Harder Markus J, Kuhn Nadine, Schrezenmeier Hubert, Höchsmann Britta, von Zabern Inge, Weinstock Christof, Simmet Thomas, Ricklin Daniel, Lambris John D, Skerra Arne, Anliker Markus, Schmidt Christoph Q
Institute of Pharmacology of Natural Products and Clinical Pharmacology, Ulm University, Ulm, Germany.
Lehrstuhl für Biologische Chemie, Technische Universität München, Freising, Germany.
Blood. 2017 Feb 23;129(8):970-980. doi: 10.1182/blood-2016-08-732800. Epub 2016 Dec 27.
Eculizumab inhibits the terminal, lytic pathway of complement by blocking the activation of the complement protein C5 and shows remarkable clinical benefits in certain complement-mediated diseases. However, several reports suggest that activation of C5 is not always completely suppressed in patients even under excess of eculizumab over C5, indicating that residual C5 activity may derogate the drug's therapeutic benefit under certain conditions. By using eculizumab and the tick-derived C5 inhibitor coversin, we determined conditions ex vivo in which C5 inhibition is incomplete. The degree of such residual lytic activity depended on the strength of the complement activator and the resulting surface density of the complement activation product C3b, which autoamplifies via the alternative pathway (AP) amplification loop. We show that at high C3b densities required for binding and activation of C5, both inhibitors reduce but do not abolish this interaction. The decrease of C5 binding to C3b clusters in the presence of C5 inhibitors correlated with the levels of residual hemolysis. However, by employing different C5 inhibitors simultaneously, residual hemolytic activity could be abolished. The importance of AP-produced C3b clusters for C5 activation in the presence of eculizumab was corroborated by the finding that residual hemolysis after forceful activation of the classical pathway could be reduced by blocking the AP. By providing insights into C5 activation and inhibition, our study delivers the rationale for the clinically observed phenomenon of residual terminal pathway activity under eculizumab treatment with important implications for anti-C5 therapy in general.
依库珠单抗通过阻断补体蛋白C5的激活来抑制补体的终末溶解途径,在某些补体介导的疾病中显示出显著的临床益处。然而,有几份报告表明,即使在依库珠单抗用量超过C5的情况下,患者体内C5的激活也并非总是被完全抑制,这表明在某些情况下,残余的C5活性可能会损害该药物的治疗效果。通过使用依库珠单抗和蜱源C5抑制剂覆盖素,我们在体外确定了C5抑制不完全的条件。这种残余溶解活性的程度取决于补体激活剂的强度以及补体激活产物C3b由此产生的表面密度,C3b通过替代途径(AP)放大环进行自身放大。我们发现,在C5结合和激活所需的高C3b密度下,两种抑制剂都能减少但不能消除这种相互作用。在存在C5抑制剂的情况下,C5与C3b簇结合的减少与残余溶血水平相关。然而,通过同时使用不同的C5抑制剂,可以消除残余溶血活性。经典途径强力激活后的残余溶血可通过阻断AP来降低,这一发现证实了在依库珠单抗存在的情况下,AP产生的C3b簇对C5激活的重要性。通过深入了解C5的激活和抑制,我们的研究为临床上观察到的依库珠单抗治疗下残余终末途径活性现象提供了理论依据,这对一般的抗C5治疗具有重要意义。