GLS1通过激活Nrf2/HO-1轴抑制过氧化氢诱导的ARPE-19细胞氧化应激、自噬与凋亡

目的探究GLS1对过氧化氢诱导的ARPE-19细胞氧化应激、自噬与凋亡的影响及机制。方法ARPE-19细胞分为对照组、H_(2)O_(2)组、H_(2)O_(2)+Vector组、H_(2)O_(2)+GLS1组,对照组细胞不做任何处理,H_(2)O_(2)组细胞用200μmol/L H_(2)O_(2)诱导48h,H_(2)O_(2)+Vector组和H_(2)O_(2)+GLS1组细胞转染Vector和GLS1质粒后用200μmol/L H_(2)O_(2)诱导48 h,比色法测定各组细胞SOD、GSH和MDA浓度,透射电镜观察各组细胞自噬小体,流式细胞术检测各组细胞凋亡水平,Western blot检测各组细胞Nrf2、HO-1、LC3-Ⅱ、p62的表达。结果与对照组比较,H_(2)O_(2)组ARPE-19细胞SOD、GSH表达显著下降,MDA显著增加,自噬小体数目显著增加,细胞凋亡显著增加,LC3-Ⅱ表达显著上调,P62、抗核因子红系2相关因子2(nuclear factor erythroid 2-related factor 2,Nrf2)、血红素氧合酶1(heme Oxygenase-1,HO-1)表达显著下调。与H_(2)O_(2)+Vector组比较,H_(2)O_(2)+GLS1组细胞SOD、GSH表达显著增加,MDA显著降低,自噬小体数目显著减少,细胞凋亡显著减少,LC3-Ⅱ表达显著下调,P62、Nrf2、HO-1表达显著上调。结论GLS1可抑制H_(2)O_(2)诱导的ARPE-19细胞氧化应激、自噬与凋亡,其机制为激活Nrf2/HO-1信号通路。

CITED2 and the modulation of the hypoxic response in cancer

CITED2(CBP/p300-interacting transactivator with Glu/Asp-rich C-terminal domain,2)is a ubiquitously expressed protein exhibiting a high affinity for the CH1 domain of the transcriptional co-activators CBP/p300,for which it competes with hypoxia-inducible factors(HIFs).CITED2 is particularly efficient in the inhibition of HIF-1α-dependent transcription in different contexts,ranging from organ development and metabolic homeostasis to tissue regeneration and immunity,being also potentially involved in various other physiological processes.In addition,CITED2 plays an important role in inhibiting HIF in some diseases,including kidney and heart diseases and type 2-diabetes.In the particular case of cancer,CITED2 either functions by promoting or suppressing cancer development depending on the context and type of tumors.For instance,CITED2 overexpression promotes breast and prostate cancers,as well as acute myeloid leukemia,while its expression is downregulated to sustain colorectal cancer and hepatocellular carcinoma.In addition,the role of CITED2 in the maintenance of cancer stem cells reveals its potential as a target in non-small cell lung carcinoma and acute myeloid leukemia,for example.But besides the wide body of evidence linking both CITED2 and HIF signaling to carcinogenesis,little data is available regarding CITED2 role as a negative regulator of HIF-1αspecifically in cancer.Therefore,comprehensive studies exploring further the interactions of these two important mediators in cancer-specific models are sorely needed and this can potentially lead to the development of novel targeted therapies.

Downregulation of miR-491-5p promotes neovascularization after traumatic brain injury

Micro RNA-491-5 p(miR-491-5 p) plays an important role in regulating cell proliferation and migration;however,the effect of miR-491-5 p on neovascularization after traumatic brain injury remains poorly understood.In this study,a controlled cortical injury model in C57 BL/6 mice and an oxygen-glucose deprivation model in microvascular endothelial cells derived from mouse brain were established to simulate traumatic brain injury in vivo and in vitro,respectively.In the in vivo model,quantitative real-time-polymerase chain reaction results showed that the expression of miR-491-5 p increased or decreased following the intracerebroventricular injection of an miR-491-5 p agomir or antagomir,respectively,and the expression of miR-491-5 p decreased slightly after traumatic brain injury.To detect the neuroprotective effects of miR-491-p,neurological severity scores,Morris water maze test,laser speckle techniques,and immunofluorescence staining were assessed,and the results revealed that miR-491-5 p downregulation alleviated neurological dysfunction,promoted the recovery of regional cerebral blood flow,increased the number of lectin-stained microvessels,and increased the survival of neurons after traumatic brain injury.During the in vitro experiments,the potential mechanism of miR-491-5 p on neovascularization was explored through quantitative real-time-polymerase chain reaction,which showed that miR-491-5 p expression increased or decreased in brain microvascular endothelial cells after transfection with an miR-491-5 p mimic or inhibitor,respectively.Dual-luciferase reporter and western blot assays verified that metallothionein-2 was a target gene for miR-491-5 p.Cell counting kit 8(CCK-8) assay,flow cytometry,and 2′,7′-dichlorofluorescein diacetate(DCFH-DA) assay results confirmed that the downregulation of miR-491-5 p increased brain microvascular endothelial cell viability,reduced cell apoptosis,and alleviated oxidative stress under oxygen-glucose deprivation conditions.Cell scratch assay,Transwell assay,tube formation assay,and western blot assay results demonstrated that miR-491-5 p downregulation promoted the migration,proliferation,and tube formation of brain microvascular endothelial cells through a metallothionein-2-dependent hypoxia-inducible factor-1α/vascular endothelial growth factor pathway.These findings confirmed that miR-491-5 p downregulation promotes neovascularization,restores cerebral blood flow,and improves the recovery of neurological function after traumatic brain injury.The mechanism may be mediated through a metallothionein-2-dependent hypoxia-inducible factor-1α/vascular endothelial growth factor signaling pathway and the alleviation of oxidative stress.All procedures were approved by Ethics Committee of the First Affiliated Hospital of Chongqing Medical University,China(approval No.2020-304) on June 22,2020.

A Correlative Study between CT Perfusion Parameters and Angiogenesis in Rabbit VX2 Liver Tumors

Objective: The purpose of this study was to evaluate the correlation between CT perfusion parameters and the hypoxia-inducible factor-1 alpha (HIF-1α), vascular en-dothelial growth factor (VEGF), matrix metalloproteinase-2 (MMP-2) and microvessel density (MVD) marked by CD34 molecular of rabbit VX2 liver tumors and to investigate the value of CT perfusion imaging in evaluating tumor angiogenesis. Material and methods: Twenty-four cases of rabbit VX2 liver tumor were performed by CT perfusion scanning. Hepatic artery perfusion (HAP), portal vein perfusion (PVP), total hepatic blood flow (THBF) and hepatic perfusion index (HPI) were measured by perfusion software. HIF-1α, VEGF and MMP-2 expression and MVD were detected in the 24 rabbit VX2 liver tumor tissue samples using immunohistochemical method. The correlation between the HIF-1α, VEGF, MMP-2 expression and MVD and CT perfusion parameters were analyzed. Results: Correlation analysis revealed that the expression of HIF-1α, MMP-2, MVD were positively related to the HAP, THBF, HPI (p < 0.01), but no relations with PVP (p > 0.05);and correlation analysis revealed that the expression of VEGF was positively related to the HAP, HPI (p 0.05). There was a positive relationship between the expression of HIF-1α, VEGF, MMP-2 and MVD (p < 0.01). Conclusions: CT perfusion imaging can reflect the blood perfusion of the rabbit VX2 liver tumors and evaluate the information of angiogenesis about tumors.

合并阻塞型睡眠呼吸暂停低通气综合征的结直肠癌患者的肠道菌群状况及其慢性间歇性缺氧状况与病理特征的关系

目的分析合并阻塞型睡眠呼吸暂停低通气综合征(OSAHS)的结直肠癌患者肠道菌群状况和病理特征。方法选择100例患者或体检者作为研究对象,其中健康者(对照组)、结直肠癌合并OSAHS患者(结直肠癌+OSAHS组)、单纯结直肠癌患者(结直肠癌组)、单纯OSAHS患者(OSAHS组)各25例。采集所有研究对象的粪便标本,检测并对比各组肠道菌群集落数。检测结直肠癌患者癌组织以及非结肠癌者肠黏膜组织的缺氧诱导因子1(HIF-1)、谷氨酰胺酶2(GLS2)的表达情况。比较4组HIF-1和GLS2的阳性率,以及结肠癌患者癌组织、癌旁组织HIF-1、GLS2表达阳性率的差异。分析结直肠癌+OSAHS患者临床病理特征与HIF-1、GLS2表达水平的关系。结果结直肠癌+OSAHS组、结直肠癌组、OSAHS组、对照组的乳酸杆菌集落数依次升高,大肠埃希菌集落数依次降低;结直肠癌+OSAHS组、结直肠癌组的脆弱拟杆菌、粪肠球菌集落数均高于OSAHS组、对照组,双歧杆菌集落数均低于OSAHS组、对照组(均P<0.05)。与对照组比较,结直肠癌+OSAHS组、结直肠癌组、OSAHS组的HIF-1、GLS2表达阳性率均升高(均P<0.05)。结直肠癌患者癌组织HIF-1、GLS2表达阳性率高于癌旁组织(均P<0.05)。结直肠癌+OSAHS患者中,浸润深度大、Dukes分期高、合并淋巴结转移的患者的GLS2阳性率升高,合并淋巴结转移的患者的HIF-1阳性率升高(均P<0.05)。结论合并OSAHS的结直肠癌患者存在明显的肠道菌群紊乱,OSAHS可能通过影响肠道菌群引起结直肠癌,并与其病理特征密切相关。

Melatonin combined with exercise cannot alleviate cerebral injury in a rat model of focal cerebral ischemia/reperfusion injury

Previous studies have demonstrated that melatonin combined with exercise can alleviate secondary damage after spinal cord injury in rats. Therefore, it is hypothesized that melatonin combined with exercise can also alleviate ischemic brain damage. In this study, adult rats were subjected to right middle cerebral artery occlusion after receiving 10 mg/kg melatonin or vehicle subcutaneously twice daily for 14 days. Forced exercise using an animal treadmill was performed at 20 m/min for 30 minutes per day for 6 days prior to middle cerebral artery occlusion. After middle cerebral artery occlusion, each rat received melatonin combined with exercise, melatonin or exercise alone equally for 7 days until sacrifice. Interestingly, rats receiving melatonin combined with exercise exhibited more severe neurological deficits than those receiving melatonin or exercise alone. Hypoxia-inducible factor la mRNA in the brain tissue was upregulated in rats receiving melatonin combined with exercise. Similarly, microtubule associated protein-2 mRNA expression was significantly upregulated in rats receiving melatonin alone. Chondroitin sulfate proteoglycan 4 （NG2） mRNA expression was significantly decreased in rats receiving melatonin combined with exercise as well as in rats receiving exercise alone. Furthermore, neural cell loss in the primary motor cortex was significantly reduced in rats receiving melatonin or exercise alone, but the change was not observed in rats receiving melatonin combined with exercise. These findings suggest that excessive intervention with melatonin, exercise or their combination may lead to negative effects on ischemia/reperfusion-induced brain damage.

Analysis of isocitrate dehydrogenase-1/2 gene mutations in gliomas

Objective To highlight recent researches which may show promise for histomolecular classification and new treatments for gliomas.Data sources All articles cited in this review were mainly searched from PubMed, which were published in English from 1996 to 2010.Study selection Original articles and critical reviews selected were relevant to the isocitrate dehydrogenase-1/2 mutation in gliomas and other tumors.Results Extraordinary high rates of somatic mutations in isocitrate dehydrogenase-1/2 occur in the majority of World Health Organization grade Ⅱ and grade Ⅲ gliomas as well as grade Ⅳ secondary glioblastomas. Isocitrate dehydrogenase-1/2 mutations are associated with younger age at diagnosis and a better prognosis in patients with mutated tumors. The functional role of isocitrate dehydrogenase-1/2 mutations in the pathogenesis of gliomas is still unclear.Conclusion Isocitrate dehydrogenase-1/2 mutations define a specific subtype of gliomas and may have great significance in the diagnosis, prognosis, and treatment of patients with these tumors.