The plasma contact system, a protease cascade at the nexus of inflammation, coagulation and immunity

Weidmann, Henri; Heikaus, Laura; Long, Andy; Naudin, Clément; Schlüter, Hartmut; Renné, Thomas

doi:10.1016/j.bbamcr.2017.07.009

Cited by 114 publications

(110 citation statements)

References 96 publications

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“…The proteases of the contact pathway play a role in inflammatory and immune processes as well as in maintaining hemostasis [102]. Kallikrein cleaves high molecular weight kininogen to the pro-inflammatory bradykinin.…”

Section: Proteases and Diseasementioning

confidence: 99%

“…Several bacterial, viral, protozoan and fungal proteases trigger inflammation by activating the intrinsic coagulation pathway [102], or act as procoagulants by non-canonical, direct activation of prothrombin [179]. Large panels of small-molecule inhibitors of the proteasome in pathogenic organisms are currently being screened for potential therapeutic benefit and minimal toxicity toward the cellular machinery of the host [180].…”

Section: Proteases and Diseasementioning

confidence: 99%

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Proteases: Pivot Points in Functional Proteomics

Verhamme

Leonard

Perkins

2018

Functional Proteomics

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Proteases drive the life cycle of all proteins, ensuring the transportation and activation of newly minted, would-be proteins into their functional form while recycling spent or unneeded proteins. Far from their image as engines of protein digestion, proteases play fundamental roles in basic physiology and regulation at multiple levels of systems biology. Proteases are intimately associated with disease and modulation of proteolytic activity is the presumed target for successful therapeutics. “Proteases: Pivot Points in Functional Proteomics” examines the crucial roles of proteolysis across a wide range of physiological processes and diseases. The existing and potential impacts of proteolysis-related activity on drug and biomarker development are presented in detail. All told the decisive roles of proteases in four major categories comprising 23 separate sub-categories are addressed. Within this construct, 15 sets of subject-specific, tabulated data are presented that include identification of proteases, protease inhibitors, substrates and their actions. Said data are derived from and confirmed by over 300 references. Cross comparison of datasets indicates that proteases, their inhibitors/promoters and substrates intersect over a range of physiological processes and diseases, both chronic and pathogenic. Indeed, “Proteases: Pivot Points …” closes by dramatizing this very point through association of (pro)Thrombin and Fibrin(ogen) with: hemostasis, innate immunity, cardiovascular and metabolic disease, cancer, neurodegeneration and bacterial self-defense.

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Section: Proteases and Diseasementioning

confidence: 99%

Section: Proteases and Diseasementioning

confidence: 99%

Proteases: Pivot Points in Functional Proteomics

Verhamme

Leonard

Perkins

2018

Functional Proteomics

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“…The role of coagulation factor XII (FXII) in the interplay between the coagulation and the complement system has been suggested since the early 1980s . FXII is primarily produced in the liver by hepatocytes and further secreted and present in plasma as an 80 kDa single‐chain zymogen at a concentration of ~30 μg/mL . Upon binding of negatively charged surfaces, lipophilic surfaces or binding toward zinc ions, FXII is either auto‐ or proteolytically activated by the two downstream serine proteases, kallikrein and plasmin, that cleave the Arg353‐Val354 bond, thereby producing a two‐chain molecule (α‐FXIIa) consisting of a disulphide‐linked heavy and a light chain of 353 and 243 amino acids, respectively .…”

Section: Introductionmentioning

confidence: 99%

Contact activation‐induced complex formation between complement factor H and coagulation factor XIIa

Thangaraj

Christiansen

Graversen

et al. 2020

Journal of Thrombosis and Haemostasis

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Background The complement and coagulation systems share an evolutionary origin with many components showing structural homology. Certain components, including complement factor H (FH) and coagulation factor XII (FXII), have separately been shown to have auxiliary activities across the two systems. Objectives The interaction between FXII and FH was investigated. Methods Using enzyme‐linked immunosorbent assay (ELISA) and surface plasmon resonance (SPR) complex formation between different FXII forms and FH was investigated. The presence of α‐FXIIa:FH complexes upon contact activation in plasma was evaluated by ELISA and immunoprecipitation. Results We identified and characterized a direct interaction between the components and demonstrated that among different forms of FXII, only the activated α‐FXIIa formed complexes with FH, with an apparent binding strength Kd of 34 ± 9 nmol/L. The complex formation involved the kringle domain of the heavy chain of FXII. C1‐inhibitor induced inhibition of α‐FXIIa did not alter the binding of α‐FXIIa toward FH. We further demonstrated the presence of α‐FXIIa:FH complexes in normal human plasma upon contact activation, indicating formation of α‐FXIIa:FH complexes as a consequence of α‐FXIIa generation. Complex formation between α‐FXIIa and FH was also assessed in hereditary angioedema (HAE) patients with C1‐inhibitor deficiency as well as rheumatoid arthritis (RA) patients with high levels of anti‐cyclic citrullinated peptide (anti‐CCP) upon contact activation. We observed elevated levels of α‐FXIIa:FH complexes in HAE patients, and equal levels of complexes in RA patients and healthy individuals upon contact activation. Conclusion A direct interaction between α‐FXIIa and FH is demonstrated. Our findings represent a new crosstalk between these systems, potentially important in the onset and pathology of inflammatory vascular diseases.

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“…HK is detectable in porcine endometrium and human placenta . HK and its D5 peptides are implicated in the regulation of diverse functions relevant to normal pregnancy and PE pathogenesis including blood pressure regulation, smooth muscle contraction, coagulation, angiogenesis, immune response, immunity, and endothelial cell migration, proliferation, and apoptosis . HK is highly concentrated in the female reproductive tract and may be an important regulator of placental vascularization and nutrient transport to the fetus …”

Section: Introductionmentioning

confidence: 99%

“…17,19 HK and its D5 peptides are implicated in the regulation of diverse functions relevant to normal pregnancy and PE pathogenesis including blood pressure regulation, smooth muscle contraction, coagulation, angiogenesis, immune response, immunity, and endothelial cell migration, proliferation, and apoptosis. 11,20,21 HK is highly concentrated in the female reproductive tract and may be an important regulator of placental vascularization and nutrient transport to the fetus. 22 Previous biomarker studies compared HK protein and/or HKderived peptide levels in normal and hypertensive pregnancies, but interpretation of the results is confounded by differing methodologies and a lack of knowledge regarding kininogen dynamics in the course of normal pregnancy.…”

Section: Introductionmentioning

confidence: 99%

Differential processing of high‐molecular‐weight kininogen during normal pregnancy

Droll

Hsu²,

Drake

et al. 2020

Rapid Comm Mass Spectrometry

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Rationale Studies identified kininogen as a potential biomarker of preeclampsia, a major cause of adverse maternal outcomes. High‐molecular‐weight kininogen (HK) and its activated form participate in numerous pathways associated with establishing and maintaining pregnancy. However, dynamic changes in HK and naturally occurring HK‐derived peptides during the natural course of pregnancy are largely unknown. Methods Longitudinal serum samples during the course of normal pregnancy (trimesters T1, T2, T3) from 60 pregnant women were analyzed by western blot with an anti‐HK antibody. Circulating peptides in longitudinal serum specimens derived from 50 participants were enriched using nanoporous silica thin films. Peptides were identified by liquid chromatography/tandem mass spectrometry (LC/MS/MS) and database searching. Relative quantification was performed using MaxQuant and in‐house scripts. Normality was evaluated by either ANOVA or Friedman tests with p < 0.05 for statistical significance. Results Western blotting revealed that HK significantly decreased during normal pregnancy (T1 vs T2, p < 0.05; T1 vs T3, p < 0.0001). A 100 kDa intermediate increased during pregnancy (T1 vs T2, p < 0.005; T1 vs T3, p < 0.01). Moreover, the heavy chain (T1 vs T2, p < 0.0001; T1 vs T3, p < 0.0001; T2 vs T3, p < 0.01) and light chain (T1 vs T2, p < 0.0001; T1 vs T3, p < 0.0001; T2 vs T3, p < 0.05) significantly increased during pregnancy. LC/MS/MS analysis identified 180 kininogen‐1 peptides, of which 167 mapped to domain 5 (D5). Seventy‐three peptides with ten or more complete data sets were included for further analysis. Seventy peptides mapped to D5, and 3, 24, and 43 peptides showed significant decrease, no trend, and significant increase, respectively, during pregnancy. Conclusions This study demonstrates dynamic changes in HK and naturally occurring HK‐derived peptides during pregnancy. Our study sheds light on the gestational changes of HK and its peptides for further validation of them as potential biomarkers for pregnancy‐related complications.

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The plasma contact system, a protease cascade at the nexus of inflammation, coagulation and immunity

Cited by 114 publications

References 96 publications

Proteases: Pivot Points in Functional Proteomics

Proteases: Pivot Points in Functional Proteomics

Contact activation‐induced complex formation between complement factor H and coagulation factor XIIa

Differential processing of high‐molecular‐weight kininogen during normal pregnancy

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