白细胞介素10工程化修饰人脐带间充质干细胞优效治疗炎症性肠病

背景:间充质干细胞来源广泛、易体外增殖,并可分泌一系列免疫调节因子抑制炎症、促进组织修复再生,广泛应用于各种疾病治疗研究。但是对于多种疾病,间充质干细胞的治疗效果有限。针对疾病特定发病机制或者干预靶点进行工程化修饰间充质干细胞是未来细胞治疗的重要发展方向。目的:白细胞介素10是一种典型的抗炎细胞因子,有助于调节免疫反应并诱导巨噬细胞向抗炎表型极化,该研究探讨白细胞介素10基因工程化修饰人脐带间充质干细胞对炎症性肠病的治疗效果。方法:通过电转染建立稳定过表达人白细胞介素10基因的人脐带间充质干细胞,并基于细胞治疗产品标准筛选出临床级细胞。给予C57BL/6J小鼠自由饮用5%葡聚糖硫酸钠盐水溶液建立急性结肠炎模型,分别在造模前1 d(尾静脉途径)与造模后第4天(腹腔途径)注射空质粒转染的人脐带间充质干细胞或过表达人白细胞介素10基因的人脐带间充质干细胞(1×10~6个/只)。在造模后第6天取结肠组织进行苏木精-伊红染色评估组织学变化,免疫荧光染色检测增殖细胞核抗原与CD31的表达。结果与结论:构建的稳定过表达白细胞介素10的工程化人脐带间充质干细胞,满足临床级人脐带间充质干细胞质量标准;人脐带间充质干细胞对小鼠急性结肠炎具有修复效果,过表达白细胞介素10基因的人脐带间充质干细胞的治疗效果更加优效,更显著地抑制急性结肠炎小鼠的体质量下降(P<0.05)、结肠缩短(P<0.05)以及结肠组织损伤(P<0.05);过表达白细胞介素10基因人脐带间充质干细胞组结肠组织切片中增殖细胞核抗原阳性细胞与CD31阳性细胞显著多于人脐带间充质干细胞组,表明过表达白细胞介素10基因的人脐带间充质干细胞可能通过显著促进肠组织细胞增殖和血管再生进而促进结肠组织修复。

Low interleukin-10 level indicates a good prognosis in Salmonella enterica serovar typhimurium-induced pediatric hemophagocytic lymphohistiocytosis:A case report

BACKGROUND Secondary hemophagocytic lymphohistiocytosis(sHLH)triggered by Salmonella enterica serovar Typhimurium is rare in pediatric patients.There is no consensus on how to treat S.typhimurium-triggered sHLH.CASE SUMMARY A 9-year-old boy with intermittent fever for 3 d presented to our hospital with positive results for S.typhimurium,human rhinovirus,and Mycoplasma pneumoniae infections.At the time of admission to our institution,the patient’s T helper 1/T helper 2 cytokine levels were 326 pg/mL for interleukin 6(IL-6),9.1 pg/mL for IL-10,and 246.7 pg/mL for interferon-gamma(IFN-γ),for which the ratio of IL-10 to IFN-γwas 0.04.In this study,the patient received meropenem,linezolid,and cefoperazone/sulbactam in combination with high-dose methylprednisolone therapy(10 mg/kg/d for 3 d)and antishock supportive treatment twice.After careful evaluation,this patient did not receive HLH chemotherapy and recovered well.CONCLUSION S.Typhimurium infection-triggered sHLH patient had a ratio of IL-10 to IFN-γ≤1.33,an IL-10 concentration≤10.0 pg/mL,and/or an IFN-γconcentration≤225 pg/mL at admission.Early antimicrobial and supportive treatment was sufficient,and the HLH-94/2004 protocol was not necessary under these conditions.

Effects of interleukin-10 treated macrophages on bone marrow mesenchymal stem cells via signal transducer and activator of transcription 3 pathway

BACKGROUND Alveolar bone defects caused by inflammation are an urgent issue in oral implant surgery that must be solved.Regulating the various phenotypes of macrophages to enhance the inflammatory environment can significantly affect the progression of diseases and tissue engineering repair process.AIM To assess the influence of interleukin-10(IL-10)on the osteogenic differentiation of bone marrow mesenchymal stem cells(BMSCs)following their interaction with macrophages in an inflammatory environment.METHODS IL-10 modulates the differentiation of peritoneal macrophages in Wistar rats in an inflammatory environment.In this study,we investigated its impact on the proliferation,migration,and osteogenesis of BMSCs.The expression levels of signal transducer and activator of transcription 3(STAT3)and its activated form,phos-phorylated-STAT3,were examined in IL-10-stimulated macrophages.Subsequently,a specific STAT3 signaling inhibitor was used to impede STAT3 signal activation to further investigate the role of STAT3 signaling.RESULTS IL-10-stimulated macrophages underwent polarization to the M2 type through substitution,and these M2 macrophages actively facilitated the osteogenic differentiation of BMSCs.Mechanistically,STAT3 signaling plays a crucial role in the process by which IL-10 influences macrophages.Specifically,IL-10 stimulated the activation of the STAT3 signaling pathway and reduced the macrophage inflammatory response,as evidenced by its diminished impact on the osteogenic differentiation of BMSCs.CONCLUSION Stimulating macrophages with IL-10 proved effective in improving the inflammatory environment and promoting the osteogenic differentiation of BMSCs.The IL-10/STAT3 signaling pathway has emerged as a key regulator in the macrophage-mediated control of BMSCs’osteogenic differentiation.

香榧花粉TgPUX10基因克隆与表达

以香榧(Torreya grandis‘Merrillii’)花粉RNA反转录的cDNA为模板,利用RT-PCR技术分离出一条类似拟南芥PUX10-like cDNA序列,命名为TgPUX10,并对该基因进行鉴定、克隆、表达分析。结果表明:TgPUX10基因的完整开放阅读框(ORF)为1437 bp,编码477个氨基酸残基。TgPUX10蛋白的氨基酸序列包含UBA、HP、UAS、UBX功能结构域。通过构建瞬时表达载体,并利用拟南芥悬浮细胞转化体系,发现TgPUX10蛋白定位于油体细胞器。在花粉萌发的0、2、4 d时,油体相关基因TgOLE及TgCLO的表达量呈下降趋势,TgPUX10的表达量显著上升,证明TgPUX10影响香榧花粉萌发,且参与油体的降解过程。TgPUX10在各品种香榧中表达较为保守。与其他品种相比,细榧(Torreya grandis‘xifei’)的花粉活性较高,萌发率达到35.5%。

Interleukin-6 in epilepsy and its neuropsychiatric comorbidities: How to bridge the gap

There is growing evidence that interleukin(IL)-6 plays an important role in neurological and psychiatric disorders.This editorial comments on the study published in the recent issue of the World Journal of Psychiatry,which employed Mendelian randomization to identify a causal relationship between IL-6 receptor blockade and decreased epilepsy incidence.The purpose of this editorial is to highlight the dual effects of IL-6 in epilepsy and its related neuropsychiatric comorbidities.IL-6 plays a critical role in the facilitation of epileptogenesis and maintenance of epileptic seizures and is implicated in neuroinflammatory proce-sses associated with epilepsy.Furthermore,IL-6 significantly influences mood regulation and cognitive dysfunction in patients with epilepsy,highlighting its involvement in neuropsychiatric comorbidities.In summary,IL-6 is not only a pivotal factor in the pathogenesis of epilepsy but also significantly contributes to the emergence of epilepsy-related neuropsychiatric complications.Future resear-ch should prioritize elucidating the specific mechanisms by which IL-6 operates across different subtypes,stages and neuropsychiatric comorbidities of epilepsy,with the aim of developing more precise and effective interventions.Furthermore,the potential of IL-6 as a biomarker for the early diagnosis and prognosis of epile-psy warrants further investigation.

Interleukin-17A facilitates tumor progression via upregulating programmed death ligand-1 expression in hepatocellular carcinoma

BACKGROUND Hepatocellular carcinoma(HCC)is an inflammation-associated tumor with a dismal prognosis.Immunotherapy has become an important treatment strategy for HCC,as immunity is closely related to inflammation in the tumor microenvir-onment.Inflammation regulates the expression of programmed death ligand-1(PD-L1)in the immunosuppressive tumor microenvironment and affects im-munotherapy efficacy.Interleukin-17A(IL-17A)is involved in the remodeling of the tumor microenvironment and plays a protumor or antitumor role in different tumors.We hypothesized that IL-17A participates in tumor progression by affe-cting the level of immune checkpoint molecules in HCC.The upregulation of PD-L1 expression in HCC cells by IL-17A was assessed by reverse transcription PCR,western blotting,and flow cytometry.Mechanistic studies were conducted with gene knockout models and pathway inhibitors.The function of IL-17A in immune evasion was explored through coculture of T cells and HCC cells.The effects of IL-17A on the malignant biological behaviors of HCC cells were evaluated in vitro,and the antitumor effects of an IL-17A inhibitor and its synergistic effects with a PD-L1 inhibitor were studied in vivo.RESULTS IL-17A upregulated PD-L1 expression in HCC cells in a dose-dependent manner,whereas IL-17A receptor knockout or treatment with a small mothers against decapentaplegic 2 inhibitor diminished the PD-L1 expression induced by IL-17A.IL-17A enhanced the survival of HCC cells in the coculture system.IL-17A increased the viability,G2/M ratio,and migration of HCC cells and decreased the apoptotic index.Cyclin D1,VEGF,MMP9,and Bcl-1 expression increased after IL-17A treatment,whereas BAX expression decreased.The combination of IL-17A and PD-L1 inhibitors showed synergistic antitumor efficacy and increased cluster of differentiation 8+T lymphocyte infiltration in an HCC mouse model.CONCLUSION IL-17A upregulates PD-L1 expression via the IL-17A receptor/phosphorylation-small mothers against decapenta-plegic 2 signaling pathway in HCC cells.Blocking IL-17A enhances the therapeutic efficacy of PD-L1 antibodies in HCC in vivo.

卵巢癌组织CLDN10、三结构域蛋白59表达及其临床意义

目的分析卵巢癌组织紧密连接蛋白10(CLDN10)、三结构域蛋白59(TRIM59)表达及其临床意义。方法该研究选取2017年2月至2019年2月在鹤壁市人民医院接受手术的112例卵巢癌病人术中切除的卵巢癌组织及癌旁组织。采用实时荧光定量PCR法检测CLDN10、TRIM59 mRNA表达;采用免疫组织化学法检测CLDN10、TRIM59蛋白表达;采用Pearson法分析CLDN10、TRIM59的相关性;CLDN10、TRIM59与预后的关系采用Kaplan-Meier生存曲线分析;卵巢癌病人预后的危险因素采用Cox回归分析。结果与癌旁组织相比,卵巢癌组织中CLDN10 mRNA表达水平(0.62±0.14比1.00±0.23)及蛋白阳性表达率(39.29%比63.39%)明显降低(P<0.05),TRIM59 mRNA表达水平(1.64±0.32比1.01±0.25)及蛋白阳性表达率(64.29%比38.39%)明显升高(P<0.05)。根据Pearson相关性分析得知,卵巢癌组织中CLDN10、TRIM59 mRNA表达水平呈负相关(P<0.05)。卵巢癌组织中CLDN10、TRIM59表达与国际妇产科联盟(FIGO分期)、分化程度、淋巴结转移有关(P<0.05)。根据Kaplan-Meier法得知,卵巢癌组织中CLDN10阳性表达病人3年生存率高于阴性表达病人(P<0.05);卵巢癌组织中TRIM59阳性表达病人3年阳性生存率低于阴性表达病人(P<0.05)。根据Cox回归分析表明,CLDN10阴性、TRIM59阳性是影响卵巢癌病人预后的危险因素[HR=2.15,95%CI:(1.15,4.00);HR=3.55,95%CI:(1.55,8.10)]。结论卵巢癌组织中CLDN10阴性、TRIM59阳性是卵巢癌预后的危险因素,二者有可能作为有价值的预后标志物。

基于鲸鱼算法的10 kV组合互感器失真电流校正

对于10 kV组合互感器而言,电流失真会使输出电流的数值水平异常增大,并且长时间不恢复至常规电流状态,从而影响互感器的正常运行。为解决上述问题,设计基于鲸鱼算法的10 kV组合互感器失真电流校正方法。构建10 kV组合互感器结构模型,完善鲸鱼算法流程,基于鲸鱼算法获取失真的电流计量数值,实现组合互感器的失真特性判定,完成基于鲸鱼算法的10 kV组合互感器失真电流校正算法的设计。实验结果表明,经过设计方法对互感器失真电流进行校正处理后,可在2 min之内将失真电流恢复至与常规电流完全相同的数值状态,校正效果较好。

Association of interleukin-6 with acute lung injury risk and disease severity in sepsis

Sepsis is a life-threatening condition caused by a dysregulated response of the body in response to an infection that harms its tissues and organs.Interleukin-6(IL-6)is a significant component of the inflammatory response as part of the pa-thogenesis of sepsis.It aids in the development of Acute lung injury and,subse-quently,multiple organ dysfunction syndrome.This letter probes into the corre-lation between plasma IL-6 levels and the risk of developing acute lung injury and multiple organ dysfunction syndrome in critically ill patients with sepsis.While it shows promising results,limitations like its observational study design,a limited sample size,a single center involvement,single-time-point measurement,and a lack of a control group restrain its cogency.The study is a big step in identifying IL-6 as a biomarker to improve patient care.

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.

Regulation of lipoxygenase-1 and Dectin-1 on interleukin-10 in mouse Aspergillus fumigatus keratitis

AIM： To investigate the regulation of lipoxygenase （LOX）-1 and Dectin-1 on interleukin-10 （IL-10） production in mice with Aspergillus fumigatus （A. fumigatus） keratitis. METHODS： The corneas of C57BL/6 mice were pretreated with LOX-1 inhibitor Poly（I） or Dectin-1 siRNA separately before the infection of A. fumigatus. Polymerase chain reaction （PCR） and Western blot were used to detect the expression of IL-10. RESULTS： The mRNA and protein expressions of IL-10 were significantly increased in mice with A. fumigatus keratitis. Compared with the group pretreated with sterile water before infection, Poly（I） pretreatment suppressed IL-10 expression significantly. Compared with the group pretreated with scrambled siRNA before infection, Dectin-1 siRNA pretreatment significantly reduced IL-10 expression in response to A. fumigatus infection. CONCLUSION： LOX-1 and Dectin-1 regulate IL-10 production in mouse A. fumigatus keratitis.

Serum Levels of Interleukin-2 and -10 in Patients with Early Syphilis

Objective: To investigate the roles of interleukin-2(IL-2) and interleukin-10 (IL-10) in pathogenesis ofearly syphilis. Methods: The serum levels of IL-2 and IL-10 in 48patients with early syphilis were detected by ABC-ELISA. Results: (1) The level of IL-2 in the patients withearly syphilis was significantly higher than that inhealthy controls, while that of IL-10 was lower(P<0.001 and P<0.001). (2) The levels of IL-2 and IL-10 were almost identical in patients with primary andsecondary syphilis (P>0.05), as well as between dif-ferent RPR titers (P>0.05). (3) After therapy, the levelof IL-2 decreased markedly (P<0.05), while that of IL-10 increase (p>0.05). (4) A significant correlation wasfound between the serum levels of IL-2 and IL-10 (r=0.5385 P<0.05). Conclusions: Th1 up-regulation occurs in patientswith early syphilis, and plays an active role in fightingagainst TP infection.

基于DSM的城市公园对PM_(2.5)和PM_(10)的消减特征研究——以南昌市人民公园为例

【目的】PM_(2.5)、PM_(10)等空气颗粒物是城市空气首要污染物,在城市空气污染中占主导地位。了解固定外源下PM_(2.5)、PM_(10)在城市绿地的消减特征,可为城市阻控空气颗粒物、缓解空气污染提供有利依据。然而目前空气颗粒物的研究大多以点测定方式量化空间结构及植被类型对空气颗粒物的影响,对固定外源污染下PM_(2.5)、PM_(10)在城市绿地空间尺度上的影响机制研究较少。【方法】研究结合DSM与地统计学,以南昌市人民公园为例,探索城市公园阻隔外源污染的空间梯度效应及空间结构类型差异。利用克里金插值法对其空间分布特征进行可视化模拟;利用Arcgis和R语言等软件分析不同空间结构PM_(2.5)、PM_(10)的浓度差异。【结果】人民公园PM_(2.5)、PM_(10)的浓度在空间分布上趋势一致,均表现为以固定外源点为核心,浓度随距离增加呈极显著梯度递减的趋势,且在中部(约距外源点150~220 m处)消减效率最高,约为全园PM_(2.5)平均消减值的7.5倍,PM_(10)平均消减值的3.8倍;PM_(2.5)、PM_(10)受多种因子影响:与空气温度、距离(主导因子)显著负相关、与相对湿度显著正相关,且PM_(2.5)、PM_(10)对不同因子响应特征存在差异;城市公园不同绿地空间结构对PM_(2.5)、PM_(10)的消减及扩散作用差异显著,受其双重影响,PM_(2.5)、PM_(10)的浓度表现为水体>广场>树林>草坪,其中PM_(2.5)受影响更显著;此外,受各因子和绿地空间结构耦合影响,部分区域PM_(2.5)、PM_(10)分布异常。【结论】以固定外源点为核心,PM_(2.5)、PM_(10)浓度随距离增加呈极显著梯度递减的趋势,且在中部消减效率最高;PM_(2.5)、PM_(10)浓度与相对湿度显著正相关,与空气温度与距离显著负相关,其中PM_(10)对距离和相对湿度响应较为明显,而PM_(2.5)受空气温度影响较大;在随距离变化基础上,不同城市绿地空间结构对PM_(2.5)、PM_(10)消减和扩散作用差异导致了局部分布差异。

白细胞介素10基因多态性和多囊卵巢综合征遗传易感性的研究

目的 探讨白细胞介素10(interleukin-10,IL-10)基因rs1800871 A/G的单核苷酸多态性(single nucleotide polymorphism, SNP)和rs1800872 T/G SNP与多囊卵巢综合征(polycystic ovary syndrome, PCOS)患者遗传易感性。方法 通过SNaPshot SNP分型方法共分析了121例PCOS患者和158例健康对照IL-10基因rs1800871 A/G和rs1800872 T/G的单核苷酸多态性。结果 病例组体重指数、肥胖家族史阳性、T水平高于对照组,FSH水平低于健康对照组(P<0.05)。采用SHEsis软件对这两个多态性位点进行分析显示,两个位点存在完全连锁现象(D'=1)。病例组与健康对照组基因型构成和等位基因差异有统计学意义(P<0.05)。Logistic回归分析结果显示,肥胖家族史、IL-10基因rs1800871A/G单核苷酸多态性是PCOS发病的危险因素(P<0.05)。结论 IL-10基因rs1800871 A/G增加了对PCOS的遗传易感性,携带AG和GG基因型可能增加了PCOS的发病风险。

外周血IL-10、IL-33及其受体sST2水平与妊娠期糖尿病患者不良妊娠结局的关系

目的 探究外周血白介素-10(IL-10)、白介素-33(IL-33)及其受体可溶性肿瘤抑制素2(sST2)水平与妊娠期糖尿病(GDM)患者不良妊娠结局的关系。方法 选取2022年7月至2023年7月在我院建档产检的GDM患者80例纳入研究组,同期在我院进行产检的健康孕产妇80例纳入对照组,比较两组产妇孕37周时的外周血IL-10、IL-33及其受体sST2水平。对研究组患者进行追踪随访,并根据不同妊娠结局将研究组分为良好结局组(获得良好妊娠结局,n=55)和不良结局组(发生不良妊娠结局,n=25),探究影响GDM患者妊娠结局的因素,以及外周血IL-10、IL-33及其受体sST2水平对不良妊娠结局的预测价值。结果 研究组和对照组患者的年龄、孕次、产次、总胆固醇、受教育年限、孕前体质量指数(BMI)比较均无显著性差异(P>0.05),但研究组分娩前BMI、胰岛素抵抗指数均显著高于对照组(P<0.05)。研究组患者的IL-10水平显著低于对照组,IL-33及sST2水平显著高于对照组(P均<0.05)。对照组发生1例产后出血,2例巨大儿,不良妊娠结局总发生率为3.75%;研究组发生3例产后出血,5例巨大儿,8例新生儿窒息,6例足月低体重儿,3例胎儿发育异常,不良妊娠结局总发生率为31.25%,显著高于对照组(P<0.05)。研究组中,不良结局组患者的IL-10水平显著低于良好结局组,IL-33及sST2水平显著高于良好结局组(P均<0.05)。经单因素及多因素分析,IL-10、IL-33、sST2、胰岛素抵抗指数均能影响GDM患者的妊娠结局(P<0.05)。经受试者工作特征(ROC)曲线分析,IL-10、IL-33、sST2对GDM患者不良妊娠结局具有一定预测价值,曲线下面积(AUC)分别为0.969、0.945、0.960(P<0.05)。结论 外周血IL-10、IL-33及其受体sST2水平在预测GDM患者的新生儿窒息、产后出血、巨大儿、足月低体重儿、胎儿发育异常等不良妊娠结局方面具有潜在的临床应用价值,有助于早期识别上述高风险患者,以采取积极有效的干预措施改善妊娠结局。

高校仪器设备10S精细化管理的研究与实践

高校仪器设备的投入不断增加,如何管好、管活仪器设备,使其在教学和科研方面发挥更大的作用,是广大高校仪器设备管理工作者努力解决的问题。四川大学经过长期积极探索与不断实践,首次提出10S精细化仪器设备管理体系,以管理促发展,理论与实践相结合,仪器设备日常管理规范化与现代化相结合,大幅提升了仪器设备管理的科学化和精细化水平,有效提高了仪器设备开放共享的效益和受益面。对10S精细化管理在仪器设备管理中的具体内容进行了阐述与分析,可为其他高校仪器设备管理提供一定的借鉴和帮助。

瑞芬太尼调节IL-10/β-内啡肽信号通路对坐骨神经损伤大鼠疼痛的影响

目的探讨瑞芬太尼对坐骨神经损伤(SNI)大鼠疼痛的影响及作用机制。方法建立SNI大鼠模型,大鼠分为假手术组、模型组、瑞芬太尼低剂量组(5μg·kg^(-1)·min^(-1))、瑞芬太尼高剂量组(20μg·kg^(-1)·min^(-1))和瑞芬太尼+抑制剂组(20μg·kg^(-1)·min^(-1)的瑞芬太尼+10μL IL-10抗体),评估大鼠疼痛阈值,统计坐骨神经指数(SFI),Masson染液评价靶肌肉萎缩情况,酶联免疫吸附法(ELISA)检测白介素(IL)-1β、IL-6、肿瘤坏死因子(TNF)-α的含量,免疫荧光检测微管相关蛋白(MAP2)的表达,Western blot检测IL-10、β-内啡肽蛋白表达。结果与假手术组比较,模型组大鼠疼痛阈值、SFI和IL-10、β-内啡肽蛋白的表达水平下降,肌肉萎缩、IL-1β、IL-6、TNF-α、MAP2表达增加(P<0.05);与模型组比较,瑞芬太尼低、高剂量组大鼠疼痛阈值、SFI和IL-10、β-内啡肽蛋白的表达水平升高,肌肉萎缩、IL-1β、IL-6、TNF-α、MAP2表达降低,且呈剂量依赖性(P<0.05);与瑞芬太尼高剂量组比较,瑞芬太尼+抑制剂组大鼠疼痛阈值、SFI和IL-10、β-内啡肽蛋白的表达水平下降,肌肉萎缩、IL-1β、IL-6、TNF-α、MAP2表达增加(P<0.05)。结论瑞芬太尼可能通过激活IL-10/β-内啡肽信号通路抑制SNI大鼠的疼痛行为。

带状疱疹后遗神经痛患者治疗前后白介素10水平与疼痛程度和持续时间的相关性分析

目的分析带状疱疹后遗神经痛患者治疗前后白介素10(IL-10)水平与疼痛程度及持续时间的相关性。方法选取2020年6月至2021年12月我院收治的105例带状疱疹后遗神经痛患者,根据患者疼痛程度将患者分为轻中度组及重度组,比较两组患者白细胞、IL-10等实验室指标水平,患者出院后随访1年,记录患者疼痛持续时间,分析IL-10等指标水平与患者疼痛程度及持续时间的相关性。结果在随访期间4例患者失联,按脱落处理,最终纳入患者101例,其中轻中度组75例,重度组26例。两组患者年龄、性别等一般资料及治疗前后白细胞、中性粒细胞百分比水平相比较,差异无统计学意义(均P>0.05)。轻中度组疼痛评分、疼痛持续时间、治疗前超敏C-反应蛋白(Hs-CRP)及IL-10水平均显著低于重度组(t=28.408,23.888,2.726,9.381;均P<0.05);治疗后两组患者各指标均较前好转,但轻中度组患者Hs-CRP及IL-10水平仍显著低于重度组患者(t=4.342,5.966;均P<0.05)。相关性分析显示,治疗前、后IL-10水平与患者疼痛严重程度及持续时间呈显著正相关(r=0.705,0.209,0.739,0.481;均P<0.001);线性回归示,治疗前IL-10及Hs-CRP水平与患者疼痛持续程度显著相关(t=5.240,5.026;均P<0.05)。结论患者治疗前后IL-10水平与患者疼痛严重程度及疼痛持续时间显著相关,可成为患者预后的可靠预测因子,有助于评估患者预后。

白细胞介素10和过氧化氢酶对急性缺血性卒中病人卒中后抑郁的预测价值

目的:探讨白细胞介素10(IL-10)和过氧化氢酶(CAT)对急性缺血性卒中病人卒中后抑郁(PSD)的预测价值。方法:151例急性缺血性卒中病人入院后24 h内测定血清IL-10、CAT水平。使用17项汉密尔顿抑郁量表(HAMD-17)来评估抑郁症状;PSD定义为HAMD评分≥8。结果:脑梗死后1个月开始随访,有51例(33.8%)被诊断为PSD。与非PSD病人相比,PSD组入院和出院时NIHSS评分较高,脑梗死体积较大,BI评分较低,mRS评分较高,血清CAT、IL-10水平较低(P<0.05)。在调整了潜在混杂因素(在单变量逻辑回归分析中,P<0.05)后,IL-10(OR=0.615,95%CI:0.410~0.923)和CAT(OR=0.757,95%CI:0.652~0.914)仍然是PSD的独立预测因子。PSD病人的IL-10水平(r=0.394,P<0.01)和CAT水平(r=0.306,P<0.01)与HAMD评分呈负相关。ROC分析显示,血清IL-10水平的截止点为2.06 pg/mL,预测PSD的AUC为0.739。同时,CAT水平的截止点为1.07 U/L,预测PSD的AUC为0.630。IL-10水平较低(<2.06 pg/mL)的病人比对应组(≥2.06 pg/mL)更容易发生PSD(OR=9.750,95%CI=2.671~35.534,P<0.01)。同样,CAT水平较低(<1.07 U/L)的病人比对应组(≥1.07 U/L)更容易发生PSD(OR=5.052,95%CI=1.256~20.322,P<0.05)。结论:血清IL-10、CAT可用作急性缺血性卒中病人PSD的独立保护性预测因子。IL-10、CAT水平低的病人在卒中后1个月更有可能发生PSD。

非小细胞肺癌组织中CLDN10和CSPG4水平表达与临床病理特征及预后的关系研究

目的探讨非小细胞肺癌(non-small cell lung cancer,NSCLC)组织中紧密连接蛋白10(claudin 10,CLDN10)和硫酸软骨素蛋白聚糖4(chondroitin sulfate proteoglycan 4,CSPG4)表达与临床病理特征和预后的关系。方法随机选取2017年1月~2018年4月于南京医科大学附属泰州市人民医院进行手术的136例NSCLC患者为研究对象,并根据随访结局(生存或死亡)分为生存组(n=63)和死亡组(n=69)。收集136例患者于手术过程中切除的癌组织及癌旁组织标本;实时荧光定量PCR(real-time fluorescence quantitative PCR,RT-qPCR)检测癌组织及癌旁组织CLDN10和CSPG4表达水平,并分别以NSCLC患者癌组织中CLDN10和CSPG4表达水平的平均数为界限,分为CLDN10高表达组(n=66),CLDN10低表达组(n=70)和CSPG4高表达组(n=71),CSPG4低表达组(n=65);采用多因素COX回归分析确定NSCLC患者预后的影响因素;采用Kaplan-Meier生存曲线分析NSCLC患者CLDN10和CSPG4表达水平与其预后的关系。结果NSCLC组织中CLDN10表达水平(0.96±0.25)低于癌旁组织(1.73±0.42),CSPG4表达水平(1.80±0.46)高于癌旁组织(1.04±0.27),差异有统计学意义(t=18.372,16.617,均P<0.05)。与生存组比较,死亡组低未分化占比、淋巴结转移占比及癌组织中CSPG4表达水平较高,CLDN10表达水平较低,差异具有统计学意义(t/χ^(2)=8.463,7.423,11.696,6.426,均P<0.05)。CLDN10高表达组五年存活率(58.46%)高于低表达组(37.31%),CSPG4低表达组患者五年存活率(55.56%)高于高表达组(40.58%),差异有统计学意义(χ^(2)=7.848,4.018,均P<0.05)。多因素COX分析结果显示,CLDN10低表达、CSPG4高表达、低分化程度、淋巴结转移是NSCLC患者预后的危险因素(HR=1.362,1.368,1.335,1.314,均P<0.05)。结论NSCLC患者癌组织中CLDN10表达水平较低,CSPG4水平较高,且与NSCLC发展和预后密切相关。