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垂体腺瘤中 BMP-4 基因的表观遗传沉默:表皮生长因子诱导再表达的潜在靶点。

Epigenomic silencing of the BMP-4 gene in pituitary adenomas: a potential target for epidrug-induced re-expression.

机构信息

Human Disease and Genomics Group, Institute of Science and Technology in Medicine, School of Medicine, Keele University, Stoke on Trent, Staffordshire ST4 7QB, United Kingdom.

出版信息

Endocrinology. 2012 Aug;153(8):3603-12. doi: 10.1210/en.2012-1231. Epub 2012 Jun 14.

Abstract

Bone morphogenetic protein (BMP)-4 is a key mediator of anterior pituitary organogenesis. However, through inappropriate expression patterns, BMP-4 is also pathogenic in a pituitary adenoma subtype-specific context. In these cases, increase or decrease in BMP-4 in lactotroph- and corticotroph-derived adenomas, respectively, is consistent with a bifunction role for this protein toward either promotion or inhibition of cell proliferation and hormone secretion. To gain insight into the aberrations responsible for differential expression, we examined BMP-4 transcript and protein expression patterns in the major adenomas subtypes. BMP-4 transcript and protein are differentially expressed and show increase in the majority of prolactinomas relative to normal pituitary, whereas the majority of other adenoma subtypes show reduced expression relative to both prolactinoma and normal pituitaries. Reduced expression of BMP-4 is not associated with change in CpG island methylation status. However, histone tail modifications are apparent, as enrichment for a modification associated with silent genes, H3K27me3, and depletion of a modification associated with active genes, H3K9Ac. In pituitary cell lines, reduced BMP-4 expression is also associated with similar histone tail modifications and contemporaneous increase in CpG island methylation. In these cells, coincubation with the demethylating agent zebularine and histone deacetylase inhibitor, trichostatin A, reversed epigenetic changes and restored expression of BMP-4. These studies show that, in contrast to prolactinomas, other adenoma subtypes show reduced expression of BMP-4 where epidrug induced reexpression, alone or in combination with conventional therapies, may offer new treatment strategies.

摘要

骨形态发生蛋白 4(BMP-4)是前垂体器官发生的关键介质。然而,通过不适当的表达模式,BMP-4 在特定的垂体腺瘤亚型中也是致病的。在这些情况下,BMP-4 在催乳素细胞和促肾上腺皮质激素细胞衍生的腺瘤中的增加或减少分别与该蛋白对细胞增殖和激素分泌的促进或抑制的双重作用一致。为了深入了解导致差异表达的异常情况,我们检查了主要腺瘤亚型中 BMP-4 转录本和蛋白表达模式。BMP-4 转录本和蛋白在大多数泌乳素瘤中表现出差异表达,相对于正常垂体,其表达增加,而大多数其他腺瘤亚型相对于泌乳素瘤和正常垂体,其表达减少。BMP-4 的表达减少与 CpG 岛甲基化状态的改变无关。然而,组蛋白尾部修饰是明显的,因为与沉默基因相关的修饰,H3K27me3 的富集,以及与活跃基因相关的修饰,H3K9Ac 的耗尽。在垂体细胞系中,BMP-4 表达的减少也与类似的组蛋白尾部修饰和同时发生的 CpG 岛甲基化增加有关。在这些细胞中,与去甲基化剂 zebularine 和组蛋白去乙酰化酶抑制剂曲古抑菌素 A 共同孵育,逆转了表观遗传变化并恢复了 BMP-4 的表达。这些研究表明,与泌乳素瘤相反,其他腺瘤亚型表现出 BMP-4 的表达减少,单独或与传统疗法联合使用,表皮诱导再表达可能提供新的治疗策略。

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