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Tumor‐specific T Cells which Form Clusters with Dendritic Cells and Tumor Cells and Deliver Macrophage‐activating Factors

机译:肿瘤特异性T细胞与树突状细胞和肿瘤细胞形成簇并提供巨噬细胞激活因子

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摘要

T cells prepared from tumor (Meth A)‐bearing mice were cocultured with homologous tumor cells and splenic dendritic cells to enrich tumor‐specific T cells by the separation of clusters. T blasts generated from clusters were capable of inhibiting the in vivo tumor cell growth. The culture supernatant of clustering cells (CLSN) was effective in activating macrophages (MØ) to be cytostatic and cytocidal against tumor cells. Moreover, it was found that CLSN contains at least 3 distinct factors; one was identified as interferon‐γ (IFN‐γ), and the others are so far unidentified, but one acts synergistically with IFN‐γ, possibly as the second signal, and the other cooperates with lipopolysaccharide but not with IFN‐γ. We propose that the tumor‐specific T cells secrete soluble mediators which cooperate with each other in MØ activation against tumor cells.
机译:从荷瘤小鼠(Meth A)制备的T细胞与同源肿瘤细胞和脾树突状细胞共培养,通过分离簇来富集肿瘤特异性T细胞。由簇产生的T胚细胞能够抑制体内肿瘤细胞的生长。群集细胞的培养上清液(CLSN)可有效激活巨噬细胞(MØ),使其具有抑制肿瘤细胞的杀伤细胞活性。此外,发现CLSN包含至少3个不同的因子。一个被鉴定为干扰素-γ(IFN-γ),到目前为止还没有被鉴定,但是一个与IFN-γ协同作用,可能是第二个信号,另一个与脂多糖协同而不与IFN-γ协同作用。我们建议肿瘤特异性T细胞分泌可溶性介体,这些介体在针对肿瘤细胞的MØ激活中相互配合。

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