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A unique catalyst for ischemia-reperfusion injury prevention

 
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A mechanism of action targeting the IRI cascade

Reducing reactive oxygen species (ROS) damage and inflammation

 

FDY-5301’s unique properties are well-suited to mitigate ischemia-reperfusion injury (IRI).

In preclinical IRI models FDY-5301, a formulation of sodium iodide, reduced tissue damage, infarct size, and inflammation. Iodide functions as a catalytic neutralizer of hydrogen peroxide (H2O2), a prominent reactive oxygen species (ROS) implicated in the IRI cascade leading to cardiomyocyte death. Iodide also acts as an immunomodulating agent.

 

A potentially powerful intervention

Iodide naturally redistributes in humans following stress. FDY-5301 enhances this response by increasing the body’s natural blood iodide levels by 1000-fold.

Sodium iodide catalytically destroys hydrogen peroxide and beneficially modulates inflammatory pathways by reducing ROS damage and inflammation. These characteristics enable FDY-5301 to potentially target the multiple pathways that cause ischemia-reperfusion injury simultaneously.

Prior to reperfusion
GIF showing animation of FDY-5201 reaching anticipated therapeutic levels in blood stream

FDY-5301 is easy to deliver prior to reperfusion and rapidly reaches anticipated therapeutic levels.

In seconds
GIF animation showing the hydrogen peroxide being destroyed in heart muscle fibers.

FDY-5301 catalytically destroys hydrogen peroxide (H2O2) to reduce cell death due to ROS burst upon reperfusion.

In minutes to hours
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FDY-5301 reduces migration of neutrophils into the damaged tissue.

In hours to days
GIF animation of a heart regaining function (going from cold to warm)

FDY-5301 reduces the cardiac inflammatory response.

 

A multi-faceted strategy for limiting IRI

By attenuating ROS, reducing neutrophil migration, and modulating the immune response, FDY-5301 is a multi-faceted strategy for limiting IRI, potentially reducing infarct size following myocardial infarction treated by PCI.

Blood cells floating through body (with reduced Nephs)

Anterior STEMI typically represents an acute occlusion of the most vital coronary artery, the left anterior descending, and its reperfusion by PCI is believed to have the most IRI-mediated damage among heart attacks as well as risk of subsequent heart failure. The potential clinical impact of IRI in anterior STEMI is being investigated in a Phase 3 clinical trial, Iocyte AMI-3.


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