AAV2-PDE6B restores retinal structure and function in the retinal degeneration 10 mouse model of retinitis pigmentosa by promoting phototransduction and inhibiting apoptosis

Retinitis pigmentosa is a group of inherited diseases that lead to retinal degeneration and photoreceptor cell death.However,there is no effective treatment for retinitis pigmentosa caused by PDE6B mutation.Adeno-associated virus(AAV)-mediated gene therapy is a promising strategy for treating retinitis pigmentosa.The aim of this study was to explore the molecular mechanisms by which AAV2-PDE6B rescues retinal function.To do this,we injected retinal degeneration 10(rd10)mice subretinally with AAV2-PDE6B and assessed the therapeutic effects on retinal function and structure using dark-and light-adapted electroretinogram,optical coherence tomography,and immunofluorescence.Data-independent acquisition-mass spectrometry-based proteomic analysis was conducted to investigate protein expression levels and pathway enrichment,and the results from this analysis were verified by real-time polymerase chain reaction and western blotting.AAV2-PDE6B injection significantly upregulated PDE6βexpression,preserved electroretinogram responses,and preserved outer nuclear layer thickness in rd10 mice.Differentially expressed proteins between wild-type and rd10 mice were closely related to visual perception,and treating rd10 mice with AAV2-PDE6B restored differentially expressed protein expression to levels similar to those seen in wild-type mice.Kyoto Encyclopedia of Genes and Genome analysis showed that the differentially expressed proteins whose expression was most significantly altered by AAV2-PDE6B injection were enriched in phototransduction pathways.Furthermore,the phototransductionrelated proteins Pde6α,Rom1,Rho,Aldh1a1,and Rbp1 exhibited opposite expression patterns in rd10 mice with or without AAV2-PDE6B treatment.Finally,Bax/Bcl-2,p-ERK/ERK,and p-c-Fos/c-Fos expression levels decreased in rd10 mice following AAV2-PDE6B treatment.Our data suggest that AAV2-PDE6B-mediated gene therapy promotes phototransduction and inhibits apoptosis by inhibiting the ERK signaling pathway and upregulating Bcl-2/Bax expression in retinitis pigmentosa.

Lp-PLA2与sLOX-1在急性脑梗死中的意义

目的探讨脂蛋白相关磷脂酶A2(Lp-PLA2)与可溶性凝集素样氧化型低密度脂蛋白受体1(sLOX-1)对急性脑梗死的发生、复发及TOAST分型的关系。方法选取2021年7月至2023年1月,我院收治的急性脑梗死患者181例,健康对照组154例。急性脑梗死患者根据病史被分为首发和复发;根据TOAST分型被分为大动脉粥样硬化型(LAA),小动脉闭塞型(SAO)。比较各组间Lp-PLA2与sLOX-1的水平差异;采用Logistic回归分析急性脑梗死复发的危险因素。结果疾病组的Lp-PLA2、sLOX-1水平显著高于健康对照组,差异有统计学意义;复发组Lp-PLA2、sLOX-1显著高于首发组,差异有统计学意义;sLOX-1水平在LAA组显著高于SAO(P=0.047),Lp-PLA2在两组间差异无统计学意义。结论Lp-PLA2与sLOX-1与急性脑梗死相关,是急性脑梗死复发的危险因素。此外,sLOX-1与急性脑梗死的病因相关。

原发性高血压患者Lp(a)、Lp-PLA2水平与血压变异性的相关性

目的通过研究原发性高血压(EH)患者的血清Lp(a)、Lp-PLA2水平与血压变异性(BPV)的特征,进一步探讨EH患者血清中Lp(a)和Lp-PLA2水平与BPV之间的关系。方法选取2022年9月至2023年9月于内蒙古自治区人民医院门诊及住院诊疗的EH患者240例。将患者分为A组:Lp(a)、Lp-PLA2均正常,115例;B组:仅Lp(a)升高,48例;C组:仅Lp-PLA2升高,42例;D组:Lp(a)、Lp-PLA2均升高,35例。探索Lp(a)和Lp-PLA2水平与血压变异性之间的相关性。结果B组各时段变异系数(CV)均高于A组(P<0.05);C组24 h SBPCV、24 h DBP CV、nSBP CV、dDBP CV、dSBP CV高于A组(P<0.05);D组各时段CV均高于A组(P<0.05)。Lp(a)、Lp-PLA2与BPV呈正相关(rs>0,P<0.05)。B组、C组以及D组的Lp(a)、Lp-PLA2和24 h SBP CV、24 h DBP CV间均呈显著正相关关系(rs>0,P<0.05)。结论EH患者血清Lp(a)、Lp-PLA2水平与BPV呈正相关,且血清Lp(a)、Lp-PLA2均升高的患者BPV也升高。

Identification of hub genes associated with Helicobacter pylori infection and type 2 diabetes mellitus:A pilot bioinformatics study

BACKGROUND Helicobacter pylori(H.pylori)infection is related to various extragastric diseases including type 2 diabetes mellitus(T2DM).However,the possible mechanisms connecting H.pylori infection and T2DM remain unknown.AIM To explore potential molecular connections between H.pylori infection and T2DM.METHODS We extracted gene expression arrays from three online datasets(GSE60427,GSE27411 and GSE115601).Differentially expressed genes(DEGs)commonly present in patients with H.pylori infection and T2DM were identified.Hub genes were validated using human gastric biopsy samples.Correlations between hub genes and immune cell infiltration,miRNAs,and transcription factors(TFs)were further analyzed.RESULTS A total of 67 DEGs were commonly presented in patients with H.pylori infection and T2DM.Five significantly upregulated hub genes,including TLR4,ITGAM,C5AR1,FCER1G,and FCGR2A,were finally identified,all of which are closely related to immune cell infiltration.The gene-miRNA analysis detected 13 miRNAs with at least two gene cross-links.TF-gene interaction networks showed that TLR4 was coregulated by 26 TFs,the largest number of TFs among the 5 hub genes.CONCLUSION We identified five hub genes that may have molecular connections between H.pylori infection and T2DM.This study provides new insights into the pathogenesis of H.pylori-induced onset of T2DM.

Regulatory potential of soil available carbon,nitrogen,and functional genes on N_(2)O emissions in two upland plantation systems

Dynamic nitrification and denitrification processes are affected by changes in soil redox conditions,and they play a vital role in regulating soil N_(2)O emissions in rice-based cultivation.It is imperative to understand the influences of different upland crop planting systems on soil N_(2)O emissions.In this study,we focused on two representative rotation systems in Central China:rapeseed–rice(RR)and wheat–rice(WR).We examined the biotic and abiotic processes underlying the impacts of these upland plantings on soil N_(2)O emissions.The results revealed that during the rapeseed-cultivated seasons in the RR rotation system,the average N_(2)O emissions were 1.24±0.20 and 0.81±0.11 kg N ha^(–1)for the first and second seasons,respectively.These values were comparable to the N_(2)O emissions observed during the first and second wheat-cultivated seasons in the WR rotation system(0.98±0.25 and 0.70±0.04 kg N ha^(–1),respectively).This suggests that upland cultivation has minimal impacts on soil N_(2)O emissions in the two rotation systems.Strong positive correlations were found between N_(2)O fluxes and soil ammonium(NH_(4)^(+)),nitrate(NO_(3)^(–)),microbial biomass nitrogen(MBN),and the ratio of soil dissolved organic carbon(DOC)to NO_(3)^(–)in both RR and WR rotation systems.Moreover,the presence of the AOA-amoA and nirK genes were positively associated with soil N_(2)O fluxes in the RR and WR systems,respectively.This implies that these genes may have different potential roles in facilitating microbial N_(2)O production in various upland plantation models.By using a structural equation model,we found that soil moisture,mineral N,MBN,and the AOA-amoA gene accounted for over 50%of the effects on N_(2)O emissions in the RR rotation system.In the WR rotation system,soil moisture,mineral N,MBN,and the AOA-amoA and nirK genes had a combined impact of over 70%on N_(2)O emissions.These findings demonstrate the interactive effects of functional genes and soil factors,including soil physical characteristics,available carbon and nitrogen,and their ratio,on soil N_(2)O emissions during upland cultivation seasons under rice-upland rotations.

应用Minigene剪接变异体分析技术诊断PMM2基因非经典剪接位点新变异的致病性

目的:研究Minigene剪接变异体分析技术在诊断磷酸甘露糖变位酶2(PMM2)相关先天性糖基化障碍(PMM2-CDG)中的价值,探讨磷酸甘露糖变位酶2(PMM2)基因剪接位点新变异对其转录产物的影响。方法:通过对1例PMM2-CDG患儿进行高通量测序查找可能的遗传学病因,利用Minigene剪接变异体分析技术,研究PMM2基因新剪接位点变异的致病性。根据美国医学遗传学与基因组学学会(ACMG)指南,判断新变异的致病性。结果:遗传学分析发现患儿系PMM2基因母源性c.691G>A(p.Val231Met)变异和父源性c.447+5G>A变异复合杂合子。Minigene剪接变异体分析发现:变异c.447+5G>A导致PMM2基因转录产物形成r.348_447del转录本,为致病性PMM2基因变异。患儿的临床特征为皮肤巩膜黄染,血清总胆红素、非结合胆红素和总胆汁酸明显升高,白蛋白明显降低,甲胎蛋白、铁蛋白和促甲状腺素等升高,对症支持治疗效果欠佳。结论:Minigene剪接变异体分析可为PMM2-CDG确诊和家系遗传咨询提供新的分子标记物,扩展了PMM2基因变异谱,为该病的临床诊治提供新的参考依据。

Vanillylacetone attenuates cadmium chloride-induced hippocampal damage and memory loss through upregulation of nuclear factor erythroid 2-related factor 2 gene and protein expression

Memory loss and dementia are major public health concerns with a substantial economic burden.Oxidative stress has been shown to play a crucial role in the pathophysiology of hippocampal damage-induced memory impairment.To investigate whether the antioxidant and anti-inflammatory compound vanillyla cetone(zingerone) can protect against hippocampal damage and memory loss induced by cadmium chloride(CdCl_(2)) administration in rats,we explo red the potential involvement of the nuclear factor erythroid 2-related factor 2(Nrf2) signaling pathway,which is known to modulate oxidative stress and inflammation.Sixty healt hy male Wistar rats were divided into five groups:vehicle-treated(control),vanillylacetone,CdCl_(2),vanillylacetone+ CdCl_(2),vanillylacetone+ CdCl_(2)+ brusatol(a selective pharmacological N rf2inhibitor) groups.Vanillylacetone effectively attenuated CdCl_(2)-induced damage in the dental gyrus of the hippocampus and improved the memory function assessed by the Morris Water Maze test.Additionally,vanillylacetone markedly decreased the hippocampal tissue levels of inflammatory biomarkers(interleukin-6,tumor necrosis factor-α,intracellular cell adhesive molecules) and apoptosis biomarkers(Bax and cleaved caspase-3).The control and CdCl_(2)-treated groups treated with va nillylacetone showed reduced generation of reactive oxygen species,decreased malondialdehyde levels,and increased superoxide dismutase and glutathione activities,along with significant elevation of nuclear Nrf2 mRNA and protein expression in hippocampal tissue.All the protective effects of vanillylacetone we re substantially blocked by the co-administration of brusatol(a selective N rf2 inhibitor).Va nillylacetone mitigated hippocampal damage and memory loss induced by CdCl_(2),at least in part, by activating the nuclear transcription factor Nrf2.Additionally,vanillylacetone exerted its potent antioxidant and antiinflammatory actions.

To Analyze the Sensitivity of RT-PCR Assays Employing S Gene Target Failure with Whole Genome Sequencing Data during Third Wave by SARS-CoV-2 Omicron Variant

Introduction: Omicron is a highly divergent variant of concern (VOCs) of a severe acute respiratory syndrome SARS-CoV-2. It carries a high number of mutations in its spike protein hence;it is more transmissible in the community by immune evasion mechanisms. Due to mutation within S gene, most Omicron variants have reported S gene target failure (SGTF) with some commercially available PCR kits. Such diagnostic features can be used as markers to screen Omicron. However, Whole Genome Sequencing (WGS) is the only gold standard approach to confirm novel microorganisms at genetically level as similar mutations can also be found in other variants that are circulating at low frequencies worldwide. This Retrospective study is aimed to assess RT-PCR sensitivity in the detection of S gene target failure in comparison with whole genome sequencing to detect variants of Omicron. Methods: We have analysed retrospective data of SARS-CoV-2 positive RT-PCR samples for S gene target failure (SGTF) with TaqPath COVID-19 RT-PCR Combo Kit (ThermoFisher) and combined with sequencing technologies to study the emerged pattern of SARS-CoV-2 variants during third wave at the tertiary care centre, Surat. Results: From the first day of December 2021 till the end of February 2022, a total of 321,803 diagnostic RT-PCR tests for SARS-CoV-2 were performed, of which 20,566 positive cases were reported at our tertiary care centre with an average cumulative positivity of 6.39% over a period of three months. In the month of December 21 samples characterized by the SGTF (70/129) were suggestive of being infected by the Omicron variant and identified as Omicron (B.1.1.529 lineage) when sequence. In the month of January, we analysed a subset of samples (n = 618) with SGTF (24%) and without SGTF (76%) with Ct values Conclusions: During the COVID-19 pandemic, it took almost more than 15 days to diagnose infection and identify pathogen by sequencing technology. In contrast to that molecular assay provided quick identification with the help of SGTF phenomenon within 5 hours of duration. This strategy helps scientists and health policymakers for the quick isolation and identification of clusters. That ultimately results in a decreased transmission of pathogen among the community.

Evaluating serum CXCL12,sCD22,Lp-PLA2 levels and ratios as biomarkers for diagnosis of Alzheimer's disease

BACKGROUND Grasping the underlying mechanisms of Alzheimer's disease(AD)is still a work in progress,and existing diagnostic techniques encounter various obstacles.Therefore,the discovery of dependable biomarkers is essential for early detection,tracking the disease's advancement,and steering treatment strategies.AIM To explore the diagnostic potential of serum CXCL12,sCD22,Lp-PLA2,and their ratios in AD,aiming to enhance early detection and inform targeted treatment strategies.METHODS The study was conducted in Dongying people's Hospital from January 2021 to December 2022.Participants included 60 AD patients(AD group)and 60 healthy people(control group).Using a prospective case-control design,the levels of CXCL12,sCD22 and Lp-PLA2 and their ratios were detected by enzyme-linked immunosorbent assay kit in the diagnosis of AD.The differences between the two groups were analyzed by statistical methods,and the corresponding ratio was constructed to improve the specificity and sensitivity of diagnosis.RESULTS Serum CXCL12 levels were higher in the AD group(47.2±8.5 ng/mL)than the control group(32.8±5.7 ng/mL,P<0.001),while sCD22 levels were lower(14.3±2.1 ng/mL vs 18.9±3.4 ng/mL,P<0.01).Lp-PLA2 levels were also higher in the AD group(112.5±20.6 ng/mL vs 89.7±15.2 ng/mL,P<0.05).Significant differences were noted in CXCL12/sCD22(3.3 vs 1.7,P<0.001)and Lp-PLA-2/sCD22 ratios(8.0 vs 5.2,P<0.05)between the groups.Receiver operating characteristic analysis confirmed high sensitivity and specificity of these markers and their ratios in distinguishing AD,with area under the curves ranging from CONCLUSION Serum CXCL12 and Lp-PLA2 levels were significantly increased,while sCD22 were significantly decreased,as well as increases in the ratios of CXCL12/sCD22 and Lp-PLA2/sCD22,are closely related to the onset of AD.These biomarkers and their ratios can be used as potential diagnostic indicators for AD,providing an important clinical reference for early intervention and treatment.

Analysis of SMOC2 gene variants in familial and nonfamilial primary open angle glaucoma Pakistani patients

AIM:To find out the association of secreted protein acidic and rich in cysteine(SPARC)-related modular calcium binding 2(SMOC2)gene variants rs2255680 and rs13208776 with genotypic and phenotypic characteristics in both familial and non-familial primary open angle glaucoma(POAG)patients.METHODS:A total of 212 POAG patients,comprising 124 familial and 88 non-familial,were enrolled.For genotyping the SMOC2 variant rs2255680,amplification refractory mutation system(ARMS)-polymerase chain reaction(PCR)method and PCR-restriction fragment length polymorphism(PCR-RFLP)were utilized for analyzing rs13208776 variant.RESULTS:The mean age of familial POAG patients was 50.92±9.12y,with 78 males and 46 females.The mean age of non-familial POAG patients was 53.14±13.44y,with 52 males and 36 females.The SMOC2 gene variant rs13208776 showed the significant association with POAG between familial and non-familial groups.The homozygous G/G variant was frequent among non-familial(60.2%)whereas the heterozygous G/A variant was more frequent in familial POAG patients(46%).There were significant differences in G/A variant between familial and non-familial glaucoma patients,and the risk was decreased to 0.53-fold in non-familial glaucoma patients[odds ratio(OR):0.53;95%confidence interval(CI):0.29-0.94;P=0.033]in codominant model.The risk was further reduced to 0.49-fold(95%CI:0.28-0.86;P=0.012)in dominant model for non-familial patients.No significant association of SMOC2 gene variant rs2255680 between familial and non-familial glaucoma patients was found in our population.The haplotype analysis showed the decreased risk for TA[OR:0.48(95%CI:0.29-0.79);P=0.004]and an increased risk for TG[OR=2.28(95%CI:1.22-4.25);P=0.01]haplotypes.CONCLUSION:Current findings show significant association of SMOC2 gene variant rs13208776 with POAG between familial and non-familial Pakistani patients.

Pathogenesis of chronic enteropathy associated with the SLCO2A1 gene:Hypotheses and conundrums

Chronic enteropathy associated with the SLCO2A1 gene(CEAS)is a complex gastroenterological condition characterized by multiple ulcers in the small intestine with chronic bleeding and protein loss.This review explores the potential mechanisms underlying the pathogenesis of CEAS,focusing on the role of SLCO2A1-encoded prostaglandin transporter OATP2A1 and its impact on prostaglandin E2(PGE2)levels.Studies have suggested that elevated PGE2 levels contribute to mucosal damage,inflammation,and disruption of the intestinal barrier.The effects of PGE2 on macrophage activation and Maxi-Cl channel functionality,as well as its interaction with nonsteroidal anti-inflammatory drugs play crucial roles in the progression of CEAS.Understanding the balance between its protective and pro-inflammatory effects and the complex interactions within the gastrointestinal tract can shed light on potential therapeutic targets for CEAS and guide the development of novel,targeted therapies.

Transglutaminase 2 serves as a pathogenic hub gene of KRAS mutant colon cancer based on integrated analysis

BACKGROUND Colon cancer is acknowledged as one of the most common malignancies worldwide,ranking third in United States regarding incidence and mortality.Notably,approximately 40%of colon cancer cases harbor oncogenic KRAS mutations,resulting in the continuous activation of epidermal growth factor receptor signaling.AIM To investigate the key pathogenic genes in KRAS mutant colon cancer holds considerable importance.METHODS Weighted gene co-expression network analysis,in combination with additional bioinformatics analysis,were conducted to screen the key factors driving the progression of KRAS mutant colon cancer.Meanwhile,various in vitro experiments were also conducted to explore the biological function of transglutaminase 2(TGM2).RESULTS Integrated analysis demonstrated that TGM2 acted as an independent prognostic factor for progression-free survival.Immunohistochemical analysis on tissue microarrays revealed that TGM2 was associated with an elevated probability of perineural invasion in patients with KRAS mutant colon cancer.Additionally,biological roles of the key gene TGM2 was also assessed,suggesting that the downregulation of TGM2 attenuated the proliferation,invasion,and migration of the KRAS mutant colon cancer cell line.CONCLUSION This study underscores the potential significance of TGM2 in the progression of KRAS mutant colon cancer.This insight not only offers a theoretical foundation for therapeutic approaches but also highlights the need for additional clinical trials and fundamental research to support our preliminary findings.

脑梗死血清MMP-9、Lp-PLA2、Hcy水平与早期神经功能恶化的关系研究

目的探究脑梗死患者血清基质金属蛋白酶-9(MMP-9)、脂蛋白相关磷脂酶A2(Lp-PLA2)、同型半胱氨酸(Hcy)水平与早期神经功能恶化(END)的联系。方法纳入2020年4月至2023年4月于本院收治的脑梗死患者112例,根据是否发生END分为恶化组、非恶化组,对比两组患者一般资料、MMP-9、Lp-PLA2及Hcy水平的差异,进行多因素Logistic回归分析,评估脑梗死患者END影响因素,绘制ROC曲线,分析血清MMP-9、Lp-PLA2、Hcy水平与END的关系。结果112例脑梗死患者中,有79例未发生END作为非恶化组,占比70.54%;33例发生END的患者作为恶化组,占比29.46%。对比两组性别、年龄、身体质量指数(BMI)、高血压病情、糖尿病病情、高脂症均无明显差异(P>0.05)。恶化组舒张压、发病至治疗时间、入院NIHSS评分、MMP-9、Lp-PLA2、Hcy高于非恶化组,差异有统计学意义(P<0.05)。多因素分析显示MMP-9、Lp-PLA2、Hcy均为脑梗死患者发生END的独立影响因素(P<0.05)。ROC曲线分析,血清MMP-9、Lp-PLA2、Hcy预测AIS患者不良预后的曲线下面积(AUC)分别为0.914、0.867、0.883,敏感度分别为0.909、0.836、0.879,特异度分别是0.797、0.962和0.823。结论MMP-9、Lp-PLA2、Hcy水平与脑梗死患者END密切相关,其可能是通过调节机体炎症反应、血脑屏障损伤进程影响患者的神经功能,可为脑梗死患者END预测提供可靠信息。

血清Lp-PLA2、TNF-α、Hcy水平与急性脑梗死患者神经功能缺损程度的关系及预后价值

目的 探讨血清脂蛋白相关磷脂酶A2(Lp-PLA2)、肿瘤坏死因子α(TNF-α)、同型半胱氨酸(Hcy)水平与急性脑梗死(ACI)患者神经功能缺损程度的关系及预后价值。方法 回顾性选取2021年03月—2023年11月我院120例ACI患者,根据美国国立卫生研究院卒中量表(NIHSS)分为轻度组、中度组、重度组,另选取同期健康体检者60例为对照组,并根据改良Rankin Scale(MRS)量表分为预后良好、预后不良患者。比较4组及不同预后患者血清Lp-PLA2、TNF-α、Hcy水平,分析各指标与ACI患者神经功能缺损程度的相关性,受试者工作特征(ROC)分析各指标联合检测对预后不良的预测价值。结果 各组入院时血清Lp-PLA2、TNF-α、Hcy水平对比,其中重度组>中度组>轻度组>对照组(P<0.05);预后不良者血清Lp-PLA2、TNF-α、Hcy水平高于预后良好者(P<0.05);血清Lp-PLA2、TNF-α、Hcy水平与ACI患者神经功能缺损程度呈正相关(P<0.05);血清Lp-PLA2、TNF-α、Hcy联合预测ACI患者预后不良的曲线下面积(AUC)为0.897(P<0.05)。结论 血清Lp-PLA2、TNF-α、Hcy水平与神经功能缺损程度密切相关,对ACI患者预后有一定预测价值。

Gene expression analysis of cytokines and MMPs in melatonin and rhBMP-2 enhanced bone remodeling

BACKGROUND In the medical and dental fields,there is a need for studies of new therapeutic approaches for the treatment of bone defects that cause extensive bone loss.Melatonin may be an important endogenous biological factor for bone remodeling,and growth factors may enhance the repair process.AIM To evaluate the gene expression of cytokines(IL-1β,IL-6,IL-10 and TNF-α),markers of osteoclastogenesis(RANK,RANKL and OPG)and MMPs(MMP-1,MMP-2,MMP-8 and MMP-13)from the treatment of melatonin associated with an osteogenic membrane and rhBMP-2 on the recovery of a bone injury.METHODS Sixty-four rats were used and divided into 9 experimental groups and were formed according to the treatment carried out in the region of the bone lesion,which varied between the combination of 1,10 and 100μmol/L of melatonin.Gene Expression analysis was performed using real time-PCR by reading the concentration of total RNA and reverse transcription.RESULTS There were differences between groups when compared with clot or scaffold control,and improvement with a higher concentration of melatonin or rhBMP-2.The combination melatonin(1μg)with 5μg of rhBMP-2,using the guided bone regeneration technique,demonstrated some effects,albeit mild,on bone repair of critical bone defects.CONCLUSION This indicates that the approach for administering these substances needs to be reassessed,with the goal of ensuring their direct application to the affected area.Therefore,future research must be carried out,seeking to produce materials with these ideal characteristics.

Identification of M2 macrophage-related genes for establishing a prognostic model in pancreatic cancer: FCGR3A as key gene

Background:Pancreatic ductal adenocarcinoma(PDAC)has a rich and complex tumor immune microenvironment(TIME).M2 macrophages are among the most extensively infiltrated immune cells in the TIME and are necessary for the growth and migration of cancers.However,the mechanisms and targets mediating M2 macrophage infiltration in pancreatic cancer remain elusive.Methods:The M2 macrophage infiltration score of patients was assessed using the xCell algorithm.Using weighted gene co-expression network analysis(WGCNA),module genes associated with M2 macrophages were identified,and a predictive model was designed.The variations in immunological cell patterns,cancer mutations,and enrichment pathways between the cohorts with the high-and low-risk were examined.Additionally,the expression of FCGR3A and RNASE2,as well as their association with M2 macrophages were evaluated using the HPA,TNMplot,and GEPIA2 databases and verified by tissue immunofluorescence staining.Moreover,in vitro cell experiments were conducted,where FCGR3A was knocked down in pancreatic cancer cells using siRNA to analyze its effects on M2 macrophage infiltration,tumor proliferation,and metastasis.Results:The prognosis of patients in high-risk and low-risk groups was successfully distinguished using a prognostic risk score model of M2 macrophage-related genes(p=0.024).Between the high-and low-risk cohorts,there have been notable variations in immune cell infiltration patterns,tumor mutations,and biological functions.The risk score was linked to the manifestation of prevalent immunological checkpoints,immunological scores,and stroma values(all p<0.05).In vitro experiments and tissue immunofluorescence staining revealed that FCGR3A can promote the infiltration or polarization of M2 macrophages and enhance tumor proliferation and migration.Conclusions:In this study,an M2 macrophage-related pancreatic cancer risk score model was established,and found that FCGR3A was correlated with tumor formation,metastasis,and M2 macrophage infiltration.

血清NT-proBNP、cTnⅠ、Lp-PLA2联合检测对妊娠期高血压孕妇妊娠结局的预测价值

目的分析血清NT-proBNP、cTnⅠ、Lp-PLA2联合检测对妊娠期高血压孕妇妊娠结局的预测价值。方法92例妊娠期高血压孕妇根据妊娠结局分为不良结局组、正常结局组,比较两组确诊时的血清NT-proBNP、cTnⅠ、Lp-PLA2水平,评价各指标单独及联合检测对妊娠结局的预测效能。结果不良结局组的血清NT-proBNP、cTnⅠ、Lp-PLA2水平均高于正常结局组(P<0.05)。ROC曲线显示,血清NT-proBNP、cTnⅠ、Lp-PLA2三项指标联合检测预测妊娠期高血压孕妇妊娠结局的AUC为0.932,高于各指标单独检测。结论血清NT-proBNP、cTnⅠ、Lp-PLA2联合检测预测妊娠期高血压孕妇妊娠结局的效能较高。

血清Lp-PLA2、Aβ_(1-42)联合Fazekas评分对脑小血管病认知障碍的预测价值

目的探讨血清Lp-PLA2、Aβ_(1-42)联合Fazekas评分对脑小血管病患者认知障碍的预测价值。方法选取2021年3月至2022年12月我院收治的94例脑小血管病患者,根据蒙特利尔认知评估量表评分分为认知障碍组和认知正常组,比较两组的Lp-PLA2、Aβ_(1-42)水平以及Fazekas评分,分析Lp-PLA2、Aβ_(1-42)水平联合Fazekas评分预测脑小血管病患者发生认知障碍的效能。结果认知障碍组的Lp-PLA2、Aβ_(1-42)水平及Fazekas评分均高于认知正常组(P<0.05)。ROC曲线显示,Lp-PLA2、Aβ_(1-42)水平联合Fazekas评分预测脑小血管病患者认知障碍的效能高于单一指标(P<0.05)。结论血清Lp-PLA2、Aβ_(1-42)水平联合Fazekas评分预测脑小血管病患者发生认知障碍的应用价值高。

进展性脑梗死与血糖、血脂、Lp-PLA2等危险因素相关性研究

探究进展性脑梗死(CI)同Lp-PLA2、血脂、血糖等危险因子之间的关联性。方法 研究对象是本院2015年9月至2021年1月期间183名已确诊CI病人,分组情况为进展组101例,非进展组82例。观察两组患者基础疾病如高血压、糖尿病、中风、房颤、颈部血管斑块等分布情况,并比较两组患者血糖、血脂、Lp-PLA2、D-二聚体等指标的差异。进一步分析血糖、血脂、Lp-PLA2与进展性脑梗死患者疾病严重程度NIHSS评分之间的相关性。结果 常见发病危险因素比较,相较非进展组糖尿病(DM)病史所占比例,进展组显著偏高(P<0.05)。LDL、糖化血红蛋白、Lp-PLA2等结果比较,进展组高于非进展组(P<0.05)。相关性分析提示,总胆固醇、低密度脂蛋白、Lp-PLA2与疾病严重程度NIHSS评分呈正相关(P<0.05),空腹血糖(FBG)、糖化血红蛋白(HbA1c)同疾病严重程度NIHSS评分存在紧密联系(P<0.01)。回归分析提示,低密度脂蛋白、空腹血糖对疾病严重程度NIHSS评分具有显著影响(P<0.05,P<0.01)。结论 血糖、LDL、Lp-PLA2均是脑梗死的高危因素,并与进展性脑梗死的发生存在一定相关性。

血清HCY、Lp-PLA2水平在缺血性脑卒中充氧回输血疗效中应用

目的临床分析血清同型半胱氨酸(HCY)、脂蛋白相关性磷脂酶A2(Lp-PLA2)水平在缺血性脑卒中充氧回输血疗效中的应用效果。方法选取2019年12月—2022年12月山东省德州市陵城区人民医院收治的80例缺血性脑卒中患者为试验组,同时选取同期德州市陵城区人民医院收治的80名健康体检者为对照组;再根据美国国立卫生研究所卒中量表(NIHSS)评分,将试验组分为轻度组(<5分)25例、中度组(5~15分)30例、重度组(>15分)25例,进行回顾性研究。比较两组患者血清HCY、Lp-PLA2、LPA水平,同时对患者给予充氧回输血治疗,比较试验组患者治疗前后HCY、Lp-PLA2、LPA水平。结果试验组患者的HCY、Lp-PLA2、LPA水平高于对照组,差异有统计学意义(P<0.05)。轻、中、重度组HCY、Lp-PLA2、LPA水平比较,差异有统计学意义(P<0.05),其中重度组患者的HCY、Lp-PLA2、LPA水平高于轻度组与中度组,中度组HCY、Lp-PLA2、LPA水平高于轻度,差异有统计学意义(P<0.05)。治疗后试验组患者的HCY、Lp-PLA2、LPA水平均低于治疗前,差异有统计学意义(P<0.05)。治疗后试验组的血浆黏度、全血高切黏度、全血低切黏度、红细胞压积及血小板黏附率均较治疗前降低,差异有统计学意义(P<0.05)。结论缺血性脑卒中患者血清HCY、Lp-PLA2水平较高,且在缺血性脑卒中患者充氧回输血过程中监测血清HCY、Lp-PLA2水平,可作为患者病情监测及预后评估的有效指标。