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Journal ArticleDOI

Glial Fibrillary Acidic Protein: GFAP-Thirty-One Years (1969–2000)

Lawrence F. Eng, +2 more
- 01 Oct 2000 - 
- Vol. 25, Iss: 9, pp 1439-1451
TLDR
While the structural function of GFAP has become more acceptable, the use ofGFAP antibodies and promoters continue to be valuable in studying CNS injury, disease, and development.
Abstract
It is now well established that the glial fibrillary acidic protein (GFAP) is the principal 8-9 nm intermediate filament in mature astrocytes of the central nervous system (CNS). Over a decade ago, the value of GFAP as a prototype antigen in nervous tissue identification and as a standard marker for fundamental and applied research at an interdisciplinary level was recognized (Raine, 135). As a member of the cytoskeletal protein family, GFAP is thought to be important in modulating astrocyte motility and shape by providing structural stability to astrocytic processes. In the CNS of higher vertebrates, following injury, either as a result of trauma, disease, genetic disorders, or chemical insult, astrocytes become reactive and respond in a typical manner, termed astrogliosis. Astrogliosis is characterized by rapid synthesis of GFAP and is demonstrated by increase in protein content or by immunostaining with GFAP antibody. In addition to the major application of GFAP antisera for routine use in astrocyte identification in the CNS, the molecular cloning of the mouse gene in 1985 has opened a new and rich realm for GFAP studies. These include antisense, null mice, and numerous promoter studies. Studies showing that mice lacking GFAP are hypersensitive to cervical spinal cord injury caused by sudden acceleration of the head have provided more direct evidence for a structural role of GFAP. While the structural function of GFAP has become more acceptable, the use of GFAP antibodies and promoters continue to be valuable in studying CNS injury, disease, and development.

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Citations
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Journal ArticleDOI

Astrocytes: biology and pathology

TL;DR: Astrocyte functions in healthy CNS, mechanisms and functions of reactive astrogliosis and glial scar formation, and ways in which reactive astrocytes may cause or contribute to specific CNS disorders and lesions are reviewed.
Journal ArticleDOI

Diffusion in brain extracellular space.

TL;DR: Experimental studies with the real-time iontophoresis method employing the cation tetramethylammonium in normal brain tissue improve the conception of ECS structure and the roles of glia and extracellular matrix in modulating the ECS microenvironment.
Journal ArticleDOI

Physiology of astroglia

TL;DR: Astrocytes are tightly integrated into neural networks and act within the context of neural tissue; astrocytes control homeostasis of the CNS at all levels of organization from molecular to the whole organ.
Journal ArticleDOI

Glia and pain: Is chronic pain a gliopathy?

Ru-Rong Ji, +1 more
- 20 Jun 2013 - 
TL;DR: Chronic pain could be a result of "gliopathy," that is, dysregulation of glial functions in the central and peripheral nervous system, and an update on recent advances is provided and remaining questions are discussed.
Journal ArticleDOI

Astrocytes and brain injury.

TL;DR: Astrocytes are the most numerous cell type in the central nervous system and provide structural, trophic, and metabolic support to neurons and modulate synaptic activity, and their death or survival may affect the ultimate clinical outcome and rehabilitation.
References
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Journal ArticleDOI

Brain interleukin 1 and S-100 immunoreactivity are elevated in Down syndrome and Alzheimer disease

TL;DR: The data suggest that increased expression of S-100 in Down syndrome, resulting from duplication of the gene on chromosome 21 that encodes the beta subunit ofS-100, may be augmented by elevation of interleukin 1, which may promote the astrogliosis in Alzheimer disease.
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Molecular profile of reactive astrocytes—Implications for their role in neurologic disease

TL;DR: A summary of molecules whose levels of expression differentiate activated from resting astrocytes is provided and it becomes apparent that reactive astroCytes may benefit the injured nervous system by participating in diverse biological processes.
Journal ArticleDOI

Localization of the glial fibrillary acidic protein in astrocytes by immunofluorescence

TL;DR: The glial fibrillary acidic (GFA) protein, a brain specific protein extracted from severely gliosed human tissue, is not species specific; cross-reaction occurs between anti-human GFA protein antibodies and brain extracts of rabbit, guinea pig, rat and dog.
Journal ArticleDOI

Leukocyte Infiltration, Neuronal Degeneration, and Neurite Outgrowth after Ablation of Scar-Forming, Reactive Astrocytes in Adult Transgenic Mice

TL;DR: These findings show that genetic targeting can be used to ablate scar-forming astrocytes and demonstrate roles for astroCytes in regulating leukocyte trafficking, repairing the BBB, protecting neurons, and restricting nerve fiber growth after injury in the adult central nervous system.
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