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DOI: 10.1055/s-0042-1751304
Aquaporin 4 and its Relationship with Brain Astrocytomas – Literature Review
Aquaporina 4 e sua Relação com Astrocitomas Cerebrais – Revisão da LiteraturaAuthors
Funding There was not financial support.
Abstract
Background Aquaporins (AQPs) are a family of membrane proteins that regulate the osmotic permeability of the plasma membrane. There are described in the literature a total of 13 types of Aquaporins in mammals, each with different places of expression. In addition to water, some AQPs allow the passage of glycerol and ammonia, being called Aquaglyceroproteins. In the central nervous system, AQPs 1 and 4 are expressed, being responsible for the water regulation in the blood-brain barrier. These two AQPs are believed to participate in the pathophysiological process that governs the behavior of various CNS diseases, such as trauma and primary tumors. More particularly, there are quite controversial data in the literature on the expression of AQP4 in tumors and its relationship with disease progression and treatment possibility.
Objective This paper aims to perform a literature review on the function and expression of AQP4 in the CNS and primary tumors of this system, to compile what is in the literature on the subject and raise new possible research hypotheses.
Methods The PUBMED platform was used for bibliographic survey using “Aquaporin 4,” “expression” and “astrocytomas” as keywords. Articles older than 2008 and articles that did not address AQP4 expression in astrocytomas were excluded. In the selected articles, the following topics were investigated: AQP4 structure, brain and tumor localization, and relationship with peritumoral edema.
Results Regarding the structure and location of AQP4, the literature presents two isoforms of AQP4: M1 and M23. Both form clusters of AQP4 called “orthogonal arrays of proteins - OAPs.” In the tumor tissue, the literature shows a decrease in the formation of OAPs and an increase in the expression of both AQP4 isoforms, besides losing their polarity, diffusing through the cytoplasmic membrane. As for the function of AQP4 in tumors, AQP4 assists in cell migration and invasion, in addition to participating in cell proliferation and apoptosis. Regarding the relationship with cerebral edema, there are controversial knowledge. Studies have shown that increased AQP4 aggravates cytotoxic edema of tumor cells and, by assisting in cell migration and angiogenesis, indirectly assist in the formation of vasogenic edema by breaking the blood-brain barrier. Other studies, however, point to the increase in AQP4 as a protective mechanism to combat vasogenic edema that occurs in tumor formation. Furthermore, the literature presents a therapeutic proposal in which, by inhibiting AQP4 expression, tumor migration and cerebral edema decrease in rats with glioblastoma.
Discussion As shown in the literature, there is a difference in histopathological structure between high and low grade gliomas. However, there are common changes between them. These common changes could then be used as a factor of severity or evolution of low-grade to high-grade tumors. Moreover, it is not yet possible to perceive the true relationship of AQP4 expression and increased VEGF evolution of peritumoral edema. Finally, it can be hypothesized that since the expression ratio between AQP4 isoforms in normal tissue is greater than in some tumors, the decrease in this ratio is due either to decreased M23 expression or increased of the isoform M1.
Conclusion Further studies are needed to understand the physiology and pathophysiology involving AQP4 in astrocytomas to create effective therapeutic proposals to combat this disease.
Resumo
Introdução As aquaporinas (AQPs) são uma família de proteínas de membrana que regulam a permeabilidade osmótica da membrana plasmática. Existem descritos na literatura um total de 13 tipos de aquaporinas em mamíferos, cada um com diferentes locais de expressão. Além da água, alguns AQPs permitem a passagem de glicerol e amônia, sendo chamados de aquagliceroproteínas. No sistema nervoso central, as AQPs 1 e 4 são expressas, sendo responsáveis pela regulação da água na barreira hematoencefálica. Acredita-se que esses dois AQPs participem do processo fisiopatológico que regula o comportamento de várias doenças do SNC, como trauma e tumores primários. Mais particularmente, há dados bastante controversos na literatura sobre a expressão de AQP4 em tumores e sua relação com a progressão da doença e possibilidade de tratamento.
Objetivo Este artigo tem como objetivo realizar uma revisão da literatura sobre a função e expressão da AQP4 no SNC e tumores primários deste sistema, a fim de compilar o que está na literatura sobre o assunto e levantar novas hipóteses de pesquisa possíveis.
Método A plataforma PUBMED foi utilizada para levantamento bibliográfico utilizando “Aquaporin 4,” “expression” e “astrocitomas” como palavras-chave. Artigos com idade superior a 2008 e artigos que não abordaram a expressão de AQP4 em astrocitomas foram excluídos. Nos artigos selecionados, foram investigados os seguintes tópicos: estrutura da AQP4, localização do cérebro e do tumor e relação com o edema peritumoral.
Resultados Em relação à estrutura e localização da AQP4, a literatura apresenta duas isoformas da AQP4: M1 e M23. Ambos formam aglomerados de AQP4 chamados “arranjos ortogonais de proteínas - OAPs.” No tecido tumoral, a literatura mostra uma diminuição na formação de OAPs e um aumento na expressão de ambas as isoformas AQP4, além de perder sua polaridade, difundindo através da membrana citoplasmática. Quanto à função da AQP4 nos tumores, a AQP4 auxilia na migração e invasão celular, além de participar da proliferação celular e apoptose. Em relação à relação com o edema cerebral, existem controvérsias. Estudos demonstram que o aumento da AQP4 agrava o edema citotóxico das células tumorais e, auxiliando na migração celular e na angiogênese, auxilia indiretamente na formação de edema vasogênico por quebra da barreira hematoencefálica. Outros estudos, no entanto, apontam para o aumento da AQP4 como mecanismo protetor para combater o edema vasogênico que ocorre na formação de tumores. Além disso, a literatura apresenta uma proposta terapêutica em que, ao inibir a expressão da AQP4, a migração tumoral e o edema cerebral diminuem em ratos com glioblastoma.
Discussão Como mostrado na literatura, há uma diferença na estrutura histopatológica entre os gliomas de alto e baixo grau. No entanto, existem mudanças comuns entre eles. Estas alterações comuns poderiam então ser usadas como um fator de gravidade ou evolução de tumores de baixo grau a alto grau. Além disso, ainda não é possível perceber a verdadeira relação entre a expressão da AQP4 e o aumento da evolução do VEGF no edema peritumoral. Finalmente, pode-se supor que, como a razão de expressão entre as isoformas de AQP4 no tecido normal é maior do que em alguns tumores, a diminuição dessa razão é devida à diminuição da expressão de M23 ou ao aumento da isoforma M1.
Conclusão: Novos estudos são necessários para compreender a fisiologia e a fisiopatologia da AQP4 em astrocitomas, a fim de criar propostas terapêuticas efetivas para combater essa doença.
Publikationsverlauf
Eingereicht: 18. April 2021
Angenommen: 16. Juni 2021
Artikel online veröffentlicht:
28. Juni 2023
© 2023. Sociedade Brasileira de Neurocirurgia. This is an open access article published by Thieme under the terms of the Creative Commons Attribution-NonDerivative-NonCommercial License, permitting copying and reproduction so long as the original work is given appropriate credit. Contents may not be used for commecial purposes, or adapted, remixed, transformed or built upon. (https://creativecommons.org/licenses/by-nc-nd/4.0/)
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References
- 1 Verkman AS. Aquaporins in clinical medicine. Annu Rev Med 2012; 63 (01) 303-316
- 2 Filippidis AS, Carozza RB, Rekate HL. Aquaporins in Brain Edema and Neuropathological Conditions. Int J Mol Sci 2016; 18 (01) 55
- 3 Lan Y-L, Wang X, Lou J-C, Ma X-C, Zhang B. The potential roles of aquaporin 4 in malignant gliomas. Oncotarget 2017; 8 (19) 32345-32355 http://www.oncotarget.com/fulltext/16017 cited2018Oct25 [Internet]
- 4 Noell S, Wolburg-Buchholz K, Mack AF. et al. Dynamics of expression patterns of AQP4, dystroglycan, agrin and matrix metalloproteinases in human glioblastoma. Cell Tissue Res 2012; 347 (02) 429-441
- 5 Saito M, Tanaka H, Sasaki M, Kurose H, Nakahata N. Involvement of aquaporin in thromboxane A2 receptor-mediated, G 12/13/RhoA/NHE-sensitive cell swelling in 1321N1 human astrocytoma cells. Cell Signal 2010; 22 (01) 41-46
- 6 Wang J, Feng L, Zhu Z. et al. Aquaporins as diagnostic and therapeutic targets in cancer: how far we are?. J Transl Med 2015; 13 (01) 96 http://www.translational-medicine.com/content/13/1/96 cited2019Sep23 [Internet]
- 7 Ding T, Gu F, Fu L, Ma Y-J. Aquaporin-4 in glioma invasion and an analysis of molecular mechanisms. J Clin Neurosci 2010; 17 (11) 1359-1361
- 8 Nico B, Mangieri D, Tamma R. et al. Aquaporin-4 contributes to the resolution of peritumoural brain oedema in human glioblastoma multiforme after combined chemotherapy and radiotherapy. Eur J Cancer 2009; 45 (18) 3315-3325
- 9 Zhao W-J, Zhang W, Li G-L, Cui Y, Shi Z-F, Yuan F. Differential expression of MMP-9 and AQP4 in human glioma samples. Folia Neuropathol 2012; 50 (02) 176-186
- 10 Ding T, Zhou Y, Sun K. et al. Knockdown a water channel protein, aquaporin-4, induced glioblastoma cell apoptosis. PLoS One 2013; 8 (08) e66751
- 11 Yool AJ, Brown EA, Flynn GA. Roles for novel pharmacological blockers of aquaporins in the treatment of brain oedema and cancer. Clin Exp Pharmacol Physiol 2010; 37 (04) 403-409
- 12 Smith AJ, Jin B-J, Ratelade J, Verkman AS. Aggregation state determines the localization and function of M1- and M23-aquaporin-4 in astrocytes. J Cell Biol 2014; 204 (04) 559-573
- 13 Noell S, Ritz R, Wolburg-Buchholz K, Wolburg H, Fallier-Becker P. An allograft glioma model reveals the dependence of aquaporin-4 expression on the brain microenvironment. PLoS One 2012; 7 (05) e36555
- 14 Maugeri R, Schiera G, Di Liegro CM, Fricano A, Iacopino DG, Di Liegro I. Aquaporins and Brain Tumors. Int J Mol Sci 2016; 17 (07) 1029
- 15 Fallier-Becker P, Nieser M, Wenzel U, Ritz R, Noell S. Is Upregulation of Aquaporin 4-M1 Isoform Responsible for the Loss of Typical Orthogonal Arrays of Particles in Astrocytomas?. Int J Mol Sci 2016; 17 (08) 1230
- 16 Noell S, Fallier-Becker P, Deutsch U, Mack AF, Wolburg H. Agrin defines polarized distribution of orthogonal arrays of particles in astrocytes. Cell Tissue Res 2009; 337 (02) 185-195
- 17 Nduom EK, Yang C, Merrill MJ, Zhuang Z, Lonser RR. Characterization of the blood-brain barrier of metastatic and primary malignant neoplasms. J Neurosurg 2013; 119 (02) 427-433
- 18 Li Y, Hu H, Liu J, Zhu Q, Gu R. Effects of aquaporin 4 and inward rectifier potassium channel 4.1 on medullospinal edema after methylprednisolone treatment to suppress acute spinal cord injury in rats. Acta Cir Bras 2018; 33 (02) 175-184
- 19 Ding T, Ma Y, Li W. et al. Role of aquaporin-4 in the regulation of migration and invasion of human glioma cells. Int J Oncol 2011; 38 (06) 1521-1531
- 20 Wolburg H, Noell S, Fallier-Becker P, Mack AF, Wolburg-Buchholz K. The disturbed blood-brain barrier in human glioblastoma. Mol Aspects Med 2012; 33 (5-6): 579-589
- 21 Mou K, Chen M, Mao Q. et al. AQP-4 in peritumoral edematous tissue is correlated with the degree of glioma and with expression of VEGF and HIF-alpha. J Neurooncol 2010; 100 (03) 375-383
- 22 Tan Y, Zhang H, Wang XC, Qin JB, Wang L. The value of multi ultra high-b-value DWI in grading cerebral astrocytomas and its association with aquaporin-4. Br J Radiol 2018; 91 (1086): 20170696
- 23 Isoardo G, Morra I, Chiarle G. et al. Different aquaporin-4 expression in glioblastoma multiforme patients with and without seizures. Mol Med 2012; 18 (01) 1147-1151
- 24 DeLay M, Jahangiri A, Carbonell WS. et al. Microarray analysis verifies two distinct phenotypes of glioblastomas resistant to antiangiogenic therapy. Clin Cancer Res 2012; 18 (10) 2930-2942
- 25 Tan Y, Zhang H, Zhao R-F, Wang X-C, Qin J-B, Wu X-F. Comparison of the values of MRI diffusion kurtosis imaging and diffusion tensor imaging in cerebral astrocytoma grading and their association with aquaporin-4. Neurol India 2016; 64 (02) 265-272
- 26 Wang D, Owler BK. Expression of AQP1 and AQP4 in paediatric brain tumours. J Clin Neurosci 2011; 18 (01) 122-127
- 27 Hong CS, Ho W, Piazza MG, Ray-Chaudhury A, Zhuang Z, Heiss JD. Characterization of the blood brain barrier in pediatric central nervous system neoplasms. J Interdiscip Histopathol 2016; 4 (02) 29-33
- 28 Schoenegger K, Oberndorfer S, Wuschitz B. et al. Peritumoral edema on MRI at initial diagnosis: an independent prognostic factor for glioblastoma?. Eur J Neurol 2009; 16 (07) 874-878
- 29 Fazzina G, Amorini AM, Marmarou CR. et al. The protein kinase C activator phorbol myristate acetate decreases brain edema by aquaporin 4 downregulation after middle cerebral artery occlusion in the rat. J Neurotrauma 2010; 27 (02) 453-461
- 30 Yang B, Zador Z, Verkman AS. Glial cell aquaporin-4 overexpression in transgenic mice accelerates cytotoxic brain swelling. J Biol Chem 2008; 283 (22) 15280-15286
- 31 Yang L, Wang X, Zhen S, Zhang S, Kang D, Lin Z. Aquaporin-4 upregulated expression in glioma tissue is a reaction to glioma-associated edema induced by vascular endothelial growth factor. Oncol Rep 2012; 28 (05) 1633-1638
- 32 Henker C, Kriesen T, Fürst K. et al. Effect of 10 different polymorphisms on preoperative volumetric characteristics of glioblastoma multiforme. J Neurooncol 2016; 126 (03) 585-592
- 33 Thrane AS, Rangroo Thrane V, Nedergaard M. Drowning stars: reassessing the role of astrocytes in brain edema. Trends Neurosci 2014; 37 (11) 620-628
- 34 Wang BF, Cui ZW, Zhong ZH. et al. Curcumin attenuates brain edema in mice with intracerebral hemorrhage through inhibition of AQP4 and AQP9 expression. Acta Pharmacol Sin 2015; 36 (08) 939-948