肿瘤抗原P1A与细胞因子mGM-CSF共表达载体的构建和表达

目的 :构建并鉴定细胞因子mGM CSF和肿瘤特异抗原P1A共表达载体 ,为研究新型的肿瘤疫苗提供新的策略。方法 :以PCR方法从pCI neo P1A中扩增出P1A编码基因片段 ,构建于pRSC质粒上 ;再从pORF mGM CSF中扩增出mGM CSF基因片段 ,插入pRSC P1A重组质粒P1A基因的上游。以酶切和DNA测序进行鉴定。并将鉴定过的重组质粒以脂质体法转染 772 1细胞 ,用RT PCR法鉴定转染细胞中P1A基因和mGM CSF基因的表达。结果 :经酶切鉴定和DNA测序证实mGM CSF和P1A重组质粒构建正确 ,并在转染此质粒的 772 1细胞中检测出了P1A和mGM CSF基因的表达。结论 :成功构建mGM CSF和P1A的共表达载体 。

The development and functions of CD41 T cells expressing a transgenic TCR specific for an MHC-I-restricted tumor antigenic epitope

It has been reported that the ratio of CD41 to CD81 T cells has no bias in a few class I major histocompatibility complex(MHC-I)-restricted T-cell receptor(TCR)-transgenic mice specific for alloantigens or autoantigens,in which most CD41 T cells express an MHC-I-restricted TCR.In this study,we further showed that more than 50%of CD41 T cells in MHC-I-restricted P1A tumor antigen-specific TCR(P1ATCR)-transgenic mice could specifically bind to MHC-I/P1A peptide complex.P1A peptide could stimulate the transgenic CD41 T cells to proliferate and secrete both type 1 helper T cell and type 2 helper T cell cytokines.The activated CD41 T cells also showed cytotoxicity against P1A-expressing tumor cells.The analysis of TCR a-chains showed that these CD41 T cells were selected by co-expressing endogenous TCRs.Our results show that CD41 T cells from P1ATCR transgenic mice co-expressed an MHC-I-restricted transgenic TCR and another rearranged endogenous TCRs,both of which were functional.