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分枝杆菌水溶性化合物和合成的胞壁酰二肽对巨噬细胞的激活作用。

Macrophage activation by mycobacterial water soluble compounds and synthetic muramyl dipeptide.

作者信息

Wahl S M, Wahl L M, McCarthy J B, Chedid L, Mergenhagen S E

出版信息

J Immunol. 1979 Jun;122(6):2226-31.

PMID:221582
Abstract

The adjuvant effects of mycobacteria can be replaced by more chemically defined isolates of the cell walls including a water soluble fraction (WSA) and by the synthetic analog N-acetyl-muramyl-L-alanyl-D-isoglutamine (MDP), which is the minimal structure required for adjuvanticity. These compounds can directly activate macrophages as determined by an increase in spreading and adherence and by an elevated synthesis of the enzyme collagenase. Moreover, this increase in collagenase production is modulated by enhanced production of prostaglandins that influences intracellular levels of cyclic AMP. In addition, both MDP and WSA induced macrophages to produce a biologically active mediator that triggers quiescent fibroblasts into active proliferation. It thus appears that a mechanism for mycobacterial adjuvant action as determined with MDP and WSA is via activation of macrophages, which may then precipitate a multiplicity of other reactions resulting in enhanced immune phenomena. Furthermore, the granulomatous and fibrotic reactions associated with mycobacterial infection may be a consequence of this direct activation of macrophages.

摘要

分枝杆菌的佐剂效应可以被细胞壁中化学定义更明确的分离物所取代,包括水溶性部分(WSA),以及合成类似物N-乙酰-胞壁酰-L-丙氨酰-D-异谷氨酰胺(MDP),后者是佐剂活性所需的最小结构。这些化合物可通过细胞铺展和黏附增加以及胶原酶合成增加来直接激活巨噬细胞。此外,胶原酶产生的增加受到前列腺素产生增加的调节,而前列腺素会影响细胞内环磷酸腺苷(cAMP)的水平。此外,MDP和WSA均可诱导巨噬细胞产生一种生物活性介质,该介质可触发静止的成纤维细胞进入活跃增殖状态。因此,用MDP和WSA确定的分枝杆菌佐剂作用机制似乎是通过激活巨噬细胞,进而可能引发多种其他反应,导致免疫现象增强。此外,与分枝杆菌感染相关的肉芽肿和纤维化反应可能是巨噬细胞这种直接激活的结果。

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