The Serine Protease Domain of MASP-3: Enzymatic Properties and Crystal Structure in Complex with Ecotin

Gaboriaud, Christine; Gupta, Rajesh Kumar; Martin, Lydie; Lacroix, Monique; Serre, Laurence; Teillet, F; Arlaud, Gérard J.; Rossi, Véronique; Thielens, Nicole M.

doi:10.1371/journal.pone.0067962

Cited by 21 publications

(25 citation statements)

References 64 publications

(112 reference statements)

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“…We could not detect any inhibition of C1r, while ecotin inhibited C1s with a 25.15±4.45 μM K I value representing a very weak inhibition. These findings are in agreement with previous SPR-based results of Gaboriaud et al [23] who immobilized ecotin on the chip and by injecting up to 2 μM C1s or C1r catalytic fragments, did not detect any interaction.…”

Section: E Coli Ecotin Is a Weak Inhibitor Of C1s While It Is Inactisupporting

confidence: 93%

“…Ecotin orthologs are potent inhibitors of MASP-2 with K I values in the 10 −8 -10 −9 M range ( Fig 1, Table 1). E. coli ecotin inhibits MASP-2 with a K I of 11 nM, which is close to the SPRbased K D value of 24.7 nM reported by Gaboriaud et al [23]. Importantly, most ecotin orthologs are as good, or even better MASP-2 inhibitors than SGMI-2, a monospecific, high-affinity inhibitor of the enzyme we developed previously via directed evolution [21].…”

Section: Ecotin Orthologs Are Potent Masp-2 Inhibitorssupporting

confidence: 85%

“…It is worth noting that, by using SPR, Gaboriaud et al measured a much weaker, 600 nM affinity between E. coli ecotin and MASP-3 [23]. An important difference between the two experiments is that they used a single MASP-3 SP domain construct, which lacked even the SP-structure stabilizing activation peptide.…”

Section: Ecotin Orthologs Are Highly Potent Masp-3 Inhibitorsmentioning

confidence: 99%

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Ecotin, a microbial inhibitor of serine proteases, blocks multiple complement dependent and independent microbicidal activities of human serum

et al. 2019

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Ecotin is a serine protease inhibitor produced by hundreds of microbial species, including pathogens. Here we show, that ecotin orthologs from Escherichia coli, Yersinia pestis, Pseudomonas aeruginosa and Leishmania major are potent inhibitors of MASP-1 and MASP-2, the two key activator proteases of the complement lectin pathway. Factor D is the key activator protease of another complement activation route, the alternative pathway. We show that ecotin inhibits MASP-3, which is the sole factor D activator in resting human blood. In pathway-specific ELISA tests, we found that all ecotin orthologs are potent lectin pathway inhibitors, and at high concentration, they block the alternative pathway as well. In flow cytometry experiments, we compared the extent of complement-mediated opsonization and lysis of wild-type and ecotin-knockout variants of two E. coli strains carrying different surface lipopolysaccharides. We show, that endogenous ecotin provides significant protections against these microbicidal activities for both bacteria. By using pathway specific complement inhibitors, we detected classical-, lectin-and alternative pathway-driven complement attack from normal serum, with the relative contributions of the activation routes depending on the lipopolysaccharide type. Moreover, in cell proliferation experiments we observed an additional, complement-unrelated antimicrobial activity exerted by heat-inactivated serum. While ecotin-knockout cells are highly vulnerable to these activities, endogenous ecotin of wild-type bacteria provides complete protection against the lectin pathwayrelated and the complement-unrelated attack, and partial protection against the alternative pathway-related damage. In all, ecotin emerges as a potent, versatile self-defense tool that blocks multiple antimicrobial activities of the serum. These findings suggest that ecotin might be a relevant antimicrobial drug target.Bloodstream infections are major cause of morbidity and mortality in many countries around the globe. As the number of multi-drug resistant pathogenic strains is growing, it is urgent to identify their virulence factors and unveil the corresponding mechanisms of action that enable the pathogen to avoid potent immune response. A microbial inhibitor of serine proteases, ecotin was previously implicated in protecting various pathogenic bacteria and eukaryotic Leishmania species against the host immune system by inhibiting leukocyte elastase. However, the interaction of ecotin with the complement system, which provides a first line defense against pathogens, remained unexplored. We found that ecotin blocks activation of the complement lectin pathway by inhibiting its key activator enzymes, MASP-1 and MASP-2. Furthermore, by inhibiting MASP-3, ecotin also disrupts a fundamental link between the lectin-and the alternative pathways. We provide evidence that E. coli cells devoid of ecotin are extremely vulnerable to complement-mediated lysis and they are also potently killed by some complement-independent antimicrobial factors o...

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Section: E Coli Ecotin Is a Weak Inhibitor Of C1s While It Is Inactisupporting

confidence: 93%

Section: Ecotin Orthologs Are Potent Masp-2 Inhibitorssupporting

confidence: 85%

Section: Ecotin Orthologs Are Highly Potent Masp-3 Inhibitorsmentioning

confidence: 99%

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Ecotin, a microbial inhibitor of serine proteases, blocks multiple complement dependent and independent microbicidal activities of human serum

et al. 2019

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“…Inhibition of the LP is influenced by MASP-3, MAp44, and MAp19 proteins, which share high sequence homology with MASP-1 and -2 and have similar binding affinity to MBL and ficolins ( 70 , 86 ). These proteins may compete with MASP-1 and -2, but are unable to cleave MASP, C2, and C4 preventing further activation of the LP cascade (Figure 4 D).…”

Section: Structural Basis Of Complement Activation and Regulationmentioning

confidence: 99%

Complement System Part I â€“ Molecular Mechanisms of Activation and Regulation

et al. 2015

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Complement is a complex innate immune surveillance system, playing a key role in defense against pathogens and in host homeostasis. The complement system is initiated by conformational changes in recognition molecular complexes upon sensing danger signals. The subsequent cascade of enzymatic reactions is tightly regulated to assure that complement is activated only at specific locations requiring defense against pathogens, thus avoiding host tissue damage. Here, we discuss the recent advances describing the molecular and structural basis of activation and regulation of the complement pathways and their implication on physiology and pathology. This article will review the mechanisms of activation of alternative, classical, and lectin pathways, the formation of C3 and C5 convertases, the action of anaphylatoxins, and the membrane-attack-complex. We will also discuss the importance of structure–function relationships using the example of atypical hemolytic uremic syndrome. Lastly, we will discuss the development and benefits of therapies using complement inhibitors.

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“…The structure of zymogen MASP-3 also shows that the CCP1-CCP2 and the CCP2-SP interfaces have some flexibility. Interestingly, while mutant proenzyme and inhibited active MASP-3 (Gaboriaud et al, 2013) fragments have been crystallized successfully, the wild-type enzyme by itself has so far resisted crystallization.…”

Section: Proenzyme Masp Structuresmentioning

confidence: 99%

Multiple roles of complement MASP-1 at the interface of innate immune response and coagulation

Dobó

Schroeder

Jenny

et al. 2014

Molecular Immunology

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MASP-1 is a versatile serine protease that cleaves a number of substrates in human blood. In recent years it became evident that besides playing a crucial role in complement activation MASP-1 also triggers other cascade systems and even cells to mount a more powerful innate immune response. In this review we summarize the latest discoveries about the diverse functions of this multi-faceted protease. Recent studies revealed that among MBLassociated serine proteases, MASP-1 is the one responsible for triggering the lectin pathway via its ability to rapidly autoactivate then cleave MASP-2, and possibly MASP-3. The crystal structure of MASP-1 explains its more relaxed substrate specificity compared to the related complement enzymes. Due to the relaxed specificity, MASP-1 interacts with the coagulation cascade and the kinin generating system, and it can also activate endothelial cells eliciting pro-inflammatory signaling.

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The Serine Protease Domain of MASP-3: Enzymatic Properties and Crystal Structure in Complex with Ecotin

Cited by 21 publications

References 64 publications

Ecotin, a microbial inhibitor of serine proteases, blocks multiple complement dependent and independent microbicidal activities of human serum

Ecotin, a microbial inhibitor of serine proteases, blocks multiple complement dependent and independent microbicidal activities of human serum

Complement System Part I â€“ Molecular Mechanisms of Activation and Regulation

Multiple roles of complement MASP-1 at the interface of innate immune response and coagulation

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