analyses. Nine of 11 prolactinomas readily expressed multiple ER variants (delta 2ER, delta 4ER, 5ER, and delta 7ER), whereas 6 of 11 tumors showed faint expression of delta 3ER. Four of 7 glycoprotein hormone-producing tumors that synthesized FSH beta expressed delta 2ER, delta 5ER, and delta 7ER. In 9 GH- and 10 ACTH-secreting tumors examined, the expression of normal and variant ER was restricted to tumors that also exhibited scattered PRL immunoreactivity. Variant and normal ER were not found in three null cell tumors (oncocytomas) that showed negative immunoreactivity for all pituitary hormones or their subunits. In contrast, only delta 4ER and delta 7ER were uniformly detected in normal pituitaries. delta 6ER was not detected in any normal or neoplastic pituitary specimen studied. We conclude that multiple alternatively spliced ER variants are coexpressed with normal ER in a tumor phenotype-specific manner. In addition, ER variants delta 2ER and delta 5ER were found to be tumor specific. Future functional studies will be required to determine whether coexpression of multiple ER variants along with normal ER confers a pathophysiological role in pituitary hormone regulation and/or tumor cell proliferation.

摘要

雌激素(E2)对垂体细胞具有有充分文献记载的促有丝分裂和激素调节作用,这是通过其核受体(ER)介导的,ER是v-erbA癌基因的细胞同源物。通过选择性外显子剪接产生的ER异构体,称为ER变体δ2ER至δ7ER,已在乳腺癌中被鉴定出来,并被推测在肿瘤发生和/或激素抵抗的发展中具有重要的发病机制和临床意义。由于垂体肿瘤,尤其是催乳素瘤,已知是E2依赖性的,我们使用逆转录PCR和Southern印迹分析,研究了40例不同表型的人类垂体肿瘤和正常垂体组织中选择性剪接的ER变体信使核糖核酸的表达。11例催乳素瘤中有9例容易表达多种ER变体(δ2ER、δ4ER、δ5ER和δ7ER),而11例肿瘤中有6例显示δ3ER表达微弱。7例合成促卵泡激素β的糖蛋白激素分泌肿瘤中有4例表达δ2ER、δ5ER和δ7ER。在检测的9例生长激素分泌肿瘤和10例促肾上腺皮质激素分泌肿瘤中,正常和变体ER的表达仅限于也表现出散在催乳素免疫反应性的肿瘤。在3例对所有垂体激素或其亚基均呈阴性免疫反应的无功能细胞瘤(嗜酸细胞瘤)中未发现变体和正常ER。相比之下,在正常垂体中仅均匀检测到δ4ER和δ7ER。在所研究的任何正常或肿瘤性垂体标本中均未检测到δ6ER。我们得出结论,多种选择性剪接的ER变体与正常ER以肿瘤表型特异性方式共表达。此外,发现ER变体δ2ER和δ5ER是肿瘤特异性的。未来需要进行功能研究,以确定多种ER变体与正常ER的共表达是否在垂体激素调节和/或肿瘤细胞增殖中赋予病理生理作用。

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