Bladder Function Restored in Animals with Severe Spinal Cord Injury

Posted: Published on June 26th, 2013

This post was added by Dr Simmons

Newswise For the first time, researchers have restored significant bladder function through nerve regeneration in rats with the most severe spinal cord injuries (SCI). The breakthrough paired a traditional nerve bridge graft with a novel combination of scar degrading and growth factor treatments to grow new nerve cells from the thoracic level to the lower spinal cord region. Details of the discovery appear in the June 26 issue of the Journal of Neuroscience.

Neuroscientists from Case Western Reserve University School of Medicine and Cleveland Clinic built a regeneration bridge across a lesion in animals with complete gap transections of their spinal cords. Although the animals did not regain the ability to walk, the procedure did allow them to recover a strong level of bladder control.

Jerry Silver, PhD, professor of neurosciences at the School of Medicine, and Yu-Shang Lee, PhD, assistant staff scientist in the Lerner Research Institute of Cleveland Clinic, created the bridge using a scaffold of multiple segments of the animals own peripheral nerves. Key to the regeneration was surrounding the graft and both spinal cord stumps with a stimulating growth factor and an enzyme to dissolve scar tissue, which inhibits the nerve fibers from crossing over the bridge and traveling down the spinal cord.

While urinary control is complex and recovery took several months, it was clear that this primitive function lost to spinal cord injury does possess the capacity to rewire itself, even when a relatively small number of axons are regenerated, Silver said.

The spinal cords role in bladder function is critical, as it relays information between the brain and body. After suffering SCI, urinary dysfunction occurs. The loss of control happens because the axons, or nerve fibers which transmit information from neuron to neuron, are disconnected from the brain stem where the bodys urination commands reside.

The creation of the neural bridge, which spans the open cavity between the severed ends of the spinal cord, kills the axons that normally reside within the nerve. However, the glial cells of the bridge, called Schwann cells, which form an aligned growth promoting pathway, remain alive in the nerve and encourage the severed nearby axons in the spinal cord to enter the bridge and regrow.

Establishing functional regeneration across the gap and down the rats spinal cord presented challenges. The first obstacle was coaxing the regenerating axons to enter and transcend the bridge. Then the axons had to grow well beyond the bridge and form connections capable of relaying nerve signals once they arrived at their destination approximately two centimeters down the spinal cord.

To achieve these results, Silver and Lee added Fibroblast Growth Factor to help align the Schwann cells in the graft with the scar tissue cells at the bridges interfaces. Next, they injected an enzyme called chondroitinase to break down inhibitory molecules that often form in scar tissue and curtail regeneration at both ends of the bridge.

We were especially surprised and excited to discover that once a permissive environment was created, a subset of neurons situated largely within the brainstem, which play important roles in bladder function, slowly re-grew lengthy axons far down the cord, said Dr. Silver.

The model is highly relevant to people with a complete SCI, a total loss of function below the lesion, referred to as an A grade in the American Spinal Injury Associations impairment scale. The Cleveland-based teams work offers hope that the approach ultimately could translate to restoration of bodily functions for paralyzed humans.

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Bladder Function Restored in Animals with Severe Spinal Cord Injury

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