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T细胞亚群在破坏13762A大鼠乳腺腺癌已形成转移灶中的作用。

Role of T-cell subsets in the destruction of established metastases of 13762A rat mammary adenocarcinoma.

作者信息

Howell L E, Kreider J W, Bartlett G L

出版信息

J Natl Cancer Inst. 1986 Jul;77(1):187-93.

PMID:3487670
Abstract

The 13762A rat mammary adenocarcinoma metastasizes with high frequency to regional lymph nodes and lungs. The intratumoral injection of Corynebacterium parvum on day 7 followed by primary tumor excision on day 20 significantly prolonged survival and cured 10-40% of syngeneic F344 rats. Established metastases were destroyed by the treatment, and strong and specific tumor rejection immunity was induced. The purpose of the present study was to determine if T-cells were required for the C. parvum treatment to be effective and to identify the subsets of T-lymphocytes that might participate in the response. The results indicated that rats depleted by either neonatal thymectomy or a combination of adult thymectomy, 900 rad, and bone marrow reconstitution did not inhibit tumor growth after C. parvum treatment. Restoration of depleted rats with lymph node cells permitted effective treatment. The lymph node cells that were responsible for restoration expressed both W3/13 (pan-T-cell) and W3/25 (helper T-cell) membrane-associated differentiation antigens. T-cells that bore the MRC OX8 (cytotoxic-suppressor T-cell) antigen did not restore the response to C. parvum treatment. The effect of lymph node restoration was markedly potentiated by simultaneous administration of thymocytes, a T-cell population that expresses both W3/25 and MRC OX8 antigens. In conclusion, the cytotoxic-suppressor T-cells were ineffective in the restoration of T-cell-depleted, tumor-bearing rats to benefit from C. parvum but helper T-cells were highly effective, and their activity was strongly potentiated by administration of thymocyte amplifier cells.

摘要

13762A大鼠乳腺腺癌极易转移至局部淋巴结和肺部。在第7天瘤内注射短小棒状杆菌,然后在第20天切除原发肿瘤,可显著延长同基因F344大鼠的生存期,并使10% - 40%的大鼠治愈。已形成的转移灶经该治疗后被破坏,并诱导出强烈而特异的肿瘤排斥免疫。本研究的目的是确定短小棒状杆菌治疗有效是否需要T细胞,并鉴定可能参与该反应的T淋巴细胞亚群。结果表明,新生期胸腺切除或成年期胸腺切除、900拉德照射及骨髓重建联合处理使T细胞耗竭的大鼠,在接受短小棒状杆菌治疗后肿瘤生长未受抑制。用淋巴结细胞恢复T细胞耗竭的大鼠后,治疗变得有效。负责恢复的淋巴结细胞表达W3/13(全T细胞)和W3/25(辅助性T细胞)膜相关分化抗原。带有MRC OX8(细胞毒性 - 抑制性T细胞)抗原的T细胞不能恢复对短小棒状杆菌治疗的反应。同时给予胸腺细胞(一种表达W3/25和MRC OX8抗原的T细胞群体)可显著增强淋巴结恢复的效果。总之,细胞毒性 - 抑制性T细胞在恢复T细胞耗竭的荷瘤大鼠以从短小棒状杆菌治疗中获益方面无效,但辅助性T细胞非常有效,并且给予胸腺细胞扩增细胞可强烈增强其活性。

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