Coagulation factor V mediates inhibition of tissue factor signaling by activated protein C in mice

Liang, Hai; Kerschen, E. J.; Basu, Sreemanti; Hernández, Irene; Zogg, Mark; Song, Jia; Hessner, Martin J.; Toso, Raffaella; Rezaie, Alireza R.; Fernández, José A.; Camire, Rodney M.; Ruf, Wolfram; Griffin, John H.; Weiler, Hartmut

doi:10.1182/blood-2015-05-644401

Cited by 28 publications

(32 citation statements)

References 57 publications

(80 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Additionally, the PROWESS trial found heterozygous factor V leiden carriers displayed reduced mortality in the setting of sepsis(22). In subsequent mouse studies, Liang et al identified protein C cleaved factor V as a crucial cofactor inhibiting a novel inflammatory tissue factor signaling pathway mediated by activated protein C(23). Discovery of factor V’s role in a new murine protein C mediated inflammatory pathway is exciting and insinuates factor V may play an even larger function in dictating the balance of hypocoagulability, hypercoagulability, and inflammation after trauma.…”

Section: Discussionmentioning

confidence: 99%

Individual clotting factor contributions to mortality following trauma

Kunitake

Howard

Kornblith

et al. 2017

Journal of Trauma and Acute Care Surgery

View full text Add to dashboard Cite

BACKGROUND Acute traumatic coagulopathy (ATC) afflicts 20–30% of trauma patients, but the extensive collinearity of the coagulation cascade complicates attempts to clarify global clotting factor dysfunction. This study aims to characterize phenotypes of clotting factor dysfunction and their contributions to mortality after major trauma. METHODS This prospective cohort study examines all adult trauma patients of the highest activation level presenting to San Francisco General Hospital between 2/2005 and 2/2015. Factors II, V, VII, VIII, IX, X, and protein C activity on admission and mortality status at 28 days were assessed. Predictors of 28-day mortality in univariate analysis were included in multiple logistic regression controlling for traumatic brain injury (TBI), acidosis, age, and mechanism of injury. Principal component analysis (PCA) was utilized to identify phenotypic coagulation. RESULTS Complete coagulation factor data was available for 876/1,429 (61%). In multiple logistic regression, factors V (OR: 0.86, CI95%: 0.76–0.97), VIII (OR: 0.97, CI95%: 0.95–0.99), X (OR: 0.79, CI95%: 0.68–0.92), and protein C (OR: 1.17, CI95%: 1.05–1.30) significantly predicted 28-day mortality after controlling for age, base deficit, mechanism of injury, and TBI. PCA identified 2 significant principal components (Phenotypes 1 and 2) that accounted for 66.3% of the total variance. Phenotype 1 (factors II, VII, IX, X, and protein C abnormalities) explained 49.3% and was associated with increased injury, coagulopathy, TBI, and mortality. Phenotype 2 (factors V and VIII abnormalities) explained 17.0% and was associated with increased coagulopathy, blunt injury, and mortality. Only Phenotype 2 remained significantly associated with 28-day mortality in multiple logistic regression. CONCLUSIONS PCA identified 2 distinct phenotypes within the entirety of global clotting factor abnormalities, and these findings substantiate the crucial association of factors V and VIII on mortality following trauma. This may be the first step toward identifying unique phenotypes after injury and personalizing hemostatic resuscitation. LEVEL OF EVIDENCE Prognostic study, Level III

show abstract

Section: Discussionmentioning

confidence: 99%

Individual clotting factor contributions to mortality following trauma

Kunitake

Howard

Kornblith

et al. 2017

Journal of Trauma and Acute Care Surgery

View full text Add to dashboard Cite

show abstract

“…In the presence of NAPc2, the TF-induced TRIF response was not only preserved, but stabilization of the ternary complex with NAPc2 prevented the suppression of TF signaling by aPC. This signaling role of aPC is, similar to aPC anticoagulant activity, dependent on protein S as well as FV anticoagulant cofactor function that is lost in FV Leiden (90). These data suggest that EPCR ligand occupancy by either FXa or aPC determines TLR4-TRIF activation and indicate a control switch function for EPCR in the hardwiring of innate immune and coagulation signaling.…”

Section: Coagulation Signaling Of Immune Cellsmentioning

confidence: 96%

Targeting clotting proteins in cancer therapy – progress and challenges

Ruf

Rothmeier

Graf

2016

Thrombosis Research

Self Cite

View full text Add to dashboard Cite

Cancer-associated thrombosis remains a significant complication in the clinical management of cancer and interactions of the hemostatic system with cancer biology continue to be elucidated. Here, we review recent progress in our understanding of tissue factor (TF) regulation and procoagulant activation, TF signaling in cancer and immune cells, and the expanding roles of the coagulation system in stem cell niches and the tumor microenvironment. The extravascular functions of coagulant and anti-coagulant pathways have significant implications not only for tumor progression, but also for the selection of appropriate target specific anticoagulants in the therapy of cancer patients.

show abstract

“…144–146 Blood coagulation and primary hemostasis evolved as important defense mechanisms to prevent bleeding, 147 and a primary function of the vascular TM/aPC/EPCR pathway is to counterbalance intravascular thrombosis and maintain endothelial quiescence. With new functions emerging in our understanding of EPCR in BM LT-HSCs and the challenge of deciphering the mechanisms of the tight regulation by distinct PAR1 signaling, 6 new questions arise on the relevance of the hemostatic system for human stem cell physiology, and future studies will enhance our understanding of the role of PAR1 and NO signaling in clinical G-CSF– and AMD3100-induced HSPC mobilization.…”

Section: Concluding Remarks and Perspectivesmentioning

confidence: 99%

“…Since the first cloning and identification of EPCR as the physiological receptor for the powerful anticoagulant aPC 143 and the discovery of EPCR/aPC/PAR1 anticoagulant signaling, 14 additional evidence emerged for a close interaction between the coagulation systems and inflammation, cellular metabolism, angiogenesis, and innate immunity. [144][145][146] Blood coagulation and primary hemostasis evolved as important defense mechanisms to prevent bleeding, 147 and a primary function of the vascular TM/aPC/EPCR pathway is to counterbalance intravascular thrombosis and maintain endothelial quiescence. With new functions emerging in our understanding of EPCR in BM LT-HSCs and the challenge of deciphering the mechanisms of the tight regulation by distinct PAR1 signaling, 6 new questions arise on the relevance of the hemostatic system for human stem cell physiology, and future studies will enhance our understanding of the role of PAR1 and NO signaling in clinical G-CSF-and AMD3100-induced HSPC mobilization.…”

Section: Concluding Remarks and Perspectivesmentioning

confidence: 99%

Regulation of long‐term repopulating hematopoietic stem cells by EPCR/PAR1 signaling

Gur-Cohen

Graf

Esmon

et al. 2016

Annals of the New York Academy of Sciences

Self Cite

View full text Add to dashboard Cite

The common developmental origin of endothelial and hematopoietic cells is manifested by coexpression of several cell surface receptors. Adult murine bone marrow (BM) long-term repopulating hematopoietic stem cells (LT-HSCs), endowed with the highest repopulation and self-renewal potential, express endothelial protein C receptor (EPCR), which is used as a marker to isolate them. EPCR/PAR1 signaling in endothelial cells has anticoagulant and anti-inflammatory roles, while thrombin/PAR1 signaling induces coagulation and inflammation. Recent studies define two new PAR1-mediated signaling cascades that regulate EPCR+ LT-HSC BM retention and egress. EPCR/PAR1 signaling facilitates LT-HSC BM repopulation, retention, survival, and chemotherapy resistance by restricting nitric oxide (NO) production, maintaining NOlow LT-HSC BM retention with increased VLA4 expression, affinity, and adhesion. Conversely, acute stress and clinical mobilization upregulate thrombin generation and activate different PAR1 signaling which overcomes BM EPCR+ LT-HSC retention, inducing their recruitment to the bloodstream. Thrombin/PAR1 signaling induces NO generation, TACE-mediated EPCR shedding, and upregulation of CXCR4 and PAR1, leading to CXCL12-mediated stem and progenitor cell mobilization. This review discusses new roles for factors traditionally viewed as coagulation related, which independently act in the BM to regulate PAR1 signaling in bone- and blood-forming progenitor cells, navigating their fate by controlling NO production.

show abstract

Coagulation factor V mediates inhibition of tissue factor signaling by activated protein C in mice

Cited by 28 publications

References 57 publications

Individual clotting factor contributions to mortality following trauma

Individual clotting factor contributions to mortality following trauma

Targeting clotting proteins in cancer therapy – progress and challenges

Regulation of long‐term repopulating hematopoietic stem cells by EPCR/PAR1 signaling

Contact Info

Product

Resources

About