葛根芩连汤通过IRS-1/PI3K/AKT通路对胃肠湿热型2型糖尿病大鼠糖脂代谢的影响

目的探究葛根芩连汤通过胰岛素受体底物-1(IRS-1)/磷脂酰肌醇3激酶(PI3K)/蛋白激酶B(AKT)通路对胃肠湿热型2型糖尿病大鼠糖脂代谢的影响。方法将40只SD大鼠随机分为正常组(2 mL生理盐水灌胃)、造模组(2 mL生理盐水灌胃)、二甲双胍组(4.17 mg/100 g二甲双胍灌胃)和葛根芩连汤组(1 g/100 g葛根芩连汤灌胃),每组10只。采用高脂高糖饲料加腹腔注射链脲佐菌素(STZ)构建2型糖尿病大鼠模型,随后喂食油脂、42°白酒及蜂蜜水构建胃肠湿热型2型糖尿病大鼠模型。测量各组大鼠不同时间节点体质量,血糖仪测定空腹血糖(FBG);ELISA检测空腹胰岛素(FINS)、三酰甘油(TG)、总胆固醇(TC)、白细胞介素-6(IL-6)、肿瘤坏死因子-α(TNF-α)水平变化、计算胰岛素抵抗指数(HOMA-IR);HE染色检测肝组织病理学变化;检测肝组织过氧化氢酶(CAT)、谷胱甘肽过氧化物酶(GSH-Px)、超氧化物歧化酶(SOD)及丙二醛(MDA)含量变化。Western blot检测肝组织IRS-1、PI3K、p-PI3K、AKT及p-AKT蛋白变化。结果与正常组比较,造模组大鼠体质量、FBG、FINS及HOMA-IR、GSH-Px、CAT、SOD、IRS-1、p-PI3K/PI3K及p-AKT/AKT水平均明显下降(P<0.05)、TG、TC、IL-6、TNF-α及MDA含量均显著升高(P<0.05),可见局灶性肝实质损失。与造模组比较,二甲双胍组及葛根芩连汤组大鼠体质量、FBG、FINS及HOMA-IR、GSH-Px、CAT、SOD、IRS-1、p-PI3K/PI3K及p-AKT/AKT水平均明显升高(P<0.05)、TG、TC、IL-6、TNF-α及MDA含量均显著降低(P<0.05),显示正常的肝实质。结论葛根芩连汤可明显改善胃肠湿热型2型糖尿病糖脂紊乱,可能是通过IRS-1/PI3K/AKT通路发挥作用。

血清IRS-1和CTRP3水平与妊娠糖尿病患者不良妊娠结局的相关性

目的分析血清胰岛素底物受体-1(IRS-1)、C1q肿瘤坏死因子相关蛋白-3(CTRP3)水平与妊娠糖尿病(GDM)患者不良妊娠结局的相关性。方法采用前瞻性研究,选取2021年1月至2023年12月在陕西中医药大学第二附属医院分娩的132例GDM孕妇为患病组[年龄(28.76±3.18)岁,体重指数(BMI)为(25.72±2.82)kg/m^(2),孕周(38.06±1.42)周,经产孕妇66例,阴道分娩82例],根据妊娠结局分为良好结局组(80例)与不良结局组(52例);另选同期分娩的健康孕妇132名为对照组[年龄(28.65±3.06)岁,BMI(25.31±2.67)kg/m^(2),孕周(38.21±1.33)周,经产孕妇60例,阴道分娩86例]。对不同妊娠结局GDM患者临床资料进行单因素分析,多因素logistic回归分析孕妇不良妊娠结局的影响因素,绘制受试者操作特征曲线(ROC)分析IRS-1、CTRP3对GDM患者不良妊娠结局的诊断价值,分析IRS-1、CTRP3与临床指标及孕妇妊娠结局的相关性。统计学方法采用χ^(2)检验、t检验、Pearson及Spearman相关性分析。结果患病组血清IRS-1、CTRP3水平均低于对照组[(1.82±0.21)μg/L比(2.33±0.28)μg/L、(353.51±38.14)ng/L比(425.95±45.21)ng/L],差异均有统计学意义(t=16.74、14.07,均P<0.05);不良结局组血清IRS-1、CTRP3水平均低于良好结局组,空腹血糖(FBG)、糖化血红蛋白(HbAlc)、胰岛素抵抗指数(HOMA-IR)水平均高于良好结局组,差异均有统计学意义(t=8.61、7.49、7.26、8.40、32.73,均P<0.05);FBG、HbAlc、HOMA-IR水平升高均为影响患者不良妊娠结局的危险因素[比值比(OR)=1.498,95%置信区间(CI)1.099~2.042;OR=1.698,95%CI 1.092~2.639;OR=2.014,95%CI 1.063~3.816;均P<0.05],IRS-1、CTRP3均为影响患者不良妊娠结局的保护因素[OR=0.774,95%CI 0.621~0.964;OR=0.731,95%CI 0.573~0.932;均P<0.05];ROC显示,IRS-1、CTRP3联合诊断患者不良妊娠结局的曲线下面积(AUC)为0.899,联合诊断的AUC优于IRS-1、CTRP3单独诊断(Z=2.094、2.056,均P<0.05);IRS-1、CTRP3与孕妇妊娠结局及FBG、HbAlc、HOMA-IR均呈负相关(均P<0.05)。结论不良妊娠结局GDM患者血清IRS-1、CTRP3水平降低,二者联合对患者不良妊娠结局有一定预测价值。

Glucagon-like peptide-1 receptor agonists as a possible intervention to delay the onset of type 1 diabetes:A new horizon

Type 1 diabetes(T1D)is a chronic autoimmune condition that destroys insulinproducing beta cells in the pancreas,leading to insulin deficiency and hyperglycemia.The management of T1D primarily focuses on exogenous insulin replacement to control blood glucose levels.However,this approach does not address the underlying autoimmune process or prevent the progressive loss of beta cells.Recent research has explored the potential of glucagon-like peptide-1 receptor agonists(GLP-1RAs)as a novel intervention to modify the disease course and delay the onset of T1D.GLP-1RAs are medications initially developed for treating type 2 diabetes.They exert their effects by enhancing glucose-dependent insulin secretion,suppressing glucagon secretion,and slowing gastric emptying.Emerging evidence suggests that GLP-1RAs may also benefit the treatment of newly diagnosed patients with T1D.This article aims to highlight the potential of GLP-1RAs as an intervention to delay the onset of T1D,possibly through their potential immunomodulatory and anti-inflammatory effects and preservation of beta-cells.This article aims to explore the potential of shifting the paradigm of T1D management from reactive insulin replacement to proactive disease modification,which should open new avenues for preventing and treating T1D,improving the quality of life and long-term outcomes for individuals at risk of T1D.

Fixed-ratio combinations of basal insulin and glucagon-like peptide-1 receptor agonists as a promising strategy for treating diabetes

The maintenance of appropriate glycemic control is important for the prevention of diabetic complications in people with type 2 diabetes(T2D). Numerous oral antidiabetic drugs are now clinically available, but in particular, the introduction of injection regimens using insulin and/or glucagon-like peptide-1 receptor agonist(GLP-1RA)s represents promising step-up options for oral antidiabetic drug treatment. The recently licensed fixed-ratio combination(FRC) products,which comprise basal insulin and a GLP-1RA, have potent anti-hyperglycemic effects and reduce the undesirable side-effects of each component, such as body weight gain, hypoglycemia, and gastrointestinal symptoms. Two FRCs-insulin degludec/Liraglutide and insulin glargine/Lixisenatide-are now clinically available and, to date, several phase Ⅱ/Ⅲ trials have been conducted in particular groups of subjects with T2D. However, their utility in real-world clinical settings is of interest for most clinicians. Recently reported real-world clinical trials of these two FRCs in various situations have demonstrated their efficacy regarding glycemic control and the quality of life of people with T2D. Their long-term safety and efficacy require confirmation, but a treatment strategy that includes an FRC may be compatible with the concept of “well-balanced” therapy in certain groups of patients with T2D who have inadequate glycemic control.

Simiao Wan alleviates obesity-associated insulin resistance via PKCε/IRS-1/PI3K/Akt signaling pathway based on network pharmacology analysis and experimental validation

Background:The purpose of the study was to investigatethe active ingredients and potential biochemicalmechanisms of Simiao Wan(SMW)in obesity-associated insulin resistance.Methods:An integrated network pharmacology method to screen the active compoundsand candidate targets,construct the protein-protein-interaction network,and ingredients-targets-pathways network was constructed for topological analysis to identify core targets and main ingredients.To find the possible signaling pathways,enrichment analysis was performed.Further,a model of insulin resistance in HL-7702 cells was established to verify the impact of SMW and the regulatory processes.Results:An overall of 63 active components and 151 candidate targets were obtained,in which flavonoids were the main ingredients.Enrichment analysis indicated that the PI3K-Akt signaling pathway was the potential pathway regulated by SMW in obesity-associated insulin resistance treatment.The result showed that SMW could significantly ameliorate insulin sensitivity,increase glucose synthesis and glucose utilization and reduce intracellular lipids accumulation in hepatocytes.Also,SMW inhibited diacylglycerols accumulation-induced PKCεactivity and decreased its translocation to the membrane.Conclusion:SMW ameliorated obesity-associated insulin resistance through PKCε/IRS-1/PI3K/Akt signaling axis in hepatocytes,providing a new strategy for metabolic disease treatment.

达格列净联合胰高血糖素样肽-1受体激动剂对2型糖尿病的疗效研究

目的探讨达格列净联合胰高血糖素样肽-1受体激动剂(GLP-1 RAs)对2型糖尿病患者血液流变学及胰岛素抵抗的影响。方法将2020年11月—2022年10月泉州市中医院收治的102例2型糖尿病患者随机分为2组,每组51例。对照组给予达格列净治疗,研究组采用达格列净联合GLP-1 RAs(利拉鲁肽)的治疗方案。比较2组临床疗效、血糖指标[空腹血糖(FBG)、餐后2 h血糖(2 hPG)、糖化血红蛋白(HbA1c)]、空腹胰岛素(FINS)及胰岛素抵抗[胰岛素抵抗指数(HOMA-IR)、胰岛素分泌指数(HOMA-β)]、血脂指标[总胆固醇(TC)、甘油三酯(TG)、高密度脂蛋白胆固醇(HDL-C)、低密度脂蛋白胆固醇(LDL-C)]、血液流变学指标[红细胞聚集指数(EAI)、红细胞压积(HCT)、红细胞变形指数(EDI)、血浆黏度(PV)]和不良反应。结果研究组总有效率为94.12%,高于对照组的80.39%,差异有统计学意义(P<0.05)。研究组和对照组治疗后FBG、2 hPG、HbAlc、BMI均低于治疗前,且研究组治疗后FBG、2 hPG、HbAlc水平低于对照组,差异有统计学意义(P<0.05)。治疗后,研究组FINS、HOMA-β水平高于对照组,HOMA-IR水平低于对照组,差异有统计学意义(P<0.05)。研究组和对照组治疗后HDL-C均高于治疗前,TC、TG、LDL-C水平均低于治疗前;研究组治疗后HDL-C水平高于对照组,TC、TG、LDL-C水平低于对照组,差异均有统计学意义(P<0.05)。治疗后,研究组和对照组EAI、HCT、EDI、PV水平均低于治疗前,且研究组EAI、HCT、EDI、PV水平低于对照组,差异均有统计学意义(P<0.05)。研究组不良反应总发生率为11.76%,与对照组的9.80%比较,差异无统计学意义(P>0.05)。结论达格列净联合GLP-1 RAs(利拉鲁肽)治疗2型糖尿病的疗效确切,可有效调节患者血糖及血脂水平,缓解胰岛素抵抗,改善血液流变学指标。

子宫内膜癌患者血清sVEGFR1、YKL-40、IGF-1表达水平及临床意义研究

目的探究子宫内膜癌患者血清可溶性血管内皮生长因子受体1(sVEGFR1)、甲壳质酶蛋白40(YKL-40)、胰岛素样生长因子1(IGF-1)表达水平及临床意义。方法择取本院100例子宫内膜癌患者作为观察组;另选取同期100例健康体检者作为对照组。比较两组sVEGFR1、YKL-40、IGF-1表达水平并分析观察组不同分期表达水平。结果观察组sVEGFR1表达水平较对照组低,YKL-40、IGF-1表达水平较对照组高,差异有统计学意义(P<0.05)。观察组Ⅰ~Ⅳ期sVEGFR1表达水平明显降低,YKL-40、IGF-1表达水平升高,差异有统计学意义(P<0.05)。结论在子宫内膜癌患者中,sVEGFR1、YKL-40、IGF-1均出现异常表达,不同分期患者存在较大差异,可为疾病诊断与分期提供可靠的数据参考。

Blockade of insulin receptor substrate-1 inhibits biological behavior of choroidal endothelial cells

AIM: To investigate the effects of blockade of insulin receptor substrate-1(IRS-1) on the bio-function of tube formation of human choroidal endothelial cells(HCECs).METHODS: Quantitative reverse transcriptionpolymerase chain reaction(RT-PCR) and Western blot were performed to determine the expression level of IRS-1 and phospho-IRS-1 in HCECs. Tube formation of HCECs was analyzed using three dimensional in vitro Matrigel assay with or without IRS-1 blockage via IRS-1 inhibitor(GS-101) and vascular endothelial growth factor receptor 2(VEGFR2) inhibitor. In addition, cell counting kit(CCK)-8 and Transwell migration assay were exerted to analyze the effects of blockade of IRS-1 on the bio-function of proliferation and migration of HCECs, respectively. The apoptosis of HCECs was examined using flow cytometry(FCM).RESULTS: RT-PCR and Western blot revealed that IRS-1 phospho-IRS-1 were expressed in HCECs and the expression level was enhanced by stimulation of VEGF-A. The number of tube formation was decreased significantly in GS-101 treated groups compared to phosphate buffered saline(PBS) treated control groups. Furthermore, both cell proliferation and migration of HCECs were decreased in the presence of GS-101. FCM analysis showed that the apoptosis of HCECs was enhanced when the cells were treated with GS-101. Western blot also showed that the expression level of cleaved-caspase 3 in GS-101 treated group was higher than that in control group.CONCLUSION: Blockade of IRS-1 can inhibit tube formation of HCECs through reducing cell proliferation and migration and promoting cell apoptosis.

雷公藤多苷联合他克莫司及激素治疗难治性肾病综合征的效果及对血清sTNF-R1、IGFBP-2、CFH水平的影响

目的 探讨雷公藤多苷联合他克莫司及激素治疗难治性肾病综合征(RNS)的疗效对血清可溶性肿瘤坏死因子受体1(s TNF-R1)、胰岛素样生长因子结合蛋白-2(IGFBP-2)、补体因子H(CFH)水平的影响。方法 研究对象为2018年8月至2021年8月于江南大学附属医院治疗的RNS患者102例,以随机数字表法分为对照组(n=51,采取甲泼尼龙片加他克莫司胶囊治疗)和观察组(n=51,在对照组基础上给予雷公藤多苷片治疗)。评估两组的治疗效果、血清相关指标,统计两组的不良反应。结果 观察组治疗总有效率(96.08%)高于对照组(80.39%)(χ^(2)=6.044,P=0.014);治疗后,观察组患者血清白蛋白、CFH水平[分别为(36.54±8.11) g·L^(-1)、(586.20±100.72)μg·m L^(-1)],高于对照组[分别为(32.58±6.12) g·L^(-1)、(540.11±100.47)μg·m L^(-1)],差异均有统计学意义(t=2.783,P=0.006;t=2.314,P=0.023);观察组患者24 h尿蛋白、肌酐、s TNF-R1、IGFBP-2水平[分别为(2.67±0.69) g、(82.25±16.13)μmol·L^(-1)、(1.56±0.45) ng·m L^(-1)、(51.34±10.44) ng·m L^(-1)],低于对照组[分别为(3.24±1.02) g、(92.68±17.35)μmol·L^(-1)、(1.91±0.58) ng·m L^(-1)、(57.79±12.58) ng·m L^(-1)],差异均有统计学意义(t=3.306,P=0.001;t=3.135,P=0.002;t=3.405,P=0.001;t=2.820,P=0.005);观察组复发率(1.96%)低于对照组(13.73%)(χ^(2)=4.883,P=0.027)。结论 公藤多苷联合他克莫司及激素治疗RNS效果佳,降低复发率,改善肾功能,减轻炎症,有望作为辅助治疗RNS的药物。

替米沙坦通过直接抑制Kv2.1通道促进离体大鼠的胰岛素分泌

目的研究替米沙坦促进大鼠胰岛素分泌作用相关的信号通路。方法(1)分离成年Wistar大鼠胰腺获得胰岛和胰岛细胞,通过胰岛素分泌实验观察药物对胰岛素分泌的影响,通过钙成像实验和全细胞膜片钳技术观察药物对β细胞内Ca^(2+)浓度的变化和对离子通道的作用。(2)使用过表达电压门控性钾(voltage-gated potassium channel,Kv)通道2.1亚型(Kv2.1)的慢病毒转染中国仓鼠卵巢(Chinese hamster ovary,CHO)细胞构建CHO-Kv2.1细胞系,使用膜片钳技术观察替米沙坦对Kv2.1通道的直接作用。结果缬沙坦和厄贝沙坦无类似替米沙坦的高糖浓度下促胰岛素分泌、升高β细胞内Ca^(2+)浓度和抑制β细胞的Kv通道等作用。过氧化物酶体增殖物激活受体γ(peroxisome proliferator-activated receptorγ,PPARγ)阻断剂GW9662亦未阻断替米沙坦的上述作用。而替米沙坦可以浓度依赖性地抑制CHO-Kv2.1细胞的Kv2.1通道电流。结论替米沙坦的促胰岛素分泌作用可能与血管紧张素Ⅱ-1型(angiotensin II type 1,AT-1)受体和PPARγ无关,但至少与对Kv2.1通道的直接抑制作用有关。

CXCR1、ESM-1及IGFBP-2与COPD合并肺部感染患者疾病严重程度、预后的关系

目的 分析血清趋化因子受体1(CXCR1)、内皮细胞特异性分子-1(ESM-1)、胰岛素样生长因子结合蛋白2(IGFBP-2)水平与慢性阻塞性肺疾病(COPD)合并肺部感染患者疾病严重程度、预后的关系。方法 选取2021年1月至2023年1月于阜阳市人民医院就诊的COPD患者325例,根据肺部感染情况分为感染组及未感染组。比较两组入院时的血清CXCR1、ESM-1、IGFBP-2水平及常规感染指标[C-反应蛋白(CRP)、降钙素原(PCT)]水平,采用Pearson相关分析感染组上述指标的关系。比较不同病情严重程度COPD合并肺部感染患者入院时的CXCR1、ESM-1、IGFBP-2水平。对感染组患者跟踪随访6个月或死亡止,根据预后情况分为存活亚组及死亡亚组,比较两亚组患者入院时的血清CXCR1、ESM-1、IGFBP-2水平;采用受试者工作曲线(ROC)分析上述指标对COPD合并肺部感染患者死亡的预测价值。结果 325例COPD患者包括感染组109例及未感染组216例。感染组患者入院时的血清CXCR1、ESM-1、IGFBP-2、CRP、PCT水平高于未感染组,差异有统计学意义(P<0.05)。不同病情严重程度COPD合并肺部感染患者入院时的血清CXCR1、ESM-1、IGFBP-2水平比较差异有统计学意义(P<0.05)。Pearson相关分析显示,感染组入院时的血清CRP水平与CXCR1、ESM-1水平呈正相关(P<0.05)。随访期间感染组死亡19例(17.43%),存活90例(82.57%),死亡亚组入院时的血清CXCR1、ESM-1、IGFBP-2水平高于存活亚组,差异有统计学意义(P<0.05)。ROC结果显示,血清CXCR1、IGFBP-2水平预测COPD合并肺部感染患者死亡具有一定局限性(AUC=0.636、0.769),ESM-1的预测效能较好(AUC=0.827),CXCR1+ESM-1+IGFBP-2三项联合诊断的预测效能最佳(AUC=0.904)。结论 血清CXCR1、ESM-1、IGFBP-2水平在COPD合并肺部感染患者的疾病严重程度及预后评估方面具有一定指导意义。

吐根碱通过GLP-1R促进大鼠胰岛组织胰岛素分泌作用的研究

目的探讨吐根碱通过胰高血糖素样肽-1受体(glucagon-like peptide-1 receptor,GLP-1R)促进离体大鼠胰岛组织胰岛素分泌作用。方法分离大鼠胰岛组织进行胰岛素分泌实验,根据实验设计使用不同浓度的吐根碱(2、10、50μmol·L^(-1))、不同浓度葡萄糖(2.8、11.1、16.7 mmol·L^(-1))以及特异性GLP-1R拮抗剂Exendin(9-39)孵育胰岛组织。酶联放射免疫的检测方法测定每组上清液胰岛素分泌量。使用SYBYL-X2.0软件将小分子化合物与GLP-1R(PDB代码:5NX2)进行对接。结果胰岛素分泌实验结果显示在高糖(11.1 mmol·L^(-1))条件下,胰岛素分泌量在吐根碱作用下明显升高,且具有剂量依赖性。低糖(2.8 mmol·L^(-1))条件下,胰岛素分泌量在吐根碱干预下没有明显变化,但在高糖(11.1、16.7 mmol·L^(-1))条件下,胰岛素分泌量在吐根碱作用下明显升高,具有类似GLP-1R激动剂葡萄糖浓度依赖性促胰岛素分泌特点。吐根碱与GLP-1R对接打分是Total Score=6.82,C Score=5,表明吐根碱与GLP-1R有良好的亲和力。当GLP-1R被Exendin(9-39)阻断后,吐根碱促胰岛素分泌作用明显降低。结论吐根碱通过激活GLP-1R发挥促离体大鼠胰岛组织胰岛素分泌作用。

胰高血糖素样肽-1/葡萄糖依赖性促胰岛素多肽双受体激动剂替西帕肽

新型胰高血糖素样肽-1/葡萄糖依赖性促胰岛素多肽(GLP-1/GIP)双受体激动剂替西帕肽,临床显示具有较强的降糖效果,并且减轻体质量效果非常显著,可以提高胰岛素敏感性,同时具有优越的心血管保护作用和改善非酒精性脂肪性肝病/非酒精性脂肪性肝炎(NAFLD/NASH)的作用,并且副作用小,依从性好。替西帕肽作为双肠道激素激动剂对改善代谢水平显示出强大的潜力。该文就GLP-1/GIP双受体激动剂替西帕肽的作用机制和临床研究进行综述。

高血压合并焦虑病人血清微RNA-451a、胰岛素样生长因子-1受体表达水平与焦虑程度的关系

目的探讨高血压合并焦虑病人血清微RNA-451a(miR-451a)、胰岛素样生长因子-1受体(IGF1R)表达水平与焦虑程度的关系。方法选取2020年2月至2022年1月在汉中市中心医院进行治疗的高血压病人160例,根据临床诊断和汉密尔顿焦虑量表(HAMA)评估将病人分为高血压组60例、高血压合并轻度焦虑情绪组48例、高血压合并中度焦虑情绪组32例和高血压合并重度焦虑情绪组20例,收集整理所有病例的临床基础资料。采用实时荧光定量PCR法检测血清miR-451a表达水平、ELISA法检测血清IGF1R表达水平;比较分析高血压病人和高血压合并焦虑情绪病人的临床病理特征;采用Pearson法分析HAMA评分与血清miR-451a、IGF1R表达水平的相关性;采用logistic回归分析高血压合并焦虑的影响因素。结果高血压组、轻度焦虑、中度焦虑和重度焦虑组病人血清miR-451a水平依次降低(0.88±0.30,0.59±0.14,0.48±0.11,0.38±0.09),IGF1R水平依次升高[(2.14±0.60)μg/L,(2.66±0.62)μg/L,(3.08±0.66)μg/L,(3.51±0.74)μg/L];血清miR-451a水平与HAMA评分呈负相关(r=−0.50,P<0.05),血清IGF1R水平与HAMA评分呈正相关(r=0.43,P<0.05);高血压合并焦虑组收缩压[(142.26±18.51)mmHg,(135.29±17.84)mmHg]、舒张压[(84.25±11.30)mmHg,(78.23±10.25)mmHg]、C-反应蛋白[(4.47±0.96)mg/L,(4.16±0.91)mg/L]、IL-6水平[(36.95±6.31)μg/L,(27.48±5.49)μg/L]显著高于高血压组,IL-10水平[(12.34±3.26)ng/L,(16.24±3.91)ng/L]显著低于高血压组(P<0.05);多因素logistic回归分析结果显示,收缩压[OR 95%CI=1.33(1.06,1.67)]、舒张压[OR 95%CI=1.20(1.00,1.45)]、IL-6[OR 95%CI=1.89(1.22,2.93)]、IL-10[OR 95%CI=0.38(0.17,2.93)]、miR-451a[OR 95%CI=0.01(0.00,0.47)]、IGF1R[OR 95%CI=7.62(1.21,48.03)]水平为高血压合并焦虑的影响因素(P<0.05)。结论高血压合并焦虑病人血清中miR-451a低表达,IGF1R高表达,且与病人焦虑程度密切相关。

子宫内膜癌组织中ZEB2和IGF1R表达情况及其与患者淋巴结转移及预后的关系

目的探讨E盒结合锌指蛋白2(ZEB2)和胰岛素样生长因子1受体(IGF1R)在子宫内膜癌组织中的表达情况及其与淋巴结转移及预后的关系。方法选取2018年6月至2020年6月邯郸市中心医院收治的137例行手术治疗的子宫内膜癌患者作为研究对象,收集患者在手术过程中切除的癌组织及癌旁组织。采用免疫组化方法检测组织中ZEB2和IGF1R的表达情况,进一步分析患者的病理特征与ZEB2和IGF1R表达情况的关系及不同临床特征与淋巴结转移的关系。进行定期随访,根据随访结果采用Kaplan-Meier法分析患者预后生存情况,采用Cox回归模型进行患者预后不良的多因素分析。结果子宫内膜癌组织中ZEB2和IGF1R阳性表达率均高于癌旁组织(P<0.05)。子宫内膜癌组织中ZEB2和IGF1R表达水平与与国际妇产科联盟(FIGO)分期、淋巴结是否转移有关(P<0.05)。淋巴结转移情况与肿瘤直径、FIGO分期有关(P<0.05)。子宫内膜癌组织ZEB2阳性表达患者3年生存率低于ZEB2阴性表达患者(P<0.05),子宫内膜癌组织IGF1R阳性表达患者3年生存率低于IGF1R阴性表达患者(P<0.05)。FIGO分期、淋巴结转移、ZEB2和IGF1R阳性表达均为子宫内膜癌患者预后不良的影响因素(P<0.05)。结论与癌旁组织比较,子宫内膜癌组织中ZEB2和IGF1R阳性表达率较高,且与患者的FIGO分期、淋巴结转移情况有关。

lncRNA DSCAM-AS1通过miR-144-5p/IRS2轴对甲状腺乳头状癌细胞的影响

目的:探究长链非编码RNA(lncRNA)唐氏综合征细胞黏附分子反义1(DSCAM-AS1)通过微小RNA(miR)-144-5p/胰岛素受体底物2(IRS2)轴促进甲状腺乳头状癌(PTC)细胞生长和侵袭的作用。方法:将PTC细胞株TPC-1随机分为对照组(Control组,完全培养基正常培养)、si-NC组(转染si-NC)、si-DSCAM-AS1组(转染si-DSCAM-AS1)、si-DSCAM-AS1+inhibitor NC组(si-DSCAM-AS1与inhibitor NC共转染)、si-DSCAM-AS1+miR-144-5p inhibitor组(si-DSCAM-AS1与miR-144-5p inhibitor共转染)。RT-qPCR法检测DSCAM-AS1、miR-144-5p和IRS2 mRNA的表达;CCK-8法检测细胞增殖能力;Transwell实验检测细胞的侵袭能力;Western blot检测IRS2蛋白的表达。双荧光素酶报告基因实验验证靶向关系。结果:与Control组相比,si-DSCAM-AS1组TPC-1细胞DSCAM-AS1表达、吸光度(A450)值、细胞侵袭数目、IRS2表达显著降低(P<0.05),miR-144-5p表达显著升高(P<0.05)。与si-DSCAM-AS1组相比,si-DSCAM-AS1+miR-144-5p inhibitor组A450值、细胞侵袭数目、IRS2表达显著升高(P<0.05),miR-144-5p表达显著降低(P<0.05)。DSCAM-AS1靶向负调控miR-144-5p表达,miR-144-5p靶向负调控IRS2表达。结论:沉默DSCAM-AS1可能通过上调miR-144-5p来抑制IRS2蛋白的表达,从而抑制PTC细胞生长和侵袭。

栀子苷调节HMGB1-RAGE信号通路对妊娠期糖尿病大鼠胰岛素抵抗的影响

目的探讨栀子苷(GP)调节高迁移率组框1-晚期糖基化终产物信号通路(HMGB1-RAGE信号通路)对妊娠期糖尿病大鼠胰岛素抵抗的影响。方法建立妊娠期糖尿病大鼠模型(GDM),分为对照组(Control组)、模型组(GDM组)、栀子苷低剂量组(GP-L组,200 mg·kg^(-1)·d^(-1)GP)、栀子苷中剂量组(GP-M组,400 mg·kg^(-1)·d^(-1)GP)、栀子苷高剂量组(GP-H组,500 mg·kg^(-1)·d^(-1)GP),HMGB1抑制剂Glycyrrhizin组(Gly组,50 mg·kg^(-1)·d^(-1)Gly)。ELISA法检测IL-1β、IL-6和TNF-α水平;试剂盒测定空腹胰岛素(FINS)、总胆固醇(TC)、三酰甘油(TG)、低密度脂蛋白胆固醇(LDL-C)、高密度脂蛋白胆固醇(HDL-C)、血清中GLUT4和CTRP3蛋白浓度;HE染色观察肝组织病理学变化;PAS染色观察肝糖原表达情况;Western blot测定HMGB1和RAGE蛋白表达。结果与Control组相比,GDM组肝组织结构损伤、脂肪沉积增多,肝糖原表达(0.17±0.02)显著降低(P<0.05),IL-1β(35.34±3.52)、IL-6(24.31±2.32)、TNF-α(38.96±2.25)、FBG(13.21±1.06)、FINS(20.43±1.65)、HOMA-IR(11.99±1.20)、TC(3.11±0.56)、TG(1.91±0.35)、LDL-C(1.49±0.19)、HMGB1(1.28±0.13)和RAGE(1.43±0.15)水平及TG/HDL-C比值(2.81±0.26)显著升高(P<0.05),HDL-C(0.68±0.07)、GLUT4(2.21±0.61)和CTRP3(299.21±31.43)水平显著降低(P<0.05);与GDM组相比,GP-L、GP-M、GP-H和Gly组肝组织结构整齐,细胞形态正常,脂肪沉积较少;肝组织染色均匀,糖原表达(0.31±0.04、0.44±0.03、0.56±0.05、0.59±0.07b)显著增加(P<0.05),且药物治疗组呈剂量依赖性增加(P<0.05),GP-L、GP-M、GP-H和Gly组IL-1β(分别为30.81±2.41、27.65±2.03、21.54±2.12、21.68±1.97)、IL-6(分别为21.05±1.28、17.35±1.04、12.37±1.16、12.69±1.05)、TNF-α(分别为32.17±2.03、29.18±1.74、22.69±1.41、23.17±1.12)、FBG(分别为11.86±1.19、9.38±1.06、7.07±1.14、6.96±1.08)、FINS(分别为17.06±1.37、14.60±1.16、11.03±1.25、11.76±1.11)、HOMA-IR(分别为8.99±1.22、6.07±0.91、3.47±0.43、3.64±0.14)、TC(分别为2.64±0.16、1.83±0.12、1.43±0.04、1.36±0.38)、TG(分别为1.67±0.21、1.41±0.19、1.17±0.23、1.20±0.11)、LDL-C(分别为1.36±0.16、1.17±0.13、0.96±0.06、0.87±0.04)、HMGB1(分别为0.94±0.10、0.54±0.05、0.35±0.07、0.30±0.2)、RAGE水平(分别为1.21±0.10、0.98±0.06、0.77±0.09、0.69±0.05)及TG/HDL-C比值(分别为2.06±0.21、1.48±0.11、0.98±0.12、1.03±0.10)显著降低(P<0.05),HDL-C浓度(分别为0.81±0.06、0.95±0.09、1.19±0.13、1.16±0.21)、GLUT4(分别为3.06±0.49、4.18±1.10、5.41±0.96、5.25±0.82)和CTRP3(分别为362.43±30.27、427.25±45.41、481.16±44.23、473.53±41.38)水平显著升高,且药物治疗组呈剂量依赖性(P<0.05)。结论栀子苷通过抑制HMGB1-RAGE信号通路抑制妊娠期糖尿病大鼠胰岛素抵抗。

IRS-1/PI3K/Akt2信号通路调控miR-139-5p对2型糖尿病大鼠的干预效果

目的分析基于胰岛素受体底物1(IRS-1)/磷脂酰肌醇3激酶(PI3K)/蛋白激酶B(Akt2)信号通路调控微小核糖核酸139-5p(miR-139-5p)对2型糖尿病大鼠的干预效果。方法选取52只雄性SPF级Wistar大鼠,12只大鼠作为对照组,另外40只建立2型糖尿病模型,将建模成功36只大鼠采用随机数字表法分为模型组、沉默组、过表达组,每组各12只。对照组、模型组大鼠注射同剂量0.9%氯化钠溶液,沉默组大鼠尾静脉注射10μL miR-139-5p沉默慢病毒悬液,过表达组大鼠尾静脉注射10μL miR-139-5p过表达慢病毒悬液,于miR-139-5p转染后,对各组大鼠毛发光泽度、活动、形态等一般情况进行观察。对各组大鼠miR-139-5p、IRS-1、PI3K、Akt2表达量、血糖相关指标[胰岛素抵抗指数(HOMA-IR)、空腹胰岛素、空腹血糖、胰岛β细胞功能指数(HOMA-β)]、炎症因子[白细胞介素6(IL-6)、肿瘤坏死因子α(TNF-α)]水平、血脂变化水平、IRS-1/PI3K/Akt2信号通路蛋白表达量进行检测。结果与对照组相比,模型组、沉默组、过表达组miR-139-5p表达量、HOMA-β、IRS-1、PI3K、Akt2 mRNA表达量、IRS-1、磷酸化IRS-1(p-IRS-1)、PI3K、磷酸化PI3K(p-PI3K)、Akt2、磷酸化Akt2(p-Akt2)表达量均降低,HOMA-IR、空腹胰岛素、空腹血糖、IL-6、TNF-α、总胆固醇、甘油三酯均升高,差异均有统计学意义(P<0.05);与模型组相比,沉默组、过表达组miR-139-5p表达量、HOMA-IR、空腹胰岛素、空腹血糖、IL-6、TNF-α、总胆固醇、甘油三酯均降低,HOMA-β、IRS-1、PI3K、Akt2 mRNA表达量、IRS-1、p-IRS-1、PI3K、p-PI3K、Akt2、p-Akt2表达量均升高,差异均有统计学意义(P<0.05);与沉默组相比,过表达组miR-139-5p相对表达量、HOMA-IR、空腹胰岛素、空腹血糖、IL-6、TNF-α、总胆固醇、甘油三酯降低,HOMA-β、IRS-1、PI3K、Akt2 mRNA表达量、IRS-1、p-IRS-1、PI3K、p-PI3K、Akt2、p-Akt2表达量升高,差异均有统计学意义(P<0.05)。结论上调miR-139-5p表达,可调节2型糖尿病大鼠体内血糖、血脂水平,其机制可能与IRS-1/PI3K/Akt2信号通路有关。

Ginsenoside F1 administration promotes UCP1-dependent fat browning and ameliorates obesity-associated insulin resistance

Obesity-induced type 2 diabetes is mainly due to excessive free fatty acids leading to insulin resistance.Increasing thermogenesis is regarded as an effective strategy for hypolipidemia and hypoglycemia.Ginsenoside is a natural active component in Panax ginseng C.A.Meyer,and some of them enhance thermogenesis.However,there are few studies on the mechanism and target of ginsenosides enhancing thermogenesis.Using thermogenic protein uncoupling protein 1(UCP1)-luciferase reporter assay,we identifi ed ginsenoside F1 as a novel UCP1 activator in the ginsenosides library.Using pull down assay and inhibitor interference,we found F1 binds toβ3-adrenergic receptors(β3-AR)to enhance UCP1 expression via cAMP/PKA/CREB pathway.We also investigated the ability of F1 on energy metabolism in obesity-induced diabetic mice,including body weight,body composition and energy expenditure.The results of proteomics showed that F1 signifi cantly up-regulated thermogenesis proteins and lipolytic proteins,but down-regulated fatty acid synthesis proteins.Ginsenoside F1 increased thermogenesis and ameliorated insulin resistance specifi cally by promoting the browning of white adipose tissue in obese mice.Additionally,ginsenoside F1 improves norepinephrine-induced insulin resistance in adipocytes and hepatocytes,and shows a stronger mitochondria respiration ability than norepinephrine.These fi ndings suggest that ginsenoside F1 is a promising lead compound in the improvement of insulin resistance.

AT1 receptor downregulation:A mechanism for improving glucose homeostasis

There is a pathophysiological correlation between arterial hypertension and diabetes mellitus, established since the pre-diabetic state in the entity known as insulin resistance. It is known that high concentrations of angiotensin-Ⅱ enable chronic activation of the AT1 receptor, promoting sustained vasoconstriction and the consequent development of high blood pressure. Furthermore, the chronic activation of the AT1 receptor has been associated with the development of insulin resistance. From a molecular outlook, the AT1 receptor signaling pathway can activate the JNK kinase. Once activated, this kinase can block the insulin signaling pathway, favoring the resistance to this hormone. In accordance with the previously mentioned mechanisms, the negative regulation of the AT1receptor could have beneficial effects in treating metabolic syndrome and type 2diabetes mellitus. This review explains the clinical correlation of the metabolic response that diabetic patients present when receiving negatively regulatory drugs of the AT1 receptor.