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首页> 外文期刊>Oncology reports >Recombinant Salmonella-based CEACAM6 and 4-1BBL vaccine enhances T-cell immunity and inhibits the development of colorectal cancer in rats: In vivo effects of vaccine containing 4-1BBL and CEACAM6
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Recombinant Salmonella-based CEACAM6 and 4-1BBL vaccine enhances T-cell immunity and inhibits the development of colorectal cancer in rats: In vivo effects of vaccine containing 4-1BBL and CEACAM6

机译:基于沙门氏菌的重组CEACAM6和4-1BBL疫苗增强大鼠T细胞免疫力并抑制大肠癌的发展:含有4-1BBL和CEACAM6的疫苗的体内作用

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The present study aimed to determine the effect of recombinant Salmonella (SL3261)-based CEACAM6 and 4-1BB ligand (4-1BBL) vaccine on the development of colorectal cancer in rats and the potential immune mechanisms involved. Attenuated Salmonella typhimurium (vaccine strain)-carrying plasmids pIRES-CEACAM6, pIRES-4-1BBL and pIRES-CEACAM6-4-1BBL were constructed. The rats were administered subcutaneous injections of 1,2-dimethyl-hydrazine (DMH) once a week for 18 weeks. Eight weeks after the first injection, the rats were divided into the pIRES/SL3261, pIRES-4-1BBL/SL3261, pIRES-CEACAM6/SL3261 and pIRES-CEACAM6-4-1BBL/SL3261 groups, and fed with corresponding vaccine strains. The rats were then sacrificed, the number of colon tumors were recorded, and the Dukes' stage were evaluated. CD3, CD4, CD8, CD56, FOXP3 and CEACAM6 expression in tumor tissues was determined by immunohistochemical staining. Compared with the expression levels in the pIRES/SL3261 group, similar levels of CD3(+), CD8(+) and CD56(+) expression were identified for the pIRES-CEACAM6/SL3261 group of rats. Additionally, a comparable number of tumors was detected in the pIRES-4-1BBL/SL3261 and pIRES-CEACAM6/SL3261 groups. By contrast, a significantly fewer number of tumors, albeit with a higher density of CD3(+)CD8(+), CD56(+) and a lower density of Foxp3(+) tumor-infiltrating lymphocyte (TIL) cells was detected in the pIRES-CEACAM6-4-1BBL/SL3261 group of rats. The results indicated that vaccination with recombinant attenuated Salmonella harboring the CEACAM6 and 4-1BBL gene efficiently increased the number of CD3(+)CD8(+) TIL and NK cells, decreased the number of FOXP3 cells and inhibited the development of DMH-induced colorectal cancer in rats.
机译:本研究旨在确定基于重组沙门氏菌(SL3261)的CEACAM6和4-1BB配体(4-1BBL)疫苗对大鼠大肠癌发展的影响以及潜在的免疫机制。构建了携带减毒鼠伤寒沙门氏菌(疫苗株)的质粒pIRES-CEACAM6,pIRES-4-1BBL和pIRES-CEACAM6-4-1BBL。每周一次给大鼠皮下注射1,2-二甲基肼(DMH),持续18周。首次注射后八周,将大鼠分为pIRES / SL3261,pIRES-4-1BBL / SL3261,pIRES-CEACAM6 / SL3261和pIRES-CEACAM6-4-1BBL / SL3261组,并喂以相应的疫苗株。然后处死大鼠,记录结肠肿瘤的数目,并评估Dukes阶段。通过免疫组织化学染色确定肿瘤组织中的CD3,CD4,CD8,CD56,FOXP3和CEACAM6表达。与pIRES / SL3261组的表达水平相比,pIRES-CEACAM6 / SL3261组的大鼠CD3(+),CD8(+)和CD56(+)表达水平相似。此外,在pIRES-4-1BBL / SL3261和pIRES-CEACAM6 / SL3261组中检测到相当数量的肿瘤。相比之下,尽管肿瘤中CD3(+)CD8(+),CD56(+)的密度较高,而Foxp3(+)肿瘤浸润淋巴细胞(TIL)的密度较低,但肿瘤的数量却明显减少。 pIRES-CEACAM6-4-1BBL / SL3261组的大鼠。结果表明,带有CEACAM6和4-1BBL基因的重组减毒沙门氏菌疫苗有效地增加了CD3(+)CD8(+)TIL和NK细胞的数量,减少了FOXP3细胞的数量并抑制了DMH诱导的结直肠癌的发展。大鼠癌症。

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