Artificial Blood

November 12, 2014 by

Nov. 7, 2014

By Medical Discovery News

Red blood cells

In the series “True Blood,” the invention of artificial blood allows vampires to live among humans without inciting fear. In the real world, however, artificial blood would have very different effects, as 85 million units of blood are donated worldwide and there is always a demand for more. An artificial blood substitute free of infectious agents that could be stored at room temperature and used on anyone regardless of blood type would be revolutionary.

That is exactly what a group of scientists at the University of Essex in England are working on, although the search for an artificial blood substitute started 80 years ago. All red blood cells contain a molecule called hemoglobin, which acquires oxygen from the lungs and distributes it to cells throughout the body. Their plan is to make an artificial hemoglobin-based oxygen carrier (HBOC) that could be used in place of blood.

HBOCs are created using hemoglobin molecules derived from a variety of sources, including expired human blood, human placentas, cow blood, and genetically engineered bacteria. The problem is that free hemoglobin, which exists outside the protective environment of red blood cells, breaks down quickly and is quite toxic. Therefore, HBOCs are not approved for use in most of the world due to their ineffectiveness and toxicity.

The active group in hemoglobin that binds to oxygen is called heme, which can actually be quite toxic. Scientists have found a variety of ways to modify hemoglobin to increase its stability but safety issues still remain. If the hemoglobin’s processing system is overwhelmed, a person may develop jaundice, which causes the skin and whites of the eyes to turn yellow. Too much free hemoglobin can also cause serious liver and kidney damage. When free hemoglobins, not whole red blood cells, are infused, the human body’s natural system for dealing and disposing of this molecule is overwhelmed, leading to toxicity. That is why blood substitutes consisting of free hemoglobin have been plagued with problems, such as an increase in deaths and heart attacks.

But scientists involved in this latest effort to produce a blood substitute have been reengineering the hemoglobin molecule. They are introducing specific amino acids, which are the building blocks of proteins, into hemoglobin in an effort to detoxify it. Preliminary results indicate that this approach may work. They have already created some hemoglobin molecules that are much less reactive and are predicted to be less toxic when used in animals or people.

If successful, this HBOC would be a universal product, meaning it could be used on everyone and there would be no need to waste time on testing for blood types. It would also be sterile, free of any of the infectious agents that donated blood must be tested for. Instead of refrigeration, it could have a long shelf life at room temperature, perhaps years, so it could be stockpiled in case of major emergencies. It could even be kept on board ambulances and at remote locations far from hospitals. The search for an effective and nontoxic blood substitute is one the medical field’s Holy Grails, and if proven successful, these scientists may have finally found it.

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Hope for Sickle Cell

September 20, 2014 by

Sept. 19, 2014

By Medical Discovery News

While sickle cell disease has long been studied, a recent discovery revealed that the disease significantly increases the levels of a molecule called sphingosine-1-phosphate (S1P), which is generated by an enzyme called sphingosine kinase 1 (SphK1). Inhibiting the enzyme SphK1 was found to reduce the severity of sickle cell disease in mice, which will hopefully lead to new drugs that target SphK1in order to treat sickle cell disease in humans.

Sickle cell disease is caused by a change in the gene that is responsible for a type of hemoglobin, the protein molecule in red blood cells that carries oxygen. This tiny change results in hemoglobin clumping together, changing the shape of red blood cells.

The name for sickle cell disease actually comes from misshapen red blood cells. Rather than being shaped like a disk, or a donut without a whole, sickle cells are shaped like a crescent, sort of bending over on themselves. The normal shape is critical to red blood cells’ ability to easily travel through blood vessels and deliver oxygen to cells and tissues. Sickle cells become inflexible and stick to each other, blocking the flow of blood through blood vessels.

Symptoms of the disease begin to appear at about four months of age. Normally, red blood cells live for about 120 days. Sickle cells only survive 10-20 days. Although the bone marrow tries to compensate for the rapid loss of red blood cells, it cannot keep up. The disease causes pain, anemia, organ damage, and possibly infections.

Although the symptoms and their severity vary, most people with sickle cell disease will have periodic crises lasting hours or days. Symptoms include fatigue, paleness, shortness of breath, increased heart rate, jaundice, and pain. Long-term damage can occur in the spleen, eyes, and other organs, and sickle cell disease increases the risk of stroke. People who only inherit one copy of the sickle cell hemoglobin gene have a milder case of the disease than those who inherit two copies, one from each parent.

Current treatments only reduce the number and the severity of crises using hydroxyrurea, blood transfusions, pain medications, and antibiotics. As the disease advances, dialysis, kidney transplants, eye surgeries, gall bladder removal, and other treatments may be necessary. The only cure for the disease is a bone marrow transplant, which is not an option for everyone.

So it’s pretty exciting that when scientists found that levels of S1P were elevated in mice with sickle cell disease, they inhibited the enzyme SphK1 to reduce the levels of S1P. As a result, red blood cells lived longer and had less sickling. The mice also had less inflammation and tissue damage, which would reduce damage to red blood cells and prevent symptoms of the disease. When they engineered sickle cell disease mice without the gene for the enzyme SphK1 that makes S1P, again the mice had less sickling and symptoms.

How does S1P influence sickling? Apparently, it binds directly to hemoglobin and reduces its ability to collect and carry oxygen, which causes the characteristic folding of cells. S1P has other roles in the body, so it is unknown whether inhibitors to SphK1 can safely and effectively be used in humans to treat sickle cell disease.

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