Influence of vascular endothelial growth factor and radiation on gap junctional intercellular communication in glioblastoma multiforme cell lines

Glioblastoma multiforme （GBM） is a highly aggressive glial brain tumor with an unfavorable prognosis despite all current therapies including surgery, radiation and chemotherapy. One characteristic of this tumor is a strong synthesis of vascular endothelial growth factor （VEGF）, an angiogenesis factor, followed by pronounced vascularization. VEGF became a target in the treatment of GBM, for example with bevacizumab or the tyrosine kinase inhibitor axitinib, which blocks VEGF receptors. To improve patients＇ prognosis, new targets in the treatment of GBM are under investigations. The role of gap junctions in GBM remains un- known, but some experimental therapies affect these intercellular channels to treat the tumor. Gap junctions are composed of connexins to allow the transport of small molecules between adjacent cells through gap junc- tional intercellular communication （GJIC）. Based on data derived from astrocytes in former studies, which show that VEGF is able to enhance GJIC, the current study analyzed the effects of VEGF, radiation therapy and VEGF receptor blockade by axitinib on GJIC in human GBM cell lines U-87 and U-251. While VEGF is able to induce GJIC in U-251 cells but not in U-87 cells, radiation enhances GJIC in both cell lines. VEGF reocptor blockade by axitinib diminishes radiation induced effects in U-251 partially, while increases GJIC in U-87 cells. Our data indicate that VEGF and radiation are both modifying components of GJ1C in pathologic brain tumor tissue.

Regulation Effect of Vascular Endothelial Growth Factor on Human Fetal Choroid Vascularization

Purpose:To investigate the spatial and temporal regulation effect of vascular endothelial growth factor(VEGF)on human fetal choroid vascularization.Methods:The eyeballs of 54human fetuses from the 9th week to the40th week due to accidental abortion were studied by immunohistochemically staining for the expression of VEGF and proliferation cell nuclear antigen(PCNA).Results:(1)The distribution of VEGF expression in the retinal pigment epithelium(RPE)decreased with the increase of age,the peak of which was between the 9th and 14th week,(2)PCNAimmunoreactivity was localized within choriocapillaris endothe-lium,THe expression level decreased alone with fetus age,In this period the chori-ocapillaris endothelium kept proliferation,differentiation.canalization and remodelled to form the choroid vessels.(3)Statistically significant correlations were shown between the expression of VEGF in the PRE and that of PCNAin choriocapillaris endothelium(r=0.933,P<0.01).Conclusion:VEGF expression in PRE was positively involved in modulating human fetal choroid vascularization.Eye Science2000;16:11-14.

Regulation effect of vascular endothelial growth factor on vascularization and angiogenesis in developmental human fetal retinas

目的 :研究血管内皮生长因子 ( Vascular endothelial growth factor VEGF)对人胚胎视网膜血管发生的调节作用。方法 :收集 54例 9～ 4 0周龄胎儿眼球后壁标本 ,免疫组织化学染色 ,光镜观察。结果 :1VEGF在视网膜的表达呈波峰式分布 ,高峰在 9～ 13周及 2 6周左右。 2节细胞层的梭形细胞(血管内皮细胞前体细胞 )、血管内皮细胞呈增殖细胞核抗原 ( Proliferation cell nucelear antigen,PCNA)免疫反应阳性 ,水平波动 ,高峰在 9～ 13周及 2 1周前后 ,此期间梭形细胞不断增殖、分化形成内皮细胞索 ,经改建形成视网膜内层血管 ,2 6、34周起见内核层内、外缘血管内皮细胞呈 PCNA免疫反应阳性 ,并保持至足月。 3视网膜 VEGF表达量与梭形细胞、血管内皮细胞 PCNA表达量呈显著正相关( r=0 .736,P<0 .0 1)。结论

红景天苷对血管生成及骨血管偶联的影响

目的探讨红景天苷对血管生成及骨血管偶联的影响。方法采用MTS法探究成骨细胞条件培养液对血管内皮细胞增殖活性的影响;采用Transwell小室迁移实验探究成骨细胞条件培养液对血管内皮细胞迁移数量的影响;Matrigel管腔形成实验探究成骨细胞条件培养液对管腔形成长度的影响;胎鼠跖骨血管生成实验用于研究红景天苷对内皮细胞出芽面积的影响。结果与条件培养液组比较,经红景天苷处理后的条件培养液组细胞活性明显升高,差异均具有统计学意义(P<0.01);红景天苷组的血管内皮细胞的迁移数量及HUVEC管腔形成长度与条件培养液组相比显著增加,差异有统计学意义(P<0.01);红景天苷和血管内皮生长因子(VEGF)处理组的内皮细胞出芽面积均明显大于对照组,差异有统计学意义(P<0.01),且上述作用均能被抗VEGF抗体Avastin阻断。结论红景天苷是一种较好的促血管生成药物单体,且可通过上调VEGF的表达水平促进骨血管偶联。

Electro-acupuncture at Conception and Governor vessels and transplantation of umbilical cord bloodderived mesenchymal stem cells for treating cerebral ischemia/reperfusion injury

Mesenchymal stem cell transplantation is a novel means of treating cerebral ischemia/reper- fusion, and can promote angiogenesis and neurological functional recovery. Acupuncture at Conception and Governor vessels also has positive effects as a treatment for cerebral ischemia/ reperfusion. Therefore, we hypothesized that electro-acupuncture at Conception and Governor vessels plus mesenchymal stem cell transplantation may have better therapeutic effects on the promotion of angiogenesis and recovery of neurological function than either treatment alone. In the present study, human umbilical cord blood-derived mesenchymal stem cells were isolated, cultured, identified and intracranially transplanted into the striatum and subcortex of rats at 24 hours following cerebral ischemia/reperfusion. Subsequently, rats were electro-acupunctured at Conception and Governor vessels at 24 hours after transplantation. Modified neurological severity scores and immunohistochemistry findings revealed that the combined interventions of electro-acupuncture and mesenchymal stem cell transplantation clearly improved neurological impairment and up-regulated vascular endothelial growth factor expression around the isch- emic focus. The combined intervention provided a better outcome than mesenchymal stem cell transplantation alone. These findings demonstrate that electro-acupuncture at Conception and Governor vessels and mesenchymal stem cell transplantation have synergetic effects on promot- ing neurological function recovery and angiogenesis in rats after cerebral ischemia/reperfusion.

Revisiting tumor angiogenesis:vessel co-option,vessel remodeling,and cancer cell-derived vasculature formation

Tumor growth and metastasis depend on the establishment of tumor vasculature to provide oxygen,nutrients,and other essential factors.The well-known vascular endothelial growth factor(VEGF) signaling is crucial for sprouting angiogenesis as well as recruitment of circulating progenitor endothelial cells to tumor vasculature,which has become therapeutic targets in clinical practice.However,the survival benefits gained from targeting VEGF signaling have been very limited,with the inevitable development of treatment resistance.In this article,we discuss the most recent findings and understanding on how solid tumors evade VEGF-targeted therapy,with a special focus on vessel co-option,vessel remodeling,and tumor cell-derived vasculature establishment.Vessel co-option may occur in tumors independently of sprouting angiogenesis,and sprouting angiogenesis is not always required for tumor growth.The differences between vessel-like structure and tubule-like structure formed by tumor cells are also introduced.The exploration of the underlying mechanisms of these alternative angiogenic approaches would not only widen our knowledge of tumor angiogenesis but also provide novel therapeutic targets for better controlling cancer growth and metastasis.

Microvessel density is a prognostic marker of human gastric cancer

AIM: To investigate whether microvessel density (MVD) is related with prognosis in gastric cancer patients, and the expression of cyclooxygenase-2 (COX-2) and vessel endothelial growth factor (VEGF) so as to determine the possible role of COX-2 and VEGF in gastric cancer angiogenesis.METHODS: Forty-seven formalin-fixed paraffin-embedded tissue samples of gastric cancer were evaluated for COX-2, VEGF by immunohitochemical staining. To assess tumor angiogenesis, MVD was determined by immunohitochemical staining of endothelial protein factor Ⅷ-related antigen. The relationship among COX-2 and VEGF expression, MVD, and clinicopathologic parameters was analyzed. RESULTS: Among the 67 samples, high MVD was significantly associated with lymph node metastasis and poor survival. Multivariate survival analysis showed that MVD value and lymph node metastasis were independent prognostic factors. The expression rate of COX-2 and VEGF was significantly higher than that of the adjacent tissues. COX-2 and VEGF expression in gastric cancer was significantly correlated with tumor differentiation and depth of invasion, but not with survival. The mean MVD value of COX-2 or VEGF positive tumors was higher than that of COX-2 or VEGF negative tumors. A significant correlation was found between the expressions of COX-2and VEGF. CONCLUSION: MVD may be one of the important prognostic factors for gastric cancer patients. COX-2 and VEGF may play an important role in tumor progression by stimulating angiogenesis. VEGF might play a main role in the COX-2 angiogenic pathway. The inhibition of angiogenesis or COX-2, VEGF activity may have an important therapeutic benefit in the control of gastric cancer.

微RNA-140-5p靶向调节血管内皮生长因子表达对高糖诱导的人视网膜血管内皮细胞增殖、迁移和管腔形成的影响

目的 探讨微RNA(miR)-140-5p靶向调节血管内皮生长因子(VEGF)表达对高糖诱导的人视网膜血管内皮细胞(hRECs)增殖、迁移和管腔形成的影响。方法 将对数生长期hRECs细胞分为正常对照组、高糖组、miR-140-5p组、阴性对照(NC)组、高糖+miR-140-5p组。正常对照组和高糖组细胞不做任何转染,miR-140-5p组和高糖+miR-140-5p组细胞转染miR-140-5p模拟物(miR-140-5p mimics),NC组细胞转染阴性对照模拟物(mimics NC)。高糖组和高糖+miR-140-5p组细胞用含30 mmol·L^(-1)葡萄糖的培养基制备高糖模型。应用实时荧光定量聚合酶链式反应法检测各组细胞中miR-140-5p表达水平,噻唑蓝法检测各组细胞增殖能力,Transwell法检测各组细胞迁移能力,管腔形成实验检测各组细胞成管能力,Western blot法检测各组细胞中VEGF蛋白的表达。将40只Sprague Dawley大鼠随机分成正常对照组、糖尿病模型组、糖尿病+NC组、糖尿病+miR-140-5p组,每组10只。除正常对照组外,其余各组大鼠腹腔注射65 mg·kg^(-1)链脲佐菌素制备糖尿病模型,正常对照组和糖尿病模型组大鼠尾静脉注射200μL生理盐水,糖尿病+miR-140-5p组大鼠尾静脉注射200μL miR-140-5p,糖尿病+NC组大鼠尾静脉注射200μL mimics NC,每日1次,持续给药7 d;再继续饲养8周,大鼠麻醉后,取视网膜,苏木精-伊红染色观察miR-140-5p对糖尿病模型大鼠视网膜血管生成的影响。结果 高糖组、高糖+miR-140-5p组细胞中miR-140-5p相对表达量显著低于正常对照组,miR-140-5p组细胞中miR-140-5p相对表达量显著高于正常对照组(P<0.01);NC组与正常对照组细胞中miR-140-5p相对表达量比较差异无统计学意义(P>0.05)。miR-140-5p组、NC组、高糖+miR-140-5p组细胞中miR-140-5p相对表达量显著高于高糖组(P<0.01)。NC组、高糖+miR-140-5p组细胞中miR-140-5p相对表达量显著低于miR-140-5p组(P<0.01)。高糖+miR-140-5p组细胞中miR-140-5p相对表达量显著低于NC组(P<0.05)。培养24、48、72 h时,高糖组细胞增殖率均显著高于正常对照组(P<0.01),miR-140-5p组、NC组与正常对照组细胞增殖率比较差异均无统计学意义(P>0.05)。培养24 h时,高糖+miR-140-5p组与正常对照组细胞增殖率比较差异无统计学意义(P>0.05);培养48、72 h时,高糖+miR-140-5p组细胞增殖率显著高于正常对照组(P<0.01)。培养24、48、72 h时,miR-140-5p组、NC组、高糖+miR-140-5p组细胞增殖率均显著低于高糖组(P<0.05)。培养24、48、72 h时,NC组与miR-140-5p组细胞增殖率比较差异均无统计学意义(P>0.05)。培养24 h时,高糖+miR-140-5p组细胞增殖率与miR-140-5p组、NC组比较差异无统计学意义(P>0.05);培养48、72 h时,高糖+miR-140-5p组细胞增殖率显著高于miR-140-5p组和NC组(P<0.01)。高糖组迁移细胞数显著高于正常对照组,miR-140-5p组、NC组迁移细胞数显著低于正常对照组(P<0.01)。高糖+miR-140-5p组与正常对照组迁移细胞数比较差异无统计学意义(P>0.05)。miR-140-5p组、NC组、高糖+miR-140-5p组迁移细胞数显著低于高糖组(P<0.01)。NC组、高糖+miR-140-5p组迁移细胞数均显著高于miR-140-5p组(P<0.01)。高糖+miR-140-5p组迁移细胞数显著高于NC组(P<0.01)。高糖组管腔形成数量显著高于正常对照组,miR-140-5p组、NC组细胞管腔形成数量显著低于正常对照组(P<0.01);高糖+miR-140-5p组与正常对照组细胞管腔形成数量比较差异无统计学意义(P>0.05)。miR-140-5p组、NC组、高糖+miR-140-5p组细胞管腔形成数量均显著低于高糖组(P<0.01)。NC组、高糖+miR-140-5p组细胞管腔形成数量均显著高于miR-140-5p组(P<0.05)。高糖+miR-140-5p组细胞管腔形成数量显著高于NC组(P<0.05)。高糖组、高糖+miR-140-5p组细胞中VEGF蛋白相对表达量显著高于正常对照组,miR-140-5p组细胞中VEGF蛋白相对表达量显著低于正常对照组(P<0.05);NC组与正常对照组细胞中VEGF蛋白相对表达量比较差异无统计学意义(P>0.05)。miR-140-5p组、NC组、高糖+miR-140-5p组细胞中VEGF蛋白相对表达量显著低于高糖组(P<0.01)。NC组、高糖+miR-140-5p组细胞中VEGF蛋白相对表达量显著高于miR-140-5p组(P<0.01)。高糖+miR-140-5p组细胞中VEGF蛋白相对表达量显著高于NC组(P<0.05)。正常对照组大鼠靠近视乳头处的视网膜血管整体呈“树状结构”,内极部毛细血管分布较致密,外极部毛细血管分布较疏松,血管壁均匀。糖尿病模型组大鼠视网膜血管的“树状结构”被破坏,毛细血管分布不均匀,毛细血管瘤形成。糖尿病+NC组大鼠视网膜血管损伤与糖尿病模型组相当。糖尿病+miR-140-5p组大鼠视网膜血管的损伤情况有所好转,毛细血管瘤减少。结论 miR-140-5p可以抑制hRECs在高糖条件下的增殖、迁移及成管能力,缓解糖尿病大鼠视网膜血管病变,其作用可能是通过miR-140-5p靶向调控VEGF的表达而实现。

The lymphatic system:a therapeutic target for central nervous system disorders

The lymphatic vasculature forms an organized network that covers the whole body and is involved in fluid homeostasis,metabolite clearance,and immune surveillance.The recent identification of functional lymphatic vessels in the meninges of the brain and the spinal cord has provided novel insights into neurophysiology.They emerge as major pathways for fluid exchange.The abundance of immune cells in lymphatic vessels and meninges also suggests that lymphatic vessels are actively involved in neuroimmunity.The lymphatic system,through its role in the clearance of neurotoxic proteins,autoimmune cell infiltration,and the transmission of pro-inflammatory signals,participates in the pathogenesis of a variety of neurological disorders,including neurodegenerative and neuroinflammatory diseases and traumatic injury.Vascular endothelial growth factor C is the master regulator of lymphangiogenesis,a process that is critical for the maintenance of central nervous system homeostasis.In this review,we summarize current knowledge and recent advances relating to the anatomical features and immunological functions of the lymphatic system of the central nervous system and highlight its potential as a therapeutic target for neurological disorders and central nervous system repair.

钙敏感受体在高血压大鼠心肌重塑和视网膜血管病变中的作用研究

背景临床中对于高血压靶器官损害主要以全身降压辅以局部用药治疗为主,但因各组织对药物的反应不同甚至相斥,治疗效果不佳。现已关注到钙敏感受体(CaSR)与高血压的关系,然而其在高血压视网膜疾病中的作用和机制仍缺乏相关研究。目的探讨CaSR在高血压视网膜中的表达水平以及其与高血压心肌重塑、视网膜血管改变的关系。方法2021年5—12月选取10只8周龄健康正常血压大鼠(WKY)作为WKY组,20只同周龄同源的自发性高血压大鼠(SHR)随机分为SHR组及抑制剂(SHR+NPS2143)组。SHR+NPS2143组腹腔注射CaSR抑制剂NPS2143,WKY组和SHR组注射等量的0.9%氯化钠溶液,共注射16周。干预0周、16周通过无创血压仪监测大鼠血压;干预0周、16周分别选取5只大鼠处死,通过马松(Masson)染色观察大鼠心肌胶原沉积,通过苏木素-伊红(HE)染色检测视网膜病理变化;通过免疫组织化学染色、实时荧光定量PCR(qRT-PCR)观察CaSR和血管内皮生长因子A(VEGFA)在视网膜的分布和表达。结果SHR组干预0周、16周收缩压(SBP)、舒张压(DBP)、平均动脉压(MAP)高于WKY组(P<0.05);SHR组干预16周SBP、DBP、MAP均低于SHR+NPS2143组(P<0.05);SHR组、SHR+NPS2143组干预16周SBP、DBP、MAP均高于干预0周(P<0.05)。SHR组干预16周心脏/体质量(HW/BW%)和左心室/体质量(LVW/BW%)、心肌组织胶原容积分数(CVF)高于WKY组,低于SHR+NPS2143组(P<0.05);SHR组、SHR+NPS2143组干预16周HW/BW%、LVW/BW%、CVF高于干预0周(P<0.05)。SHR组干预0周、16周视网膜总厚度、内丛状层厚度高于WKY组(P<0.05);SHR组干预16周视网膜总厚度、内丛状层厚度低于SHR+NPS2143组(P<0.05);SHR组干预16周视网膜内核层厚度高于WKY组、低于SHR+NPS2143组(P<0.05)。干预16周SHR组视网膜中CaSR低于WKY组、高于SHR+NPS2143组(P<0.05);SHR组视网膜中VEGFA高于WKY组、低于SHR+NPS2143组(P<0.05)。结论应用CaSR抑制剂,可减少CaSR活化,促进视网膜中VEGFA表达增加,加剧高血压引起的心肌重塑与视网膜血管病变的发展。

促心脏淋巴管生成与基于抗心肌纤维化治疗心血管疾病研究进展

淋巴管是一种低压、盲端管状结构,在维持组织液体稳态、免疫细胞运输以及膳食脂质摄取和运输中发挥着重要作用,并参与免疫反应。淋巴管生成的抑制参与了缺血性损伤或压力超负荷后的心脏水肿和心脏重构。新的研究表明,促进淋巴管的生长、重塑和功能发挥可以在一些病理生理条件下减少炎症和减轻疾病严重程度。因此,促进淋巴管生成在心血管疾病中可能成为一种很有前途的治疗方法。当淋巴管重塑不足或适应不良时,它会导致淋巴运输功能障碍,导致慢性间质水肿和炎症,从而触发间质纤维化的发展。本文主要综述了心脏淋巴管在心血管疾病中的作用,介绍了心脏淋巴转运不良与心肌纤维化的相关性以及淋巴管生成在心血管疾病中的潜在益处。以期为心血管疾病的诊治提供新的思路和靶点。

益气活血生肌方对难愈性创面愈合及血管再生的影响

目的探讨益气活血生肌方对糖尿病大鼠溃疡创面愈合及血管再生的影响。方法按照随机数字表法将60只SPF级体重281~320 g,8~10周龄的雄性SD大鼠分成给药组、难愈性创面组、正常创面组、四君子汤组,每组15只。其中,给药组、难愈性创面组及四君子汤组采用链脲佐菌素法制作成糖尿病模型,48 h后空腹血糖>16.7 mmol/L,出现多尿、多饮等情况,提示造模成功。所有大鼠均于背部制作皮肤缺损创面,给药组及四君子汤组分别用3 ml益气活血生肌方及四君子汤灌胃,其他组用3 ml双蒸水灌胃,早晚各一次。于术后的第5、10、20天每组随机取5只大鼠,测量创面大小,计算创面愈合率;采用苏木精-伊红染色观察并计算溃疡创面毛细血管的数量,采用酶联免疫吸附试验法检测大鼠血液中血管内皮生长因子(VEGF)的含量,采用Western blot法检测创面局部组织VEGF、转化生长因子-β1(TGF-β1)和Smad 3的含量。结果术后第20天各组创面愈合率、血清VEGF表达水平、创面局部组织VEGF蛋白表达水平高于术后第5、10天,术后第10天各组创面愈合率、血清VEGF表达水平、创面局部组织VEGF蛋白表达水平高于本组术后第5天(P<0.05)。术后第20天给药组和正常创面组TGF-β1和Smad3蛋白表达水平低于术后第5、10天,术后第10天给药组和正常创面组TGF-β1和Smad3蛋白表达水平低于术后第5天(P<0.05),术后第20天难愈性创面组TGF-β1蛋白表达水平低于术后第5、10天(P<0.05)。术后第10、20天难愈性创面组Smad3蛋白表达水平高于术后第5天(P<0.05)。术后第5天,难愈性创面组创面愈合率低于正常创面组(P<0.05)。术后第10、20天,难愈性创面组创面愈合率低于正常创面组,给药组创面愈合率高于难愈性创面组(P<0.05)。术后各时间点难愈性创面组血清VEGF表达水平、创面局部组织VEGF蛋白表达水平低于正常创面组,给药组血清VEGF表达水平、创面局部组织VEGF蛋白表达水平高于难愈性创面组(P<0.05)。术后第5、10天,难愈性创面组TGF-β1和Smad3蛋白表达水平低于正常创面组,给药组TGF-β1和Smad3蛋白表达水平高于难愈性创面组(P<0.05);术后第20天,难愈性创面组TGF-β1和Smad3蛋白表达水平高于正常创面组,给药组TGF-β1和Smad3蛋白表达水平低于难愈性创面组(P<0.05)。病理学观察发现给药组炎症细胞浸润及组织坏死较难愈性创面组轻,毛细血管生成明显。结论益气活血生肌方能促进糖尿病大鼠VEGF的分泌,调节TGF-β1、Smad3蛋白的表达量,促进新生血管生成,进而促进难愈性创面愈合。

胰岛素样生长因子1在脑小血管病诊治中研究进展

脑小血管病作为老年人认知障碍发生的最重要血管因素,同时与老年人的步态、情绪障碍密切相关。由于脑小血管病的发病机制尚不明确,缺乏特异性治疗手段。胰岛素样生长因子1参与胚胎发育和神经发生,在正常生长发育中发挥重要作用。在脑小血管病发生发展过程中,目前研究提示IGF-1通过改善内皮功能、保护血脑屏障完整性、调节神经血管单元功能、改善脑白质病变和减轻神经炎症等发挥保护作用。本文通过复习文献,总结IGF-1在脑小血管病发生发展中的研究现状,提出进一步在脑小血管病中开展IGF-1相关研究的重要意义,并为脑小血管病的诊治提供新的探索方向。

口腔癌VEGF-C mRNA表达和血管及淋巴管生成与淋巴道转移关系的研究

背景与目的:VEGF-C与癌周的淋巴管血管生成以及肿瘤的淋巴道转移可能有密切的关系,本研究探讨口腔鳞癌组织血管、淋巴管密度与VEGF-CmRNA表达及淋巴道转移的关系。方法:VEGF-C逆转录PCR(RT-PCR),血管、淋巴管酶组化染色、光镜及图像分析观察血管、淋巴管总体面数密度(TNa)。结果:VEGF-CmRNA表达阳性的淋巴管TNa(26.42±5.85)明显高于阴性淋巴管TNa(17.34±6.48)(P<0.01);VEGF-CmRNA表达阳性的血管TNa(35.16±15.55)略高于阴性的血管TNa(33.49±13.73)(P>0.05)。淋巴结转移组血管TNa(44.19±14.29)比无淋巴结转移组TNa(30.61±11.82)增加(P<0.01)、淋巴结转移组淋巴管TNa(30.67±5.76)比无淋巴结转移组TNa(21.94±5.84)增加(P<0.01)。结论:VEGF-C主要介导了癌周淋巴管生成,对血管生成有一定影响;血管、淋巴管密度的同时增加可能与VEGF、VEGF-C及其受体的协同表达有一定关系。

双龙丸对大鼠实验性心肌梗死血管新生的影响与分子学机制

目的探讨双龙丸对缺血心肌血管新生的影响和分子学机制。方法 63只Wistar大鼠参照Drexler法结扎冠状动脉左前降支 ,制成急性心肌梗死 (AMI)模型。随机分为双龙丸大剂量组 (6 72 g/kg)、双龙丸小剂量组 (3 36g/kg)、AMI对照组 (生理盐水灌胃 ) ,另取 11只大鼠为正常对照组 (生理盐水灌胃 ) ,各组治疗观察半数至 2w、半数至 4w结束。应用免疫组化两步法检测AMI大鼠缺血心肌新生血管数量、免疫组化SP法检测缺血心肌血管内皮生长因子 (VEGF)和碱性成纤维细胞生长因子 (bFGF)的表达、逆转录多聚酶链反应 (RT PCR)法检测缺血心肌VEGFmRNA和bFGFmRNA的表达。结果双龙丸大、小剂量组各期的缺血心肌新生血管数均比AMI对照组增多 ,且第 4w比第 2w更显著 ;第 2w时 ,大剂量组VEGF较AMI对照组、bFGF较小剂量组和AMI对照组均增高 ,大剂量组 4w时VEGF较 2w降低 ;大、小剂量组各期VEGFmRNA的表达均比AMI对照组增高 ,其第 4w均较第 2w为低 ;而bFGFmRNA的表达则仅见大剂量组第 2w时高于其他组 ;以上各组比较均具有显著性差异 (P <0 0 5— 0 0 1)。结论双龙丸能够促进缺血心肌血管新生 ;大剂量应用对VEGF。

电针预处理对脑缺血再灌注大鼠骨髓和血浆中EPCs及VEGF的影响

目的:观察电针预处理对脑缺血再灌注损伤大鼠骨髓和外周血中内皮祖细胞(EPCs)、血管内皮生长因子(VEGF)的影响,研究电针预处理减轻脑缺血再灌注损伤机制。方法:将大鼠用抽签法随机分组,分为治疗组、模型组、假手术组和正常对照组。将大鼠造模脑缺血再灌注后,在第12,24,48小时分别将各组大鼠留取标本,用流式细胞仪检测其骨髓和外周血中EPCs的百分比变化。用ELISA法检测骨髓和血清中VEGF的浓度。结果:脑缺血再灌注损伤的大鼠较正常大鼠的骨髓和外周血中EPCs和VEGF的含量增加。电针预处理过的脑缺血再灌注损伤大鼠较未经过预处理的大鼠的骨髓和外周血中EPCs和VEGF的含量增加;随着电针预处理后时间的延长,EPCs和VEGF的含量增加越多。结论:电针预处理可以通过提高脑缺血再灌注损伤大鼠骨髓和外周血中VEGF的浓度,VEGF作用于EPCs的表面受体VEGFR2,从而加速EPCs的动员和迁移入血。

口腔鳞状细胞癌中血管内皮生长因子-C的表达及其与血管、淋巴管生成、淋巴结转移的关系

目的探讨血管内皮生长因子-C(VEGF-C)在口腔鳞状细胞癌(OSCC)组织中的表达情况及其与血管、淋巴管生成、淋巴结转移之间的关系。方法调查拥有完整临床病理资料的67例口腔鳞癌患者的手术切除标本,采用SP免疫组化技术检测VEGF-C的表达情况并分析其与微血管密度(MVD)、淋巴管密度(LVD)及其他临床病理指标的关系。结果晚期病例、淋巴结转移阳性病例的VEGF-C表达明显升高(P值分别为0.015和<0.001),而VEGF-C表达与患者性别、肿瘤部位、肿瘤分化程度无关(P>0.05)。VEGF-C高表达组的LVD明显高于VEGF-C低表达组(P=0.001),但两组间MVD无统计学差异(P=0.125)。此外,淋巴结转移阳性组的LVD明显高于淋巴结转移阴性组(P=0.026)。结论 VEGF-C可能主要通过参与诱导口腔鳞癌淋巴管生成促进淋巴结转移。

大肠癌中VEGF-D、VEGFR-3表达及淋巴管生成关系的研究

目的探讨大肠癌中VEGF-D、VEGFR-3的表达、D2-40阳性淋巴管特点以及淋巴管生成,分析与其临床生物学行为及预后的关系。方法免疫组织化学法检测148例大肠癌VEGF-D、VEGFR-3表达及淋巴管密度(LVD)。结果大肠癌中VEGF-D、VEGFR-3在淋巴结转移组阳性率(79%、52%)高于无淋巴结转移组(61%、34%),复发转移组阳性率(82%、52%)高于无复发转移组(59%、34%),生存期≤3年组阳性率(81%、62%)高于生存期>3年组(59%、35%)(均P<0.05);VEGF-D在淋巴管受累组阳性率(85%)高于无淋巴管受累组(60%)(P<0.05);LVD值在溃疡型和浸润型组中高于肿块型组,Dukes'C、D期高于DukesA、B期,淋巴结转移组高于无淋巴结转移组,淋巴管受累组高于无淋巴管受累组,复发转移组高于无复发转移组,生存期≤3年组高于生存期>3年组(均P<0.05)。结论大肠癌中VEGF-D、VEGFR-3表达升高与促进淋巴管生成和淋巴结转移、复发转移和预后不良有关。

靶向VEGFR-3载阿霉素脂质微泡超声造影剂体外显影及寻靶能力的实验研究

目的:制备一种靶向淋巴管内皮细胞载阿霉素脂质微泡超声造影剂,并考察其体外显影及寻靶能力。方法:制备生物素化抗VEGFR-3单克隆抗体,检测其生物素化程度;用机械振荡法,及生物素-亲和素桥连方式构建靶向VEGFR-3载阿霉素的脂质超声微泡。检测其一般特性;行体外超声,观察其显影效果;并在荧光下观察靶向载药微泡在体外与细胞的结合能力,与载药非靶向微泡做比较。结果:每个单抗分子平均可与9个生物素分子结合,所制备的载药靶向脂质微泡超声造影剂分散度佳,其平均粒径为1.66μm;体外超声显影,载药靶向脂质微泡呈高回声,回声强度随浓度及机械指数减小而降低;体外寻靶试验显示,该靶向载药脂质微泡较多并牢固的聚集在淋巴管内皮细胞表面。结论:成功制备的靶向VEGFR-3载阿霉素脂质微泡超声造影剂,有较高的包封率及载药率,其在体外有增强超声显影效果,并对淋巴管内皮细胞亲和力有较强的特异性。

GM-CSF对诱导人血管内皮细胞血管形成的影响及VEGF的作用

目的:研究炎性因子粒细胞-巨噬细胞集落刺激因子(GM-CSF)对诱导人血管内皮细胞血管形成的影响及血管内皮生长因子(VEGF)的作用,为探讨GM-CSF和VEGF与动脉粥样硬化斑块内血管新生及斑块稳定性之间的关系提供实验基础。方法:在Matrigel上诱导人脐带静脉内皮细胞(HUVECs)形成管腔结构,从而建立稳定的血管形成的体外培养体系,然后施加实验因素。分别检测rhGM-CSF的浓度效应和时间效应,及加入VEGF165的作用。然后各实验组用CD34免疫细胞化学染色,光学显微镜下计数各组管腔数。最后用统计学方法进行分析。结果:应用Matrigel可在体外诱导培养的HUVECs形成管腔结构。rhGM-CSF作用后,培养体系的管腔数逐渐增多,呈剂量及时间依赖效应;加入VEGF165后,管腔数显著增多。结论:应用Matrigel可在体外诱导培养的HUVECs形成管腔结构。GM-CSF可以促进体外诱导人血管内皮细胞血管形成,并在一定范围内呈剂量及时间依赖效应。VEGF可以促进体外诱导人血管内皮细胞血管形成。