Proteolytic properties of single-chain factor XII: a mechanism for triggering contact activation

Ivanov, Ivan; Matafonov, Anton; Sun, Mao-fu; Cheng, Qiufang; Dickeson, S. Kent; Verhamme, Ingrid M.; Emsley, Jonas; Gailani, David

doi:10.1182/blood-2016-10-744110

Cited by 76 publications

(136 citation statements)

References 53 publications

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“…While coagulation through the intrinsic pathway begins with fXII activation, the mechanism that initiates the process has been uncertain. The data presented here suggest that fXII expresses sufficient proteolytic activity in its single-chain form to initiate surface-dependent contact activation [69**]. Given the low level of activity relative to α-fXIIa, sc-fXII activity is probably most important early in contact activation.…”

Section: Conclusion and Future Considerationsmentioning

confidence: 99%

“…The consequences of cleavage after Arg343 are not clear. To test the hypothesis that sc-fXII is a protease, we replaced Arg334, Arg343, and Arg353 with alanine [69**]. The resulting protein, designated fXII-T (for “triple” mutant), does not undergo autocatalysis to α-fXIIa in the presence of polyphosphate, and is resistant to cleavage by α-kal and fXIIa.…”

Section: Factor XII Activationmentioning

confidence: 99%

“…When wild type fXII (fXII-WT) is mixed with PPK at plasma concentrations there is reciprocal conversion of the proteins to α-fXIIa and α-kal (Figure 4A) [69**,70]. Initiation of this process is often attributed to traces of α-fXIIa in fXII preparations.…”

Section: The Activity Of Fxii-tmentioning

confidence: 99%

“…Initiation of this process is often attributed to traces of α-fXIIa in fXII preparations. However, when fXII-WT is replaced by fXII-T, PPK is still converted to α-kal, although at a lower rate than with fXII-WT [69**]. PPK activation by fXII-T turns out to be four orders of magnitude slower than with α-fXIIa.…”

Section: The Activity Of Fxii-tmentioning

confidence: 99%

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Single-chain factor XII: a new form of activated factor XII

Ivanov

Matafonov

Gailani

2017

Current Opinion in Hematology

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Purpose Exposure of blood to foreign surfaces induces reciprocal conversion of the plasma proteins factor XII (fXII) and plasma prekallikrein (PPK) to the proteases α-fXIIa and α-kallikrein. This process, called contact activation, has a range of effects on host defense mechanisms, including promoting coagulation. The nature of the triggering mechanism for contact activation is debated. One hypothesis predicts that fXII has protease activity, either intrinsically or upon surface-binding, that initiates contact activation. We tested this by assessing the proteolytic activity of a recombinant fXII variant that cannot be converted to α-fXIIa. Recent findings The proteolytic activity of fXII-T (for “triple” mutant), a variant with alanine substitutions for arginine at activation cleavage sites (Arg334, Arg344, and Arg353) was tested with known α-fXIIa substrates. FXII-T activates PPK in solution, and the reaction is enhanced by polyphosphate, an inducer of contact activation released from platelets. In the presence of polyphosphate, fXII-T converts fXII to α-fXIIa, and also converts the coagulation protein factor XI to its active form. Summary The findings support the hypothesis that contact activation is initiated through activity intrinsic to single-chain fXII, and indicate that pre-existing α-fXIIa is not required for induction of contact activation.

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Section: Conclusion and Future Considerationsmentioning

confidence: 99%

Section: Factor XII Activationmentioning

confidence: 99%

Section: The Activity Of Fxii-tmentioning

confidence: 99%

Section: The Activity Of Fxii-tmentioning

confidence: 99%

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Single-chain factor XII: a new form of activated factor XII

Ivanov

Matafonov

Gailani

2017

Current Opinion in Hematology

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“…n In this issue of Blood, Gluckman et al confirm the role of HLA identical sibling transplantation in sickle cell disease (SCD) with a 5-year overall survival of 95% when performed at an early age (,16 years) and using bone marrow as the source of stem cells. 1 A lthough SCD is the most common inherited hemoglobinopathy worldwide, and most patients suffer from life-threatening complications, fewer transplants have been performed compared with the number carried out for thalassemia major. Past indications for stem cell transplantation (SCT) reserved this procedure for patients with significant sicklerelated morbidity, such as recurrent pain crises leading to multiple hospitalizations, stroke or acute chest syndrome, sickle lung disease, and sickle nephropathy.…”

mentioning

confidence: 99%

Contact ignition by single-chain XIIa

Meijers

2017

Blood

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Mechanisms for Reduced Fibrin Clot Formation on Liquid‐Infused Surfaces

Hong

Ruhoff

Mathur

et al. 2022

Adv Healthcare Materials

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Biomedical devices are prone to blood clot formation (thrombosis), and liquid-infused surfaces (LIS) are effective in reducing the thrombotic response. However, the mechanisms that underpin this performance, and in particular the role of the lubricant, are not well understood. In this work, it is investigated whether the mechanism of LIS action is related to i) inhibition of factor XII (FXII) activation and the contact pathway; ii) reduced fibrin density of clots formed on surfaces; iii) increased mobility of proteins or cells on the surface due to the interfacial flow of the lubricant. The chosen LIS is covalently tethered, nanostructured layers of perfluorocarbons, infused with thin films of medical-grade perfluorodecalin (tethered-liquid perfluorocarbon), prepared with chemical vapor deposition previously optimized to retain lubricant under flow. Results show that in the absence of external flow, interfacial mobility is inherently higher at the liquid-blood interface, making it a key contributor to the low thrombogenicity of LIS, as FXII activity and fibrin density are equivalent at the interface. The findings of this study advance the understanding of the anti-thrombotic behavior of LIS-coated biomedical devices for future coating design. More broadly, enhanced interfacial mobility may be an important, underexplored mechanism for the anti-fouling behavior of surface coatings.

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Proteolytic properties of single-chain factor XII: a mechanism for triggering contact activation

Cited by 76 publications

References 53 publications

Single-chain factor XII: a new form of activated factor XII

Single-chain factor XII: a new form of activated factor XII

Contact ignition by single-chain XIIa

Mechanisms for Reduced Fibrin Clot Formation on Liquid‐Infused Surfaces

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