蜕膜CXCR6^(+/-)单核-巨噬细胞在人早孕期母胎界面的表型差异

目的分析正常早孕期和不明原因自然流产妇女蜕膜组织中CXCR6^+单核-巨噬细胞比例及表型差异。方法收集上海复旦大学附属妇产科医院门诊手术室正常早孕期(40例)和不明原因自然流产(20例)妇女的蜕膜组织,分离蜕膜免疫细胞群,采用流式细胞术分析正常早孕组及不明原因自然流产组蜕膜免疫细胞中单核-巨噬细胞所占比例的差异;比较两组妇女蜕膜单核-巨噬细胞(dMΦ)表面CXCR6^+、CD80、CD206的表达差异。结果不明原因自然流产组CD14+dMΦ在蜕膜免疫细胞群(DIC)中所占比例为(9.9±1.63)%,正常早孕期组CD14+dMΦ在DIC中所占比例为(8.9±0.88)%,两组差异并无显著性(P>0.05);正常早孕组CXCR6^+在dMΦ的表达率为(40.0±1.90)%,而不明原因自然流产组表达率为(31.22±2.38)%,二者比较有显著差异(P<0.05);正常早孕组CD206、CD80在CXCR6^+dMΦ中的表达均显著高于CXCR6^-dMΦ(P<0.05),不明原因自然流产组CD206在CXCR6^+dMΦ的表达显著高于CXCR6^-dMΦ(P<0.01),CD80并无显著变化(P>0.05);与正常早孕组相比,不明原因自然流产组CD206在CXCR6^(+/-)dMΦ中的表达均显著降低(P<0.05),CD80在CXCR6^-dMΦ中表达则显著升高(P<0.05),在CXCR6^+dMΦ中的表达无显著差异(P>0.05)。结论不明原因自然流产妇女中,蜕膜单核巨噬细胞数量并无显著的变化,CXCR6^+dMΦ、表面分子CD206的表达明显降低及CD80的表达明显升高,提示CXCR6^+dMΦ可能参与了自然流产的发病机制。

Study of targeted and controlled release of 5-fluorouracil-loaded PLA nanoparticles and microspheres on treatment of gastric tumor

The aim of this paper was to evaluate controlled release behavior and the therapeutic efficacy of 5-FU-loaded Poly(lactic acid) (PLA)microspheres to human gastric cancer xenograft, and the targeting effect of VEGF/5-FU loaded PLA nanoparticles. 5-FU-loaded PLA microspheres were prepared by an emulsion evaporation method, and were characterized by scanning electron microscopy (SEM). 5-FU loaded PLA nanoparticles were characterized by (TEM), and particle size analyzer determined the distribution of nanoparticles size. The release performances of 5-FU microspheres in vitro were studied in PH 7.4 phosphate buffered saline. The therapeutic efficacy of 5-FU-loaded PLA microspheres in vivo were studied using MGC-803 (human stomach cancer) xenograft. 32 nude mice were divided into four groups (n =8), 5-FU loaded PLA microspheres were injected at tumor site. VEGF121 monoclonal antibody was connected with 5-FU loaded PLA nanoparticles through carbodimide. The targeted effect of VEGF 5-FU loaded nanoparticles in vivo were observed by single photon emission computed tomography (SPECT) after tail vein injection at 1 h and 2 h. SEM observation showed that microspheres were spherical, and the diameters of two kinds of microspheres were 1 μm and 5 μm respectively. The mean diameter of nanoparticles was 191.0 nm, and the index of polydispersity was 0.202. The drug was released following biphasic kinetics, initial burst and the following steady phase. 1 μm and 5 μm 5-FU-loaded microspheres both resulted in increased life span (1 μm microspheres median survival time=40.63 days, 5 μm microspheres median survival time=62.25 days), against 5-FU pure drug (median survival time=14.5 days). These results strongly suggest that 5-FU-loaded PLA microspheres increase life span of nude mice bearing MGC-803 tumors. After injection for 2 h, almost all the VEGF/5-FU loaded PLA nanoparticles could centralize at the human gastric cancer xenograft sites. That demonstrated VEGF monoclonal antibody remain its bioactivity after connection with nanoparticles, VEGF/5-FU loaded PLA nanoparticles had very exact targeting function for gastric tumor xenograft.