Rational Engineering of a Minimized Immune Inhibitor with Unique Triple-Targeting Properties

Schmidt, Christoph Q.; Bai, Hongjun; Lin, Zhuoer; Risitano, Antonio M.; Barlow, Paul N.; Ricklin, Daniel; Lambris, John D.

doi:10.4049/jimmunol.1203548

Cited by 118 publications

(202 citation statements)

References 59 publications

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“…This is consistent with previous data showing that the C3-opsonintargeting inhibitors mini-FH and TT30 efficiently control AP activation in several assays. 38,44,45,49,50 As observed for the double inhibition of C5 in NHS (above), addition of coversin or PAS-coversin to the patientderived, eculizumab-containing serum completely stopped the residual hemolysis if compared with eculizumab alone. We verified that the patient sera indeed contained an excess amount of eculizumab over C5 ( Figure 1F).…”

Section: Single C5 Inhibition Only Partially Blocks Tp Activationmentioning

confidence: 78%

“…Immobilization of 800 response units (RUs) of C3b onto the carboxymethyldextran surface of a sensor chip via standard amine coupling enabled binding of mini-FH ( Figure 3A) as expected. 38,45 In contrast, no binding of C5 to amine coupled C3b was observed. However, when additional 900 RUs of C3b molecules were immobilized in a more physiological manner employing onchip assembled C3 convertases, C5 did efficiently adhere to such "physiologically" immobilized C3b in a concentration-dependent way ( Figure 3B).…”

Section: Residual Lysis Under C5 Inhibition Is Influenced By Ap Activitymentioning

confidence: 94%

“…As a control, the minimized, engineered version of the natural AP-specific regulator FH, mini-FH, was included; mini-FH regulates the complement cascade upstream of C5 activation and inhibits at the level of activated C3. 38 All inhibitors showed a clear concentration-dependent inhibition of hemolysis, but only mini-FH inhibited lysis completely, while all C5 inhibitors in the assay reached a plateau of background lysis and failed to completely inhibit hemolysis, even at higher inhibitor concentrations ( Figure 1B). Of note, the level of background hemolysis was different for the C5 inhibitors.…”

Section: Single C5 Inhibition Only Partially Blocks Tp Activationmentioning

confidence: 95%

“…The minimized engineered version of the natural AP regulator FH, mini-FH, and the C-terminal FH fragment, FH18-20, which harbors the FH host surface recognition patch, were produced as described previously. 38,39 Hemolysis and bacterial lysis assays CP activity was measured with a standard heterologous hemolysis assay using antibody-sensitized sheep erythrocytes (shRBCs). 40 Alternatively, a very sensitive homologous assay with antibody-sensitized PNH-RBCs was adapted from the procedure of Rosse.…”

Section: Proteinsmentioning

confidence: 99%

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Incomplete inhibition by eculizumab: mechanistic evidence for residual C5 activity during strong complement activation

Harder

Kuhn

Schrezenmeier

et al. 2017

Blood

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115

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• Strong complement activation overrides the terminal pathway inhibition by the anti-C5 antibody eculizumab.• The more powerful complement is activated, the less effective is terminal pathway inhibition by diverse anti-C5 agents.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. (Blood. 2017;129(8):970-980)

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Section: Single C5 Inhibition Only Partially Blocks Tp Activationmentioning

confidence: 78%

Section: Residual Lysis Under C5 Inhibition Is Influenced By Ap Activitymentioning

confidence: 94%

Section: Single C5 Inhibition Only Partially Blocks Tp Activationmentioning

confidence: 95%

Section: Proteinsmentioning

confidence: 99%

See 2 more Smart Citations

Incomplete inhibition by eculizumab: mechanistic evidence for residual C5 activity during strong complement activation

Harder

Kuhn

Schrezenmeier

et al. 2017

Blood

Self Cite

115

125

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“…Mini-FH has high affinity for C3b and C3d and showed better inhibitory function in vitro compared to native FH. 56,57 In addition, as with eculizumab, safety issues still have to be defined with regard to infectious complications. A more specific approach to inhibit complement activation via the classical pathway on the level of C3 has been described by Yazdanbaksh and co-workers.…”

mentioning

confidence: 99%

Complement inhibitors to treat IgM-mediated autoimmune hemolysis

Wouters

2015

Haematologica

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© F e r r a t a S t o r t i F o u n d a t i o n Complement systemThe complement system is an evolutionary highly conserved cascade system that makes up part of the innate immune system. [7][8][9] Complement activation can occur via three distinct pathways (classical pathway (CP), lectin pathway (LP) and alternative pathway (AP) that converge at the level of C3 cleavage and eventually lead to a common terminal pathway (TP) ( Figure 1A).The AP can be initiated by spontaneous hydrolysis of the central complement component into C3b(H 2 O). C3b(H 2 O) is an acceptor for the next AP protein Factor B (FB) which is then cleaved by the serine protease factor D (FD), resulting Complement inhibition in AIHA haematologica | 2015; 100 (11) 1389 The lectin pathway is initiated by binding of MBL (or ficolins) to sugar structures followed by activation of C2 and C4 by MASP1/MASP2, leading to the formation of lectin C3 convertase (C2aC4b). (E) C3-activation by the classical, lectin or alternative C3 convertase results in the formation of the C5 convertase. C5 convertase subsequently activates C5 resulting in the formation of the membrane attack complex (MAC). C: complement factor; MAC: membrane attack complex; MBL: mannan binding lectin; MASP: MBL-associated serine protease; P: properdin; C1-inh: C1-inhibitor; FI: factor I; CR1: complement receptor 1; MCP: membrane co-factor protein; DAF: decay accelerating factor; C4BP: C4-binding protein; FH: factor H. A B C D E © F e r r a t a S t o r t i F o u n d a t i o nin the fluid phase C3 convertase (C3b(H 2 O)Bb), that can cleave multiple C3 molecules into C3b and C3a. C3b binds to nucleophilic targets on cell membranes 10 and C3a acts as a pro-inflammatory anaphylatoxin ( Figure 1B). Low-level activation of C3 can significantly be accelerated through a positive feedback loop resulting in the formation of additional alternative C3 convertases on the surface (C3bBb) that are stabilized by properdin (P) and eventually give rise to the formation of a C5 convertase (C3bBbC3b), which subsequently cleaves C5 into C5b and C5a.10 C5b attaches to the surface and subsequently binds to C6, C7 and C8 to form the C5bC8 complex allowing polymerization of C9 to form the membrane attack complex (MAC), which inserts into target membranes and induces cell lysis ( Figure 1A and E). 11,12 Next to lysis by the MAC, cleavage of both C3 and C5 results in the generation of pro-inflammatory anaphylatoxins (C3a, C5a) that attract and activate leukocytes 13 and C3b opsonization of the target surface facilitates uptake by phagocytic cells in the liver and spleen.During evolution complement activation became more specific by the development of recognition molecules. The CP is initiated by binding of C1q to the Fc-part of IgM or IgG complexed with their target antigens. IgM is most efficient in complement activation, due to its polymeric nature. Human IgG activates complement in the order IgG3>IgG1>IgG2, whereas IgG4 does not activate complement at all.14 As the affinity of C1q for a single IgG Fc tail is...

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Toward complement inhibition 2.0: Next generation anticomplement agents for paroxysmal nocturnal hemoglobinuria

Risitano

Marotta

2018

American J Hematol

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Therapeutic complement inhibition by eculizumab has revolutionized the treatment of paroxysmal nocturnal hemoglobinuria (PNH) with a major impact on its natural history. Nevertheless, emerging unmet clinical needs may benefit from the development of novel complement inhibitors. Novel strategies of complement inhibition exploit different agents targeting C5, as well as compound intercepting the complement cascade at the level of its key component C3, or even upstream at the level of components involved in complement alternative pathway initiation. Many of these agents are already in their clinical development; preliminary data together with a deep understanding of PNH biology may help to anticipate their possible clinical effect. Novel anti-C5 agents include monoclonal antibodies (even long-lasting) as well as other small molecules bioavailable by subcutaneous administration; an anti-C5 small interfering RNA has been developed too. All these anti-C5 agents seem to recapitulate safety and efficacy of current eculizumab treatment; their main improvement pertains to better patient's convenience due to longer dosing interval and/or possible subcutaneous self-administration. The possibility of achieving a deeper C5 inhibition has been shown as well, but its actual clinical meaning remains to be elucidated. Upstream complement inhibitors include the anti-C3 small peptide compstatin (and its derivatives), and small inhibitors of complement factor D or complement factor B. This class of compounds anticipates a possible efficacy in prevention of C3-mediated extravascular hemolysis, in addition to inhibition of intravascular hemolysis, eventually leading to improved hematological responses. The availability of all these compounds will result soon in a substantial improvement of PNH management.

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Rational Engineering of a Minimized Immune Inhibitor with Unique Triple-Targeting Properties

Cited by 118 publications

References 59 publications

Incomplete inhibition by eculizumab: mechanistic evidence for residual C5 activity during strong complement activation

Incomplete inhibition by eculizumab: mechanistic evidence for residual C5 activity during strong complement activation

Complement inhibitors to treat IgM-mediated autoimmune hemolysis

Toward complement inhibition 2.0: Next generation anticomplement agents for paroxysmal nocturnal hemoglobinuria

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