Shimizu Takashi, Kida Yutaka, Kuwano Koichi
Department of Bacteriology, Kurume University School of Medicine, Kurume, Japan.
Immunology. 2007 Aug;121(4):473-83. doi: 10.1111/j.1365-2567.2007.02594.x. Epub 2007 Apr 13.
Pathogenesis of Mycoplasma pneumoniae infection is considered to be in part attributed to excessive immune responses. Recently, a mycoplasma lipoprotein has been shown to induce nuclear factor kappaB (NF-kappaB) activation through toll-like receptor 1 (TLR1), TLR2 and TLR6. In this study, we examined the ability of lipoproteins from M. pneumoniae to activate NF-kappaB through TLR1- and TLR2-dependent, but TLR6-independent, pathways, and the active components responsible for the NF-kappaB activation through the TLR6-independent pathway were identified. The active lipoproteins were found to be MPN611 and MPN162 of M. pneumoniae (designated N-ALP1 and N-ALP2, respectively). Purified N-ALP1 and N-ALP2 from M. pneumoniae and triacylated partial synthetic lipopeptides of N-ALP1 and N-ALP2 augmented the levels of NF-kappaB induction through TLR1- and TLR2-dependent pathways, whereas diacylated partial synthetic lipopeptides of N-ALP1 and N-ALP2 activated NF-kappaB through TLR1-, TLR2- and TLR6-dependent pathways. These data suggest that N-ALP1 and N-ALP2 would be triacylated lipoproteins. The activity of N-ALP1 and N-ALP2 was decreased with a pretreatment of lipoprotein lipase, and partially decreased by protease treatment, indicating that the lipid moiety of N-ALP1 and N-ALP2 is critical for the NF-kappaB activation. Thus, triacylated lipoproteins derived from M. pneumoniae might activate NF-kappaB through TLR1 and TLR2, but not TLR6.
肺炎支原体感染的发病机制被认为部分归因于过度的免疫反应。最近,一种支原体脂蛋白已被证明可通过Toll样受体1(TLR1)、TLR2和TLR6诱导核因子κB(NF-κB)活化。在本研究中,我们检测了肺炎支原体脂蛋白通过TLR1和TLR2依赖性但TLR6非依赖性途径激活NF-κB的能力,并鉴定了通过TLR6非依赖性途径负责NF-κB激活的活性成分。发现活性脂蛋白是肺炎支原体的MPN611和MPN162(分别命名为N-ALP1和N-ALP2)。从肺炎支原体中纯化的N-ALP1和N-ALP2以及N-ALP1和N-ALP2的三酰化部分合成脂肽通过TLR1和TLR2依赖性途径增加了NF-κB诱导水平,而N-ALP1和N-ALP2的二酰化部分合成脂肽通过TLR1、TLR2和TLR6依赖性途径激活NF-κB。这些数据表明N-ALP1和N-ALP2是三酰化脂蛋白。用脂蛋白脂肪酶预处理后,N-ALP1和N-ALP2的活性降低,蛋白酶处理使其部分降低,表明N-ALP1和N-ALP2的脂质部分对NF-κB激活至关重要。因此,源自肺炎支原体的三酰化脂蛋白可能通过TLR1和TLR2而非TLR6激活NF-κB。