Coversin Blocked in Vitro Hemolysis in an Eculizumab-Resistant PNH Patient with the C5 Polymorphism (c.2654G&gt;A)

Ueda, Yutaka; Osato, Makiko; Weston‐Davies, Wynne; Nunn, Miles A.; Hayashi, Satoru; Nishimura, Junichi; Kanakura, Yuzuru

doi:10.1182/blood.v126.23.2138.2138

Cited by 6 publications

(3 citation statements)

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“…Moreover, it could be shown that the C5 complement inhibitor OmCI, which binds at a site distinct from eculizumab 30 , was, in contrast to eculizumab, able to completely prevent the haemolysis induced by the mutant C5 molecules. Considering that OmCI, also known as coversin, was earlier reported as a possible therapeutic 30 45 46 47 48 with low immunogenicity 45 and is currently undergoing clinical trial, and given the results presented here, OmCI could represent an alternative future treatment strategy for patients responding poorly to eculizumab due to a missense mutation in eculizumab’s epitope on C5. Taken together our work outlines a general strategy for precision medicine based on detailed epitope mapping and genetic profiling, which should be transferable to several other diseases and therapies, and which would allow for correct treatment on those who will benefit while sparing expense and side effects for non-responders.…”

Section: Discussionmentioning

confidence: 84%

Stratification of responders towards eculizumab using a structural epitope mapping strategy

Volk

Berglund

et al. 2016

Sci Rep

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The complement component 5 (C5)-binding antibody eculizumab is used to treat patients with paroxysmal nocturnal hemoglobinuria (PNH) and atypical haemolytic uremic syndrome (aHUS). As recently reported there is a need for a precise classification of eculizumab responsive patients to allow for a safe and cost-effective treatment. To allow for such stratification, knowledge of the precise binding site of the drug on its target is crucial. Using a structural epitope mapping strategy based on bacterial surface display, flow cytometric sorting and validation via haemolytic activity testing, we identified six residues essential for binding of eculizumab to C5. This epitope co-localizes with the contact area recently identified by crystallography and includes positions in C5 mutated in non-responders. The identified epitope also includes residue W917, which is unique for human C5 and explains the observed lack of cross-reactivity for eculizumab with other primates. We could demonstrate that Ornithodorus moubata complement inhibitor (OmCI), in contrast to eculizumab, maintained anti-haemolytic function for mutations in any of the six epitope residues, thus representing a possible alternative treatment for patients non-responsive to eculizumab. The method for stratification of patients described here allows for precision medicine and should be applicable to several other diseases and therapeutics.

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Section: Discussionmentioning

confidence: 84%

Stratification of responders towards eculizumab using a structural epitope mapping strategy

Volk

Berglund

et al. 2016

Sci Rep

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“…A plethora of agents is currently in the pipeline of several pharmaceutical companies; they can be divided according to their target in the complement cascade (Figure ; Table ). Inhibitors of the effector pathway target C5, and include at least 6 novel mAb‐derived compounds, a small‐interfering RNA (siRNA) and 2 small molecules . A second group of inhibitors intercept the complement cascade upstream C5; they include broad inhibitors of C3 and agents which specifically target complement activating pathways—classical (CCP), alternative (CAP), and mannose/lectine (CMP) ones (Figure ; Table ) .…”

Section: Novel Strategies Of Complement Inhibitionmentioning

confidence: 99%

“…Coversin is a 16 kDa protein derived from the tick Ornithodoros moubata able to prevent C5 cleavage by its convertases; its in vitro efficacy in PNH has been already documented, even in patients carrying C5 polymorphisms . In a phase I study in healthy volunteers coversin was shown bioavailable after SC injections, with excellent PK and PD in absence of immunogenicity and of other safety concerns .…”

Section: Novel Strategies Of Complement Inhibitionmentioning

confidence: 99%

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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Second-Generation C5 Inhibitors for Paroxysmal Nocturnal Hemoglobinuria

Fattizzo

Kulasekararaj

2020

BioDrugs

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Coversin Blocked in Vitro Hemolysis in an Eculizumab-Resistant PNH Patient with the C5 Polymorphism (c.2654G>A)

Cited by 6 publications

References 0 publications

Stratification of responders towards eculizumab using a structural epitope mapping strategy

Stratification of responders towards eculizumab using a structural epitope mapping strategy

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

Second-Generation C5 Inhibitors for Paroxysmal Nocturnal Hemoglobinuria

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