Hetland G, Bungum L
Institute of Medical Biology, University of Tromsø, Norway.
APMIS. 1988 Jan;96(1):89-92.
Endotoxin-stimulated human peritoneal macrophages were cultured in serum-free medium with agarose beads. Monospecific antibodies to human C3c, C3g, C5, C6, C7, C8, C9 and to C9-neoantigen bound to the beads. This shows that activated C3 and the terminal complement complex (TCC), made from complement components C5 to C9, were generated on the beads. De novo synthesis was confirmed by agarose binding of tritium-labelled protein. Moreover, C3-derivatives and C9-neoantigen were detected on normal serum-treated agarose beads but not on beads kept in factor B-depleted or heat-inactivated sera, implying that an intact alternative complement pathway was required for our findings. The macrophages thus synthesize the active complement components of the alternative and terminal pathways in vitro.
内毒素刺激的人腹膜巨噬细胞在含有琼脂糖珠的无血清培养基中培养。与珠子结合的针对人C3c、C3g、C5、C6、C7、C8、C9以及C9新抗原的单特异性抗体。这表明在珠子上产生了由补体成分C5至C9组成的活化C3和末端补体复合物(TCC)。通过氚标记蛋白的琼脂糖结合证实了从头合成。此外,在正常血清处理的琼脂糖珠上检测到C3衍生物和C9新抗原,但在保存在B因子缺失或热灭活血清中的珠子上未检测到,这意味着完整的替代补体途径是我们研究结果所必需的。因此,巨噬细胞在体外合成替代途径和末端途径的活性补体成分。
