Abstract

This project aims to provide proof-of-principle for the novel concept that the natural protein C pathway couples and coordinates the function of the hematopoietic system to the activation state of the blood coagulation system. We propose that the key components of the natural protein C anticoagulant and cytoprotective pathway, i.e. the endothelial protein C receptor (EPCR), the modulator of thrombin function thrombomodulin (Thbd), and the key effector protease of the protein C pathway, activated protein C (aPC), regulate in a physiologically relevant manner the function of hematopoietic stem and progenitor cells (HSPC). Expression of EPCR and Thbd on HSPC enables the hematopoietic system to sense and respond to the presence of the coagulation proteases thrombin and aPC generated in the HSPC micro-environment. As coagulation system activation is an intrinsic part of the response to injury, the protein C system adapts hematopoiesis to the specific challenges posed by inflammatory stress or similar pathological conditions.
AIM 1 is based on the novel observation that the protein C system protects HSPC against otherwise lethal radiation exposure, and investigates the mechanistic details mediating this protection against injury.
AIM 2 answers the question whether systemic alterations of coagulation system activity, as they may occur during inflammation, cancer, cardiovascular events, and many other disease, change the quality or quantity of the hematopoietic output;and whether this interaction between coagulation and hematopoiesis is again mediated through the activity of the protein C system.
AIM 3 investigates how the protein C pathway regulates the response of the hematopoietic system to chemokine- or inflammation-induced HSPC mobilization. Pilot studies suggest that the protein C pathway may have profound effects on the efficacy of clinically employed mobilization protocols for stem cells, and may provide signals to hematopoietic stem cells that trigger the rapid production of regulatory immune cells. To test these hypotheses we utilize genetically engineered mice lacking the key receptors EPCR and Thbd, and conduct in vivo tests that reveal how disruption of the protein C pathway, or pharmacologic manipulation thereof by infusion of aPC, affects hematopoiesis. Beyond documenting a novel physiologic connection between blood coagulation and hematopoiesis, outcomes of the study lay the groundwork for the rationale design of therapeutic applications and interventions targeting this cross-talk. These discoveries have the potential to significantly impact the current understanding of hematopoiesis and approaches to its pharmacologic manipulation.

Public Health Relevance

The study investigates a novel interaction between the blood coagulation mechanism and the function of the hematopoietic system, that is mediated by the natural protein C pathway, and points to novel approaches towards improving transfusion protocols, emerging cellular therapies, and immune functions of hematopoietic stem cells.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Program Projects (P01)
Project #
2P01HL044612-21
Application #
8063271
Study Section
Heart, Lung, and Blood Initial Review Group (HLBP)
Project Start
Project End
Budget Start
2010-12-01
Budget End
2011-11-30
Support Year
21
Fiscal Year
2011
Total Cost
$324,718
Indirect Cost

  Institution

Name
Bloodcenter of Wisconsin, Inc.
Department
Type
DUNS #
057163172
City
Milwaukee
State
WI
Country
United States
Zip Code
53233

  Publications

Zeng, Hu; Yu, Mei; Tan, Haiyan et al. (2018) Discrete roles and bifurcation of PTEN signaling and mTORC1-mediated anabolic metabolism underlie IL-7-driven B lymphopoiesis. Sci Adv 4:eaar5701
Kanaji, Sachiko; Orje, Jennifer N; Kanaji, Taisuke et al. (2018) Humanized GPIb?-von Willebrand factor interaction in the mouse. Blood Adv 2:2522-2532
Baumgartner, C K; Mattson, J G; Weiler, H et al. (2017) Targeting factor VIII expression to platelets for hemophilia A gene therapy does not induce an apparent thrombotic risk in mice. J Thromb Haemost 15:98-109
Zhang, Nanyan; Zhi, Huiying; Curtis, Brian R et al. (2016) CRISPR/Cas9-mediated conversion of human platelet alloantigen allotypes. Blood 127:675-80
Chen, Yuhong; Zheng, Yongwei; You, Xiaona et al. (2016) Kras Is Critical for B Cell Lymphopoiesis. J Immunol 196:1678-85
Newman, Debra K; Fu, Guoping; Adams, Tamara et al. (2016) The adhesion molecule PECAM-1 enhances the TGF-?-mediated inhibition of T cell function. Sci Signal 9:ra27
Chen, Yingyu; Schroeder, Jocelyn A; Chen, Juan et al. (2016) The immunogenicity of platelet-derived FVIII in hemophilia A mice with or without preexisting anti-FVIII immunity. Blood 127:1346-54
Santoso, Sentot; Wihadmadyatami, Hevi; Bakchoul, Tamam et al. (2016) Antiendothelial ?v?3 Antibodies Are a Major Cause of Intracranial Bleeding in Fetal/Neonatal Alloimmune Thrombocytopenia. Arterioscler Thromb Vasc Biol 36:1517-24
Zhi, Huiying; Dai, Jing; Liu, Junling et al. (2015) Platelet Activation and Thrombus Formation over IgG Immune Complexes Requires Integrin ?IIb?3 and Lyn Kinase. PLoS One 10:e0135738
Liang, Hai Po H; Kerschen, Edward J; Basu, Sreemanti et al. (2015) Coagulation factor V mediates inhibition of tissue factor signaling by activated protein C in mice. Blood 126:2415-23

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