Abstract

Treatment of acute ischemic stroke with tPA can significantly improve neurological outcomes. However, many patients do not recanalize with one recent study showing that only 53% of patients receiving IV tPA were recanalized at 24 hours. And while endovascular therapy can significantly increase reperfusion rates in patients with large vessel disease, not all occlusions are accessible for endovascular treatment and many community hospitals are not able to perform these procedures. Thus, for many patients thrombolysis remains the only treatment option. In addition to the limited efficacy of tPA, thrombolysis carries a small but significant risk of symptomatic intracerebral hemorrhage (sICH), increasing from ~0.5% in untreated patients to up to 5% in some studies. Importantly, the risk of fatal ICH with thrombolysis rises to ~2% in patients treated with the current recommended dose of tPA. Studies with lower doses of tPA show a reduction in sICH however these studies have not demonstrated noninferiority of the lower dose compared to standard therapy. In contrast to stroke, dosing recommendations of thrombolytic tPA for myocardial infarction or pulmonary embolism can be nearly 2-fold higher than the dose for ischemic stroke, suggesting that the balance between safety and efficacy in stroke may limit the potential efficacy of tPA. Thus, understanding the molecular pathways triggered by thrombolytic tPA that increase the incidence of hemorrhagic conversion could profoundly improve the treatment of ischemic stroke. By targeting these pathways and reducing the risk of sICH it should be possible to not only make thrombolysis safer but also to make it more effective by permitting increased doses of tPA to be used to promote reperfusion in more patients. In earlier work, we established an association between tPA?mediated cell signaling in the neurovascular unit (NVU) and blood brain barrier (BBB) regulation. Acting through tPA cleavage and activation of platelet- derived growth factor C (PDGF-C) and binding of active PDGF-C to the PDGF receptor ? (PDGFR?) on perivascular astrocytes, this pathways induces increased vascular permeability and thrombolysis associated hemorrhage. In the present application we present data demonstrating that tPA mediated PDGFR? signaling in perivascular astrocytes enhances the activity of VEGF-A in the neurovascular unit leading to BBB breakdown through disruption of endothelial cell tight junction complexes. This hypothesis is based upon strong preliminary data linking tPA to the phosphorylation of the tight junction protein occludin at S490 and to increased BBB permeability. This activity is dependent on PKC?, and inhibition PKC? or expression of a non- phosphorylatable occludin mutant, significantly reduces thrombolytic tPA-associated ICH in a murine model of thrombotic stroke with thrombolysis.

Public Health Relevance

Worldwide more than 15 million people who suffer from stroke each year, with nearly 800,000 patients in the U.S. The standard treatment for a stroke caused by a blood clot is lysis of the clot with tissue plasminogen activator (tPA). However, in patients treated with tPA only approximately 50% have restoration of blood flow, and treatment with tPA carries a significant risk of bleeding in the brain. The studies proposed here will investigate pathways that induce bleeding in the brain and may identify drugs that will permit safer and more effective treatments for stroke.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL055374-21
Application #
9996762
Study Section
Hemostasis and Thrombosis Study Section (HT)
Program Officer
Sarkar, Rita
Project Start
1995-08-01
Project End
2023-06-30
Budget Start
2020-07-01
Budget End
2021-06-30
Support Year
21
Fiscal Year
2020
Total Cost
Indirect Cost

  Institution

Name
University of Michigan Ann Arbor
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
073133571
City
Ann Arbor
State
MI
Country
United States
Zip Code
48109

  Publications

Waack, Ursula; Warnock, Mark; Yee, Andrew et al. (2018) CpaA Is a Glycan-Specific Adamalysin-like Protease Secreted by Acinetobacter baumannii That Inactivates Coagulation Factor XII. MBio 9:
Bondu, Virginie; Bitting, Casey; Poland, Valerie L et al. (2018) Upregulation of P2Y2R, Active uPA, and PAI-1 Are Essential Components of Hantavirus Cardiopulmonary Syndrome. Front Cell Infect Microbiol 8:169
Wahlgren, N; Thorén, M; Höjeberg, B et al. (2017) Randomized assessment of imatinib in patients with acute ischaemic stroke treated with intravenous thrombolysis. J Intern Med 281:273-283
Bohannon, Kevin P; Bittner, Mary A; Lawrence, Daniel A et al. (2017) Slow fusion pore expansion creates a unique reaction chamber for co-packaged cargo. J Gen Physiol 149:921-934
Su, Enming Joseph; Cao, Chunzhang; Fredriksson, Linda et al. (2017) Microglial-mediated PDGF-CC activation increases cerebrovascular permeability during ischemic stroke. Acta Neuropathol 134:585-604
Fredriksson, Linda; Lawrence, Daniel A; Medcalf, Robert L (2017) tPA Modulation of the Blood-Brain Barrier: A Unifying Explanation for the Pleiotropic Effects of tPA in the CNS. Semin Thromb Hemost 43:154-168
Carlson, Karen-Sue B; Nguyen, Lan; Schwartz, Kat et al. (2016) Neuroserpin Differentiates Between Forms of Tissue Type Plasminogen Activator via pH Dependent Deacylation. Front Cell Neurosci 10:154
Lewandowski, Sebastian A; Fredriksson, Linda; Lawrence, Daniel A et al. (2016) Pharmacological targeting of the PDGF-CC signaling pathway for blood-brain barrier restoration in neurological disorders. Pharmacol Ther 167:108-119
Medcalf, Robert L; Lawrence, Daniel A (2016) Editorial: The Role of the Plasminogen Activating System in Neurobiology. Front Cell Neurosci 10:222
Szabo, R; Samson, A L; Lawrence, D A et al. (2016) Passenger mutations and aberrant gene expression in congenic tissue plasminogen activator-deficient mouse strains. J Thromb Haemost 14:1618-28

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