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使用正丁醇从细胞和质膜中提取小鼠肿瘤特异性抗原:秋水仙碱提高抗原产量

Extraction of a murine tumor-specific antigen from cells and plasma membranes using 1-butanol: augmentation of antigen yield by colchicine.

作者信息

LeGrue S J, Kahan B D

出版信息

Cancer Res. 1985 May;45(5):1926-9.

PMID:4039219
Abstract

The purpose of this investigation was to examine the ability of single-phase aqueous solutions of 1-butanol to release immunoprotective tumor antigen activity from partially purified plasma membranes of the methylcholanthrene-induced fibrosarcoma, MCA-F. Tumor antigen activity was assessed by s.c. immunization of syngeneic C3H/HeJ mice 10 days prior to supralethal challenge. Although brief incubation of intact MCA-F cells in 2.5% butanol releases potent immunoprotective activity, application of this protocol to plasma membranes did not result in antigen extraction. Modification of the extraction protocol using higher concentrations of butanol and longer extraction times did release measurable tumor antigen activity. However, a significant amount of the membrane-associated activity remained with the insoluble membrane fraction, as demonstrated by the immunoprotective capacity of the extracted membranes. The dramatic difference in the extractability of antigen from intact cells and plasma membranes suggested that membrane architecture may influence antigen release. To investigate this possibility, we extracted with butanol MCA-F cells that had been preincubated in colchicine. Treatment of cells with colchicine significantly potentiated the extraction of tumor antigen activity. Augmentation of antigen yield was also observed when plasma membranes were pretreated with colchicine prior to 2.5% butanol extraction. These results suggest that the tumor-specific transplantation antigen may be directly or indirectly associated with the cytoskeleton underlying the plasma membrane.

摘要

本研究的目的是检测1-丁醇单相水溶液从甲基胆蒽诱导的纤维肉瘤(MCA-F)部分纯化的质膜中释放免疫保护性肿瘤抗原活性的能力。在超致死性攻击前10天,通过对同基因C3H/HeJ小鼠进行皮下免疫来评估肿瘤抗原活性。尽管将完整的MCA-F细胞在2.5%丁醇中短暂孵育可释放强大的免疫保护活性,但将该方案应用于质膜并未导致抗原提取。使用更高浓度的丁醇和更长的提取时间对提取方案进行修改确实释放出了可测量的肿瘤抗原活性。然而,如提取的膜的免疫保护能力所示,大量与膜相关的活性仍保留在不溶性膜部分。从完整细胞和质膜中提取抗原的能力存在显著差异,这表明膜结构可能影响抗原释放。为了研究这种可能性,我们用丁醇提取了预先在秋水仙碱中孵育的MCA-F细胞。用秋水仙碱处理细胞显著增强了肿瘤抗原活性的提取。当质膜在2.5%丁醇提取前用秋水仙碱预处理时,也观察到抗原产量增加。这些结果表明,肿瘤特异性移植抗原可能直接或间接与质膜下方的细胞骨架相关。

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