CXCR4 MFAP2 KLF4在分化型甲状腺癌中的表达及对预后的预测价值研究

目的:研究趋化因子4受体(CXCR4)、微纤维相关蛋白2(MFAP2)、Krüppel样因子4(KLF4)在分化型甲状腺癌(DTC)中的表达及对预后的预测价值。方法:选择我院2019年7月至2020年7月收治的113例DTC患者,术中留取其肿瘤组织及癌旁正常组织。采用蛋白免疫印迹法检测DTC组织及癌旁正常组织中CXCR4、MFAP2、KLF4表达水平,分析CXCR4、MFAP2、KLF4表达水平与DTC临床病理特征的关系。对DTC患者进行3年随访,统计3年总生存情况,比较死亡组与存活组CXCR4、MFAP2、KLF4表达水平,采用ROC曲线分析CXCR4、MFAP2、KLF4对DTC预后的预测价值,采用Cox回归模型进行DTC预后单因素和多因素分析。结果:与癌旁正常组织比较,DTC组织CXCR4、MFAP2蛋白表达量显著升高(P<0.05),KLF4蛋白表达量显著降低(P<0.05)。TNM分期Ⅲ期、发生淋巴结转移、肿瘤低分化者CXCR4、MFAP2蛋白表达量显著高于TNM分期Ⅰ+Ⅱ期、未发生淋巴结转移、肿瘤中高分化者(P<0.05),TNM分期Ⅲ期、发生淋巴结转移、肿瘤低分化者KLF4蛋白表达量显著低于TNM分期Ⅰ+Ⅱ期、未发生淋巴结转移、肿瘤中高分化者(P<0.05)。113例DTC患者随访3年期间失访8例,最终获得随访者105例。死亡组患者CXCR4、MFAP2蛋白表达量显著高于存活组(P<0.05),KLF4蛋白表达量显著低于存活组(P<0.05)。绘制ROC曲线发现,CXCR4、MFAP2、KLF4单独或联合预测DTC预后的AUC(95%CI)分别为0.692(0.562~0.823)、0.729(0.590~0.869)、0.766(0.622~0.910)、0.832(0.690~0.975),联合预测的效能显著优于单项检测(P<0.05)。Cox回归分析显示,淋巴结转移、TNM分期Ⅲ期、肿瘤低分化、CXCR4表达升高、MFAP2表达升高、KLF4表达降低是DTC预后的危险因素(P<0.05)。结论:分化型甲状腺癌患者肿瘤组织中CXCR4、MFAP2呈高表达,KLF4呈低表达,其表达水平与淋巴结转移、肿瘤分化程度、TNM分期及3年总生存率相关,三者联合检测有助于预测分化型甲状腺癌预后。

Chemokine receptor CXCR4-prognostic factor for gastrointestinal tumors

To review the implication of CXCR4 for gastrointestinal cancer, a "Pubmed" analysis was performed in order to evaluate the relevance of CXCR4 and its ligands for gastrointestinal cancers. Search terms applied were "cancer, malignoma, esophageal, gastric, colon, colorectal, hepatic, pancreatic, CXCR4, SDF-1α, and SDF-1b". CXCR4 expression correlated with dissemination of diverse gastrointestinal malignomas. The CXCR4 ligand SDF-1α might act as "chemorepellent" while SDF-1b might act as "chemorepellent" for CTLs, inducing tumor rejection. The paracrine expression of SDF-1α was furthermore closely associated with neoangiogenesis. CXCR4 and its ligands influence the dissemination, immune rejection, and neoangiogenesis of human gastrointestinal cancers. Inhibition of CXCR4 might be an interesting therapeutic option.

CXCL12 Retargeting of an Oncolytic Adenovirus Vector to the Chemokine CXCR4 and CXCR7 Receptors in Breast Cancer

Breast cancer is the most frequently diagnosed cancer in women under 60, and the second most diagnosed cancer in women over 60. While significant progress has been made in developing targeted therapies for breast cancer, advanced breast cancer continues to have high mortality, with poor 5-year survival rates. Thus, current therapies are insufficient in treating advanced stages of breast cancer;new treatments are sorely needed to address the complexity of advanced-stage breast cancer. Oncolytic virotherapy has been explored as a therapeutic approach capable of systemic administration, targeting cancer cells, and sparing normal tissue. In particular, oncolytic adenoviruses have been exploited as viral vectors due to their ease of manipulation, production, and demonstrated clinical safety profile. In this study, we engineered an oncolytic adenovirus to target the chemokine receptors CXCR4 and CXCR7. The overexpression of CXCR4 and CXCR7 is implicated in the initiation, survival, progress, and metastasis of breast cancer. Both receptors bind to the ligand, CXCL12 (SDF-1), which has been identified to play a crucial role in the metastasis of breast cancer cells. This study incorporated a T4 fibritin protein fused to CXCL12 into the tail domain of an adenovirus fiber to retarget the vector to the CXCR4 and CXCR7 chemokine receptors. We showed that the modified virus targets and infects CXCR4- and CXCR7-overexpressing breast cancer cells more efficiently than a wild-type control vector. In addition, the substitution of the wild-type fiber and knob with the modified chimeric fiber did not interfere with oncolytic capability. Overall, the results of this study demonstrate the feasibility of retargeting adenovirus vectors to chemokine receptor-positive tumors.

吴茱萸碱调节SDF-1α/CXCR4信号通路对颅内动脉瘤血管平滑肌细胞增殖和凋亡的影响

目的探究吴茱萸碱通过调节基质细胞衍生因子1α(SDF-1α)/CXC趋化因子受体4(CXCR4)信号通路对颅内动脉瘤(IA)血管平滑肌细胞(VSMCs)的增殖和凋亡的作用。方法24只小鼠随机分为对照组和IA组,每组12只。IA组通过定位手术注射弹性蛋白酶制造IA模型小鼠,然后通过HE染色观察动脉组织变化。随后将小鼠主动脉血管平滑肌细胞(MOVAS)先用MTT法检测吴茱萸碱浓度对细胞的活性影响,然后将MOVAS分为ctrl组、Model组(H_(2)O_(2)诱导损伤组)、低浓度吴茱萸碱组(0.50μmol/L)、高浓度吴茱萸碱组(1.00μmol/L)、高浓度吴茱萸碱+CTCE-0214组(1.00μmol/L吴茱萸碱+10 mg/kg SDF-1α/CXCR4激活剂)。CCK-8试剂盒检测细胞活性;流式细胞术检测细胞凋亡;Western blot检测SDF-1α、CXCR4、BAX、增殖细胞核抗原(PCNA)、平滑肌22α(SM22α)和平滑肌α肌动蛋白(α-SMA)的蛋白表达。结果与对照组正常动脉组织比较,IA组的IA组织出现明显的病理变化,损伤严重。在MOVAS细胞实验中,与ctrl组比较,Model组的细胞凋亡率、SDF-1α、CXCR4、BAX蛋白表达增加,而细胞存活率、PCNA、SM22α、α-SMA含量降低(P<0.05)。与Model组比较,低浓度吴茱萸碱组、高浓度吴茱萸碱组的细胞凋亡率、SDF-1α、CXCR4、BAX蛋白表达降低,而细胞存活率、PCNA、SM22α、α-SMA含量升高(P<0.05);与高浓度吴茱萸碱组比较,高浓度吴茱萸碱+CTCE-0214组细胞凋亡率、SDF-1α、CXCR4、BAX蛋白表达升高,而细胞存活率、PCNA、SM22α、α-SMA含量降低(P<0.05)。结论吴茱萸碱可能通过抑制SDF-1α/CXCR4信号通路进而抑制颅内动脉瘤血管平滑肌细胞的凋亡,促进其增殖。

血清CXCR4水平与颅内动脉粥样硬化性狭窄的相关性研究

目的探讨血清中C-X-C基序趋化因子受体4(C-X-C motif chemokine receptor 4,CXCR4)水平与颅内动脉粥样硬化性狭窄(intracranial atherosclerotic stenosis,ICAS)的关系。方法该研究为病例对照研究。连续性纳入自2022年3月至2023年4月于北京医院神经内科住院治疗的缺血性脑血管病患者。应用颅内动脉检查(MRA、CTA或DSA)评估患者颅内动脉粥样硬化情况,将患者分为ICAS组(颅内动脉狭窄≥50%)和对照组(颅内动脉狭窄<50%),检测两组患者的血清CXCR4水平,通过多因素分析探讨CXCR4水平与ICAS的相关性。根据颅内动脉狭窄程度将ICAS组患者进一步分为中度狭窄组(50%≤颅内动脉狭窄<70%)及重度狭窄组(70%≤颅内动脉狭窄≤100%),比较各组间CXCR4水平的差异。结果共纳入患者264例,其中ICAS组173例〔男125例;年龄(69.05±11.06)岁〕,对照组91例〔男56例;年龄(66.96±11.12)岁〕。ICAS组CXCR4水平高于对照组〔(320.00±46.90)ng/L比(304.00±51.54)ng/L,t=2.472,P=0.014〕。校正相关混杂因素后,Logistic回归分析结果提示CXCR4水平升高〔OR(95%CI):1.007(1.002~1.013),P=0.011〕是ICAS的独立影响因素。ICAS中、重度狭窄组及对照组间CXCR4水平差异有统计学意义(F=5.527,P=0.004),且ICAS重度狭窄组患者血清中CXCR4水平明显高于对照组〔(324.82±45.87)ng/L比(304.00±51.54)ng/L,t=3.132,P=0.002〕及ICAS中度狭窄组〔(324.82±45.87)ng/L比(307.47±47.72)ng/L,t=2.118,P=0.035〕。结论血清CXCR4水平在ICAS患者中升高是ICAS的独立影响因素,有作为评估ICAS潜在生物标志物的潜力。

甲基莲心碱调节SDF-1/CXCR4信号通路对糖尿病肾病的影响

目的·探讨甲基莲心碱(neferine,Nef)对糖尿病肾病(diabetic nephropathy,DN)大鼠肾组织的作用及其相关机制。方法·采用高脂饲料喂食联合腹腔注射链脲佐菌素的方法构建DN模型大鼠,并将造模成功的大鼠随机分为DN组、Nef(低、中、高)剂量组、Nef高剂量+通路拮抗剂(AMD3100)组,每组10只。同时,选10只普通大鼠作为正常组。检测6组大鼠的空腹血糖(fasting blood glucose,FBG)、24 h尿蛋白、血清糖化血红蛋白(glycosylated hemoglobin,HbA1c)、血清肌酐(serum creatinine,Scr)、尿素氮(blood urea nitrogen,BUN)水平及肾指数。分别采用苏木精-伊红(hematoxylin-eosin,H-E)染色、马松(Masson)染色观察6组大鼠的肾组织的病理变化。采用硫代巴比妥酸(thiobarbituric acid,TBA)法检测肾组织丙二醛(malondialdehyde,MDA)含量,分别采用水溶性四氮唑(water soluble tetrazolium,WST-1)法、钼酸铵法检测肾组织超氧化物歧化酶(superoxide dismutase,SOD)、过氧化氢酶(catalase,CAT)的活性。分别采用实时荧光定量PCR(quantitative real-time PCR,qPCR)和蛋白质印迹法(Western blotting)检测肾组织中基质细胞衍生因子-1(stromal cell-derived factor-1,SDF-1)、CXC趋化因子受体4(CXC chemokine receptor 4,CXCR4)的mRNA以及蛋白表达。采用高糖(30 mmol/L葡萄糖)诱导大鼠肾小管上皮细胞NRK-52E,以建立DN细胞模型。将该细胞分为对照组、高糖(HG)组、HG+Nef(低、中、高)剂量组(即HG+Nef-L、M、H组)、HG+Nef-H+AMD3100组。分别采用WST-1法、钼酸铵法检测模型细胞中SOD、CAT活性,采用TBA法检测MDA含量,分别采用qPCR、Western blotting检测SDF-1、CXCR4的mRNA及蛋白表达,采用CCK-8法、流式细胞术检测细胞活力和凋亡率。结果·与DN组比较,Nef(低、中、高)剂量组和Nef高剂量+AMD3100组大鼠的FBG、24 h尿蛋白、HbA1c、Scr、BUN水平以及肾指数、MDA水平均较低,SDF-1、CXCR4的mRNA和蛋白表达以及SOD、CAT活性均较高(均P<0.05),肾组织病理损伤、纤维化程度有所减轻,且均呈剂量依赖性;AMD3100能减弱高剂量Nef对DN大鼠的肾保护作用。与HG组比较,HG+Nef-L、M、H组NRK-52E细胞的活力,SOD、CAT活性,SDF-1、CXCR4的mRNA和蛋白表达均较高,MDA含量及凋亡率均较低(均P<0.05);AMD3100可逆转Nef-H对NRK-52E细胞损伤的保护作用。结论·Nef可能通过激活SDF-1/CXCR4信号通路来控制DN大鼠的血糖水平并提高其抗氧化能力,从而发挥肾保护作用。

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.

SDF-1/CXCR4信号轴在MSCs修复损伤组织中作用的研究进展

骨髓间充质干细胞(mesenchymal stem cells,MSCs)具有自我更新和多向分化潜能,在损伤组织修复中起着重要作用。基质细胞衍生因子-1(stromal cell-derived factor-1,SDF-1)/CXC趋化因子受体4(CXC chemokine receptor 4,CXCR4)信号轴是由SDF-1与其受体CXCR4相互作用构成的耦联分子对,能够进行细胞间信号转导、诱导细胞的定向迁移,参与细胞的多种生物学过程。研究证实,SDF-1/CXCR4信号轴在MSCs参与心肌缺血、肾脏病变、骨组织损伤等损伤组织修复过程中有重要的促趋化和增殖的作用。本文简要介绍了SDF-1和CXCR4的分子结构,重点阐述了SDF-1/CXCR4信号轴在MSCs参与相关损伤组织修复中的作用,归纳总结了该领域的研究进展,并展望了该领域未来的发展方向,为深入理解SDF-1/CXCR4信号轴及其在MSCs参与组织损伤修复过程中的作用提供理论基础,也为临床上更好地将MSCs应用于损伤组织修复提供参考。

C-X-C chemokine receptor type 7 antibody enhances neural plasticity after ischemic stroke

Stromal cell-derived factor-1 and its receptor C-X-C chemokine receptor 4(CXCR4) have been shown to regulate neural regeneration after stroke.Howeve r,whether stromal cell-derived factor-1 receptor CXCR7,which is widely distributed in the develo ping and adult central nervous system,participates in neural regeneration remains poorly unde rstood.In this study,we established rat models of focal cerebral ischemia by injecting endothelin-1 into the cerebral co rtex and striatum.Starting on day 7 after injury,CXCR7-neutralizing antibody was injected into the lateral ventricle using a micro drug delivery system for 6 consecutive days.Our results showed that CXCR7-neutralizing antibody increased the total length and number of sprouting co rticospinal tra ct fibers in rats with cerebral ischemia,increased the expression of vesicular glutamate transporter 1 and growth-related protein 43,marke rs of the denervated spinal cord synapses,and promoted the differentiation and maturation of oligodendrocyte progenitor cells in the striatum.In addition,CXCR7 antibody increased the expression of CXCR4 in the striatum,increased the protein expression of RAS and ERK1/2 associated with the RAS/ERK signaling pathway,and im proved rat motor function.These findings suggest that CXCR7 improved neural functional recovery after ischemic stroke by promoting axonal regeneration,synaptogenesis,and myelin regeneration,which may be achieved by activation of CXCR4 and the RAS/ERK1/2 signaling pathway.

Chemokine receptor 4 gene silencing blocks neuroblastoma metastasis in vitro

This study investigated the effects of small interfering RNA （siRNA）-mediated silencing of chemokine receptor 4 （CXCR4） on the invasion capacity of human neuroblastoma cell line SH-SY5Y in vitro. Three siRNAs targeting CXCR4 were chemically synthesized and individually transfected into SH-SY5Y cells. Expression of CXCR4 mRNA and protein was signiifcantly sup-pressed in transfected cells by all three sequence-speciifc siRNAs compared with control groups. Furthermore, the invasion capacity of SH-SY5Y cells was signiifcantly decreased following trans-fection with CXCR4-speciifc siRNA compared with the control groups. These data demonstrate that down-regulation of CXCR4 can inhibit in vitro invasion of neuroblastoma.

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.

脂联素调控SDF-1α/CXCR4信号轴在炎症微环境下牙周膜干细胞成骨分化中的作用

目的 研究脂联素通过调控基质细胞衍生因子-1α(SDF-1α)/CXC趋化因子受体4(CXCR4)信号轴对炎症微环境下牙周膜干细胞(PDLSCs)成骨分化中的影响。方法 原代培养PDLSCs后取第三代细胞进行分组处理,进行成骨分化诱导并用10 ng/mL肿瘤坏死因子-α(TNF-α)模拟微炎症环境、用10μg/mL脂联素处理、转染阴性对照(NC)或SDF-1α的siRNA。成骨诱导第3、5、7 d时,检测碱性磷酸酶(ALP)活性,骨钙素(OCN)、骨保护素(OPN)、SDF-1α、CXCR4的m RNA表达,SDF-1α的含量;成骨诱导第21 d时,进行茜素红染色、观察钙盐沉积情况。结果 炎症微环境下PDSCSs的成骨分化及SDF-1α/CXCR4信号轴的激活均受到抑制;脂联素在炎症微环境下促进PDSCSs的成骨分化及SDF-1α/CXCR4信号轴的激活;转染SDF-1α的siRNA后,SDF-1α/CXCR4信号轴的激活受到抑制,脂联素在炎症微环境下促进PDSCSs成骨分化的作用也被抑制。结论 脂联素通过激活SDF-1α/CXCR4信号轴促进炎症微环境下PDSCSs的成骨分化。

NONHSAT248596.1内源性竞争miR-146a-5p调控骨关节炎软骨退变的机制

背景:目前已有针对lncRNA\miRNA\mRNA的共表达网络对骨关节炎发生发展调控机制的研究,课题组前期研究已通过数据库筛选出符合条件的NONHSAT248596.1和miR-146a-5p,尚缺乏体内实验来验证上述调控机制。目的:探究NONHSAT248596.1在基质细胞衍生因子1/4型趋化因子受体轴介导体内骨关节炎软骨退变进程中对miR-146a-5p发挥的竞争性内源性RNA调控作用。方法:取36只新西兰兔,通过向右侧后肢膝关节注射基质细胞衍生因子1溶液建立骨关节炎模型,采用随机数字表法分4组,lncRNA组、miRNA组、ceRNA组、对照组分别向造模膝关节内注射NONHSAT248596.1过表达的慢病毒载体、miR-146a-5p过表达的慢病毒载体、miR-146a-5p+NONHSAT248596.1过表达的慢病毒载体及空慢病毒载体。造模第4,8,12周,取膝关节软骨组织和软骨下骨组织进行相关检测。结果与结论:①苏木精-伊红与番红O固绿染色显示,4组软骨组织都有不同程度的退变表现,造模第4周时,lncRNA组软骨组织中的软骨细胞肿胀、细胞极性消失,细胞外基质破坏,出现表层糜烂、裂缝形成和软骨组织局部或全层缺失,并随时间延长软骨损伤程度逐渐加重,4组中miRNA组关节软骨炎症进展最缓慢;②qRT-PCR检测显示,相同时间点下,lncRNA组软骨组织中NONHSAT248596.1、4型趋化因子受体、基质金属蛋白酶3,9及13的mRNA表达量高于其他3组(P<0.05),miR-146a-5p、聚集蛋白聚糖及Ⅱ型胶原的mRNA表达量低于其他3组(P<0.05);造模后第8,12周,miRNA组软骨组织中的NONHSAT248596.1、4型趋化因子受体、基质金属蛋白酶3,9及13的mRNA表达量低于ceRNA组、对照组(P<0.05),miR-146a-5p、聚集蛋白聚糖及Ⅱ型胶原的mRNA表达量高于ceRNA组、对照组(P<0.05);③Western Blot检测显示,相同时间点下,lncRNA组软骨组织中的聚集蛋白聚糖及Ⅱ型胶原蛋白表达量始终低于其他3组(P<0.05);miRNA组造模后第8,12周软骨组织中的聚集蛋白聚糖及Ⅱ型胶原蛋白表达量高于ceRNA组、对照组(P<0.05);④结果表明,miR-146a-5p作为NONHSAT248596.1的作用靶点会受到其竞争性内源性RNA的作用造成活性被抑制,NONHSAT248596.1作用于miR-146a-5p后调控基质细胞衍生因子1/4型趋化因子受体轴,影响骨关节炎软骨组织中基质金属蛋白、Ⅱ型胶原、聚集蛋白聚糖的表达,造成细胞外基质的降解及蛋白多糖的丢失。

RGS4蛋白、CXCR4、TOPOⅡα在小儿肾母细胞瘤组织中的表达及其与临床病理特征和预后的关系

目的探究蛋白信号调节因子4(RGS4)、趋化因子受体趋化因子受体4(CX-CR4)、拓扑异构酶Ⅱα(TOPOⅡα)在小儿肾母细胞瘤组织中的表达及其与临床病理特征和预后的关系。方法选取2017年1月至2020年1月于海南医学院第二附属医院行手术治疗的肾母细胞瘤40例患儿为研究对象,并留距离癌组织边缘>4 cm的癌旁组织40例作为对照。探究RGS4蛋白、CXCR4、TOPOⅡα表达水平与肾母细胞瘤患儿临床病理特征及生存时间之间的关系。结果与癌旁组织对比,肾母细胞瘤组织中TOPOⅡα、CXCR4的高表达率升高,RGS4蛋白高表达率下降(P<0.05)。RGS4蛋白与淋巴结转移、病理种类、复发转移、TNM分期呈负相关;CXCR4、TOPOⅡα与其呈正相关(P<0.05)。RGS4蛋白、CXCR4、TOPOⅡα与复发转移、病理种类、淋巴结转移、TNM分期有关(P<0.05)。RGS4蛋白高表达者总生存率较高,CXCR4、TOPOⅡα高表达的患儿总生存率较低。结论小儿肾母细胞瘤组织中RGS4蛋白、CXCR4及TOPOⅡα的表达变化与临床病理特征变化和预后生存密切相关。

血清SDF-1α、CXCR4与糖尿病足溃疡感染、病情程度及预后的相关性

目的探讨血清基质细胞衍生因子-1α(SDF-1α)、趋化因子受体4(CXCR4)与糖尿病足溃疡(DFU)患者感染、病情程度及预后的相关性。方法回顾性选取2020年9月至2022年5月在北京市大兴区人民医院进行治疗的150例DFU患者作为观察对象。根据DFU严重程度进行分级:Wagner分级1级32例,2级39例,3级45例,4级34例。按照DFU感染严重程度分级,无感染23例,轻度感染42例,中度感染48例,重度感染37例。根据患者6个月内预后情况将患者分为预后良好组103例与预后不良组47例。收集患者临床资料[年龄、性别、合并疾病(高血压、糖尿病肾病、周围神经病变、糖尿病视网膜病变)感染程度、Wagner分级、白细胞计数、空腹血糖、糖化血红蛋白(HbA1c)、超敏C-反应蛋白(hs-CRP)、降钙素原及血脂水平],采用酶联免疫吸附试验检测血清SDF-1α、CXCR4水平,受试者工作特征(ROC)曲线分析血清SDF-1α、CXCR4对DFU患者预后不良的诊断价值,Logistics回归分析影响DFU患者预后不良的危险因素。结果DFU患者血清SDF-1α、CXCR4水平随着感染严重程度及Wagner分级升高而逐渐降低,差异均有统计学意义(P<0.05)。预后不良组与预后良好组年龄、性别、合并疾病患者比例及白细胞计数、空腹血糖、HbA1c、血脂水平之间比较,差异均无统计学意义(P>0.05);与预后良好组比较,预后不良组糖尿病病程,中、重度感染,Wagner分级3~4级患者比例及血清hs-CRP、降钙素原水平显著升高,SDF-1α、CXCR4水平显著降低,差异均有统计学意义(P<0.05)。糖尿病病程、Wagner分级、hs-CRP是影响DFU患者预后不良的独立危险因素(P<0.05),SDF-1α、CXCR4是影响DFU患者预后不良的保护因素(P<0.05)。血清SDF-1α、CXCR4联合诊断DFU患者预后不良的AUC为0.914(95%CI:0.858~0.954),敏感度为87.23%,特异度为84.47%,血清SDF-1α、CXCR4联合诊断DFU预后不良的AUC显著高于血清SDF-1α、CXCR4单独诊断(Z=2.081,P=0.037;Z=2.146,P=0.031)。结论DFU患者血清SDF-1α、CXCR4水平随感染及病情严重程度升高而降低,与患者预后有关,二者联合对DFU患者预后不良有一定诊断价值。

基于SDF-1/CXCR4信号通路中医药治疗骨类相关疾病研究进展

基质细胞衍生因子1(SDF-1)及其受体趋化因子受体-4(CXCR4)组成的生物轴与多种信号通路有着密切的联系,二者在人体多种细胞与组织中均有表达,且两者结合参与多种炎症和疾病的发生、发展过程,其具体作用在骨相关疾病的实验及临床研究中均得到证实。中医理论认为“肾主骨”,肾与骨的关系非常密切,肾脏亏虚,则骨失所养,筋失所依,进而诱发骨类疾病的发生。除此之外肝、脾二脏在骨类疾病的发生中也扮演着重要角色,肝脏亏虚,筋失所养,筋有束骨之功,骨弱则筋病,筋废则骨病;脾主肌肉,肌肉与骨骼协同发挥运动功能。中医药对于骨类疾病的治疗有着独特优势,可通过补肾、健脾、调肝等中医不同治法对骨类疾病进行治疗,从而达到一定效果。该文基于SDF-1/CXCR4信号通路对中医药治疗骨类相关疾病(骨质疏松症、骨性关节炎、骨折、椎间盘退变、强直性脊柱炎)的实验及临床研究进展进行综述。

五味子甲素对去卵巢骨质疏松大鼠SDF-1/CXCR4信号通路的影响

目的探究五味子甲素对去卵巢骨质疏松症大鼠的治疗作用以及对基质细胞衍生因子-1(SDF-1)/CXC趋化因子受体4(CXCR4)信号通路的影响。方法采用去卵巢法构建骨质疏松症大鼠模型,将建模成功的60只大鼠随机分为模型组、五味子甲素低(20 mg/kg)、高(40 mg/kg)剂量组、阿仑膦酸钠(1 mg/kg)组、五味子甲素高剂量+SDF-1/CXCR4通路抑制剂(AMD3100)(40 mg/kg+5 mg/kg)组,每组12只。另取12只大鼠作为假手术组(手术过程中仅暴露卵巢不切除)。建模结束后,各组给予对应药物干预,每天1次,连续12周。采用双能X射线骨密度仪检测大鼠左、右股骨骨密度(BMD);酶联免疫吸附法检测大鼠血清中Ⅰ型胶原交联羧基末端肽(CTX-Ⅰ)、骨钙素(OC)水平;HE染色观察大鼠股骨组织病理学变化;荧光定量PCR法检测大鼠股骨组织中SDF-1、CXCR4信使RNA(mRNA)水平;蛋白印迹法检测大鼠股骨组织中SDF-1、CXCR4蛋白水平。结果假手术组大鼠股骨组织骨小梁结构正常,排列规则;与假手术组相比,模型组大鼠股骨组织骨小梁稀疏断裂,数量减少,排列紊乱,左、右股骨BMD、血清中OC、CTX-Ⅰ水平、股骨组织中SDF-1、CXCR4 mRNA和蛋白水平显著降低(P<0.05);与模型组相比,五味子甲素低、高剂量组大鼠股骨组织病变程度依次减轻,左、右股骨BMD、血清中OC、CTX-Ⅰ水平、股骨组织中SDF-1、CXCR4 mRNA和蛋白水平依次升高(P<0.05);阿仑膦酸钠组和五味子甲素高剂量组大鼠股骨组织病理学变化及各项指标差异比较均无统计学意义(P>0.05);AMD3100可逆转高剂量五味子甲素对骨质疏松症大鼠上述指标的改善效果(P<0.05)。结论五味子甲素可抑制骨质疏松症大鼠BMD的下降,减轻大鼠股骨组织病变,改善大鼠骨质疏松,其机制可能与激活SDF-1/CXCR4信号通路有关。

AMD3100下调CA9与CXCR4表达逆转索拉菲尼耐药

目的 研究AMD3100通过调控碳酸酐酶Ⅸ(CA9)和趋化因子受体4(CXCR4)逆转人肝癌细胞对索拉菲尼的耐药性机制。方法 以人肝癌细胞Huh7和HepG2为研究对象,建立索拉菲尼耐药株Huh7/Sor和HepG2/Sor;检测索拉菲尼单独或联合使用AMD3100对Huh7、HepG2、Huh7/Sor、HepG2/Sor细胞增殖的影响;观察索拉菲尼耐药细胞与非耐药细胞侵袭能力的区别,AMD3100对肝癌细胞侵袭能力的影响;索拉菲尼单独或联合使用AMD3100对Huh7、HepG2、Huh7/Sor和HepG2/Sor细胞的CA9和CXCR4蛋白表达的调控作用。结果与对照组比较,AMD3100 (50μmol/L)可提高索拉菲尼对Huh7/Sor和HepG2/Sor细胞的增殖抑制作用(P <0.05);与Huh7细胞比较,索拉菲尼耐药株Huh7/Sor细胞的侵袭能力增强(P <0.05),AMD3100(50μmol/L)可降低Huh7和Huh7/Sor细胞的侵袭能力(P <0.05);与Huh7和HepG2细胞比较,Huh7/Sor和HepG2/Sor细胞的CA9和CXCR4蛋白表达增加(P <0.05),AMD3100(50μmol/L)可下调Huh7、HepG2、Huh7/Sor和HepG2/Sor细胞的CA9和CXCR4蛋白表达(P <0.05)。结论AMD3100可能通过下调CA9、CXCR4表达降低人肝癌细胞对索拉菲尼耐药性,增强索拉菲尼对人肝癌细胞的增殖和侵袭抑制。

CXCL12-CXCR4轴在慢性淋巴细胞白血病中的研究进展

慢性淋巴细胞白血病(chronic lymphocytic leukemia,CLL)是一种惰性恶性肿瘤,其特征在于成熟但功能失调的B淋巴细胞产生增加。趋化因子受体4(CXCR4)在CLL淋巴细胞上高表达且过与其相应的配体结合促进CLL细胞的动员、迁移、增殖和存活。据最近相关文献报道,趋化因子12-趋化因子受体4(CXCL12-CXCR4)轴通过激活多种信号通路及造血干细胞的迁移和归巢对骨髓中的生态环境进行调节,已成为CLL治疗靶点,尤其CXCR4靶向示踪剂临床上的研究非常活跃。但CXCR4在CLL中作用的相关文献较少。本文就CXCL12-CXCR4轴在CLL中的表达、作用机制、靶向治疗等方面的研究进展做一综述。

中重度宫腔粘连组织中SDF-1、CXCR4的表达

目的:探究中重度宫腔粘连(IUA)组织中基质细胞衍生因子-1(SDF-1)、趋化因子受体4(CXCR4)表达。方法:选取2019年4月-2022年4月本院确诊IUA中重度并行宫腔镜手术治疗的患者132例为IUA组,其中中度51例、重度81例;经宫腔镜确诊子宫纵隔患者132例为对照组,收集2组一般资料及性激素指标,免疫组化测定组织中SDF-1、CXCR4蛋白表达,Kaplan-Meier分析SDF-1、CXCR4表达与手术预后的关系;多因素Cox回归分析影响预后因素。结果:IUA组妊娠次数、分娩次数及妊娠相关宫腔手术次数均多于对照组,SDF-1阳性率(81.1%)高于对照组(25.0%),CXCR4阳性率(77.3%)高于对照组(20.5%),且重度IUA患者SDF-1阳性率(90.1%)、CXCR4阳性率(87.7%)高于中度IUA患者(66.7%、60.8%)(均P<0.05)。治疗无效者中SDF-1阳性表达患者占比(29.0%)高于阴性表达患者(12.0%),CXCR4阳性表达患者占比(31.4%)高于阴性表达患者(6.7%)(均P<0.001)。Cox回归分析,SDF-1、CXCR4是IUA患者预后的独立危险因素(P<0.05)。结论:IUA患者粘连组织中SDF-1、CXCR4阳性率提高,且与IUA患者病情严重程度及预后均有关。