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纸质出版日期:2005
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董晓辉, 董竞成. 黄芪注射液增强树突细胞的抗肺癌作用[J]. 中国实验方剂学杂志, 2005,11(1):25-28.
DONG Xiao-hui, DONG Jing-cheng. Effects of Dendritic-cells Combined with Astragalus on Lewis Lung Cancer[J]. Chinese journal of experimental traditional medical formulae, 2005, 11(1): 25-28.
目的:研究黄芪注射液联合MHC I类限制性肿瘤抗原多肽Mut1致敏的树突细胞(DCs)对肺癌小鼠的治疗作用及其免疫学原理。方法:制备小鼠骨髓来源的树突细胞
用转移性Lewis肺癌特异性多肽Mut1预激DCs并联合黄芪注射液治疗肺癌小鼠
通过FACS分析其脾细胞内T淋巴细胞比例的变化
用Elisa法检测荷瘤小鼠血清内IL-2、IL-4浓度的变化
间接提示Th1/Th2比例的变化。同时免疫正常小鼠
观察宿主对随后肿瘤细胞攻击的保护作用。结果:肿瘤抗原多肽致敏的DCs与黄芪注射液联合治疗后
比单用DCs更有效的治疗转移性肺癌
小鼠脾细胞内CD4+T和CD8+T细胞明显比例升高
联合治疗组的IL-2/IL-4比例也明显升高。在观察时间内经黄芪注射液和DCs联合免疫的小鼠成瘤率低于对照组和单用DCs组。结论:以肿瘤抗原多肽致敏的DCs与黄芪注射液联合治疗能更有效的促进荷瘤宿主的免疫应答
具有显著的体内抑制肺癌转移的效果。对正常动物免疫保护作用更加明显。
Objective:To invetigate the antitumor effects and mechanisms of tumor antigen peptide-pulsed dendritic cells combined with Astragalus.Methods:High purity DCs were obtained from 9-day culture of murine bone marrow cells.Mut1 is a MHC class I-restricted tumor antigen peptide of Lewis lung cancer.DCs were incubated with Mut1
then vaccines were established.Lung cancer were established on the mice.The tumor-bearing mice were treated and the survival period of the mice was observed.Treatment groups were divided into PBS
DC-Mut1
DC-Mut1 with Astragalus(DC-Mut1+AG).The phenotypes of splenocytes of these treated mice were detected by FACS.Interleukin-2 and interleukin-4 in the serum were measured by cytokine-specific ELISA.Normal mice developed a potent immune protection against the attack from tumor cells.The treatment groups were same as the previous groups.Results:The DC-Mut1+AG group demonstrated antitumor effects with the regression majority of tumors.The proportion of the CD4+T and CD8+T cells in DC-Mut1+AG group increased compared with that of DC-Mut1 group(P<0.05).The IL-2 level of DC-Mut1+AG group was higher than those of DC-Mut1 group.The IL-4 level of DC-Mut1+AG group was lower than that of the PBS group.Upon undergoing attack from LLC cells
DC-Mut1+AG group had no formation of tumors.In contrast
4 of all the mice(6) treated with DC-Mut1 developed tumors.Conclusion:DC-Mut1+AG could exert antitumor effects in the mice and significantly inhibit tumor metastasis
which demonstrated a specific immune protection.
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