Small-molecule factor B inhibitor for the treatment of complement-mediated diseases

Schubart, Anna; Anderson, Karen; Mainolfi, Nello; Sellner, Holger; Ehara, Takeru; Adams, Christopher M.; Sweeney, A. Mac; Liao, Sha-Mei; Crowley, Maura; Littlewood‐Evans, Amanda; Sarret, Sophie; Wieczorek, Grazyna; Perrot, Ludovic; Dubost, Valérie; Flandre, Thierry; Zhang, Yuzhou; Smith, Richard J.; Risitano, Antonio M.; Karki, Rajeshri G.; Zhang, Chun; Valeur, Eric; Sirockin, Finton; Gerhartz, Bernd; Erbel, P.; Hughes, Nicola; Smith, Thomas M.; Cumin, Frédéric; Argikar, Upendra A.; Haraldsson, Börje; Mogi, Muneto; Sedrani, Richard; Wiesmann, Christian; Jaffee, Bruce; Maibaum, Jürgen; Flohr, Stefanie; Harrison, Richard A.; Eder, Jörg

doi:10.1073/pnas.1820892116

Cited by 126 publications

(123 citation statements)

References 31 publications

(35 reference statements)

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“…As the initiating protease of the classical pathway, C1r catalyzes the first proteolytic cleavage event and thus represents the most upstream enzymatic target of the pathway. While complement-directed therapeutics continue to be dominated by antibody-based drugs, small-molecules have recently seen two major breakthroughs in the successful development of factor B and factor D-specific inhibitors [ 48 , 49 , 50 ]. In general, small-molecule drugs are afforded greater tissue penetrance relative to antibodies/biologics and can more easily cross the blood–brain barrier [ 51 , 52 ].…”

Section: Discussionmentioning

confidence: 99%

“…However, given their low molecular complexity, it is not necessarily expected that fragment hits themselves will exhibit high selectivity [ 36 ]. Nonetheless, it is encouraging that active-site targeted small-molecule inhibitors of other complement serine proteases, factor B and factor D, have ultimately overcome this same challenge of specificity [ 48 , 49 , 50 ]. Although our C1r-domain mapping and molecular dynamics studies have provided information about CMP-1696, defining the binding mode of each fragment hit identified here—including CMP-1611 using empirical experimental methods, such as x-ray crystallography coupled with rigorous MD simulations—is a key next step being actively pursued in our laboratory.…”

Section: Discussionmentioning

confidence: 99%

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Targeting the Initiator Protease of the Classical Pathway of Complement Using Fragment-Based Drug Discovery

et al. 2020

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The initiating protease of the complement classical pathway, C1r, represents an upstream and pathway-specific intervention point for complement-related autoimmune and inflammatory diseases. Yet, C1r-targeted therapeutic development is currently underrepresented relative to other complement targets. In this study, we developed a fragment-based drug discovery approach using surface plasmon resonance (SPR) and molecular modeling to identify and characterize novel C1r-binding small-molecule fragments. SPR was used to screen a 2000-compound fragment library for binding to human C1r. This led to the identification of 24 compounds that bound C1r with equilibrium dissociation constants ranging between 160–1700 µM. Two fragments, termed CMP-1611 and CMP-1696, directly inhibited classical pathway-specific complement activation in a dose-dependent manner. CMP-1611 was selective for classical pathway inhibition, while CMP-1696 also blocked the lectin pathway but not the alternative pathway. Direct binding experiments mapped the CMP-1696 binding site to the serine protease domain of C1r and molecular docking and molecular dynamics studies, combined with C1r autoactivation assays, suggest that CMP-1696 binds within the C1r active site. The group of structurally distinct fragments identified here, along with the structure–activity relationship profiling of two lead fragments, form the basis for future development of novel high-affinity C1r-binding, classical pathway-specific, small-molecule complement inhibitors.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Targeting the Initiator Protease of the Classical Pathway of Complement Using Fragment-Based Drug Discovery

et al. 2020

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“…Factor B (FB), a trypsin-like serine protease, plays an important role in central amplification of C3b production and circulates as a latent zymogen [38]. During alternative pathway activation, FB first binds to C3b [39].…”

Section: Early Phase Inhibitorsmentioning

confidence: 99%

“…Factor B and Factor D inhibitors are promising therapies for complement-mediated conditions. A recent publication by Schubart et al has demonstrated efficacy in vivo with animal studies and ex vivo with human samples, as indicated by the prevention of hemolysis of PNH erythrocytes [38].…”

Section: Early Phase Inhibitorsmentioning

confidence: 99%

Ravulizumab in the treatment of paroxysmal nocturnal hemoglobinuria

Rho

Wells

2020

Expert Opinion on Orphan Drugs

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Introduction: Eculizumab, the anti-C5 monoclonal antibody therapeutic, has revolutionized the treatment of Paroxysmal Nocturnal Hemoglobinuria (PNH) and has shown efficacy in other complementmediated disorders including atypical Hemolytic Uremic Syndrome (aHUS) and Myasthenia Gravis (MG). Despite the effectiveness of eculizumab, challenges remain in the treatment of these diseases, including breakthrough hemolysis, frequent intravenous infusions, and cost; in an effort to mitigate these challenges, the new monoclonal therapeutic ravulizumab has been developed. Areas covered: In this paper, we review the characteristics and clinical performance of ravulizumab and assess its potential utility in the treatment of PNH, and its position in this rapidly-developing therapeutic landscape. A review of published data up to Phase III of ravulizumab had been performed. Studies were identified via Google Scholar, PubMed, the United States National Library of Medicine Clinical Trials, citation chasing, and topic knowledge of the authors. Expert opinion: Ravulizumab represents an important advance in the clinical care of complementmediated disorders. Clinical trials demonstrate non-inferior efficacy and indistinguishable safety and tolerability to eculizumab, with added patient-preferred benefits including longer intervals between infusions. Though improved, physicians should be aware of the limitations of ravulizumab, including the need for intravenous infusions and possible breakthrough hemolysis.

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“…LNP023 (Novartis) относится к малым молекулам химического происхождения, основным механизмом действия которого является ингибирование фактора B системы комплемента. Подобно молекулам против фактора D [70], LNP023 предотвращает гемолиз и C3-опсонизацию ПНГ эритроцитов in vitro [71]. В настоящее время проводится клиническое исследование II фазы LNP023 в качестве дополнительной терапии у пациентов с плохим ответом на экулизумаб, проявляющимся повышением ЛДГ > 1,5 раза выше верхней границы нормы [72].…”

Section: ингибиторы проксимальной части комплементаunclassified

Biotechnological products for the treatment of complement system disorders including paroxysmal nocturnal hemoglobinuria: currently available and in development

Кудлай

Бакиров

Павлов

2020

Voprosy gematologii/onkologii i immunopatologii v pediatrii

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Paroxysmal nocturnal hemoglobinuria (PNH) is a rare acquired clonal blood disorder caused by somatic mutations in phosphatidylinositol glycan, class A gene (PIG-A) in hematopoietic stem cells which manifests as haemolytic anemia, bone marrow failure, thromboses, impaired renal function, and other severe clinical symptoms. The management of PNH is a clinical challenge requiring a comprehensive approach. Over the past decade, target therapy with eculizumab, an antibody inhibitor of terminal complement activation, has played a key role in the treatment of PNH. Eculizumab is the first humanized anti-C5 monoclonal antibody that was proven effective in inhibiting the complement system and was approved as a standard treatment for PNH in many countries. Elizaria, the first biosimilar version of eculizumab, whose similarity to the original drug in terms of efficacy and safety was demonstrated in clinical trials, has been widely used in Russia since 2019. New complement inhibitors classified by their mechanism of action into inhibitors targeting complement component C5 (the terminal pathway) and those targeting early phases of complement activation cascade (the proximal pathway) are currently in development. These new drugs include monoclonal antibodies, small molecules, small peptide inhibitors, small interfering RNA, and recombinant proteins based on endogenous regulators of complement activation.

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Small-molecule factor B inhibitor for the treatment of complement-mediated diseases

Cited by 126 publications

References 31 publications

Targeting the Initiator Protease of the Classical Pathway of Complement Using Fragment-Based Drug Discovery

Targeting the Initiator Protease of the Classical Pathway of Complement Using Fragment-Based Drug Discovery

Ravulizumab in the treatment of paroxysmal nocturnal hemoglobinuria

Biotechnological products for the treatment of complement system disorders including paroxysmal nocturnal hemoglobinuria: currently available and in development

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