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同基因小鼠体内负责肿瘤排斥的T细胞的Lyt表型。

The Lyt phenotype of the T cells responsible for in vivo tumor rejection in syngeneic mice.

作者信息

Ozawa H, Iwaguchi T, Kataoka T

出版信息

Cancer Immunol Immunother. 1986;23(1):73-7. doi: 10.1007/BF00205559.

Abstract

Spleen cells of BALB/c mice hyperimmunized with a transplantable methylcholanthrene-induced sarcoma Meth A (Meth A-Im-SPL) inhibited the growth of Meth A tumor in vivo in a tumor neutralizing test. Meth A-Im-SPL did not neutralize another antigenically distinct sarcoma, Meth 1, indicating that the antitumor activity is tumor specific. Lyt-1+2- cells of Meth A-Im-SPL (Im-Lyt-1+2-) were the effectors since in vitro treatment of Meth A-Im-SPL with anti-Thy 1.2 or anti-Lyt 1.2 antibody plus complement completely abrogated their neutralizing activity, whereas treatment with anti-Lyt 2.2 plus complement did not. To further confirm the effector activity of Im-Lyt-1+2- cells, T cell subpopulations were separated from Meth A-Im-SPL by the panning method. The purified Im-Lyt-1+2-, but not Im-Lyt-1+2+ cells neutralized the tumor in athymic nu/nu mice as efficiently as in +/+ mice, suggesting that the donor Im-Lyt-1+2- cells but not recipient T cells were primarily responsible for neutralizing the tumor. The present study, however, did not exclude the possible contribution of recipient T cells to the tumor neutralization and this is open to further investigation.

摘要

用可移植的甲基胆蒽诱导肉瘤Meth A(Meth A免疫脾细胞,Meth A-Im-SPL)超免疫的BALB/c小鼠的脾细胞,在肿瘤中和试验中可在体内抑制Meth A肿瘤的生长。Meth A-Im-SPL不能中和另一种抗原性不同的肉瘤Meth 1,这表明其抗肿瘤活性具有肿瘤特异性。Meth A-Im-SPL的Lyt-1+2-细胞(免疫Lyt-1+2-细胞)是效应细胞,因为用抗Thy 1.2或抗Lyt 1.2抗体加补体在体外处理Meth A-Im-SPL可完全消除其中和活性,而用抗Lyt 2.2加补体处理则不会。为了进一步证实免疫Lyt-1+2-细胞的效应活性,通过淘选法从Meth A-Im-SPL中分离出T细胞亚群。纯化的免疫Lyt-1+2-细胞而非免疫Lyt-1+2+细胞在无胸腺裸鼠(nu/nu)中中和肿瘤的效率与在+/+小鼠中一样高,这表明供体免疫Lyt-1+2-细胞而非受体T细胞是中和肿瘤的主要原因。然而,本研究并未排除受体T细胞对肿瘤中和可能的贡献,这有待进一步研究。

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