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胶质纤维酸性蛋白(GFAP)蛋白异构体之谜:如何推动GFAP成为神经疾病中的一种动态生物标志物。

The GFAP proteoform puzzle: How to advance GFAP as a fluid biomarker in neurological diseases.

作者信息

Gogishvili Dea, Honey Madison I J, Verberk Inge M W, Vermunt Lisa, Hol Elly M, Teunissen Charlotte E, Abeln Sanne

机构信息

Bioinformatics, Computer Science Department, Vrije Universiteit Amsterdam, Amsterdam, The Netherlands.

AI Technology for Life, Department of Computing and Information Sciences, Department of Biology, Utrecht University, Utrecht, The Netherlands.

出版信息

J Neurochem. 2025 Jan;169(1):e16226. doi: 10.1111/jnc.16226. Epub 2024 Sep 17.

Abstract

Glial fibrillary acidic protein (GFAP) is a well-established biomarker of reactive astrogliosis in the central nervous system because of its elevated levels following brain injury and various neurological disorders. The advent of ultra-sensitive methods for measuring low-abundant proteins has significantly enhanced our understanding of GFAP levels in the serum or plasma of patients with diverse neurological diseases. Clinical studies have demonstrated that GFAP holds promise both as a diagnostic and prognostic biomarker, including but not limited to individuals with Alzheimer's disease. GFAP exhibits diverse forms and structures, herein referred to as its proteoform complexity, encompassing conformational dynamics, isoforms and post-translational modifications (PTMs). In this review, we explore how the proteoform complexity of GFAP influences its detection, which may affect the differential diagnostic performance of GFAP in different biological fluids and can provide valuable insights into underlying biological processes. Additionally, proteoforms are often disease-specific, and our review provides suggestions and highlights areas to focus on for the development of new assays for measuring GFAP, including isoforms, PTMs, discharge mechanisms, breakdown products, higher-order species and interacting partners. By addressing the knowledge gaps highlighted in this review, we aim to support the clinical translation and interpretation of GFAP in both CSF and blood and the development of reliable, reproducible and specific prognostic and diagnostic tests. To enhance disease pathology comprehension and optimise GFAP as a biomarker, a thorough understanding of detected proteoforms in biofluids is essential.

摘要

胶质纤维酸性蛋白(GFAP)是中枢神经系统反应性星形胶质细胞增生的一种公认的生物标志物,因为在脑损伤和各种神经系统疾病后其水平会升高。用于测量低丰度蛋白质的超灵敏方法的出现,显著增强了我们对患有各种神经系统疾病患者血清或血浆中GFAP水平的理解。临床研究表明,GFAP作为一种诊断和预后生物标志物具有前景,包括但不限于阿尔茨海默病患者。GFAP呈现出多样的形式和结构,在此称为其蛋白质异构体复杂性,包括构象动力学、异构体和翻译后修饰(PTM)。在本综述中,我们探讨了GFAP的蛋白质异构体复杂性如何影响其检测,这可能会影响GFAP在不同生物体液中的鉴别诊断性能,并能为潜在的生物学过程提供有价值的见解。此外,蛋白质异构体通常具有疾病特异性,我们的综述提供了建议,并突出了开发测量GFAP新检测方法时需要关注的领域,包括异构体、PTM、释放机制、降解产物、高阶物种和相互作用伙伴。通过解决本综述中强调的知识空白,我们旨在支持GFAP在脑脊液和血液中的临床转化和解释,以及开发可靠、可重复和特异的预后和诊断测试。为了增强对疾病病理学的理解并优化GFAP作为生物标志物,深入了解生物体液中检测到的蛋白质异构体至关重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d5c6/11658191/43530a95841d/JNC-169-0-g002.jpg

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