The prognostic value of C-X-C motif chemokine receptor 4 in patients with sporadic malignant peripheral nerve sheath tumors

Background: Recent studies indicate that C-X-C motif chemokine receptor 4(CXCR4) and its ligand, C-X-C motif chemokine ligand 12(CXCL12), stimulate expression of the cell cycle regulatory protein Cyclin D1 in neurofibromatosis 1-associated malignant peripheral nerve sheath tumor(MPNST) cells and promote their proliferation. In this study, we measured the expression of CXCR4, CXCL12, and Cyclin D1 proteins in sporadic MPNST tissues from Chinese patients and investigated their prognostic values.Methods: CXCR4, CXCL12, and Cyclin D1 protein expression in samples from 58 Chinese patients with sporadic MPNST was assessed with immunohistochemical staining.Their prognostic values were evaluated with Kaplan-Meier analysis and a log-rank test. Multivariate Cox regression analysis was used to identify independent prognostic factors.Results: High expression of CXCR4, CXCL12, and Cyclin D1 was observed in 19(32.8%), 32(55.2%), and 16(27.6%)samples, respectively. CXCR4 expression was positively correlated with CXCL12 expression(r = 0.334, P = 0.010) and Cyclin D1 expression(r = 0.309, P = 0.018). Patients with high CXCR4 expression showed longer overall survival than those with low CXCR4 expression(χ~2 = 4.642, P = 0.031).Conclusion: High CXCR4 expression may define a specific subtype of sporadic MPNST with favorable prognosis.

Foodborne toxin Aflatoxin B_(1)induced glomerular podocyte inflammation through proteolysis of RelA,downregulation of miR-9 and CXCR4/TXNIP/NLRP3 pathway

Aflatoxin B_(1)(AFB_(1))is a naturally-occurring mycotoxin and recognized as the most toxic foodborne toxin,particularly causing damages to kidney.Glomerular podocytes are terminally differentiated epithelial cells.AFB_(1)induces podocyte inflammation,proteinuria and renal dysfunction.Studying the mechanism of AFB_(1)-induced podocyte inflammation and murine kidney dysfunction,we detected that AFB_(1)increased ubiquitindependent degradation of the transcription factor RelA through enhanced interaction of RelA with E3 ubiquitin ligase tripartite motif containing 7(TRIM7)in mouse podocyte clone-5(MPC-5)and mouse glomeruli.Reduction of RelA resulted in decreasing microRNA-9(miR-9)and activating the chemokine receptor 4(CXCR4),thioredoxin interacting protein(TXNIP),and NOD-like receptor pyrin domain-containing 3(NLRP3)signaling axis(CXCR4/TXNIP/NLRP3 pathway),leading to podocyte inflammation.We also determined that downregulation of miR-9 led to CXCR4 expression and the downstream TXNIP/NLRP3 pathway activation.Overexpression of miR-9 or deletion of CXCR4 suppressed AFB_(1)-induced CXCR4/TXNIP/NLRP3 pathway,resulting in alleviating podocyte inflammation and kidney dysfunction.Our findings indicated that ubiquitin-dependent proteolysis of RelA,downregulation of miR-9,and activation of CXCR4/TXNIP/NLRP3 pathway played an essential role in AFB_(1)-induced glomerular podocyte inflammation.Our study revealed a novel mechanism,via RelA,for the control of AFB_(1)’s nephrotoxicity,leading to an effective protection of food safety and public health.

慢性牙周炎患者血清CCL21、IRF4水平及临床意义

目的探讨慢性牙周炎患者血清CC基序趋化因子配体(CCL)21、干扰素调节因子(IRF)4水平及临床意义。方法选取2020年12月至2023年6月河北省邯郸市人民医院收治的124例慢性牙周炎患者作为患病组,另选取同期在河北省邯郸市人民医院体检的82例健康志愿者作为对照组,并根据慢性牙周炎严重程度将慢性牙周炎患者分为轻症组和中重症组。采用酶联免疫吸附试验检测所有研究对象血清CCL21、IRF4水平,评估慢性牙周炎患者的牙周临床指标[牙周袋探诊深度(PD)、附着丧失(AL)、牙龈沟出血指数(SBI)、牙龈指数(GI)、牙菌斑指数(PLI)]。采用Pearson相关分析慢性牙周炎患者血清CCL21、IRF4水平与牙周临床指标的相关性。绘制受试者工作特征(ROC)曲线分析血清CCL21、IRF4对慢性牙周炎患者病情严重程度的预测价值。结果患病组血清CCL21、IRF4水平高于对照组,差异均有统计学意义(P<0.05)。轻症组有66例患者,中重症组有58例患者。中重症组患者血清CCL21、IRF4水平及PD、SBI、AL、GI、PLI高于轻症组,差异均有统计学意义(P<0.05)。Pearson相关分析结果显示,慢性牙周炎患者血清CCL21、IRF4水平与PD、SBI、AL、GI、PLI呈正相关(P<0.05)。ROC曲线分析结果显示,2项指标联合预测中重症慢性牙周炎的曲线下面积(AUC)为0.914,大于CCL21、IRF4单独预测的AUC(Z_(联合=CCL21)=2.977,P=0.003;Z_(联合=IRF4)=2.412,P=0.016)。结论慢性牙周炎患者的血清CCL21、IRF4水平升高,且CCL21、IRF4对慢性牙周炎患者病情严重程度具有一定预测价值。

血清CX3CL1联合RBP4对急性脑梗死患者静脉溶栓预后的评估作用

目的探讨血清C-X3-C基序趋化因子配体1(CX3CL1)联合视黄醇结合蛋白4(RBP4)对急性脑梗死(ACI)患者静脉溶栓预后的评估作用。方法选取2020-01—2022-06内蒙古医科大学附属医院收治的120例ACI患者为ACI组,根据改良Rankin量表分为预后不良组和预后良好组,另选取同期60名体检健康志愿者为对照组。采用酶联免疫吸附法检测血清CX3CL1、RBP4水平。多因素Logistic回归和受试者工作特征曲线分析血清CX3CL1、RBP4水平对ACI患者静脉溶栓后预后不良的影响。结果与对照组比较,ACI组血清CX3CL1、RBP4水平升高(P<0.05)。随访3个月,120例ACI患者预后不良发生率为35.00%(42/120)。年龄、NIHSS评分、CX3CL1、RBP4为ACI患者静脉溶栓后预后不良的独立危险因素,弥散加权成像-阿尔伯塔卒中项目早期计算机断层扫描评分为独立保护因素(P<0.05)。血清CX3CL1、RBP4和二项联合评估预后不良的曲线下面积分别为0.779、0.778、0.876,二项联合的曲线下面积最大。结论ACI患者血清CX3CL1、RBP4水平升高,与静脉溶栓后预后不良独立相关且预测价值较高,可能成为ACI患者静脉溶栓后预后的辅助评估指标。

Functions and mechanisms of chemokine receptor 7 in tumors of the digestive system

Chemokine(C-X-C motif)receptor 7(CXCR7),recently termed ACKR3,belongs to the G protein-coupled cell surface receptor family,binds to stromal cellderived factor-1[SDF-1,or chemokine(C-X-C motif)ligand 12]or chemokine(CX-C motif)ligand 11,and is the most common chemokine receptor expressed in a variety of cancer cells.SDF-1 binds to its receptor chemokine(C-X-C motif)receptor 4(CXCR4)and regulates cell proliferation,survival,angiogenesis and migration.In recent years,another new receptor for SDF-1,CXCR7,has been discovered,and CXCR7 has also been found to be expressed in a variety of tumor cells and tumor-related vascular endothelial cells.Many studies have shown that CXCR7 can promote the growth and metastasis of a variety of malignant tumor cells.Unlike CXCR4,CXCR7 exhibits a slight modification in the DRYLAIV motif and does not induce intracellular Ca^2+release following ligand binding,which is essential for recruiting and activating G proteins.CXCR7 is generally thought to work in three ways:(1)Recruitingβ-arrestin 2;(2)Heterodimerizing with CXCR4;and(3)Acting as a“scavenger”of SDF-1,thus lowering the level of SDF-1 to weaken the activity of CXCR4.In the present review,the expression and role of CXCR7,as well as its prognosis in cancers of the digestive system,were investigated.

宣肺合剂联合西药治疗慢性支气管炎急性发作的疗效

目的 观察宣肺合剂联合西药治疗慢性支气管炎急性发作的疗效,及其对血清CXC趋化因子受体4(CXCR4)、半乳糖凝集素-9(Gal-9)和趋化因子3(CCL3)水平的影响。方法 选择2020年1月-2021年12月在本院诊治的慢性支气管炎急性发作的患者96例,分为观察组和对照组各48例。对照组予以常规西药治疗,观察组在对照组的基础上予以宣肺合剂治疗。比较两组治疗后的疗效和不良反应,比较治疗前后喘息、咳痰、咳嗽积分、第一秒用力呼气量(FEV1)、用力肺活量(FVC)、最大通气量(MVV)、CXCR4、Gal-9和CCL3水平的变化。结果 观察组的总有效率为95.83%,对照组的总有效率为79.17%,观察组显著优于对照组(P<0.05);两组的不良反应率差异无统计学意义(P>0.05)。两组治疗前喘息、咳痰、咳嗽积分、FEV1、FVC、MVV、CXCR4、Gal-9和CCL3水平差异无统计学意义(P>0.05);治疗后两组的喘息、咳痰、咳嗽积分、CXCR4、Gal-9和CCL3水平均较治疗前显著降低,与对照组比较观察组出现明显降低(均P<0.01);治疗后两组的FEV1、FVC和MVV水平均较治疗前显著升高,与对照组比较观察组显著升高(均P<0.01)。结论 宣肺合剂能够提高西药对慢性支气管炎急性发作的疗效,缓解症状和改善肺功能,其机制可能与降低机体CXCR4、Gal-9和CCL3的水平有关。

Overexpression of amplified in breast cancer 1 (AIB1) gene promotes lung adenocarcinoma aggressiveness in vitro and in vivo by upregulating C-X-C motif chemokine receptor 4

Background:We previously found that overexpression of the gene known as amplified in breast cancer 1(AIB1)was associated with lymph node metastasis and poor prognosis in patients with lung adenocarcinoma.However,the role of AIB1 in that malignancy remains unknown.The present study aimed to investigate the function of AIB1 in the process of lung adenocarcinoma cell metastasis.Methods:A series of in vivo and in vitro assays were performed to elucidate the function of AIB1,while real-time PCR and Western blotting were utilized to identify the potential downstream targets of AIB1 in the process of lung adenocarcinoma metastasis.Rescue experiments and in vitro assays were performed to investigate whether the invasive-ness of AIB1-induced lung adenocarcinoma was mediated by C-X-C motif chemokine receptor 4(CXCR4).Results:The ectopic overexpression of AIB1 in lung adenocarcinoma cells substantially enhanced cell migration and invasive abilities in vitro and tumor metastasis in vivo,whereas the depletion of AIB1 expression substantially inhibited lung adenocarcinoma cell migration and invasion.CXCR4 was identified as a potential downstream target of AIB1 in lung adenocarcinoma.The knockdown of AIB1 greatly reduced CXCR4 gene expression at both the transcription and protein levels,whereas the knockdown of CXCR4 in cells with AIB1 ectopic overexpression diminished AIB1-induced migration and invasion in vitro and tumor metastasis in vivo.Furthermore,we found a significant positive association between the expression of AIB1 and CXCR4 in lung adenocarcinoma patients(183 cases),and the co-overexpression of AIB1 and CXCR4 predicted the poorest prognosis.Conclusions:These findings suggest that AIB1 promotes the aggressiveness of lung adenocarcinoma in vitro and in vivo by upregulating CXCR4 and that it might be usable as a novel prognostic marker and/or therapeutic target for this disease.

The miR-9-5p/CXCL11 pathway is a key target of hydrogen sulfide-mediated inhibition of neuroinflammation in hypoxic ischemic brain injury

We previously showed that hydrogen sulfide(H2S)has a neuroprotective effect in the context of hypoxic ischemic brain injury in neonatal mice.However,the precise mechanism underlying the role of H2S in this situation remains unclear.In this study,we used a neonatal mouse model of hypoxic ischemic brain injury and a lipopolysaccharide-stimulated BV2 cell model and found that treatment with L-cysteine,a H2S precursor,attenuated the cerebral infarction and cerebral atrophy induced by hypoxia and ischemia and increased the expression of miR-9-5p and cystathionineβsynthase(a major H2S synthetase in the brain)in the prefrontal cortex.We also found that an miR-9-5p inhibitor blocked the expression of cystathionineβsynthase in the prefrontal cortex in mice with brain injury caused by hypoxia and ischemia.Furthermore,miR-9-5p overexpression increased cystathionine-β-synthase and H2S expression in the injured prefrontal cortex of mice with hypoxic ischemic brain injury.L-cysteine decreased the expression of CXCL11,an miR-9-5p target gene,in the prefrontal cortex of the mouse model and in lipopolysaccharide-stimulated BV-2 cells and increased the levels of proinflammatory cytokines BNIP3,FSTL1,SOCS2 and SOCS5,while treatment with an miR-9-5p inhibitor reversed these changes.These findings suggest that H2S can reduce neuroinflammation in a neonatal mouse model of hypoxic ischemic brain injury through regulating the miR-9-5p/CXCL11 axis and restoringβ-synthase expression,thereby playing a role in reducing neuroinflammation in hypoxic ischemic brain injury.

自身免疫性肝炎患者血清趋化因子CCL4和CXCL10水平及其临床意义探讨

目的探讨自身免疫性肝炎(AIH)患者血清趋化因子C-C-基元配体4(CCL4)和趋化因子配体10(CXCL10)水平及其临床意义。方法2016年12月~2020年12月我院收治的72例AIH患者均接受2年以上指南推荐的标准化免疫抑制治疗方案。采用ELISA法检测血清CCL4和CXCL10水平,使用全自动生化分析仪检测血生化指标,常规行肝活检。结果在2年治疗末,本组患者不完全应答47例,完全应答25例;完全应答患者血清CCL4和CXCL10水平分别为(46.4±18.4)pg/ml和(42.2±8.5)pg/ml,显著低于不完全应答患者【分别为(61.3±22.6)pg/ml和(89.1±47.4)pg/ml,P<0.05】;在72例患者中,26例患者存在凝血功能指标异常,均为不完全应答患者;完全应答患者PT、APTT和TT水平分别为(11.8±1.3)s、(29.6±2.2)s和(15.6±1.2)s,显著低于不完全应答患者【分别为(13.9±3.6)s、(41.3±6.2)s和(18.9±1.9)s,P<0.05】,而FIB水平为(3.1±0.8)g/l,显著高于不完全应答患者【(3.7±1.2)g/l,P<0.05】;凝血功能正常患者血清CCL4和CXCL10水平分别为(50.2±16.5)pg/ml和(66.3±18.2)pg/ml,显著低于凝血功能异常患者【分别为(68.0±24.2)pg/ml和(85.5±39.7)pg/ml,P<0.05】。结论AIH患者血清趋化因子CCL4和CXCL10水平可能影响治疗应答反应,且与凝血功能密切相关。检测血清CCL4和CXCL10水平可能有助于预测治疗应答。

CXCL12-CXCR4/CXCR7信号轴与PE发病关系的研究

目的通过检测子痫前期(PE)患者胎盘组织及血清中CXC趋化因子配体12(CXCL12)、CXC趋化因子受体4(CXCR4)以及CXCR7的表达水平,分析CXCR4、CXCR7、CXCL12表达与PE发病的关系。方法选取2016年9月至2017年9月扬州大学临床医学院妇产科住院分娩的产妇60例为研究对象,其中正常妊娠妇女(正常对照组)、轻度PE组及重度PE组各20例,通过免疫组织化学法和酶联免疫吸附法检测三组胎盘组织和血清中CXCL12、CXCR4以及CXCR7的表达。结果三组血清CXCL12、CXCR4、CXCR7表达比较差异有统计学意义(P<0.05),与正常对照组相比,重度PE组CXCL12、CXCR4及CXCR7表达显著降低(P<0.05);与轻度PE组相比,重度PE组CXCL12、CXCR4及CXCR7表达显著降低(P<0.05)。三组胎盘组织中CXCL12、CXCR4及CXCR7表达差异有统计学意义(P<0.05),与正常对照组相比,重度PE组胎盘组织中CXCL12、CXCR4、CXCR7的表达显著降低(均P<0.05),与轻度PE组相比,重度PE组胎盘组织中CXCL12、CXCR4、CXCR7的表达显著降低(均P<0.05)。结论 PE患者胎盘中CXCL12/CXCR4/CXCR7表达呈下降趋势,血清中CXCL12/CXCR4/CXCR7的表达呈下降趋势,可能与PE的发病有关。

CXCL10 Induces Lytic Reactivation of EBV through EXTL1

Epstein-Barr virus (EBV) infects over 90% of the global population, establishing latent infections in most individuals. Under specific conditions like inflammation and immune suppression, EBV can be reactivated, leading to the initiation and progression of related diseases. While inflammation is known to induce EBV reactivation, the precise mechanisms underlying this phenomenon remain unclear. Chemokine (C-X-C motif) ligand (CXCL10), a key inflammatory factor, plays a significant role in various infectious diseases. In this study, we investigated how CXCL10 levels regulate the transition between the latent and lytic replication phases of the EBV lifecycle using cell culture, Western blot, fluorescent quantitative PCR, immunofluorescence, and flow cytometric apoptosis assays. Our findings indicate that CXCL10 induces EBV transition from latency to lytic replication through its receptor CXCR3 by regulating the downstream effector, exostosis-like glycosyltransferase 1. Additionally, CXCL10 activates the JAK2/STAT3 pathway. This study confirms the role of CXCL10 in promoting EBV lytic replication, providing crucial insights into the pathogenic mechanisms of inflammation-triggered EBV reactivation.

CXCL4与高氧诱导新生小鼠性别差异性肺损伤的相关研究

目的:探讨肺组织CXC趋化因子配体4(chemokine C-X-C motif ligand 4,CXCL4)与高氧诱导新生小鼠性别差异性肺损伤的关系及相关机制。方法:32只C57BL/6J新生小鼠(雄性、雌性各16只)随机分为4组:高氧雄性组、高氧雌性组、空气雄性组、空气雌性组(每组8只)。高氧组小鼠置于95%氧浓度下暴露7 d,空气组于室内环境(FiO2=21%)中饲养。串联质谱标签(tandem mass tags,TMT)定量蛋白组学技术检测4组小鼠肺组织中蛋白质的表达变化,筛选差异表达的蛋白质;ELISA法检测肺组织匀浆CXCL4含量;HE染色法观察小鼠肺组织病理改变;冰冻切片免疫荧光染色检测肺组织'M4'型巨噬细胞(MMP7+ S100A8+)分布情况。结果:高氧暴露组肺组织肺泡化程度降低,辐射状肺泡计数(radial alveolar count,RAC)明显减小(P <0.001);与高氧雌性组相比,高氧雄性组RAC值下降(P <0.01)。TMT筛选出的CXCL4在高氧雄性组差异性表达上调;肺组织匀浆验证了质谱分析结果。高氧雄性小鼠肺组织MMP7+ S100A8+细胞增多。结论:高氧诱导新生小鼠肺损伤程度存在性别差异,雄性损伤程度高于雌性,可能与CXCL4诱导肺'M4'型巨噬细胞形成存在一定的相关性。

EGFR通过调控CXCR4/CXCL12信号通路对恶性外周神经鞘膜瘤细胞增殖、侵袭和迁移能力的影响

目的:探讨表皮生长因子受体(epidermal growth factor receptor,EGFR)的表达对恶性外周神经鞘膜瘤(malignant peripheral nerve sheath tumors,MPNST)细胞增殖、侵袭和迁移能力的影响,以及对C-X-C型趋化因子受体4/C-X-C型趋化因子配体12(C-X-C motif chemokine receptor 4/C-X-C motif chemokine ligand 12,CXCR4/CXCL12)信号通路的调节机制。方法:收集2017年6月至2019年6月在广州中医药大学第二临床医学院进行手术切除病灶的50例MPNST患者肿瘤组织作为观察组,50例皮肤型神经纤维瘤组织(dermal neurofibroma,DNF)作为对照组,免疫组化检测组织样本中的EGFR表达。细胞实验分为正常组(Normal组):不加任何药物,常规培养;对照组(Control组):细胞转染150 nmol/L EGFR-siRNA-NC后,常规培养;实验组(EGFR-siRNA组):细胞转染150 nmol/L EGFR-siRNA后,常规培养;5-乙炔基-2-脱氧尿嘧啶核苷(5-ethynyl-2’-deoxyuridine,EdU)标记实验检测各组细胞的增殖能力;Transwell小室实验检测各组细胞的迁移和侵袭能力;裸鼠皮下种植瘤模型检测各组细胞的体内生长与转移能力;基因芯片技术与实时荧光定量聚合酶链反应(real-time quantitative polymerase chain reaction,RT-qPCR)分析确定沉默EGFR基因后作用的靶基因;Western blot检测各组细胞中EGFR、CXCR4、CXCL12的表达。结果:免疫组化结果显示,对照组的EGFR阳性表达率为(2.35±0.32)%,MPNST患者肿瘤组织中的EGFR阳性表达率为(78.94±12.25)%,差异具有统计意义(t=123.573,均P=0.000);与Normal组相比,EGFR-siRNA组细胞的增殖能力(t=53.147,P=0.000)、侵袭与转移能力(t=26.947、34.638,P=0.000),体内生长与转移能力(t=15.683、22.197,均P=0.000)明显降低。基因芯片和RT-qPCR分析确定CXCR4、CXCL12是EGFR作用的靶基因。与Normal组相比,EGFR-siRNA组细胞中EGFR、CXCR4、CXCL12的表达明显下降(t=2.579、2.673、2.945,均P=0.000)。结论:在MPNST中,EGFR能调控CXCR4/CXCL12信号表达,调控肿瘤的生物学恶性行为,沉默EGFR表达,癌细胞的增殖、侵袭、迁移能力明显下降。

CXCL12-CXCR4在人类恶性肿瘤中的生物学功能

转移和细胞浸润是实体癌和淋巴癌治疗的难点,也是疾病复发和死亡的主要原因。癌细胞的迁移是肿瘤转移和侵袭的前提。CXCL12-CXCR4通路在实体瘤和白血病的发病中发挥重要作用。CXCL12与其受体CXCR4之间的相互作用可以激活多种信号通路,调节不同的生理和病理生理过程。因此,阻断CXCL12-CXCR4的结合和/或下游通路在治疗各种疾病和癌症方面具有临床益处。目前,已发现一些CXCL12和CXCR4拮抗剂,并通过研究证实其在抗肿瘤活性方面取得了令人鼓舞的结果;但这些药物由于其严重的毒副作用未能大规模应用于临床患者。迫切需要研发新型CXCL12-CXCR4轴拮抗剂以治疗肿瘤。本文综述了CXCR4通路在实体肿瘤和白血病中的最新研究进展,并讨论了CXCR4通路在实体肿瘤和白血病中的治疗价值和未来的研究方向。

The biological role of the CXCL12/CXCR4 axis in esophageal squamous cell carcinoma

Esophageal cancer is the eighth most common malignant tumor and the sixth leading cause of cancer-related death worldwide.Esophageal squamous cell carcinoma(ESCC)is the main histological type of esophageal cancer,and accounts for 90%of all cancer cases.Despite the progress made in surgery,chemotherapy,and radiotherapy,the mortality rate from esophageal cancer remains high,and the overall 5-year survival rate is less than 20%,even in developed countries.The C-X-C motif chemokine ligand 12(CXCL12)is a member of the CXC chemokine subgroup,which is widely expressed in a variety of tissues and cells.CXCL12 participates in the regulation of many physiological and pathological processes by binding to its specific receptor,C-X-C motif chemokine receptor type 4(CXCR4),where it causes embryonic development,immune response,and angiogenesis.In addition,increasing evidence indicates that the CXCL12/CXCR4 axis plays an important role in the biological processes of tumor cells.Studies have shown that CXCL12 and its receptor,CXCR4,are highly expressed in ESCC.This abnormal expression contributes to tumor proliferation,lymph node and distant metastases,and worsening prognosis.At present,antagonists and imaging agents against CXCL12 or CXCR4 have been developed to interfere with the malignant process and monitor metastasis of tumors.This article summarizes the structure,function,and regulatory mechanism of CXCL12/CXCR4 and its role in the malignancy of ESCC.Current results from preclinical research targeting CXCL12/CXCR4 are also summarized to provide a reference for the clinical diagnosis and treatment of ESCC.

基因干扰CXCL4对GBC-SD细胞恶性增殖和上皮间质转化的影响

目的 探究基因干扰CXCL4对GBC-SD细胞恶性增殖和上皮间质转化的影响.方法 构建shR-NACXCL4载体转染至GBC-SD细胞,将细胞随机分为3组:Control组、shRNA-NC组、CXCL4-shRNA1组.EDU染色检测细胞增殖;流式细胞仪检测细胞凋亡;荧光显微镜观测细胞上皮间质转化形态学变化;West-ern印迹检测Ki67、Survivin、Bax、Bcl-2、E-cadherin和N-cadherin蛋白表达;免疫荧光检测Vimentin含量.结果 与Control组相比,CXCL4-shRNA1组EDU阳性细胞数和Ki67、Survivin、N-cadherin蛋白水平降低,细胞凋亡率、Bax/Bcl-2比值、E-cadherin蛋白水平升高,抑制上皮间质转化,Vimentin含量降低,差异均有统计学意义(P<0.05).结论 基因干扰CXCL4抑制GBC-SD细胞恶性增殖、上皮间充质转化并促进凋亡.

Transforming growth factor-β and toll-like receptor-4 polymorphisms are not associated with fibrosis in haemochromatosis

AIM:To investigate the role of genetic polymorphisms in the progression of hepatic fibrosis in hereditary haemochromatosis.METHODS:A cohort of 245 well-characterised C282Y homozygous patients with haemochromatosis was studied,with all subjects having liver biopsy data and DNA available for testing.This study assessed the association of eight single nucleotide polymorphisms(SNPs)in a total of six genes including toll-like receptor 4(TLR4),transforming growth factor-beta(TGF-β),oxoguanine DNA glycosylase,monocyte chemoattractant protein 1,chemokine C-C motif receptor 2 and interleukin-10 with liver disease severity.Genotyping was performed using high resolution melt analysis and sequencing.The results were analysed in relation to the stage of hepatic fibrosis in multivariate analysis incorporating other cofactors including alcohol consumption and hepatic iron concentration.RESULTS:There were significant associations between the cofactors of male gender(P=0.0001),increasing age(P=0.006),alcohol consumption(P=0.0001),steatosis(P=0.03),hepatic iron concentration(P<0.0001)and the presence of hepatic fibrosis.Of the candidate gene polymorphisms studied,none showed a significant association with hepatic fibrosis in univariate or multivariate analysis incorporating cofactors.We also specifically studied patients with hepatic iron loading above threshold levels for cirrhosis and compared the genetic polymorphisms between those with no fibrosis vs cirrhosis however there was no significant effect from any of the candidate genes studied.Importantly,in this large,well characterised cohort of patients there was no association between SNPs for TGF-βor TLR4and the presence of fibrosis,cirrhosis or increasing fibrosis stage in multivariate analysis.CONCLUSION:In our large,well characterised group of haemochromatosis subjects we did not demonstrate any relationship between candidate gene polymorphisms and hepatic fibrosis or cirrhosis.

CXCL12/CXCR4通路在心脑血管疾病中的研究进展

CXC趋化因子配体12(chemokine C-X-C motif ligand 12,CXCL12)是一种能诱导细胞向损伤部位定向运动的小分子蛋白质,可诱导祖细胞归巢、迁移至病变部位以促进机体修复维持稳态。趋化因子CXCL12及其特异性受体CXC趋化因子受体4(C-X-C chemokine receptor 4,CXCR4)构成CXCL12/CXCR4生物学轴,参与炎症反应、肿瘤形成、免疫疾病的发生等。CXCL12/CXCR4在心脑血管疾病的发生发展中起重要的作用,现就CXCL12/CXCR4轴在心脑血管疾病中的作用进行综述。

免疫因子表达异常促进宫颈癌微环境免疫失衡

目的评估叉头蛋白3(Fox P3)、趋化因子配体22(CCL22)、肿瘤坏死因子受体超家族成员40(OX40)和SMAD家族成员3(Smad3)在宫颈癌免疫微环境中的调节作用和对肿瘤发生的影响。方法采用qRT-PCR方法检测宫颈癌癌灶、癌旁和正常宫颈组织中Fox P3、CCL22、OX40和Smad3的mRNA表达水平。结果与正常宫颈组织相比,Fox P3和CCL22 mRNA在癌灶(P=0.000,P=0.002)和癌旁(P=0.048,P=0.040)的表达显著升高,两者在高级别鳞癌癌灶(P=0.019,P=0.020)和癌旁(P=0.023,P=0.031)中的表达明显高于低级别鳞癌。OX40和Smad3的mRNA在癌灶中的表达明显低于正常宫颈(P=0.000,P=0.015),两者在高级别鳞癌癌灶(P=0.018,P=0.030)和癌旁(P=0.027,P=0.014)中的表达明显低于低级别鳞癌。在宫颈癌灶和癌旁中,OX40 mRNA与Smad3 mRNA(r=0.384,P=0.002;r=0.288,P=0.023)、Fox P3 mRNA与CCL22 mRNA均呈正相关(r=0.353,P=0.000;r=0.307,P=0.000),CCL22 mRNA与OX40 mRNA呈负相关(r=-0.288,P=0.031;r=-0.263,P=0.037)。Fox P3和CCL22mRNA在HPV阳性的宫颈癌灶(P=0.024,P=0.039)和癌旁(P=0.032,P=0.034)中的表达明显高于阴性组,Smad3在HPV阳性宫颈癌灶中的表达明显低于HPV阴性组(P=0.017)。结论在宫颈癌发生的微环境中,存在免疫因子Fox P3、CCL22、OX40和Smad3的转录表达异常,这种表达偏移可能导致宫颈癌局部OX40和Smad3的正性调节被削弱,而Fox P3和CCL22的免疫抑制作用增强的免疫模式,共同参与促成局部免疫失衡和肿瘤的发生。

Identification of differentially expressed genes in ulcerative colitis and verification in a colitis mouse model by bioinformatics analyses

BACKGROUND Ulcerative colitis(UC)is an inflammatory bowel disease that is difficult to diagnose and treat.To date,the degree of inflammation in patients with UC has mainly been determined by measuring the levels of nonspecific indicators,such as C-reactive protein and the erythrocyte sedimentation rate,but these indicators have an unsatisfactory specificity.In this study,we performed bioinformatics analysis using data from the National Center for Biotechnology Information-Gene Expression Omnibus(NCBI-GEO)databases and verified the selected core genes in a mouse model of dextran sulfate sodium(DSS)-induced colitis.AIM To identify UC-related differentially expressed genes(DEGs)using a bioinformatics analysis and verify them in vivo and to identify novel biomarkers and the underlying mechanisms of UC.METHODS Two microarray datasets from the NCBI-GEO database were used,and DEGs between patients with UC and healthy controls were analyzed using GEO2R and Venn diagrams.We annotated these genes based on their functions and signaling pathways,and then protein-protein interactions(PPIs)were identified using the Search Tool for the Retrieval of Interacting Genes.The data were further analyzed with Cytoscape software and the Molecular Complex Detection(MCODE)app.The core genes were selected and a Kyoto Encyclopedia of Genes and Genomes pathway enrichment analysis was performed.Finally,colitis model mice were established by administering DSS,and the top three core genes were verified in colitis mice using real-time polymerase chain reaction(PCR).RESULTS One hundred and seventy-seven DEGs,118 upregulated and 59 downregulated,were initially identified from the GEO2R analysis and predominantly participated in inflammation-related pathways.Seven clusters with close interactions in UC formed:Seventeen core genes were upregulated[C-X-C motif chemokine ligand 13(CXCL13),C-X-C motif chemokine receptor 2(CXCR2),CXCL9,CXCL5,C-C motif chemokine ligand 18,interleukin 1 beta,matrix metallopeptidase 9,CXCL3,formyl peptide receptor 1,complement component 3,CXCL8,CXCL1,CXCL10,CXCL2,CXCL6,CXCL11 and hydroxycarboxylic acid receptor 3]and one was downregulated[neuropeptide Y receptor Y1(NYP1R)]in the top cluster according to the PPI and MCODE analyses.These genes were substantially enriched in the cytokinecytokine receptor interaction and chemokine signaling pathways.The top three core genes(CXCL13,NYP1R,and CXCR2)were selected and verified in a mouse model of colitis using real-time PCR Increased expression was observed compared with the control mice,but only CXCR2 expression was significantly different.CONCLUSION Core DEGs identified in UC are related to inflammation and immunity inflammation,indicating that these reactions are core features of the pathogenesis of UC.CXCR2 may reflect the degree of inflammation in patients with UC.