Stem Cells Found to Heal Damaged Artery in Pre-Clinical Lab Study
In a recently published manuscript, scientists from the University of Pittsburgh Medical Center—including McGowan Institute for Regenerative Medicine affiliated faculty member Gerald Schatten, PhD, professor and vice chair of obstetrics, gynecology and reproductive sciences at the University of Pittsburgh, deputy director at Magee-Womens Research Institute, and director of the Pittsburgh Development Center—and the Texas Biomedical Research Institute have for the first time demonstrated that baboon embryonic stem cells can be programmed to completely restore a severely damaged artery. These early results show promise for eventually developing stem cell therapies to restore human tissues or organs damaged by age or disease.
“We first cultured the stem cells in petri dishes under special conditions to make them differentiate into cells that are the precursors of blood vessels, and we saw that we could get them to form tubular and branching structures, similar to blood vessels,” said John L. VandeBerg, PhD, Texas Biomed’s chief scientific officer.
This finding gave the team the confidence to do complex experiments to find out if these cells could actually heal a damaged artery. Human embryonic stem cells were first isolated and grown in 1998.
The scientists found that cells derived from embryonic stem cells could actually repair experimentally damaged baboon arteries and “are promising therapeutic agents for repairing damaged vasculature of people,” according to the authors.
Researchers completely removed the cells that line the inside surface from a segment of artery, and then put cells that had been derived from embryonic stem cells inside the artery. They then connected both ends of the arterial segment to plastic tubing inside a device called a bioreactor which is designed to grow cells and tissues. The scientists then pumped fluid through the artery under pressure as if blood were flowing through it. The outside of the artery was bathed in another fluid to sustain the cells located there.
Three days later, the complex structure of the inner surface was beginning to regenerate, and by 14 days, the inside of the artery had been perfectly restored to its complex natural state. It went from a non-functional tube to a complex fully functional artery.
“Just think of what this kind of treatment would mean to a patient who had just suffered a heart attack as a consequence of a damaged coronary artery. And this is the real potential of stem cell regenerative medicine—that is, a treatment with stem cells that regenerates a damaged or destroyed tissue or organ,” Dr. VandeBerg said.
To show that the artery couldn’t heal itself in the absence of stem cells, the researchers took a control arterial segment that also was stripped of the cells on its interior surface, but did not seed it with stem cells. No healing occurred.
Stains for proteins that indicate functional characteristics showed that the healed artery had completely normal function and could do everything that a normal artery does in a healthy individual.
“This is evidence that we can harness stem cells to treat the gravest of arterial injuries,” said Dr. VandeBerg.
Eventually, scientists hope to be able to take a skin cell or a white blood cell or a cell from any other tissue in the body, and induce it to become just like an embryonic stem cell in its capacity to differentiate into any tissue or organ.
“The vision of the future is, for example, for a patient with a pancreas damaged because of diabetes, doctors could take skin cells, induce them to become stem cells, and then grow a new pancreas that is just like the one before disease developed,” Dr. VandeBerg said.
Illustration: Scientists have for the first time demonstrated that baboon embryonic stem cells can be programmed to completely restore a severely damaged artery. These early results show promise for eventually developing stem cell therapies to restore human tissues or organs damaged by age or disease. – © noelleherzog/Fotolia.
Illustration: Pittsburgh Tissue Engineering Initiative.
Abstract (Endothelial reconstitution by CD34+ progenitors derived from baboon embryonic stem cells. Qiang Shi, Gerald Schatten, Vida Hodara, Calvin Simerly, John L. VandeBerg. Journal of Cellular & Molecular Medicine; (01/10/13))