Increased Midkine and Estrogen Receptor-β Expression in Human Non-Small Cell Lung Cancer

Objective： Midkine （MK）, a new member of the heparin-binding growth factor family, has been found recently to have a high expression level in many tumor specimens including lung carcinoma. Estrogens may be involved in lung carcinogenesis, and estrogen receptors, mainly estrogen receptor-β （ER-β）, are present and functional in normal lung and tumor cell lines and tissues. In addition, estrogens and growth factors may promote the progression of human non-small cell lung cancer （NSCLC）. Previously, we have immunohistochemically demonstrated that MK and ER-β proteins were overexpressed in NSCLC and their expression levels were both significantly negatively correlated with the pathological classification. The purpose of this study was to further verify their expression and its correlation with NSCLC. Methods： Taking NSCLC tissues and their corresponding paraneoplastic and normal lung as research objects, we further examined the expression of MK and ER-β by meas of RT-PCR, in situ hybridization and Western blot analyses at the levels of messenger RNA （mRNA） and protein, respectively. Results： The increased MK and ER-β mRNA expression was found in NSCLC by RT-PCR and in situ hybridization analyses. Furthermore, Western blot analysis also displayed increased expression of MK and ER-β proteins in NSCLC. Finally, their correlation analysis at the levels of mRNA and protein expression in NSCLC demonstrated that MK protein level was significantly correlated to estrogen receptor-β （P〈0.01, rs=0.535）; in spite of their correlation at the mRNA level, there was no remarkable difference between MK and ER-β （P〉0.05, rs=0.178）. Conclusion： All these results in the present study confirmed that MK and ER-β were overexpressed in human NSCLC.

Inetetamab combined with tegafur as second-line treatment for human epidermal growth factor receptor-2-positive gastric cancer: A case report

BACKGROUND Human epidermal growth factor receptor-2(HER-2)plays a vital role in tumor cell proliferation and metastasis.However,the prognosis of HER2-positive gastric cancer is poor.Inetetamab,a novel anti-HER2 targeting drug independently developed in China,exhibits more potent antibody-dependent cell-mediated cytotoxicity than trastuzumab,which is administered as the first-line treatment for HER2-positive gastric cancer in combination with chemotherapy.In this case,the efficacy and safety of inetetamab combined with tegafur was investigated as a second-line treatment for HER2-positive gastric cancer.CASE SUMMARY A 52-year-old male patient with HER2-positive gastric cancer presented with abdominal distension,poor appetite,and fatigue two years after receiving six cycles of oxaliplatin combined with tegafur as first-line treatment after surgery,followed by tegafur monotherapy for six months.The patient was diagnosed with postoperative recurrence of gastric adenocarcinoma.He received 17 cycles of a combination of inetetamab,an innovative domestically developed anti-HER2 monoclonal antibody,and tegafur chemotherapy as the second-line treatment(inetetamab 200 mg on day 1,every 3 wk combined with tegafur twice daily on days 1–14,every 3 wk).Evaluation of the efficacy of the second-line treatment revealed that the patient achieved a stable condition and progression-free survival of 17 months.He tolerated the treatment well without exhibiting any grade 3-4 adverse events.CONCLUSION Inetetamab combined with chemotherapy for the treatment of metastatic HER2-positive gastric cancer demonstrates significant survival benefits and acceptable safety.

Clinical outcomes of lenvatinib plus transarterial chemoembolization with or without programmed death receptor-1 inhibitors in unresectable hepatocellular carcinoma

BACKGROUND Programmed death receptor-1(PD-1)inhibitors have been approved as secondline treatment regimen in hepatocellular carcinoma(HCC),but it is still worth studying whether patients can benefit from PD-1 inhibitors as first-line drugs combined with targeted drugs and locoregional therapy.AIM To estimate the clinical outcome of transarterial chemoembolization(TACE)and lenvatinib plus PD-1 inhibitors for patients with unresectable HCC(uHCC).METHODS We carried out retrospective research of 65 patients with uHCC who were treated at Peking Union Medical College Hospital from September 2017 to February 2022.45 patients received the PD-1 inhibitors,lenvatinib,TACE(PD-1-Lenv-T)therapy,and 20 received the lenvatinib,TACE(Lenv-T)therapy.In terms of the dose of lenvatinib,8 mg was given orally for patients weighing less than 60 kg and 12 mg for those weighing more than 60 kg.Of the patients in the PD-1 inhibitor combination group,15 received Toripalimab,14 received Toripalimab,14 received Camrelizumab,4 received Pembrolizumab,9 received Sintilimab,and 2 received Nivolumab,1 with Tislelizumab.According to the investigators’assessment,TACE was performed every 4-6 wk when the patient had good hepatic function(Child-Pugh class A or B)until disease progression occurred.We evaluated the efficacy by the modified Response Evaluation Criteria in Solid Tumors(mRECIST criteria).We accessd the safety by the National Cancer Institute Common Terminology Criteria for Adverse Events,v 5.0.The key adverse events(AEs)after the initiation of combination therapy were observed.RESULTS Patients with uHCC who received PD-1-Lenv-T therapy(n=45)had a clearly longer overall survival than those who underwent Lenv-T therapy(n=20,26.8 vs 14.0 mo;P=0.027).The median progression-free survival time between the two treatment regimens was also measured{11.7 mo[95%confidence interval(CI):7.7-15.7]in the PD-1-Lenv-T group vs 8.5 mo(95%CI:3.0-13.9)in the Lenv-T group(P=0.028)}.The objective response rates of the PD-1-Lenv-T group and Lenv-T group were 44.4%and 20%(P=0.059)according to the mRECIST criteria,meanwhile the disease control rates were 93.3%and 64.0%(P=0.003),respectively.The type and frequency of AEs showed little distinction between patients received the two treatment regimens.CONCLUSION Our results suggest that the early combination of PD-1 inhibitors has manageable toxicity and hopeful efficacy in patients with uHCC.

Tyrosine kinase inhibitors and human epidermal growth factor receptor-2 positive breast cancer

The body of evidence investigating human epidermal growth factor receptor-2(HER2)directed therapy in patients with breast cancer(BC)has been growing within the last decade.Recently,the use of tyrosine kinase inhibitors(TKIs)has been of particular interest in the treatment of human malignancies.This literature commentary is intended to highlight the most recent findings associated with the widely-studied TKI agents and their clinical significance in improving the outcomes of HER2 positive BC.

青少年体内35种抗生素和4种β-受体激动剂的测定及暴露现状分析

为了解我国青少年体内抗生素和β-受体激动剂的暴露水平,本研究采用同位素稀释-高通量全自动固相萃取-超高效液相色谱-串联质谱法测定某中学442名青少年(11~15岁)尿液中的7类共35种抗生素(5种大环内酯类、4种四环素类、10种喹诺酮类、3种β-内酰胺类、11种磺胺类、1种喹噁啉类和1种林可酰胺类)和4种β-受体激动剂的水平。尿样测定结果采用尿肌酐进行校正,所得到的样品检出率用于统计分析。采用皮尔森卡方检验对目标物检出率与性别、年龄和体重等级间的相关性进行分析。在调整了混杂因素后,采用Logistic回归模型来评估目标物检出率与不同组别间的相关性。分析结果发现,442名青少年中有397名青少年的尿液中检出抗生素或β-受体激动剂,总体检出率为89.8%。除喹噁啉类抗生素未被检出外,实验中共有6类27种抗生素和2种β-受体激动剂被检出,检出率为0.2%~59.0%;其中强力霉素、土霉素和阿奇霉素的检出率最高,检出率分别为59.0%、56.1%和34.6%;四环素类和大环内酯类抗生素是主要检出的两类抗生素,检出率分别为81.9%和42.3%;优先作为兽用的抗生素检出率最高(85.1%),其次为人用抗生素(41.0%),β-受体激动剂的总体检出率为2.7%。统计分析发现,四环素类抗生素在男性青少年尿液中的检出率高于女性,男性检出风险是女性的2.17倍。大环内酯类抗生素在不同年龄组间的检出率存在差异,与11岁青少年组相比,12、13岁青少年组的检出风险更高。实验发现,大环内酯类抗生素的检出率与青少年的肥胖程度呈正相关;在调整了年龄和性别因素后,肥胖青少年尿液中大环内酯类抗生素的检出风险是正常体重者的2.35倍。研究结果表明,青少年普遍暴露于低剂量的抗生素,且食物和环境中的抗生素可能是青少年体内抗生素暴露的主要来源,大环内酯类抗生素的暴露可能与青少年的肥胖风险相关。

外用β受体阻滞剂和脉冲燃料激光治疗低、中风险血管瘤的效果对比

目的比较外用β受体阻滞剂和激光治疗低、中风险血管瘤的效果。方法将2018年10月—2021年9月本院收治的262例低、中风险婴幼儿血管瘤患者根据治疗方式分为脉冲燃料激光组(85例)、外用0.5%噻马洛尔组(91例)和外用2%卡替洛尔组(86例)。对比各组的疗效。脉冲燃料激光治疗采用595nm PDL联合1064nm Nd:钇铝石榴石(yttrium aluminum garnet,YAG),每月1次,持续治疗1~6月。其余两组将外用β受体阻滞剂湿敷于瘤体上,持续30min,每日湿敷2次。结果总有效率方面,激光组与噻马洛尔组的差异不明显,无统计学意义(P>0.05),但与卡替洛尔组相比,组间差异显著,有统计学意义(P<0.05)。激光组疗程为(3.47±1.46)月,明显快于外用β受体阻滞剂组,组间差异显著,有统计学意义(P<0.05)。噻马洛尔组的疗程(9.33±5.80月)较卡替洛尔组(5.57±2.57月)长,但噻马洛尔组有效率(85.4%)较卡替洛尔组(79.3%)高。三组血管瘤疗效与性别、风险等级没有相关性。浅表性血管瘤的疗效明显优于混合性。结论无论是脉冲燃料激光还是外用β受体阻滞剂均对低、中风险血管瘤有效。激光治疗较外用β受体阻滞剂控制快、疗程短。建议尽早开始治疗,最好在出生3月以内,并坚持用药保证一定的疗程,使治疗效果达到最优。

α7烟碱型乙酰胆碱受体与阿尔茨海默病的关系

背景:α7烟碱型乙酰胆碱受体在大脑皮质和海马高度表达,并在阿尔茨海默病的病理发展过程中起重要调控作用,是阿尔茨海默病治疗的潜在靶点。目的:总结α7烟碱型乙酰胆碱受体和阿尔茨海默病的密切关系和相互作用机制。方法:检索中国知网、PubMed数据库中相关文献,中文检索词为“α7烟碱型乙酰胆碱受体,阿尔茨海默病,β-淀粉样蛋白,激动剂,正变构调节剂,拮抗剂”;英文检索词为“alpha 7 nicotinic acetylcholine receptor,Alzheimer’s disease,beta amyloid protein,agonist,positive allosteric modulator,antagonist”,文献检索时限为各数据库建库至2024年7月,依据入选标准对检索结果进行录用或排除,最终纳入符合标准的83篇文献进行综述。结果与结论:α7烟碱型乙酰胆碱受体通过与β-淀粉样蛋白的相互作用减轻β-淀粉样蛋白的神经毒性,如促进阿尔茨海默病的突触可塑性和胆碱能突触的快速传递、减轻β-淀粉样蛋白诱导的神经中枢炎症反应、抵抗神经细胞凋亡,从而对阿尔茨海默病患者的脑具有保护作用等。α7烟碱型乙酰胆碱受体作为阿尔茨海默病治疗靶标具有很大的潜能,但是又存在一系列问题有待解决,比如α7烟碱型乙酰胆碱受体的脱敏性、适度活性稳定性及基因多态性等问题。筛选高特异、安全性和以α7烟碱型乙酰胆碱受体为核心的多靶点结合作用的药物,将成为未来阿尔茨海默病治疗研究的一个方向。

血清HBD-3、DCR3对复杂性肾结石患者经皮肾镜碎石术后尿路感染的预测价值

目的分析血清β-防御素-3(HBD-3)、诱骗受体3(DCR3)对复杂性肾结石患者经皮肾镜碎石术后尿路感染的预测价值。方法选取2020年1月—2022年12月河北省沧州中西医结合医院收治的112例复杂性肾结石患者为研究对象进行回顾性研究,所有患者均行经皮肾镜碎石术(PCNL),根据术后感染情况将患者分为非尿路感染组52例、尿路感染组60例。比较两组一般资料及HBD-3、DCR3水平。受试者工作特征(ROC)曲线分析C反应蛋白(CRP)、降钙素原(PCT)、HBD-3、DCR3水平对术后尿路感染的预测价值。结果与非尿路感染组比较,尿路感染组的HBD-3[(0.77±0.08)ng/mL vs.(1.36±0.25)ng/mL,P=0.001]、DCR3[(4.68±0.53)ng/mL vs.(13.21±0.28)ng/mL,P=0.001]水平较高。多因素logistics回归分析显示,泌尿道手术史、术前尿路感染、手术时间、导尿管留置时间、结石负荷、抗菌药物种类、合并肾功能障碍、术中通道类型CRP、PCT、HBD-3、DCR3为患者术后尿路感染的影响因素(P<0.05)。ROC曲线显示,CRP、PCT、CRP联合PCT准确度分别为70.54%、72.32%、78.57%;HBD-3、DCR3、HBD-3联合DCR3准确度分别为69.64%、75.89%、86.61%。结论复杂性肾结石患者术后尿路感染与多种因素相关,且术后尿路感染患者HBD-3、DCR3表达水平较高,联合检测对术后尿路感染具有较高的预测价值。

水泡性口炎病毒对体外血管内皮屏障功能的损伤作用及其机制

目的:探讨水泡性口炎病毒(VSV)对血管内皮(VE)屏障的损伤作用,并阐明其作用机制。方法:采用犬肾细胞对VSV进行扩增,采用小鼠脑血管内皮瘤bEnd. 3细胞检测VSV的半数组织培养感染剂量(TCID_(50)),采用300倍TCID_(50)进行后续实验。将bEnd. 3细胞分为感染0 h组、感染4 h组、感染8 h组和感染12 h组,进行VSV感染损伤VE屏障实验;将bEnd. 3细胞分为对照组、感染组和纠正组,进行抑制VSV复制与VE屏障恢复实验。将bEnd. 3细胞接种于Transwell小室,构建体外VE屏障模型,采用细胞电压电阻仪检测感染VSV不同时间后各组bEnd. 3细胞中跨上皮电阻(TER),采用异硫氰酸荧光素-葡聚糖渗漏实验检测各组渗透系数,采用免疫荧光染色法观察VSV感染后各组bEnd. 3细胞骨架及黏附连接(AJs)中VE-钙黏蛋白、β-连环蛋白(β-catenin)和磷酸化β-连环蛋白(p-β-catenin)定位变化,采用实时荧光定量PCR (RT-qPCR)法检测各组细胞中Wnt和β-catenin mRNA表达水平,采用Western blotting法检测各组细胞中Wnt、β-catenin和p-β-catenin表达水平。结果:VSV的TCID_(50)为10^(-4.5)·100μL^(-1)。Transwell小室实验检测,与感染0 h比较,其他各组细胞中TER明显降低(P<0.05),渗透系数明显升高(P<0.05)。免疫荧光染色,与对照组比较,感染组bEnd. 3细胞骨架紊乱,细胞间隙增大,AJs线性指数明显降低(P<0.05),β-catenin和p-β-catenin从细胞膜转移至细胞核周围。RT-qPCR法检测,与感染0 h比较,其他各组细胞中Wnt mRNA表达水平明显降低(P<0.05),β-catenin mRNA表达水平差异无统计学意义(P>0.05)。Western blotting法检测,与感染0 h比较,其他各组细胞中Wnt蛋白表达水平明显降低(P<0.05),β-catenin表达水平差异无统计学意义(P>0.05),p-β-catenin表达水平明显升高(P<0.05)。在抑制VSV复制并纠正低密度脂蛋白受体(LDLR)异常后,Transwell小室实验检测,与感染组比较,纠正组bEnd. 3细胞中TER明显升高(P<0.05),渗透系数明显降低(P<0.05)。免疫荧光染色,与感染组比较,纠正组细胞间隙减小,细胞中β-catenin和p-β-catenin核周聚集现象有所改善。RT-qPCR法检测,与感染组比较,纠正组细胞中Wnt mRNA表达水平明显升高(P<0.05)。Western blotting法检测,与感染组比较,纠正组细胞中Wnt蛋白表达水平明显升高(P<0.05),β-catenin表达水平差异无统计学意义(P>0.05),p-β-catenin表达水平明显降低(P<0.05)。结论:VSV感染后可引起LDLR失活,降低Wnt蛋白表达水平,造成β-catenin磷酸化水平升高并发生内化,破坏AJs稳定性,最终导致VE屏障损伤。

GPR120激动剂通过β-Arrestin2途径改善高糖诱导的海绵体内皮细胞功能障碍

目的探讨激活G蛋白偶联受体(GPR)120对高糖诱导的人类阴茎海绵体内皮损伤修复的影响,以期为寻找糖尿病性勃起功能障碍(DMED)新的药物开发靶点提供理论依据。方法收集海绵体植入手术患者术中废弃海绵体组织提取海绵体内皮细胞进行原代培养,用高浓度葡萄糖诱导内皮细胞损伤,再以GPR120激动剂治疗,观察对比不同处理的细胞一氧化氮(NO)释放量、细胞迁移、血管生成等功能。结果成功提取人类海绵体内皮细胞进行原代培养并鉴定;发现GPR120在人类海绵体内皮细胞中稳定表达,且与内皮型一氧化氮合酶(eNOS)存在共定位;与高糖损伤组相比,GPR120激动剂治疗组NO释放量、划痕愈合率和血管生成率均显著增加(P<0.05);沉默β-Arrestin2后GPR120激动剂失去原有的治疗效果。结论高糖培养可诱导海绵体内皮细胞功能障碍,GPR120激动剂能够治疗海绵体内皮功能障碍,沉默β-Arrestin2后GPR120激动剂无法改善内皮功能。

Activation of G-protein-coupled receptor 39 reduces neuropathic pain in a rat model

Activated G-protein-coupled receptor 39(GPR39)has been shown to attenuate inflammation by interacting with sirtuin 1(SIRT1)and peroxisome proliferator-activated receptor-γcoactivator 1α(PGC-1α).However,whether GPR39 attenuates neuropathic pain remains unclear.In this study,we established a Sprague-Dawley rat model of spared nerve injury-induced neuropathic pain and found that GPR39 expression was significantly decreased in neurons and microglia in the spinal dorsal horn compared with sham-operated rats.Intrathecal injection of TC-G 1008,a specific agonist of GPR39,significantly alleviated mechanical allodynia in the rats with spared nerve injury,improved spinal cord mitochondrial biogenesis,and alleviated neuroinflammation.These changes were abolished by GPR39 small interfering RNA(siRNA),Ex-527(SIRT1 inhibitor),and PGC-1αsiRNA.Taken together,these findings show that GPR39 activation ameliorates mechanical allodynia by activating the SIRT1/PGC-1αpathway in rats with spared nerve injury.

应激性心肌病的研究进展

应激性心肌病是以可逆性室壁运动异常为特征的一种心血管综合征,临床表现与急性冠脉综合征相似,但冠状动脉造影显示冠状动脉解剖正常。应激性心肌病的发病机制尚未完全明确,临床诊断不易,标准治疗药物存在争议,因并发症和复发风险导致预后不佳。现总结应激性心肌病的流行病学、发病机制、诊断和治疗方面的最新进展,以期为改善疾病的预后提供思路。

Argatroban promotes recovery of spinal cord injury by inhibiting the PAR1/JAK2/STAT3 signaling pathway

Argatroban is a synthetic thrombin inhibitor approved by U.S.Food and Drug Administration for the treatment of thrombosis.However,whether it plays a role in the repair of spinal cord injury is unknown.In this study,we established a rat model of T10 moderate spinal cord injury using an NYU Impactor ModerⅢand performed intraperitoneal injection of argatroban for 3 consecutive days.Our results showed that argatroban effectively promoted neurological function recovery after spinal cord injury and decreased thrombin expression and activity in the local injured spinal cord.RNA sequencing transcriptomic analysis revealed that the differentially expressed genes in the argatroban-treated group were enriched in the JAK2/STAT3 pathway,which is involved in astrogliosis and glial scar formation.Western blotting and immunofluorescence results showed that argatroban downregulated the expression of the thrombin receptor PAR1 in the injured spinal cord and the JAK2/STAT3 signal pathway.Argatroban also inhibited the activation and proliferation of astrocytes and reduced glial scar formation in the spinal cord.Taken together,these findings suggest that argatroban may inhibit astrogliosis by inhibiting the thrombin-mediated PAR1/JAK2/STAT3 signal pathway,thereby promoting the recovery of neurological function after spinal cord injury.

Reconceptualization of immune checkpoint inhibitor-associated gastritis

In recent years,with the extensive application of immunotherapy in clinical practice,it has achieved encouraging therapeutic effects.While enhancing clinical efficacy,however,it can also cause autoimmune damage,triggering immunerelated adverse events(irAEs).Reports of immunotherapy-induced gastritis have been increasing annually,but due to its atypical clinical symptoms,early diagnosis poses a certain challenge.Furthermore,it can lead to severe complications such as gastric bleeding,elevating the risk of adverse outcomes for solid tumor patients if immunotherapy is interrupted.Therefore,gaining a thorough understanding of the pathogenesis,clinical manifestations,diagnostic criteria,and treatment of immune-related gastritis is of utmost importance for early identification,diagnosis,and treatment.Additionally,the treatment of immune-related gastritis should be personalized according to the specific condition of each patient.For patients with grade 2-3 irAEs,restarting immune checkpoint inhibitors(ICIs)therapy may be considered when symptoms subside to grade 0-1.When restarting ICIs therapy,it is often recommended to use different types of ICIs.For grade 4 irAEs,permanent discontinuation of the medication is necessary.

髓系细胞触发受体2在阿尔茨海默病中的作用

阿尔茨海默病(AD)是老年性痴呆症中最常见的形式,其发病机制仍不清楚,但β淀粉样蛋白(Aβ)被认为是引起AD发病的重要原因,然而其引发AD的病理机制同样存在多种争议。最近研究显示,髓系细胞触发受体(TREM2)在AD病理进程中扮演重要角色,其不仅可以作为Aβ内化的重要受体,还可能成为生物学诊断标志物和治疗靶点,阐明TREM2的结构和功能,将为AD的防治提供重要的思路。本文将从TREM2的结构、TREM2对小胶质细胞功能的影响、TREM2在AD中的病理学作用以及靶向TREM2治疗AD的现状进行系统性综述,这些总结将为AD的基础研究提供具有价值的参考。

神经肽Y/Y1受体激活β⁃catenin信号通路介导心肌细胞损伤

目的:研究神经肽Y(neuropeptide Y,NPY)/Y1受体信号转导在心肌细胞损伤中的作用及机制。方法:C57BL/6J小鼠皮下注射异丙肾上腺素(isoprenaline,ISO)构建心肌损伤模型,腹腔注射Y1受体特异性拮抗剂BIBO3304干预。小鼠随机分为对照组(生理盐水)、ISO组[20 mg/(kg·d)ISO]、BIBO3304+ISO组[0.1 mg/(kg·d)BIBO3304+20 mg/(kg·d)ISO]、BIBO3304组[0.1 mg/(kg·d)BIBO3304],每组10只,连续给药14 d。实时定量PCR和Western blot检测小鼠心肌组织中NPY表达。HE染色和Masson染色观察各组小鼠心肌纤维结构变化和纤维化程度;定量PCR检测小鼠心肌肥大基因心房钠尿肽(atrial natriuretic peptide,ANP)、β⁃肌球蛋白重链(β⁃myosin heavy chain,β⁃MHC)mRNA表达。采用Y1受体特异性激活剂[Leu31,Pro34]⁃NPY刺激H9C2细胞,检测ANP、β⁃MHC mRNA表达;CCK⁃8检测心肌细胞活力。Western blot检测各组小鼠心肌组织和H9C2细胞中activeβ⁃catenin、磷酸化糖原合成酶激酶⁃3β(phospho⁃glycogen synthesis kinase 3β,p⁃GSK3β)、总糖原合成酶激酶⁃3β(total glyco⁃gen synthesis kinase 3β,t⁃GSK3β)蛋白表达。免疫荧光染色检测心肌细胞β⁃catenin入核情况。利用β⁃catenin特异性抑制剂ICG001处理细胞,检测[Leu31,Pro34]⁃NPY诱导的心肌细胞肥大和细胞活力变化。结果:与对照组比较,ISO组小鼠心肌组织NPY mRNA和蛋白表达均显著增加(P<0.05),心肌纤维排列紊乱,心肌纤维化程度高,心肌肥大基因表达增加。与ISO组比较,BIBO3304+ISO组小鼠心肌损伤和纤维化得到有效缓解,心肌肥大基因表达下降(P<0.01)。与对照组比较,[Leu31,Pro34]⁃NPY增加H9C2细胞ANP、β⁃MHC mRNA表达,降低心肌细胞活力(P<0.01)。与对照组比较,ISO组小鼠心肌组织activeβ⁃catenin、p⁃GSK3β表达明显上调,p⁃GSK3β/t⁃GSK3β增加;与ISO组比较,BIBO3304+ISO组心肌组织activeβ⁃catenin、p⁃GSK3β表达降低(P<0.05)。与对照组比较,[Leu31,Pro34]⁃NPY显著增加心肌细胞activeβ⁃catenin、p⁃GSK3β表达(P<0.05),促进细胞核β⁃catenin积累。与[Leu31,Pro34]⁃NPY组比较,BIBO3304抑制细胞核β⁃catenin表达,ICG001显著缓解[Leu31,Pro34]⁃NPY诱导的心肌细胞肥大和细胞活力下降(P<0.01)。结论:NPY通过Y1受体转导激活β⁃catenin信号通路介导心肌细胞损伤和心肌纤维化。

NLRP3炎症小体在阿尔兹海默症中的作用及潜在治疗靶点

阿尔兹海默症(Alzheimer’s disease,AD)是常见的神经退行性疾病,严重影响患者的生存质量。目前尚无有效的针对性治疗措施。AD发病机制复杂,是环境、遗传和年龄影响因素共同作用的结果。大脑中β-淀粉样蛋白(β-amyloid,Aβ)沉积、微管相关蛋白tau过度磷酸化形成的神经纤维缠结及神经元丢失是AD典型病理特征,大量研究证明,Aβ、tau蛋白聚集诱导核苷酸结合寡聚化结构域样受体含pyrin结构域蛋白3(nucleotide-binding oligomerization domain-like receptor pyrin domain-containing 3,NLRP3)炎症小体活化是AD炎性机制的核心环节,且以其和上下游分子为靶点的抑制剂和化合物治疗在细胞和动物模型中均发挥神经保护作用,改善空间记忆功能障碍,但临床疗效和安全性仍待研究。因此,抑制NLRP3炎症小体的活化可能是AD的潜在治疗靶点。本文以NLRP3炎症小体的活化机制和影响因素及与AD关系进行综述,并总结以NLRP3炎症小体为靶点的AD治疗药物,以期为AD等NLRP3炎症小体相关疾病提供新的治疗方向。

β-细辛醚通过抑制TRPV4的表达缓解谷氨酸诱导的Ca^(2+)超载

谷氨酸处理会导致Ca^(2+)超载,瞬时受体电位香草素受体4(transient receptor potential vanilloid 4,TRPV4)在其中的作用及可能机制尚不清楚。β-细辛醚能快速透过血脑屏障,对兴奋性毒性具有较强的神经保护作用。文章以高分化的PC12细胞为研究对象,探究β-细辛醚(15、30、60μmol/L)预处理4 h,40 mmol/L谷氨酸处理实时记录对PC12细胞Ca^(2+)浓度的影响,采用钙成像技术检测Ca^(2+)浓度的变化;采用实时荧光定量聚合酶链式反应(polymerase chain reaction,PCR)、Western Blot及免疫荧光技术检测TRPV4的mRNA和蛋白的表达;采用Lipofectiamine 2000脂质体实验转染TRPV4-siRNA和pEX-3-TRPV4,观察沉默和过表达TRPV4对谷氨酸引起Ca^(2+)超载的影响。结果表明:与正常对照组相比,谷氨酸处理5 min可诱导Ca^(2+)超载,显著提高TRPV4的mRNA和蛋白的表达;与模型组相比,β-细辛醚能够剂量依赖性地降低谷氨酸诱导的Ca^(2+)超载和TRPV4的表达;沉默TRPV4抑制细胞Ca^(2+)超载;过表达TRPV4则部分逆转β-细辛醚抑制谷氨酸诱导的Ca^(2+)超载。该研究证明,谷氨酸处理PC12细胞5 min通过上调TRPV4的表达诱导Ca^(2+)超载,β-细辛醚作为TRPV4的拮抗剂,是一种潜在的抑制兴奋性毒性的药物。

ADRB1基因多态性对比索洛尔疗效影响的Meta分析

目的基于Meta分析评价β_(1)肾上腺素受体(ADRB1)389位点(rs 1801253)基因多态性对比索洛尔疗效的影响。方法通过计算机检索中国知网、维普网、万方数据知识服务平台、Web of Science、PubMed等数据库收集关于ADRB1与比索洛尔研究的文献,检索时间为建库至2023年7月。研究人员对发表的文献进行筛选,并将纳入文献进入质量评价,提取文献数据,对纳入文献结局指标使用Review Manager 5.3软件进行Meta分析。结果最终纳入文献6篇,其中Gly389Gly(GG型)69例,Gly389Arg(GC型)458例,Arg389Arg(CC型)611例。在降收缩压、舒张压及控制心率疗效方面,GG与CC基因型差异无统计学意义(P=0.96,P=0.84,P=0.87),GC与CC基因型差异无统计学意义(P=0.43,P=0.35,P=0.07),GG与GC基因型差异亦无统计学意义(P=0.60,P=0.68,P=0.77)。结论在比索洛尔降压及控制心率方面,ADRB1389位点基因多态性对其疗效影响并不明显。GG、GC及CC 3个基因型之间均未发现明显差异。

绞股蓝总皂苷通过PPAR-γ与Wnt途径影响大鼠动脉粥样硬化及部分有效成分预测

目的探讨绞股蓝总皂苷对动脉粥样硬化大鼠主动脉炎症反应的影响及预测部分绞股蓝有效成分。方法将60只SD大鼠分为空白对照组(Nor组,)、模型组(Mod组)、辛伐他汀组(Sim组,5 mg/kg灌胃,13周)、绞股蓝总皂苷组(GPs组,160 mg/kg灌胃,13周)、GW9662组(PPAR-γ抑制剂,10 mg/kg灌胃,13周)及GPs+GW9662组[GPs 160 mg/kg及GW966210 mg/(kg·d),灌胃,13周],其中Nor组普通饮食,其他组予以高脂饲料联合腹腔注射维生素D 3以构建动脉粥样硬化大鼠模型;建模13周后取大鼠血液、胸主动脉和腹主动脉,HE切片染色观察胸主动脉组织学变化,ELISA测定血清中IL-6含量,Western blot检测腹主动脉过氧化酶体增殖物激活受体-γ(PPAR-γ),Wnt3a及β-catenin蛋白表达、qRT-PCR检测腹主动脉PPAR-γ及Wnt3a及β-catenin mRNA表达;利用分子对接初步筛选绞股蓝总皂苷与PPAR-γ亲和力较高的有效成分。结果与Nor组比较,Mod组及其他干预组大鼠主动脉切片可见AS特征性病变,其中GW9662组病变明显,辛伐他汀和绞股蓝总皂苷各干预组病变较轻;与Mor组相比,GPs组大鼠血清白细胞介素-6(IL-6)含量显著减少;与Mor组大鼠腹主动脉比较,GPs组PPAR-γ蛋白和mRNA的表达显著减少(P<0.05)、其他非阳性对照干预组均不同程度增高,而Mor组Wnt3a、β-catenin和mRNA表达与Nor组相比明显升高(P<0.05)、其他非阳性对照干预组均不同程度减少,其中GPs组显著降低;分子对接结果显示野黄芩苷、胆固醇、菜油甾醇、谷甾醇、3′-甲基鼠李素对PPAR-γ具有较强的亲和力。结论绞股蓝总皂苷可能是通过调节PPAR-γ与Wnt经典途径改善大鼠动脉粥样硬化,野黄芩苷、胆固醇、菜油甾醇、谷甾醇、3′-甲基鼠李素成分是绞股蓝部分有效成分。