Adrenergic receptors blockade alleviates dexamethasone-induced neurotoxicity in adult male Wistar rats: Distinct effects on β-arrestin2 expression and molecular markers of neural injury.

IF 2.5 4区 医学 Q3 PHARMACOLOGY & PHARMACY
DARU Journal of Pharmaceutical Sciences Pub Date : 2024-06-01 Epub Date: 2023-11-15 DOI:10.1007/s40199-023-00490-y
Rasha M S M Mohamed, Enssaf Ahmad Ahmad, Dalia M Amin, Samar Ahmed Abdo, Islam A A E-H Ibrahim, Mona F Mahmoud, Shimaa Abdelaal
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引用次数: 0

Abstract

Background: Dexamethasone-induced neurotoxicity has been previously reported. However, the molecular mechanisms are still not completely understood.

Objectives: The current work aimed to investigate the modulatory effects of α- and β-adrenergic receptors on dexamethasone-induced neurotoxicity in rats focused on changes in β-arrestin2 and molecular markers of neural injury in cerebral cortex.

Methods: Male Wistar rats were subcutaneously injected with dexamethasone (10 mg/kg/day) for 7 days to induce neural injury in the cerebral cortex. The experiment involved 5 groups: control, dexamethasone, carvedilol, propranolol, and doxazosin. In the last 3 groups, drugs were given 2 hours before dexamethasone injection. At the end of experiment, brain samples were collected for measurement of brain derived neurotrophic factor (BDNF), glial fibrillary acidic protein (GFAP), kinase activity of protein kinase B (Akt), diacylglycerol (DAG), α-smooth muscle actin (α-SMA), Smad3, β-amyloid and phospho-tau protein levels in addition to histopathological examination of brain tissue using hematoxylin-eosin, Nissl, and Sirius red stains. Moreover, β-arrestin2 levels in the cerebral cortex were measured using immunohistochemical examination.

Results: Dexamethasone slightly reduced brain weight and significantly decreased BDNF, Akt kinase activity and β-arrestin2 but markedly induced degeneration of cortical neurons and significantly increased GFAP, DAG, α-SMA, Smad3, β-amyloid and phospho-tau protein levels compared to controls. Carvedilol, propranolol, and doxazosin reversed all dexamethasone-induced molecular changes and slightly ameliorated the histopathological changes. Carvedilol significantly increased brain weight and β-arrestin2 levels compared to dexamethasone, propranolol, and doxazosin groups.

Conclusion: blocking α- and/or β-adrenergic receptors alleviate dexamethasone-induced neurotoxicity despite their distinct effects on β-arrestin2 levels in the cerebral cortex.

Abstract Image

肾上腺素能受体阻断减轻地塞米松诱导的成年雄性Wistar大鼠神经毒性:对β-arrestin2表达和神经损伤分子标志物的显著影响。
背景:地塞米松引起的神经毒性先前已有报道。然而,其分子机制尚不完全清楚。目的:研究α-和β-肾上腺素能受体对地塞米松诱导大鼠神经毒性的调节作用,重点研究脑皮层中β-阻滞蛋白2和神经损伤分子标志物的变化。方法:雄性Wistar大鼠皮下注射地塞米松(10 mg/kg/d) 7 d,诱导大脑皮层神经损伤。实验分为5组:对照组、地塞米松组、卡维地洛组、心得安组、多沙唑嗪组。后3组均在地塞米松注射前2 h给药。实验结束后,采集脑组织标本,测定脑源性神经营养因子(BDNF)、胶质纤维酸性蛋白(GFAP)、蛋白激酶B (Akt)激酶活性、二酰基甘油(DAG)、α-平滑肌肌动蛋白(α-SMA)、Smad3、β-淀粉样蛋白和磷酸化tau蛋白水平,并采用苏木精-伊红、尼索和天狼星红染色对脑组织进行组织病理学检查。免疫组化检测大鼠大脑皮层β-arrestin2水平。结果:与对照组相比,地塞米松轻度减轻脑重量,显著降低BDNF、Akt激酶活性和β-arrestin2,但显著诱导皮质神经元变性,显著增加GFAP、DAG、α-SMA、Smad3、β-淀粉样蛋白和磷酸化tau蛋白水平。卡维地洛、心得安和多沙唑嗪逆转了所有地塞米松诱导的分子变化,并略微改善了组织病理学变化。与地塞米松、心得安和多沙唑嗪组相比,卡维地洛显著增加了脑重量和β-抑制素2水平。结论:阻断α-和/或β-肾上腺素能受体可减轻地塞米松诱导的神经毒性,尽管它们对大脑皮层β-阻滞2水平有明显影响。
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来源期刊
DARU Journal of Pharmaceutical Sciences
DARU Journal of Pharmaceutical Sciences PHARMACOLOGY & PHARMACY-
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期刊介绍: DARU Journal of Pharmaceutical Sciences is a peer-reviewed journal published on behalf of Tehran University of Medical Sciences. The journal encompasses all fields of the pharmaceutical sciences and presents timely research on all areas of drug conception, design, manufacture, classification and assessment. The term DARU is derived from the Persian name meaning drug or medicine. This journal is a unique platform to improve the knowledge of researchers and scientists by publishing novel articles including basic and clinical investigations from members of the global scientific community in the forms of original articles, systematic or narrative reviews, meta-analyses, letters, and short communications.
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