首页> 外文期刊>Cytokines, cellular and molecular therapy >Intraportal and systemic allogeneic cell therapy in a murine model of hepatic metastatic breast cancer.
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Intraportal and systemic allogeneic cell therapy in a murine model of hepatic metastatic breast cancer.

机译:肝转移性乳腺癌小鼠模型中的门静脉和全身同种异体细胞治疗。

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Allogeneic immunocompetent splenocytes were tested for their ability to exert a GVT effect in a murine model of liver metastasis. Mammary carcinoma cells originating from an H-2(d) mouse were inoculated through the PV of F(1) (H-2(d/b)) mice, to mimic clinical hepatic involvement in malignant disease. Cell therapy was given either locally (PV) or systemically by IV inoculation to test differential efficacy of the GVT effect, and the differential expression of GVHD symptoms induced by diverse routes of administration. Livers of mice treated with H-2(b) derived splenocytes given PV or IV remained tumor-free for at least 4 weeks following tumor inoculation. Furthermore, all secondary recipients of adoptively transferred (AT) liver cells were tumor-free for >300 days. In contrast, all livers of untreated control mice or mice treated with syngeneic splenocytes displayed tumor metastases as early as 2 weeks following tumor inoculation, and large local tumors developed in AT secondary recipients. Our data demonstrate the efficacy of allogeneic cell therapy, given either locally or systemically, in the eradication of liver metastases. However, diverse routes of cell therapy administration did not show any difference in the expression and outcome of GVHD.
机译:测试了具有同种异体免疫能力的脾细胞在小鼠肝转移模型中发挥GVT效应的能力。通过F(1)(H-2(d / b))小鼠的PV接种源自H-2(d)小鼠的乳癌细胞,以模拟临床肝参与恶性疾病。通过局部接种(PV)或全身静脉注射来进行细胞治疗,以测试GVT效果的差异功效,以及通过多种给药途径诱导的GVHD症状的差异表达。接种疫苗后,接受H-2(b)衍生脾细胞给予PV或IV处理的小鼠肝脏无肿瘤至少持续4周。此外,所有过继转移(AT)肝细胞的次要接受者在300天内均无肿瘤。相反,未经治疗的对照小鼠或经同基因脾细胞治疗的小鼠的所有肝脏最早在肿瘤接种后2周就显示出肿瘤转移,并且在AT次要受体中形成了较大的局部肿瘤。我们的数据表明,局部或全身给予同种异体细胞疗法在根除肝转移中的功效。但是,细胞治疗的多种给药途径在GVHD的表达和结果方面均未显示任何差异。

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