Department of Biomedical Sciences, Charles E. Schmidt College of Medicine, Florida Atlantic University, Boca Raton, FL, 33431, USA.
Program in Integrative Biology, Florida Atlantic University, Boca Raton, FL, 33431, USA.
J Biomed Sci. 2020 Oct 30;27(1):99. doi: 10.1186/s12929-020-00692-5.
Global ischemia is the resulting effect of a cardiopulmonary arrest (CPA). Presently there is no effective treatment to address neurological deficits in patients who survived a CPA. Granulocyte-colony stimulating factor is a growth factor (G-CSF) with a plethora of beneficial effects, including neuroprotection. Clinical application of human G-CSF (hG-CSF) is limited due to its plasma half-life of 4 h. Therefore, novel approaches need to be investigated that would (1) enable prolonged manifestation of hG-CSF and (2) demonstrate G-CSF efficacy from studying the underlying protective mechanisms of hG-CSF. In our previous work, we used the self-complementary adeno-associated virus (stereotype2: scAAV2) as a vector to transfect the hG-CSF gene into the global ischemic brain of a mouse. As an extension of that work, we now seek to elucidate the protective mechanisms of hG-CSF gene therapy against endoplasmic reticulum induced stress, mitochondrial dynamics and autophagy in global ischemia.
A single drop of either AAV-CMV-hG-CSF or AAV-CMV-GFP was dropped into the conjunctival sac of the Swiss Webster mouse's left eye, 30-60 min after bilateral common artery occlusion (BCAO). The efficacy of the expressed hG-CSF gene product was analyzed by monitoring the expression levels of endoplasmic reticulum stress (ER), mitochondrial dynamics and autophagic proteins over 4- and 7-days post-BCAO in vulnerable brain regions including the striatum, overlying cortex (frontal brain regions) and the hippocampus (middle brain regions). Statistical analysis was performed using mostly One-Way Analysis of variance (ANOVA), except for behavioral analysis, which used Repeated Measures Two-Way ANOVA, post hoc analysis was performed using the Tukey test.
Several biomarkers that facilitated cellular death, including CHOP and GRP78 (ER stress) DRP1 (mitochondrial dynamics) and Beclin 1, p62 and LC3-ll (autophagy) were significantly downregulated by hG-CSF gene transfer. hG-CSF gene therapy also significantly upregulated antiapoptotic Bcl2 while downregulating pro-apoptotic Bax. The beneficial effects of hG-CSF gene therapy resulted in an overall improvement in functional behavior.
Taken together, this study has substantiated the approach of sustaining the protein expression of hG-CSF by eye drop administration of the hG-CSF gene. In addition, the study has validated the efficacy of using hG-CSF gene therapy against endoplasmic reticulum induced stress, mitochondrial dynamics and autophagy in global ischemia.
全球缺血是心肺骤停(CPA)的结果。目前,没有有效的治疗方法来解决 CPA 后幸存患者的神经功能缺损。粒细胞集落刺激因子(G-CSF)是一种具有多种有益作用的生长因子,包括神经保护作用。由于其血浆半衰期为 4 小时,因此临床应用人 G-CSF(hG-CSF)受到限制。因此,需要研究新的方法,这些方法将(1)能够延长 hG-CSF 的表现,(2)通过研究 hG-CSF 的潜在保护机制来证明 G-CSF 的疗效。在我们之前的工作中,我们使用自我互补腺相关病毒(2 型:scAAV2)作为载体将 hG-CSF 基因转染到小鼠的全脑缺血脑内。作为这项工作的延伸,我们现在旨在阐明 hG-CSF 基因治疗对全脑缺血诱导的内质网应激、线粒体动力学和自噬的保护机制。
在双侧颈总动脉闭塞(BCAO)后 30-60 分钟,将 AAV-CMV-hG-CSF 或 AAV-CMV-GFP 的一滴滴入瑞士 Webster 小鼠左眼的结膜囊中。通过监测易损脑区(纹状体、覆盖皮层(额叶脑区)和海马体(中脑脑区))的内质网应激(ER)、线粒体动力学和自噬蛋白的表达水平,分析表达的 hG-CSF 基因产物的疗效。统计分析主要采用单向方差分析(ANOVA),除行为分析采用重复测量双向方差分析外,采用 Tukey 检验进行事后分析。
几种促进细胞死亡的生物标志物,包括 CHOP 和 GRP78(内质网应激)DRP1(线粒体动力学)和 Beclin 1、p62 和 LC3-ll(自噬),通过 hG-CSF 基因转移显著下调。hG-CSF 基因治疗还显著上调了抗凋亡 Bcl2,同时下调了促凋亡 Bax。hG-CSF 基因治疗的有益效果导致功能行为的整体改善。
综上所述,这项研究证实了通过滴眼给予 hG-CSF 基因来维持 hG-CSF 蛋白表达的方法。此外,该研究验证了使用 hG-CSF 基因治疗对抗全脑缺血诱导的内质网应激、线粒体动力学和自噬的疗效。
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