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一种来自婴儿双歧杆菌的形态特征全新的细胞壁制剂(全肽聚糖),对小鼠已形成的肿瘤消退具有更高疗效。

A new morphologically characterized cell wall preparation (whole peptidoglycan) from Bifidobacterium infantis with a higher efficacy on the regression of an established tumor in mice.

作者信息

Sekine K, Toida T, Saito M, Kuboyama M, Kawashima T, Hashimoto Y

出版信息

Cancer Res. 1985 Mar;45(3):1300-7.

PMID:3971375
Abstract

Three kinds of morphologically distinct cell wall preparations were isolated from heat-killed Bifidobacterium infantis and examined for the relative antitumor efficacy with syngeneic Meth A fibrosarcoma in BALB/c mice. Ultrastructural examinations revealed that cell wall skeleton (CWS) did not retain morphologically recognizable cell wall structure but showed fibrous structure. By contrast, a new cell wall preparation, whole peptidoglycan (WPG), which was isolated from whole cells without being subjected to physically destructive methods, completely retained the intact cell wall structure. When WPG was disrupted by sonic treatment, it retained some degree of physical integrity of cell wall structure, as compared with CWS. The results of chemical analysis indicated that the three cell wall preparations had similar chemical properties. A single s.c. injection of either CWS, WPG, or sonicated WPG in a mixture with tumor cells resulted in a significant suppression of the tumor growth. They were of equally high activity. However, when WPG, sonicated WPG, or CWS was injected intralesionally five times into mice bearing 5-day-old tumors, the incidence of complete tumor regression was demonstrated to decrease in the order of 70, 40, and 20%, respectively. The in vitro cytotoxicity test excluded the possibility that the tumor cell destruction was the result of direct cytotoxicity of the cell wall preparations. From these findings, it was concluded that WPG was an active stimulator of host-mediated response at the tumor-growing sites.

摘要

从热灭活的婴儿双歧杆菌中分离出三种形态不同的细胞壁制剂,并在BALB/c小鼠中与同基因的Meth A纤维肉瘤一起检测其相对抗肿瘤功效。超微结构检查显示,细胞壁骨架(CWS)没有保留形态上可识别的细胞壁结构,而是呈现出纤维状结构。相比之下,一种新的细胞壁制剂,即全肽聚糖(WPG),它是从完整细胞中分离出来的,没有经过物理破坏方法,完全保留了完整的细胞壁结构。当WPG通过超声处理被破坏时,与CWS相比,它仍保留了一定程度的细胞壁结构物理完整性。化学分析结果表明,这三种细胞壁制剂具有相似的化学性质。将CWS、WPG或超声处理的WPG与肿瘤细胞混合进行单次皮下注射,均能显著抑制肿瘤生长。它们具有同样高的活性。然而,当将WPG、超声处理的WPG或CWS对携带5日龄肿瘤的小鼠进行瘤内注射5次时,完全肿瘤消退的发生率分别以70%、40%和20%的顺序降低。体外细胞毒性试验排除了肿瘤细胞破坏是细胞壁制剂直接细胞毒性结果的可能性。从这些发现可以得出结论,WPG是肿瘤生长部位宿主介导反应的活性刺激物。

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