Association between renin-angiotensin system inhibitor and the risk of CMV pneumonia:a Mendelian randomization study

Background:Cytomegalovirus(CMV)reactivation is linked to a high mortality rate,especially among the elderly.Prior research suggests that renin-angiotensin system(RAS)inhibitors may influence both the onset and prognosis of pneumonia.This study aims to examine the causal relationship between RAS inhibitor use and the risk of CMV pneumonia using Mendelian randomization(MR)analysis.Methods:We conducted an analysis using data from two genome-wide association studies(GWAS)involving individuals of European ancestry.This dataset included individuals treated with RAS inhibitors and those with CMV pneumonia.We assessed the relationship between RAS inhibitor use and CMV pneumonia risk using the inverse variance weighted(IVW)method.The results were further evaluated for pleiotropy,heterogeneity,and robustness.Results:The Mendelian randomization(MR)analysis revealed a causal relationship between RAS inhibitor use and an increased risk of CMV pneumonia(IVW:odds ratio[OR]=2.73;95%confidence interval[CI]=1.11-6.73;P=0.028).Conclusions:Our finding indicate a positive causal relationship between the use of RAS inhibitors and the onset of CMV pneumonia.

血清α1-抗胰蛋白酶、血管紧张素-Ⅱ与获得性免疫缺陷综合征患者预后的关系

目的探讨血清α1-抗胰蛋白酶(α1-AT)、血管紧张素-Ⅱ(Ang-Ⅱ)与获得性免疫缺陷综合征(AIDS)患者预后的关系。方法将该院2019年5月至2022年5月收治的97例首诊AIDS患者纳入研究作为研究组,另选取同期于该院进行体检的健康者97例作为对照组。根据病历收集患者临床资料。对纳入研究者进行α1-AT、Ang-Ⅱ水平检测,并进行分组比较。对纳入研究的AIDS患者进行为期1年的随访,观察患者预后情况,并比较不同预后患者的α1-AT、Ang-Ⅱ水平。采用单因素及多因素Logistic回归分析影响AIDS患者预后的因素。用受试者工作特征(ROC)曲线分析α1-AT、Ang-Ⅱ水平对患者预后的预测效能。结果研究组血清α1-AT和Ang-Ⅱ水平高于对照组(P<0.05)。AIDS患者1年内的预后不良发生率为23.71%(23/97)。预后不良患者血清α1-AT和Ang-Ⅱ水平高于预后良好患者(P<0.05)。单因素分析显示,预后不良患者C反应蛋白(CRP)水平、淋巴细胞计数水平、合并淋巴瘤者所占比例均高于预后良好患者,清蛋白(ALB)水平低于预后良好患者(P<0.05)。多因素Logistic回归分析显示,合并淋巴瘤(OR=2.087)、高α1-AT水平(OR=2.611)、高Ang-Ⅱ水平(OR=2.138)是影响患者预后的独立危险因素(P<0.05)。ROC曲线分析显示,α1-AT预测AIDS患者预后的曲线下面积(AUC)为0.778,Ang-Ⅱ预测的AUC为0.798,α1-AT联合Ang-Ⅱ预测的AUC为0.918。结论α1-AT和Ang-Ⅱ在AIDS患者血清中水平异常升高,而且与患者预后有关,是影响患者预后的独立危险因素。α1-AT和Ang-Ⅱ联合检测可有效预测患者预后。

The Beneficial Effect of Renin-Angiotensin-Aldosterone System Blockade in Treatment of Hypertension, Resistant to Conventional Antihypertensives, in Patients on Maintenance Hemodialysis

Background: Hypertension (HTN) is present in up to 90% of end stage kidney disease (ESRD) patients irrespective of the etiology of their kidney disease. Moreover, it is an important modifiable risk factor for progression to ESRD and its overall cardiovascular morbidity and mortality. Objective: to evaluate, prospectively, the role of Renin-Angiotensin-Aldosterone System blockade (RAAS) in HTN, resistant to 3 conventional antihypertensives, in patients on maintenance hemodialysis (MHD). Patients and methods: A total of 52 such patients were treated with Ramipril and 5 with Losartan after intolerable cough/shortness of breath following Ramipril-use. None of the patients had fluid depletion, renal artery stenosis and primary endocrinopathy. The study group was compared to a matched control group of MHD patients with normal blood pressure following 3 drugs-combination therapies. Results: All patients, with resistant HTN, had significant activation of RAAS system prior to treatment compared to inactive one in the control group. In those with resistant HTN, control of HTN, was established within 2 weeks of therapy and was associated with suppression of the RAAS. Such therapy was associated with minor side effects. Conclusion: Our study has shown that RAAS blockade is safe and effective in controlling such resistant HTN in MHD patients.

Effect of Topical Propranolol Gel on Plasma Renin,Angiotensin Ⅱ and Vascular Endothelial Growth Factor in Superficial Infantile Hemangiomas

The effect of topical propranolol gel on the levels of plasma renin,angiotensin Ⅱ（ATⅡ） and vascular endothelial growth factor（VEGF） in superficial infantile hemangiomas（IHs） was investigated. Thirty-three consecutive children with superficial IHs were observed pre-treatment,1 and 3 months after application of topical propranolol gel for the levels of plasma renin,AT Ⅱand VEGF in Department of General Surgery of Dongfang Hospital from February 2013 to February 2014. The plasma results of IHs were compared with those of 30 healthy infants of the same age from out-patient department. The clinical efficiency of topical propranolol gel at 1st,and 3rd month after application was 45%,and 82% respectively. The levels of plasma renin,AT and VEGF in patients preⅡ-treatment were higher than those in healthy infants（565.86±49.66 vs. 18.19±3.56,3.20±0.39 vs 0.30±0.03,and 362.16±27.29 vs. 85.63±8.14,P〈0.05）. The concentrations of VEGF and renin at 1st and 3rd month after treatment were decreased obviously as compared with those pre-treatment（271.51±18.59 vs. 362.16±27.29,and 405.18±42.52 vs. 565.86±49.66 P〈0.05; 240.80±19.89 vs. 362.16±27.29,and 325.90±35.78 vs. 565.86±49.66,P〈0.05,respectively）,but the levels of plasma AT declined slightly Ⅱ（2.96±0.37 vs. 3.20±0.39,and 2.47±0.27 vs. 3.20±0.39,P〉0.05）. It was indicated that the increased renin,AT Ⅱand VEGF might play a role in the onset or development of IHs. Propranolol gel may suppress the proliferation of IHs by reducing VEGF.

The Comparison Study of Renin and Angiotensin AⅡ Levels on Normal Tension Glaucoma Patients and Normal Individuals

Purpose: To investigate the levels of renin-angiotension system (RAS) components in normal tension glaucoma patients and normal controls. Methods: Blood samples were obtained from 11 normal tension glaucoma(NTG)patients and 11 age and sex matched controls. The levels of renin and angiotensin AⅡof 11 NTG patients and normal controls were examined by radio-immunity test. Statistical analyses were performed by paired t test. Results:The levels of renin of NTG patients and normal controls are (769.085±183.217) pg/ml/n and (822.035 ±124.140) pg/ml/n, while the levels of angiotensin A Ⅱof NTG patients and normal controls are (37.347±10.669)pg/ml and (24.836±10.665)pg/ml respectively. No statistically significant differences were observed between the levels of renin and angiotensin among NTG patients and normal controls. Conclusion: There were not many abnormalities of the levels of circulating rennin and angiotensin AⅡof NTG patients in our study. Eye Science 2005 ;21 :192-195.

Angiotensin II administration in severe thrombocytopenia and chronic venous thrombosis:A case report

BACKGROUND The initial trials on angiotensin II(AT II)administration indicated a high incidence of thrombocytopenia and thrombosis,as well as a positive correlation between hyperreninemia and response to the medication.CASE SUMMARY We describe a case of a patient presenting with catecholamine resistant septic shock,thrombocytopenia,deep vein thrombosis,and normal renin concentration who responded immediately to AT II treatment.We observed no worsening of thrombocytopenia and no progression of thrombosis or additional thromboses during treatment.CONCLUSION Our case underscores the need for individualized assessment of patients for potential therapy with AT II.

基于转录组学及表观遗传组学筛选与血管紧张素-Ⅱ相关的胸主动脉瘤/夹层诊断标志物

目的探讨基于转录组学及表观遗传组学筛选与血管紧张素-Ⅱ(Ang-Ⅱ)作用相关的胸主动脉瘤/夹层(Thoracic aortic aneurysms/dissection,TAAD)诊断标志物。方法利用数据集GSE35627筛选Ang-Ⅱ作用于大鼠原代主动脉平滑肌细胞的差异表达基因(DEGs)。取与Ang-Ⅱ相关数据集DEGs的交集,使用GeneMANIA数据库对交集基因进行功能分析和DO分析。使用R软件ChAMP包分析正常人和主动脉夹层(AD)患者升主动脉组织的表观基因组数据集GSE84274的差异甲基化水平,分析关键DEGs甲基化水平。使用人胸主动脉瘤(TAA)外周血样本全基因组基因表达谱数据集GSE9106 testing组绘制受试者工作特征曲线(ROC),预测诊断的有效性。结果在细胞水平、动物模型和TAAD临床病例的基础上,从GSE35627、GSE64613和GSE52093数据集得到6个交集基因:SLC7A8、WISP1、IL1R1、BCAT1、NID2及ATOH8。表观遗传组学分析发现,WISP1和NID2分别有5个和3个差异甲基化位点(DMPs)的甲基化水平存在明显差异。ROC曲线验证结果显示,WISP1的AUC为0.7,其特异度和敏感度较强,具有较高的准确性。结论通过转录组学及表观遗传组学分析可知,Ang-Ⅱ相关基因WISP1和NID2有助于TAAD的早期诊断。

妊娠高血压患者血管紧张素Ⅱ及AT1R、AT2R的表达及意义

目的:探讨妊娠高血压(HDCP)患者血管紧张素Ⅱ(AngⅡ)及AngⅡ受体-1(AT1R)和AngⅡ受体-2(AT2R)的表达及意义。方法:选取2021年1月—2022月年9月孝感市中心医院收治的90例HDCP患者作为观察组,并将观察组根据病情程度分为HDCP组、轻度子痫前期组和重度子痫前期组3个亚组,将同期产检的90例健康孕妇作为对照组。检测并比较观察组与对照组、观察组不同亚组AngⅡ水平、AT1R和AT2R阳性表达情况。结果:观察组产前母血、产后脐血AngⅡ水平低于对照组,产后母血AngⅡ水平、AT1R、AT2R总阳性率高于对照组,差异有统计学意义(P<0.05)。不同病情程度HDCP患者产前母血、产后脐血AngⅡ水平比较,HDCP组>轻度子痫前期组>重度子痫前期组;不同病情程度HDCP患者产后母血AngⅡ水平比较,HDCP组<轻度子痫前期组<重度子痫前期组;不同病情程度HDCP患者AT1R、AT2R阳性情况比较,HDCP组<轻度子痫前期组<重度子痫前期组,差异有统计学意义(P<0.05)。结论:HDCP患者母血、脐血AngⅡ存在异常表达,其AT1R、AT2R阳性率随病情加重而升高,检测上述指标有助于为HDCP发病机制、早期诊断与治疗提供参考。

三黄一龙汤对佐剂性关节炎继发心血管病变大鼠血管紧张素Ⅱ、醛固酮及相关炎性因子的影响

目的:探讨三黄一龙汤对佐剂性关节炎大鼠心脏的病理组织学、肾素-血管紧张素-醛固酮系统(RAAS)效应因子血管紧张素Ⅱ(AngⅡ)、醛固酮(ALD)和炎性因子肿瘤坏死因子-α(TNF-α)、白细胞介素-6(IL-6)表达的影响,探讨三黄一龙汤对佐剂性关节炎大鼠继发心血管病变的干预作用及调节机制。方法:70只Wistar健康雌性大鼠按照随机数字表法分为正常组、模型组、阳性药物组、三黄一龙汤低剂量组、三黄一龙汤中剂量组、三黄一龙汤高剂量组和安慰剂组,每组10只。除正常组,其余各组大鼠建立佐剂性关节炎模型。三黄一龙汤低剂量组、三黄一龙汤中剂量组、三黄一龙汤高剂量组分别给予每日生药量19.8、39.6、79.2 g/kg灌胃,阳性药物组给予来氟米特2.1 mg/kg灌胃,安慰剂组灌胃等量生理盐水,连续干预4周。苏木精-伊红(HE)染色观察心脏的病理组织学变化,酶联免疫吸附测定法、蛋白印迹法和免疫组化法检测外周血和心脏组织AngⅡ、ALD、TNF-α和IL-6的变化。结果:病理结果显示,相对于正常组,模型组继发心肌损伤,主要表现为心肌组织发生局部炎症,局部心肌细胞排列紊乱,个别大鼠心肌有轻微间质水肿。方药三黄一龙汤能够显著改善心肌损伤,使其炎症病灶缩小,水肿程度减轻,下调心脏组织AngⅡ和ALD的表达(P<0.05),降低外周血和心脏组织TNF-α、IL-6水平(P<0.05)。结论:方药三黄一龙汤可能通过抑制RAAS中AngⅡ和ALD的表达,减少TNF-α、IL-6的产生,从而缓解佐剂性关节炎继发的心血管病变。

羟基红花黄色素A抑制血管紧张素Ⅱ介导的心脏成纤维细胞肌化

目的研究羟基红花黄色素A对血管紧张素Ⅱ介导的心脏成纤维细胞向肌成纤维细胞转化的影响。方法实验细胞随机分为正常对照组、Ang-Ⅱ组、Ang-Ⅱ+HSYA(5μM)组、Ang-Ⅱ+HSYA(25μM)组、Ang-Ⅱ+HSYA(50μM)组和Ang-Ⅱ+HSYA(100μM)组。使用划痕实验和Transwell小室侵袭实验检测细胞迁移侵袭情况,DCFH-DA荧光探针检测细胞内活性氧(reactive oxygenspecies,ROS)水平,Western blot检测α-SMA、CollagenⅠ、CollagenⅢ及转化生长因子β1(transforming growthfactor-β1,TGF-β1)的蛋白表达水平。结果Ang-Ⅱ促进心脏成纤维细胞迁移、增加ROS产生;而HSYA抑制了Ang-Ⅱ介导的心脏成纤维细胞迁移以及ROS产生;Western blot发现HSYA抑制了Ang-Ⅱ介导的心脏成纤维细胞α-SMA、CollagenⅠ、CollagenⅢ及TGF-β1的蛋白表达,差异具有统计学意义(P<0.05)。结论HSYA通过减少ROS的产生和下调TGF-β1信号通路抑制Ang-Ⅱ诱导心肌成纤维细胞向肌成纤维细胞分化。

Protective effects of icariin on human umbilical vein endothelial cell injured by angiotensin Ⅱ

To investigate the effects of icariin （ICA） on angiotensin Ⅱ（Ang Ⅱ）-induced injury in human umbilical vein endothelial cells line （ECV-304）. The ECV-304 cells were cultured in vitro. After 24 h incubating with icariin, the model of AngⅡ-induced injury in ECV-304 was established. The cell viability （MTT method）, Lactate dehydrogenase （LDH） release and Nitric oxide （NO） production in the medium, the capacity of scavenging superoxide anion radicals （O2^-） and hydroxyl radicals （.OH） were measured. The activities of superoxide dismutase （SOD）, total nitric oxide synthase （T-NOS）, inducible nitric oxide synthase （iNOS） and constitutive nitric oxide synthase （cNOS） in the cells were determined. Compared with the Ang Ⅱ-treated group, ICA can significantly raise the viability of EC, increase the activities of SOD, T-NOS and cNOS, increase the production of NO, enhance the capacity of scavenging superoxide anion radicals （ O2^- ） and hydroxyl radicals（.OH）, and lower LDH leakage and iNOS activity. The results suggest that ICA can protect endothelial cells （ECV-304） from Ang II-induced injury.

木犀草素抑制AngiotensinⅡ诱导的心肌细胞肥大

研究木犀草素对血管紧张素Ⅱ诱导乳鼠心肌细胞肥大的作用。用(1—3)d新生大鼠分离心肌细胞;用徕卡倒置显微镜抓获心肌细胞图像以测量细胞直径;用BCA蛋白检测法测定心肌细胞蛋白质含量;以[3H]苯丙氨酸掺入法测定心肌细胞的蛋白质合成率。0.1μmol血管紧张素Ⅱ引起了心肌细胞直径、蛋白含量和心肌细胞蛋白质合成速率的显着增加。木犀草素预处理可剂量依赖性地减小由AngII刺激而引起的乳鼠心肌细胞直径、蛋白质含量和蛋白质的合成速率增加。结果表明,木犀草素可有效抑制血管紧张素Ⅱ诱导的心肌细胞肥大。

急性心肌梗死患者血清IL-10、Ang-Ⅱ与冠脉病变严重程度的关系

目的分析血清白细胞介素(IL)-10、血管紧张素(Ang)-Ⅱ与急性心肌梗死(AMI)患者冠状动脉狭窄程度的关系。方法本研究为前瞻性研究,以2020年4月至2022年3月急诊入院拟行血管内介入诊治的120例AMI患者作为研究对象,根据Gensini冠状动脉评分评估患者冠状动脉狭窄程度,分为轻度、中度、重度。在介入治疗前即对患者进行相关检查,检查项目包括血清IL-10、Ang-Ⅱ、肌钙蛋白I(cTnI),心肌酶[血清肌酸激酶(CK)、肌酸激酶同工酶(CK-MB)、乳酸脱氢酶(LDH)],血浆D-二聚体(D-D)等,分析血清IL-10、Ang-Ⅱ与AMI患者冠状动脉狭窄程度的关系及对冠状动脉狭窄程度的影响。结果研究中120例AMI患者,经剔除后以116例为研究对象,116例患者Gensini评分为22~76分,轻度狭窄28例,中度狭窄55例,重度狭窄33例。不同狭窄程度患者Killip分级,血清IL-10、Ang-Ⅱ、cTnI、CK、CK-MB、LDH,血浆D-D比较,差异有统计学意义(P<0.05);但不同狭窄程度患者Killip分级和血浆D-D两两比较,差异无统计学意义(P>0.05)。使用Kendall’s tau-b相关系数检验,血清IL-10、Ang-Ⅱ、cTnI、CK、CK-MB、LDH均与AMI患者冠状动脉狭窄程度呈正相关(r>0,P<0.05)。构建多元logistic回归模型提示,血清IL-10、Ang-Ⅱ高表达均能够加重AMI患者冠状动脉狭窄程度(P<0.05)。结论血清IL-10、Ang-Ⅱ均与AMI患者冠状动脉狭窄程度呈正相关,且能够促进冠状动脉狭窄进展,加重狭窄程度。

糖尿病合并颈动脉狭窄患者中AngⅡ调节T细胞活性的相关研究

目的 本研究主要探究在2型糖尿病合并颈动脉狭窄患者中T细胞活性与AngⅡ水平的相关性。方法选择我院200例患者和30例健康体检者作为研究对象,分为CA组,100例2型糖尿病合并颈动脉狭窄患者;T2DM组,100例2型糖尿病患者;对照组,30例健康体检者。收集病例资料并整理记录,检测T细胞比例,检测其转录因子T-bet、GATA3和RORγt以及其特征因子IFN-γ、IL-4和IL-17的变化;检测健康体检者外周血单核细胞中T细胞的变化。加用AngⅡ刺激剂和AngⅡ拮抗剂后观察T细胞的变化。结果 Th1和Th17阳性细胞数,其转录因子以及其表达因子在CA组明显高于T2DM组和对照组,差异有统计学意义(P <0.05)。健康体检者的外周血细胞在AngⅡ刺激剂作用下,效应性T细胞活性和T细胞的特征因子以及转录因子的表达明显增多,差异有统计学意义(P <0.05),而在AngⅡ拮抗剂作用下效应性T细胞活性和相关的表达因子表达明显减少,差异有统计学意义(P <0.05)。结论 通过调整T细胞活性和其表达因子,可能促进2型糖尿病的颈动脉狭窄形成和发展。AngⅡ可以调节T细活性及相关因子的表达,会导致合并高AngⅡ水平的T2DM患者发生颈动脉粥硬化。

PecsⅡ多模式镇痛在乳腺癌切除术中的应用效果及对术后疼痛-应激因子的影响

目的探究Ⅱ型胸神经阻滞(PecsⅡ)多模式镇痛在乳腺癌切除术中的应用效果及对术后疼痛-应激因子的影响。方法选取2020年4月—2022年3月行乳腺切除手术的成年女性乳腺癌90例,采用随机数字表法分为全身麻醉联合PecsⅡ多模式镇痛组(PGN组)、全身麻醉联合PecsⅡ组(GN组)、单纯全身麻醉组(G组),每组30例。比较3组围术期指标、手术前后疼痛-应激因子[神经肽Y(NPY)、前列腺素E 2(PGE 2)、血管紧张素Ⅰ(AngⅠ)、皮质醇(Cor)]、疼痛程度[视觉模拟评分法(VAS)评分]、镇静程度(Ramsay评分)、生活质量[癌症患者生活质量量表(EORTC QLQ-C30)评分]、功能状态(KPS评分)及不良反应发生率;统计3组乳腺癌术后疼痛综合征(PMPS)发生情况。结果3组手术时间、术中出血量、麻醉时间比较差异无统计学意义(P>0.05);PGN组术后48 h阿片类药物用量少于GN组、G组,住院时间短于GN组、G组(P<0.01)。PGN组术后12、24、48 h血清NPY、PGE 2、AngⅠ、Cor水平低于GN组、G组(P<0.01);PGN组术后2、8、12、24、48 h VAS评分、Ramsay评分低于GN组、G组(P<0.01);PGN组术后3、6个月EORTC QLQ-C30评分、KPS评分高于GN组、G组(P<0.01)。术后48 h,3组不良反应发生率比较差异无统计学意义(P>0.05)。术后6个月,PGN组PMPS发生率低于GN组、G组(P<0.05)。结论PecsⅡ多模式镇痛能提高乳腺癌切除术后镇痛、镇静效果,有效抑制疼痛-应激因子,降低PMPS发生率,有助于改善患者生活质量。

内源性H_2S抑制angiotensin Ⅱ引起的神经元活性氧水平的升高

目的:探讨内源性硫化氢(H2S)对血管紧张素Ⅱ(Ang Ⅱ)引起的延髓神经元活性氧(ROS)水平升高的作用及其可能机制。方法:首先培养原代延髓神经元;免疫荧光双标法鉴定神经元及内源性H2S生成酶胱硫醚β-合成酶(CBS)在神经元的表达;同时或单独给予Ang Ⅱ(1μmol/L)和丁酸钠(NaBu,一种CBS激动剂;100μmol/L、250μmol/L和500μmol/L),二氢乙啶荧光探针法测定ROS水平;采用总超氧化物歧化酶(SOD)活性检测试剂盒观察总SOD的活性;real-time PCR观察CBS mRNA的表达。结果:(1)原代培养的90%以上的细胞为神经元,Ang Ⅱ(1μmol/L)升高延髓神经元ROS水平;(2)Ang Ⅱ抑制神经元总SOD的活性;(3)荧光双标显示CBS在延髓神经元有表达,Ang Ⅱ可降低CBS mRNA的表达;(4)NaBu(250μmol/L和500μmol/L)显著抑制Ang Ⅱ引起的ROS水平的升高,且呈剂量依赖性效应。而NaBu单独对延髓神经元ROS水平作用不明显。结论:Ang Ⅱ引起的延髓神经元ROS水平升高至少部分是通过降低总SOD的活性和CBS mRNA的表达而实现的;而内源性H2S可能通过相反的作用抑制这一过程。

Role of the renin angiotensin system in diabetic nephropathy

Diabetic nephropathy has been the cause of lot of morbidity and mortality in the diabetic population. The renin angiotensin system (RAS) is considered to be involved in most of the pathological processes that result in diabetic nephropathy. This system has various subsystems which contribute to the disease pathology. One of these involves angiotensin II (Ang II) which shows increased activity during diabetic nephropathy. This causes hypertrophy of various renal cells and has a pressor effect on arteriolar smooth muscle resulting in increased vascular pressure. Ang II also induces inflammation, apoptosis, cell growth, migration and differentiation. Monocyte chemoattractant protein-1 production responsible for renal fibrosis is also regulated by RAS. Polymorphism of angiotensin converting enzyme (ACE) and Angiotensinogen has been shown to have effects on RAS. Available treatment modalities have proven effective in controlling the progression of nephropathy. Various drugs (based on antagonism of RAS) are currently in the market and others are still under trial. Amongst the approved drugs, ACE inhibitors and angiotensin receptor blockers (ARBs) are widely used in clinical practice. ARBs are shown to be superior to ACE inhibitors in terms of reducing proteinuria but the combined role of ARBs with ACE inhibitors in diabetic nephropathy is under debate.

AngiotensinⅡ通过氧化应激引起巨噬细胞AMPK/SIRT1能量信号紊乱

目的探讨Angiotensin Ⅱ诱导巨噬细胞氧化应激反应与AMPK/SIRT1通路活化关系的机制。方法 RAW264.7细胞正常培养后给予不同浓度的Angiotensin Ⅱ(0、0.5、1、3、10、20μmol/L)处理24 h后,Western blot检测AMPK,p-AMPK和SIRT1的表达水平变化,和用DCFH探针检测ROS水平的变化,试剂盒检测细胞上清液中SOD活性和MDA表达量;同时采用基因编辑技术将Angiotensin Ⅱ的受体AT1R成功沉默后给予Angiotensin Ⅱ刺激,检测对AMPK,p-AMPK和SIRT1蛋白水平的影响以及使用ROS的抑制剂来观察细胞AMPK和SIRT1的变化情况。结果 20μmol/L的Angiotensin Ⅱ的刺激能显著抑制蛋白AMPK的磷酸化(P<0.05),抑制SIRT1的表达;同时增加了细胞ROS的释放(P<0.05)。在检测SOD活性和MDA表达量时,0.5~10μmol/L的Angiotensin Ⅱ对细胞无明显改变(P>0.05),20μmol/L的Angiotensin Ⅱ明显抑制SOD活性(P<0.05),能显著增加MDA的产生。沉默了AT1R后,Angiotensin Ⅱ不能抑制AMPK蛋白磷酸化以及对SIRT1的表达无明显下调作用;使用ROS抑制剂后,Angiotensin Ⅱ处理无法降低细胞磷酸化AMPK和SIRT1的表达。结论 Angiotensin Ⅱ通过诱导巨噬细胞发生氧化应激反应从而引起AMPK/SIRT1信号通路的紊乱。

Renin-angiotensin system in the pathogenesis of liver fibrosis

Hepatic fibrosis is considered a common response to many chronic hepatic injuries. It is a multifunctional process that involves several cell types, cytokines, chemokines and growth factors leading to a disruption of homeostatic mechanisms that maintain the liver ecosystem. In spite of many studies regarding the development of fibrosis, the understanding of the pathogenesis remains obscure. The hepatic tissue remodeling process is highly complex, resulting from the balance between collagen degradation and synthesis. Among the many mediators that take part in this process, the components of the Renin angiotensin system （RAS） have progressively assumed an important role. Angiotensin （Ang） II acts as a profibrotic mediator and Ang-（1-7）, the newly recognized RAS component, appears to exert a counter-regulatory role in liver tissue. We briefly review the liver fibrosis process and current aspects of the RAS. This review also aims to discuss some experimental evidence regarding the participation of RAS mediators in the pathogenesis of liver fibrosis, focusing on the putative role of the ACE2-Ang-（1-7）- Mas receptor axis.

Renin angiotensin system in liver diseases: Friend or foe?

In the last three decades,the understanding of the renin angiotensin system(RAS)has been changed by the discoveries of functional local systems,novel biologically active peptides,additional specific receptors,alternative pathways of angiotensin(Ang)?Ⅱ?generation,and new roles for enzymes and precursor components other than those in Ang?Ⅱ?synthesis.In this regard,the discovery that Ang-(1-7)opposes the pressor,proliferative,pro-fibrotic,and pro-inflammatory effects mediated by Ang?Ⅱ?has contributed to the realization that the RAS is composed of two axes.The first axis consists of the angiotensin-converting enzyme(ACE),with Ang?Ⅱ?as the end product,and the angiotensin type 1(AT1)receptor as the main effector mediating the biological actions of Ang?Ⅱ.The second axis results from ACE2-mediated hydrolysis of Ang?Ⅱ,leading to the production of Ang-(1-7),with the Mas receptor as the main effector conveying the vasodilatory,antiproliferative,anti-fibrotic,and anti-inflammatory effects of Ang-(1-7).Experimental and clinical studies have shown that both axes of the RAS may take part in the pathogenesis of liver diseases.In this manuscript,we summarize the current evidence regarding the role of RAS in hepatic cirrhosis and its complications,including hemodynamic changes and hepatorenal syndrome.The therapeutic potential of the modulation of RAS molecules in liver diseases is also discussed.