Arginase-1、Glypican-3、HepPar-1在肝细胞癌中的表达及意义

目的研究肝细胞癌(hepatocellular carcinoma,HCC)、肝脏良性病变组织中精氨酸酶-1(arginase-1,Arg-1)、磷脂酰肌醇蛋白聚糖-3(glypican-3,GPC-3)、肝细胞抗原(Hep-1)的表达情况,探讨三种抗体及其他临床病理参数与肿瘤预后的相关性。方法回顾性分析156例HCC患者及146例肝脏良性病变患者的临床病理特征,免疫组织化学方法检测三种抗体的表达,并结合HCC患者随访资料行临床病理学参数与预后关系分析。结果 Arg-1、GPC-3、Hep-1在HCC及肝脏良性病变中的表达率分别为93.6%(146/156)、90.4%(141/156)、85.3%(133/156)和97.3%(142/146)、3.4%(5/146)、98.6%(144/146)。单因素分析显示肿瘤直径、肿瘤多发、脉管癌栓、谷丙转氨酶(ALT)、谷草转氨酶(AST)、白蛋白(ALB)及Arg-1是影响HCC患者术后总体生存率的预后因素;多因素COX回归分析结果显示,肿瘤直径与脉管瘤栓是影响HCC患者术后总体生存率的独立预后因素。结论联合应用Arg-1、GPC-3和Hep-1在HCC与肝脏良性结节性病变的鉴别诊断中具有重要意义。Arg-1可作为评估HCC患者预后的参考指标。

Competitive metabolism of L-arginine:arginase as a therapeutic target in asthma

Exhaled breath nitric oxide （NO） is an accepted asthma biomarker. Lung concentrations of NO and its amino acid precursor, L-arginine, are regulated by the relative expressions of the NO synthase （NOS） and arginase isoforms. Increased expression of arginase I and NOS2 occurs in murine models of allergic asthma and in biopsies of asthmatic airways. Although clinical trials involving the inhibition of NO-producing enzymes have shown mixed results, small molecule arginase inhibitors have shown potential as a therapeutic intervention in animal and cell culture models. Their transition to clinical trials is hampered by concerns regarding their safety and potential tox- icity. In this review, we discuss the paradigm of arginase and NOS competition for their substrate L-arginine in the asthmatic airway. We address the functional role of L-arginine in inflammation and the potential role of arginase inhibitors as therapeutics.

微藻生物系统去除抗生素和ARGs的研究进展

抗生素与抗生素抗性基因(ARGs)污染严重危害人类健康,微藻生物技术在处理抗生素废水过程中表现出良好的效果。文章首先总结了微藻对于不同种类抗生素的去除机理,包括生物吸附、生物累积、生物降解、光生物降解和水解挥发5种。分析了微藻在去除抗生素过程中的重要影响因素,包括pH、水力停留时间、光照、抗生素的种类与浓度和微藻的种类。并总结了微藻对ARGs的去除机制,包括移动基因元件的去除及活性氧自由基的猝灭。最后,文章指出了微藻处理抗生素废水过程中仍然存在的问题,进一步明确了今后微藻生物技术处理抗生素废水的重点研究方向。

Arginase as a Potential Target in the Treatment of Alzheimer’s Disease

Alzheimer’s disease (AD) is a slowly progressive, neurodegenerative disorder with an insidious onset that is characterized by severe decline in memory, thinking and reasoning skills. Advanced age is a prominent risk factor for AD and other metabolic diseases, such as type II diabetes and atherosclerosis. Their causal mechanisms are multifaceted and not fully understood. The precise pathophysiology of AD remains a mystery despite decades of intensive investigation. Thus far, there is no truly successful AD therapy. Arginase is the central enzyme of the urea cycle. Recent studies have identified arginase function in the brain and associated this enzyme with the development of neurodegenerative diseases. Upregulation of arginase has been shown to contribute to endothelial dysfunction, ischemia-reperfusion, atherosclerosis, diabetes, and neurodegeneration. Other state-of-the-art discoveries of the precise molecular machinery of neurodegeneration have provided new directions for the rational development of innovative therapeutic strategies in the treatment of common neurodegenerative diseases. In this context, the regulation of arginase activity appears to be a universal approach in interfering with the pathogenesis of AD and providing relief for it and other metabolic disorders. Therefore, the enzyme represents a novel therapeutic target. Arginase inhibition has been shown to reverse amyloid-driven neuronal dysfunction and microgliosis and prevent the development of other AD symptoms in rodent models of AD. Consequently, the methodology represents a promising direction for clinical development.

ADRB1 Arg389Gly多态性对比索洛尔疗效影响的Meta分析

目的探索ADRB1 Arg389Gly多态性对比索洛尔疗效的影响,为比索洛尔个体化药物治疗提供参考。方法从PubMed、Embase、Cochrane Library、中国生物医学文献服务系统、中国知网、万方等数据库系统性搜索与比索洛尔和ADRB1 Arg389Gly多态性相关的文献,检索时间为建库至2023年5月。根据研究制定的纳入与排除标准筛选、提取相关文献并进行文献质量评估。使用RevMan 5.4软件对相关结局指标进行Meta分析。结果最终纳入7项研究,共计1339人次。其中4项研究涉及比索洛尔治疗前后收缩压(SBP)和舒张压(DBP)的变化量(ΔSBP和ΔDBP),有4项研究涉及治疗前后左室射血分数(LVEF)的变化量(ΔLVEF)。研究结果显示,比索洛尔对ADRB1 Arg389Gly野生组(AA)和突变组(AG+GG)血压改善的差异均无统计学意义{ΔSBP[SMD=0.17,95%CI(-0.97,1.31),P=0.77]、ΔDBP[SMD=-0.01,95%CI(-0.65,0.62),P=0.97]};比索洛尔对两组ΔLVEF改善的差异亦无统计学意义[SMD=-0.61,95%CI(-2.74,1.53),P=0.58]。结论ADRB1 Arg389Gly多态性对比索洛尔改善心血管患者SBP、DBP和LVEF的作用无显著影响。

Helicobacter pylori arginase mutant colonizes arginase Ⅱ knockout mice

AIM: To investigate the role of host and bacterial arginases in the colonization of mice by Helicobacter pylori (H.pylori).METHODS: H.pylori produces a very powerful urease that hydrolyzes urea to carbon dioxide and ammonium,which neutralizes acid.Urease is absolutely essential to H.pylori pathogenesis;therefore,the urea substrate must be in ample supply for urease to work efficiently.The urea substrate is most likely provided by arginase activity,which hydrolyzes L-arginine to L-ornithine and urea.Previous work has demonstrated that H.pylori arginase is surprisingly not required for colonization of wild-type mice.Hence,another in vivo source of the critical urea substrate must exist.We hypothesized that the urea source was provided by host arginase Ⅱ,since this enzyme is expressed in the stomach,and H.pylori has previously been shown to induce the expression of murine gastric arginase Ⅱ.To test this hypothesis,wild-type and arginase (rocF) mutant H.pylori strain SS1 were inoculated into arginase Ⅱ knockout mice.RESULTS: Surprisingly,both the wild-type and rocF mutant bacteria still colonized arginase Ⅱ knockout mice.Moreover,feeding arginase Ⅱ knockout mice the host arginase inhibitor S-(2-boronoethyl)L-cysteine (BEC),while inhibiting > 50% of the host arginase Ⅰ?activity in several tissues,did not block the ability of the rocF mutant H.pylori to colonize.In contrast,BEC poorly inhibited H.pylori arginase activity.CONCLUSION: The in vivo source for the essential urea utilized by H.pylori urease is neither bacterial arginase nor host arginase Ⅱ;instead,either residual host arginase Ⅰ?or agmatinase is probably responsible.

C1q/TNF-related protein 1 promotes vasodilatory dysfunctions by increasing arginase 1 activity and uncoupling of endothelial nitric oxide synthase

Objective C1q/TNF-related protein(CTRP)1 was initiallyidentified as a paralog of adiponectin based on the similarity in C1q domain of these two proteins.Previously,we showed that CTRP1promotes the development of atherosclerosis by increasing endothelial adhesiveness.Here,we sought to investigate whether CTRP1 also influences vascular dilatory functions.

超声心动图指标联合血清ARG1、G6PD在脓毒症患儿预后评估中的价值

目的探讨超声心动图指标联合血清重组人精氨酸酶1(ARG1)、葡萄糖-6-磷酸脱氢酶(G6PD)在脓毒症患儿预后评估中的价值。方法将2022年5月至2023年6月该院收治的116例脓毒症患儿纳入研究作为脓毒症组。根据脓毒症病情程度,将其进一步分为一般脓毒症组(52例)、严重脓毒症组(38例)和脓毒症休克组(26例),另根据患儿预后情况将脓毒症患儿分为预后良好组(84例)和预后不良组(32例)。选取同期于该院行体检的健康儿童116例纳入研究作为对照组。采用彩色多普勒超声仪对纳入研究者进行超声检查,检测受试者左心室射血分数(LVEF)、左室舒张末内径(LVEDD)、左室舒张末容积(LVEDV)及二尖瓣舒张早期血流峰值速度(E)。采用酶联免疫吸附法(ELISA)检测血清ARG1、G6PD水平。比较脓毒症组与对照组、不同病情程度及不同预后脓毒症患儿超声心动图指标及血清ARG1、G6PD水平。采用受试者工作特征曲线(ROC)分析超声心动图指标联合血清ARG1、G6PD对脓毒症患儿预后不良的预测价值。结果与对照组比较,脓毒症组患儿LVEF、E及G6PD水平降低(P<0.05),而LVEDD、LVEDV及ARG1升高(P<0.05)。随着脓毒症病情程度的加重,脓毒症患儿LVEF、E、G6PD水平逐渐降低(P<0.05),而LVEDD、LVEDV及ARG1水平逐渐升高(P<0.05)。预后不良组脓毒症患儿LVEF、E、G6PD水平低于预后良好组(P<0.05),LVEDD、LVEDV、ARG1水平高于预后良好组(P<0.05)。ROC曲线分析显示,超声心动图指标联合血清ARG1、G6PD预测脓毒症患儿预后不良的AUC为0.971,灵敏度和特异度分别为84.4%、83.2%。结论脓毒症患儿LVEF、E、G6PD水平明显降低,LVEDD、LVEDV、ARG1水平明显升高。超声心动图指标联合血清ARG1、G6PD对脓毒症患儿预后不良具有较高的预测价值。

Performance Parameters:Demobilization Antibiotic Resistant Bacteria(ARB)and Carrying Genes(ARG)in Wastewater Disinfection

The UV irradiation is used for removing Antibiotic Resistant Bacteria(ARB)and Antibiotic Resistance Genes(ARG)from wastewater treatment.Bacteriophages are viruses that infect within bacteria,are recognized for bacterial control.The influence of some parameters in quantification and performance influencing of pathogen demobilization could be considered in disinfection of wastewater.The comparison of Polyvalent phage(NE1)versus Coliphage(NE4)in suppressing a bacterium Escherichia coli(NDM-1:b-lactam-resistant)with UV irradiation was observed the efficacy in reduction of cells in the disinfection and parameter process.The results with the effect of UV-C irradiation on NDM-1 infected with 1%of NE4 showed a decrease of cells from 8×10^(6)to 2×10^(5)in 60 min with UV-C dose.The NDM1(E.coli)was infected with 1%of NE4(Polyvalent Phage)under magnetic stirring for 1 h,the cells count was 8×10^(6).After 1 h in UV-C e×posure,the cells number reached 3×10^(5).The NDM1 that was e×posed in 1 h of UV-C irradiation and then was infected with 1%of NE4.Cells counting were done 24 h after this procedure.These cells were e×posed in UV-C and showed a reduction in the number of cells from 1×10^(8)to 4×10^(5)after 60 min.The results indicate that bacteriophages can mitigate bacteria species,and combined the conventional water disinfection technologies that can support the microbial safety control strategies.

Relationship of Transforming Growth Factor-β1 and Arginase-1 Levels with Long-term Survival after Kidney Transplantation

In this study, we compared the serum levels of transforming growth factor-β1 （TGF-β1）, interleukin-10 （IL-10）, and arginase-1 in long-term survival kidney transplant recipients （LTSKTRs） with those in short-term survival kidney transplant recipients （STSKTRs）. We then evaluated the relationship between these levels and graft function. Blood samples were collected from 50 adult LTSKTRs and 20 STSKTRs （graft survival approximately 1-3 years post-transplantation）. All patients had stable kidney function. The samples were collected at our institution during the patients＇ follow-up examinations between March 2017 and September 2017. The plasma levels of TGF-β1, IL- 10, and arginase- 1 were analyzed using enzyme-linked immunosorbent assays （ELISA）. The levels of TGF-β1 and arginase-1 were significantly higher in the LTSKTRs than in the STSKTRs. The time elapsed since transplantation was positively correlated with the levels of TGF-β1 and arginase-1 in the LTSKTRs. The estimated glomerular filtration rate was positively correlated with the TGF-β1 level, and the serum creatinine level was negatively correlated with the TGF-β1 level. Higher serum levels of TGF-β1 and arginase-1 were found in LTSKTRs than in STSKTRs, and we found that TGF-β1 was positively correlated with long-term graft survival and function. Additionally, TGF-β1 and arginase-1 levels were positively correlated with the time elapsed since transplantation. On the basis of these findings, TGF-β1 and arginase- 1 may play important roles in determining long-term graft survival. Thus, we propose that TGF-β1 and arginase-1 may potentially be used as predictive markers for evaluating long-term graft survival.

激活CB_(2)受体对MPP+诱导BV2小胶质细胞iNOS和Arg-1表达的影响

目的探讨激活大麻素Ⅱ型受体(CB_(2)受体)对1-甲基-4-苯基吡啶离子(MPP+)处理的BV2小胶质细胞M1/M2表型转化的影响。方法培养BV2小胶质细胞,将其分为对照组、MPP+组、JWH133(CB_(2)受体激动剂)+MPP+组、AM630(CB_(2)受体抑制剂)+MPP+组、JWH133+AM630+MPP+组。应用免疫印迹法检测各组诱导型一氧化氮合酶(iNOS)和精氨酸酶-1(Arg-1)蛋白的表达。结果与对照组相比,MPP+组BV2小胶质细胞iNOS蛋白表达明显上升(F=9.825,q=6.346,P<0.01);JWH133预处理抑制MPP+诱导的iNOS蛋白的上调(q=5.714,P<0.01),此抑制作用可被AM630逆转(q=4.154,P<0.05)。与MPP+组相比,JWH133预处理显著上调Arg-1蛋白表达水平(F=5.800,q=5.520,P<0.01),此作用可被AM630所阻断(q=4.155,P<0.05)。结论激活CB 2受体可抑制MPP+处理的BV2小胶质细胞M1极化,并且促进BV2小胶质细胞从M1型转化为M2型。

肝细胞癌SLeX和Arg-1表达的临床病理研究

目的探讨唾液酸化Lewis X(SLeX)和精氨酸酶-1(Arg-1)表达与肝细胞癌(HCC)临床病理特征及预后的关系。方法120例HCC手术切除标本及30例癌旁肝组织,应用EliVisionTMplus免疫组织化学染色二步法检测SLeX和Arg-1在HCC癌组织及癌旁肝组织中的表达,分析SLeX和Arg-1与HCC患者性别、年龄、肉眼类型、瘤体大小、分化等级、转移及5年生存期等临床病理特征的相关性。结果HCC癌组织SLeX和Arg-1阳性率分别为44.2%(53/120)和75.8%(91/120),癌旁肝组织分别为3.3%(1/30)和100.0%(30/30),差异有统计学意义(均P<0.05)。SLeX和Arg-1表达与性别、年龄、肉眼类型、瘤体大小无关(均P>0.05)。在低分化、有转移和5年内死亡患者中SLeX高表达,Arg-1低表达,呈负相关性(r=-0.31)。结论SLeX和Arg-1与HCC发生发展显著相关,SLeX表达上调和(或)Arg-1表达下调均预示HCC分化差、易转移、预后不良。

ATP1A3基因Arg756位点变异相关疾病

ATP1A3基因变异相关神经系统疾病临床表现及后遗症不一,目前OMIM记录的表型有四种:RDP、AHC、CAPOS综合征、DEE99。随着越来越多的病例报道非典型和重叠表现,ATP1A3变异相关疾病现被视为一组谱系疾病,但某些位点变异与特定表型相关。p.Arg756位点变异存在一定共同表现:1) 首次发病年龄小,多由发热诱发并有复发病程;2) 核心症状为脑病,可表现为嗜睡、易激惹、淡漠等;3) 几乎所有患者均出现共济失调,而且持续存在;4) 部分患者可有肌张力改变、构音障碍、吞咽困难、肌力下降、惊厥发作、眼球异常运动、发育倒退。变异导致Na+/K+-ATP酶功能改变的致病机制尚不清楚。

三肽D-Trp-Arg-Leu-NH2抑制B16黑色素瘤细胞黑色素合成的机制

为了研究三肽D-Trp-Arg-Leu-NH2(dWRL)对小鼠B16细胞的酪氨酸酶(TYR)活性、黑色素合成及相关基因和蛋白表达的影响,探讨dWRL抑制黑色素生成的可能机制,我们体外培养小鼠B16细胞,采用MTT法测定细胞增殖情况、L-多巴氧化法测定TYR活性、氢氧化钠裂解法测定细胞黑色素含量、qRT-PCR和Western Blot法分别检测药物作用后B16细胞中小眼畸形相关转录因子(MITF)、TYR的mRNA和蛋白表达水平。结果显示三肽dWRL在试验浓度范围内可明显抑制α-黑色素细胞刺激素(α-MSH)诱导的B16细胞内TYR活性、黑色素合成量及MITF、TYR基因及蛋白的表达量,且呈浓度依赖性。所以三肽dWRL在体外能抑制B16细胞黑色素的合成,上述变化可能是通过下调MITF和TYR的基因转录和蛋白表达作用来完成。

Rare manifestation of familial vitreous amyloidosis caused by Gly103Arg transthyretin

AIM:To identify and analyze the genotype of the patients with special ocular manifestations of familial vitreous amyloidosis(FVA)in a Chinese Han family.METHODS:Pars plana vitrectomy(PPV)surgery was performed on a 52-year-old Chinese woman presented with vitreous amyloidosis and progressive visual impairment,without evidence of cardiac,renal,gastrointestinal,central nervous system or peripheral nervous system dysfunction.During the surgery,the patient presented with a gray-white dense and thick cotton woollike change in the vitreous body,accompanied by complete retinal detachment.Additionally,hard,free and movable yellow-white deposits were observed in the posterior pole and surrounding retina,the vitreous and subretinal deposits were examined by Congo red staining and immunohistochemical pathological examination,and whole exome sequencing was performed on blood samples from the patient and her cousin.RESULTS:During the operation,it was discovered that there was a complete detachment of the retina and a significant amount of hard,free-floating yellow-white deposits were observed beneath the posterior pole and surrounding retina.This is an exceedingly rare ocular manifestation.Pathological examination of the vitreous and subretinal deposit specimens revealed positive Congo red staining,as well as elevated vascular endothelial growth factor(VEGF)expression in vascular endothelial cells within the sediment specimens upon immunohistochemical examination.The patient and her cousin both exhibited a heterozygous mutation in Glyl03Arg within the transthyretin(TTR)gene,resulting in a substitution of glycine(Gly)at position 103 with arginine(Arg).CONCLUSION:FVA may present with various ocular manifestations,but panretinal detachment is a rare occurrence.In cases where retinal detachment persists for an extended period of time,amyloid deposits may form under the retina through retinal tears,leading to subretinal deposits that can impede retinal reattachment and negatively impact visual prognosis.Elevated levels of VEGF in the eyes of FVA patients may indicate an overexpression state,necessitating careful postoperative follow-up.The heterozygous mutation Gly103Arg may represent a unique pathogenic site in Chinese individuals.

饮水系统中抗生素抗性基因赋存特征及健康风险评估

近几年抗生素抗性基因(ARGs)作为一种新型污染物在世界各地的水体、土壤中被频繁检出,其在环境中大量扩散和增殖十分容易导致微生物获得抗生素抗性,对人体健康产生潜在威胁。结合国内外文献报道数据,介绍了ARGs在城市饮水系统中污染现状,描述了其赋存特征,发现在国内外城市饮水系统中ARGs的数量不容小觑,数量最高可达1.38×105 copies·ml-1。其次对城市饮水系统中常用工艺对ARGs的赋存与传播影响因素进行了总结,发现城市常用水处理工艺对ARGs的灭杀效果差,甚至对其富集和繁殖往往起着促进作用;在不同的环境影响因素中,微生物群落结构是影响ARGs的主要驱动力,其次是重金属。最后提出ARGs对人体可能造成的健康威胁以及现有健康风险评估方法的局限性,并对未来ARGs的研究进行了展望。

短肽AKRA(Ala-Lys-Arg-Ala)对酒精性肝损伤保护作用的研究

该研究采用一种短肽AKRA(Ala-Lys-Arg-Ala)分别处理人源肝细胞LO2和酒精性肝损伤小鼠,从体内和体外分别进行验证,研究AKRA是否能够缓解由偶氮二异丁脒盐酸盐(2,2′-azobis-2-methyl-propanimidamide,AAPH)在肝细胞内引起的氧化应激和食用酒精在实验动物体内造成的酒精性肝损伤。取处于对数生长期的LO2细胞,分为正常组和AKRA处理组,采用细胞增殖-毒性检测法(cell counting kit-8,CCK8)测定并计算细胞活力。采用AAPH诱导LO2细胞氧化损伤;然后以不同浓度AKRA处理细胞,检测LO2细胞中超氧化物歧化酶(superoxide dismutase,SOD)、过氧化氢酶(catalase,CAT)、谷胱甘肽还原型(glutathione,GSH)活力和丙二醛(malondialdehyde,MDA)含量;通过蛋白免疫印迹(Western blotting,WB)评价氧化、自噬和炎症相关标志性蛋白表达情况;利用食用酒精灌胃小鼠制备酒精性肝损伤病理模型同时,通过腹腔注射高、中、低剂量AKRA注射液,连续30 d,处死小鼠并观察肝组织病理形态学改变;并进行小鼠生理生化和肝脏中氧化相关指标的检测。结果提示,AKRA在0~6.4 mg/mL对LO2细胞增殖无明显影响和毒性作用,细胞活力正常;AKRA能够不同程度改善由AAPH处理引起的CAT、GSH、SOD等抗氧化酶的活性改变,并降低MDA含量;进一步研究发现,AKRA可促进核因子E-2-相关因子(nuclear factor erythroid-2-related factor 2,Nrf2)与Kelch样ECH关联蛋白1(Kelch-like ECH-associated protein 1,Keap1)解离,并进入细胞核,调控下游抗氧化及抗炎蛋白的表达水平;AKRA促进P62蛋白(sequestosome 1)降解,LC3蛋白(light chain 3)生成,从而提高自噬活性。此外,AKRA腹腔注射后,酒精引起的小鼠肝组织细胞变性程度较轻;血清中谷草转氨酶(aspartate aminotransferase,AST)、谷丙转氨酶(alanine aminotransferase,ALT)和碱性磷酸酶(alkaline phosphatase,ALP)下降,总胆固醇(total cholesterol,T-cho/TC)、甘油三酯(triglyceride,TG)、低密度脂蛋白(low density lipoprotein,LDL)水平降低,而高密度脂蛋白(high density lipoprotein,HDL)水平升高,氧化相关指标CAT、GSH及SOD活性出现不同程度的改善和MDA含量降低。通过该研究可知,短肽AKRA可能通过调控肝细胞抗氧化水平,提高自噬活性及抗炎能力达到缓解肝损伤的目的。

早期胃癌肿瘤浸润深度与癌组织PD-L1、Arg-1表达的关系

目的 探讨早期胃癌肿瘤浸润深度与癌组织程序性死亡配体-1(PD-L1)、精氨酸酶-1(Arg-1)表达的关系。方法 回顾性选取2020年1月至2022年1月在琼海市人民医院治疗的早期胃癌患者110例,采用免疫组织化学染色法检测胃癌组织和癌旁组织的PD-L1、Arg-1表达,内镜检查早期胃癌浸润深度情况,分析早期胃癌浸润深度的影响因素。结果 早期胃癌组织PD-L1和Arg-1阳性表达率分别为58.18%和76.36%,均明显高于癌旁组织(22.73%、30.91%),差异均有统计学意义(P<0.05)。合并溃疡、病变边缘有隆起、PD-L1阳性表达、Arg-1阳性表达组织黏膜下层深浸润比例分别为54.35%、51.16%、43.75%和39.29%,明显高于未合并溃疡、病变边缘无隆起、PD-L1阴性表达、Arg-1阴性表达组织(15.63%、19.40%、15.22%和7.69%),差异均有统计学意义(P<0.05)。肿瘤大小>1 cm、未分化型组织PD-L1阳性表达率分别为73.33%和97.67%,Arg-1阳性表达率分别为95.56%和93.02%,明显高于肿瘤大小≤1 cm(47.69%、63.08%)、分化型组织(32.84%、65.67%),差异均有统计学意义(P<0.05)。Logistic回归分析显示合并溃疡、病变边缘隆起、PD-L1和Arg-1表达是黏膜下层深浸润的影响因素(OR=2.779,95%CI:1.540~5.013;OR=2.596,95%CI:1.667~4.043;OR=1.976,95%CI:1.378~2.834;OR=1.749,95%CI:1.321~2.315;P<0.05)。结论 早期胃癌肿瘤组织PD-L1、Arg-1表达上调,与肿瘤大小及组织分化有关,同时PD-L1、Arg-1表达是肿瘤浸润深度的影响因素。

急性缺血性脑卒中患者血清IRAK4、ARG1、UCH-L1的表达及其预测价值

目的分析急性缺血性脑卒中患者血清白介素1受体关联激酶4(IRAK4)、重组人精氨酸酶1(ARG1)、泛素羧基末端水解酶L1(UCH-L1)的表达及其预测价值。方法选取2021年7月至2022年7月周口东新医院收治的52例急性缺血性脑卒中患者为研究组,另选取同期于周口东新医院进行健康体检的志愿者50例为对照组。检测两组IRAK4、ARG1、UCH-L1水平。结果与对照组相比,研究组IRAK4(310.44±40.36)μg/L VS(360.59±52.88)μg/L、ARG1(80.59±9.01)ng/mL VS(109.58±11.73)ng/mL、UCH-L1(0.90±0.11)μg/L VS(1.62±0.20)μg/L水平较高(P<0.05)。与研究组轻度患者相比,中度、重度患者IRAK4(340.55±48.36)μg/L VS(359.73±50.93)μg/L VS(385.83±53.79)μg/L、ARG1(92.36±10.37)ng/mL VS(106.88±11.50)ng/mL VS(135.52±12.59)ng/mL、UCH-L1(1.21±0.16)μg/L VS(1.60±0.19)μg/L VS(2.14±0.23)μg/L水平较高(P<0.05);与中度患者相比,重度患者IRAK4(359.73±50.93)μg/L VS(385.83±53.79)μg/L、ARG1(106.88±11.50)μg/L VS(135.52±12.59)μg/L、UCH-L1(1.60±0.19)μg/L VS(2.14±0.23)μg/L水平较高(P<0.05)。结论急性缺血性脑卒中患者IRAK4、ARG1、UCH-L1表达较高,且随病情严重程度的加重、预后不良的发生,IRAK4、ARG1、UCH-L1表达水平升高加剧,IRAK4、ARG1、UCH-L1三者联合检测对急性缺血性脑卒中患者预后不良的预测价值较高。