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在体内或体外被激活至溶细胞阶段的巨噬细胞中核糖体RNA的积累失衡。

Imbalanced accumulation of ribosomal RNA in macrophages activated in vivo or in vitro to a cytolytic stage.

作者信息

Varesio L

出版信息

J Immunol. 1985 Feb;134(2):1262-7.

PMID:3965571
Abstract

Previous studies have shown that peritoneal murine macrophages activated in vivo and in vitro to a tumoricidal stage have a depressed rate of RNA synthesis. In attempting to clarify the differences in RNA metabolism between noncytotoxic and tumoricidal macrophages, we have studied the relative accumulation of various species of RNA in macrophages activated in vivo and in vitro with the use of agarose gel electrophoresis. Macrophages activated in vitro to a cytotoxic stage with supernatants containing lymphokines (LK) and traces of lipopolysaccharide (LPS) have an imbalanced accumulation of mature ribosomal RNA (rRNA), with a decreased accumulation of 28S rRNA compared to 18S rRNA. In contrast, macrophages primed in vitro with LK free of detectable endotoxins that exhibit suppressive rather than tumoricidal activity do not manifest a decreased 28S:18S rRNA ratio. The conclusion that the decreased 28S:18S rRNA ratio was associated with the activation of macrophages to a cytolytic stage was supported by the finding that cytotoxic macrophages activated in vivo by i.p. injection of Propionibacterium acnes (formerly designated C. parvum) also demonstrated a decreased accumulation of 28S comparable with that observed in in vitro-activated macrophages. Moreover, activated macrophages that lost their cytolytic activity upon prolonged in vitro culture had an augmented accumulation of 28S rRNA. These results provide the first direct evidence that the expression of cytolytic activity is associated with modulation of a specific class of RNA. The unbalanced accumulation of rRNA appears to be a late molecular event in the activation process occurring during the transition from primed to cytotoxic macrophages, because inflammatory and primed macrophages had normal rRNA accumulation. A model of macrophage activation accounting for these results is proposed.

摘要

先前的研究表明,在体内和体外被激活至杀肿瘤阶段的腹膜小鼠巨噬细胞,其RNA合成速率降低。为了阐明非细胞毒性巨噬细胞和杀肿瘤巨噬细胞在RNA代谢方面的差异,我们利用琼脂糖凝胶电泳研究了体内和体外激活的巨噬细胞中各种RNA的相对积累情况。用含有淋巴因子(LK)和微量脂多糖(LPS)的上清液在体外激活至细胞毒性阶段的巨噬细胞,成熟核糖体RNA(rRNA)的积累失衡,与18S rRNA相比,28S rRNA的积累减少。相比之下,用不含可检测内毒素的LK在体外预处理的巨噬细胞表现出抑制而非杀肿瘤活性,其28S:18S rRNA比值并未降低。腹腔注射痤疮丙酸杆菌(原称短小棒状杆菌)在体内激活的细胞毒性巨噬细胞也表现出与体外激活的巨噬细胞相当的28S积累减少,这一发现支持了28S:18S rRNA比值降低与巨噬细胞激活至溶细胞阶段相关的结论。此外,在体外长期培养后失去溶细胞活性的激活巨噬细胞,其28S rRNA的积累增加。这些结果提供了首个直接证据,表明溶细胞活性的表达与特定一类RNA的调节有关。rRNA的不平衡积累似乎是激活过程中的一个晚期分子事件,发生在从预处理巨噬细胞向细胞毒性巨噬细胞转变的过程中,因为炎症巨噬细胞和预处理巨噬细胞的rRNA积累正常。本文提出了一个解释这些结果的巨噬细胞激活模型。

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