垂体瘤的预后生物标志物:系统综述。

TouchREVIEWS in endocrinology Pub Date : 2023-11-01 Epub Date: 2023-08-09 DOI:10.17925/EE.2023.19.2.12
Eirini Papadimitriou, Eleftherios Chatzellis, Anastasia Dimitriadi, Gregory A Kaltsas, Stamatios Theocharis, Krystallenia I Alexandraki
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引用次数: 0

摘要

垂体瘤(PTs)是第二大最常见的颅内肿瘤。虽然大多数垂体瘤表现为良性,但也可能具有侵袭性,并对治疗产生抗药性。本综述旨在报告最近发现的可能具有预后价值的生物标志物。与非侵袭性或非复发性垂体癌或正常垂体癌相比,评估侵袭性/复发性垂体癌的潜在预后生物标志物或治疗靶点的研究被纳入本综述。在纳入的 28 项研究中,对超过 911 例 PT 进行了评估。通过系统性检索发现了一些可能与PT疾病复发或侵袭呈正相关的生物标志物的表达,这些标志物根据作用进行了分组:(1)对抗生长信号不敏感:小染色体维护蛋白7;(2)逃避免疫系统:环氧化酶 2、精氨酸酶 1、程序性细胞死亡蛋白 1(PD-1)/程序性死亡配体 2、分化簇(CD)80/CD86;(3) 持续血管生成:内皮细胞特异性分子、成纤维细胞生长因子受体、基质金属蛋白酶 9、垂体瘤转化基因;(4) 生长信号自给自足:表皮生长因子受体;(5) 组织侵袭:基质金属蛋白酶 9、筋膜蛋白。与疾病复发或侵袭呈负相关的生物标志物包括(1) 对抗生长信号不敏感:转化生长因子 β1、Smad 蛋白;(2) 持续血管生成:金属蛋白酶组织抑制剂 1;(3) 组织侵袭:Wnt抑制因子1;(4) 其他:胶质纤维酸性蛋白和细胞角蛋白的共同表达,以及雌激素受体α36和α66。而细胞周期蛋白A、细胞毒性T淋巴细胞相关蛋白4、S100蛋白、ephrin受体、galectin-3、神经细胞粘附分子、蛋白酪氨酸磷酸酶4A3和类固醇生成因子1与PT的侵袭或复发无明显关联。为了开发更个性化的 PT 治疗方法,同时由于目前针对复发性 PT 和侵袭研究的分子靶点数量有限,通过精心设计的介入研究更好地了解这些生物标志物中最相关的生物标志物将有助于更好地了解 PT 的分子特征。这也将满足对可治疗分子靶点的更多需求。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Prognostic Biomarkers in Pituitary Tumours: A Systematic Review.

Pituitary tumours (PTs) are the second most common intracranial tumour. Although the majority show benign behaviour, they may exert aggressive behaviour and can be resistant to treatment. The aim of this review is to report the recently identified biomarkers that might have possible prognostic value. Studies evaluating potentially prognostic biomarkers or a therapeutic target in invasive/recurrent PTs compared with either non-invasive or non-recurrent PTs or normal pituitaries are included in this review. In the 28 included studies, more than 911 PTs were evaluated. A systematic search identified the expression of a number of biomarkers that may be positively correlated with disease recurrence or invasion in PT, grouped according to role: (1) insensitivity to anti-growth signals: minichromosome maintenance protein 7; (2) evasion of the immune system: cyclooxygenase 2, arginase 1, programmed cell death protein 1 (PD-1)/programmed death ligand 2, cluster of differentiation (CD) 80/CD86; (3) sustained angiogenesis: endothelial cell-specific molecule, fibroblast growth factor receptor, matrix metalloproteinase 9, pituitary tumour transforming gene; (4) self-sufficiency in growth signals: epidermal growth factor receptor; and (5) tissue invasion: matrix metalloproteinase 9, fascin protein. Biomarkers with a negative correlation with disease recurrence or invasion include: (1) insensitivity to anti-growth signals: transforming growth factor β1, Smad proteins; (2) sustained angiogenesis: tissue inhibitor of metalloproteinase 1; (3) tissue invasion: Wnt inhibitory factor 1; and (4) miscellaneous: co-expression of glial fibrillary acidic protein and cytokeratin, and oestrogen receptors α36 and α66. PD-1/programmed cell death ligand 1 showed no clear association with invasion or recurrence, while cyclin A, cytotoxic T lymphocyte-associated protein 4, S100 protein, ephrin receptor, galectin-3 , neural cell adhesion molecule, protein tyrosine phosphatase 4A3 and steroidogenic factor 1 had no association with invasion or recurrence of PT. With the aim to develop a more personalized approach to the treatment of PT, and because of the limited number of molecular targets currently studied in the context of recurrent PT and invasion, a better understanding of the most relevant of these biomarkers by well-d esigned interventional studies will lead to a better understanding of the molecular profile of PT. This should also meet the increased need of treatable molecular targets.

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