Loos M, Clas F, Fischer W
Infect Immun. 1986 Sep;53(3):595-9. doi: 10.1128/iai.53.3.595-599.1986.
Glycerophosphate-containing lipoteichoic acids (LTAs) interact with the first component of the classical complement pathway (C1). This resulted in the activation of the classical complement pathway in serum, shown by the consumption of C1, C2, and C4. The dose-dependent interaction of LTAs with purified C1 and C1q was dependent on the negative charges of the phosphate groups of LTA. It was reduced by charge compensation through D-alanine ester substituents and by sterical hindrance through di- and trihexosyl residues linked to position 2 of the glycerol moieties. The charge density of LTA may also play a role: poly(digalactosylglycerophosphate) LTAs, in which the phosphate groups are in a greater distance from each other, were less effective, and the loss of micellar organization by deacylation of LTA drastically reduced the complement activation capacity.
含甘油磷酸的脂磷壁酸(LTA)与经典补体途径的第一成分(C1)相互作用。这导致血清中经典补体途径的激活,表现为C1、C2和C4的消耗。LTA与纯化的C1和C1q的剂量依赖性相互作用取决于LTA磷酸基团的负电荷。通过D - 丙氨酸酯取代基进行电荷补偿以及通过与甘油部分2位相连的二糖基和三糖基残基产生空间位阻可使其降低。LTA的电荷密度也可能起作用:聚(二半乳糖基甘油磷酸)LTA中磷酸基团彼此距离更远,其效果较差,并且LTA脱酰基导致的胶束结构丧失极大地降低了补体激活能力。