微卫星不稳定型胃癌及微卫星稳定型胃癌的免疫分型及预后分析

目的探讨CD8、CD68、PD-1及PD-L1在微卫星稳定型(MSS)/不稳定型(MSI)胃癌中的表达水平及微卫星状态对胃癌的预后影响。方法收集空军军医大学第一附属医院消化病医院2012年3月至2012年8月连续的胃癌病例,记录其临床病理学资料及随访结果。采用免疫组织化学染色法检测60例胃癌石蜡切片中错配修复分子MLH1、MSH2、MSH6、PMS2,CD8、CD68、PD-1、PD-L1表达水平。采用Log-rank法分析不同组间的生存预后。结果 60例胃癌中MSI胃癌病例15例(25.0%)。MSS胃癌及MSI胃癌中CD8、PD-1及PD-L1表达无统计学差异,CD68在MSS胃癌中表达高于MSI胃癌(P=0.046)。MSI胃癌以Ⅱ型免疫分型(CD8-PD-L1-)为主,占46.67%,MSS胃癌以Ⅱ型和Ⅳ型(CD8+PD-L1-)为主,占33.33%和31.11%。MSI胃癌5年疾病无进展(P=0.036)及总体生存预后(P=0.041)优于MSS胃癌。结论 MSI胃癌组织微环境存在钝性免疫反应,但生存预后较好。

新生血管特异性结合肽GX1二聚体抑制大鼠视网膜微血管内皮细胞血管生成的实验研究

目的:探讨新生血管特异性结合肽GX1二聚体对视网膜新生血管生成的影响。方法:化学合成GX1二聚体、GX1单体、对照肽二聚体,通过CCK-8实验、管状结构形成实验、迁移实验研究GX1二聚体对大鼠视网膜内皮细胞(RMEC)增殖、微管形成、迁移能力的影响,流式细胞学技术分析其对细胞周期分布和凋亡的影响。结果:CCK-8结果显示,与对照肽二聚体及阴性对照组相比,100-200μM GX1二聚体及单体均可抑制RMEC增殖(P<0.05),且随着GX1二聚体及单体浓度升高,抑制作用逐渐增强,呈剂量依赖性;各浓度GX1二聚体均较单体抑制作用增强,并有统计学差异(P<0.05)。管状结构形成实验、细胞损伤迁移实验结果显示与对照肽二聚体及PBS组相比,GX1二聚体及GX1单体均可明显抑制视网膜内皮细胞管状结构的形成及迁移,且二聚体抑制作用强于单体;对照肽二聚体仅有轻微的抑制视网膜内皮细胞管状结构形成的作用,对细胞迁移无明显抑制作用。流式细胞术分析显示与对照肽及阴性对照组相比,GX1二聚体及GX1单体均可诱导细胞凋亡(P<0.05),且GX1二聚体的诱导作用强于GX1单体(P<0.05),而对细胞周期分布则无明显影响。结论:GX1二聚体和GX1单体均可抑制视网膜新生血管内皮细胞增殖、微管形成、迁移能力及诱导凋亡,且GX1二聚体较GX1单体作用增强。GX1二聚体有望代替单体成为糖尿病视网膜病变新生血管靶向治疗小肽类药物。

Screening of specific binding peptide targeting blood vessel of human esophageal cancer in vivo in mice

Background Cancer of the esophagus and gastroesophageal junction remains a virulent malignancy with poor prognosis. Rapid progresses were made in chemotherapeutic agents and the development of molecular markers allowed better identification of candidates for targeted therapy. This study aimed to identify the candidate peptides used for anti-angiogenic therapy of esophageal cancer by in vivo screening C7C peptide library for peptides binding specifically to blood vessels of human esophageal cancer.Methods The phage displayed C7C peptide library was injected intravenously into mice bearing human esophageal tumor xenografts under renal capsule. After 5 rounds of screening, 13 clones were picked up individually and sequenced.During each round of screening, titers of phage recovery were calculated from tumor xenograft and control tissues.Homing of these 9 peptides to tumor vessel was detected by calculating phage titers in the tumor xenograft and control tissues （lung and spleen） after each phage was injected into mice model, and compared with the distribution of phage M13 and Ⅷ-related antigen in tumor xenograft by immunohistochemical staining. Comparisons among groups of data were made using one-way analysis of variance （ANOVA）, followed by the Bonferroni multiple comparisons test.Results The number of phage recovered from tumor tissue of each round increased gradually in tumor group while decreased in control groups （P 〈0.01 in tumor and spleen, P 〈0.05 in lung）. Immunohistochemical staining showed similar staining pattern with M13 antibody or Ⅷ-related antigen antibody, suggesting that phages displaying the selected peptides could home to blood vessel of human esophageal cancer. According to their DNA, 9 corresponding peptide sequences were deduced. And the homing ability to blood vessel of phages displaying the selected peptides was confirmed by comparing with their recovery in tumor and control tissues. Two motifs, YSXNXW and PXNXXN, were also obtained by analyzing the homology of these peptide sequences. The staining distribution of phage with the sequence of PNPNNST was similar to that of the blood vessel marker factor Ⅷ-related antigen staining. After sequencing, each phage with the selected peptide of PNPNNST with 1.0×1011 pfu/ml was injected intravenously into mice. The homing ability to tumor vessel of these 9 kinds of peptides in the xenograft was higher than control tissues （lung and spleen）.Conclusion Nine peptides obtained from in vivo screening homed to the blood vessel of human esophageal cancer,and the two motifs of YSXNXW and PXNXXN are the possible biochemical recognition units binding to vascular endothelial cells of esophageal cancer.

克罗恩病患者用药变化10年回顾性分析

目的 总结空军军医大学西京医院消化内科克罗恩病(CD)患者10年的用药趋势变化。方法 回顾性分析2010—2019年10年间,西京医院IBD中心确诊CD患者的临床一般信息资料、患者用药情况,其中将CD患者根据用药时间段分为2010—2014年组与2015—2019年组,分别分析两组CD患者的一般情况和用药趋势,再根据患者性别和年龄(≤40岁和>40岁)进行亚组分析。结果 2015—2019年组与2010—2014年组分别纳入164和140例CD患者,2010—2014年组和2015—2019年组患者年龄和女性比例比较[(37.2±14.5)岁比(34.7±13.7)岁,30.0%(42/140)比40.9%(67/164)],差异均无统计学意义(P>0.05)。2015—2019年组免疫抑制剂和生物制剂使用率均高于2010—2014年组[50.6%(83/164)比32.1%(45/140)、52.4%(86/164)比23.6%(33/140)],差异均有统计学意义(χ^(2)=10.566、χ^(2)=26.421,P<0.001)。2010—2014年组和2015—2019年组组内女性和男性CD患者的年龄、5-ASA(5-氨基水杨酸)类、激素、免疫抑制剂和生物制剂的使用率比较,差异均无统计学意义(P>0.05)。2015—2019年组组内≥40岁患者生物制剂使用率明显低于<40岁组[34.0%(18/53)比61.3%(68/111)],差异具有统计学意义(P=0.001)。结论 与2010—2014年相比,2015—2019年间,西京医院单中心CD患者数量基本保持稳定,CD患者的生物制剂和免疫抑制剂使用率明显增高;不同性别患者的用药情况基本一致。2015—2019年间,生物制剂使用率增加主要表现为年轻患者(<40岁)使用率增加。