Washington

An experimental technique that uses transplanted fetal tissue to treat Parkinson's disease is not yet ready for widespread use, according to a study published online last week.

In the study, surgeons transplanted nerve tissue from aborted fetuses into the brains of patients with Parkinson's disease. The disease destroys neurons that produce the chemical dopamine, which is required for normal brain function. The transplanted tissue is intended to replace these damaged cells.

But the average condition of the 23 patients who received the treatment did not improve significantly compared with a group of 11 who did not have it. The researchers, led by Warren Olanow of the Mount Sinai School of Medicine in New York, measured whether the treatment affected the symptoms of the disease, such as muscle tremors, speech and mental abilities (C. W. Olanow et al. Ann. Neurol. 54, doi:10.1002/ana.10720; 2003).

An earlier trial, led by Curt Freed of the University of Colorado Health Sciences Center in Denver, also found that patients did not benefit as a group from fetal tissue transplants (C. R. Freed et al. N. Engl. J. Med. 344, 710–719; 2001). And both trials found that the procedure caused some patients to suffer jerky involuntary movements, or dyskinesias, as a side effect. More than half of the patients in the latest trial had dyskinesias, compared with 15% of those in the earlier trial.

The results may have implications for other research using aborted fetal tissue — and, perhaps, for future therapies that might use laboratory-grown stem cells to replace defective tissue. Some researchers fear that the negative results will reduce support for the politically controversial stem-cell therapies.

Researchers say that previous trials of fetal cell transplants for Parkinson's disease have been encouraging, as they have worked in some patients. But they feel that they cannot proceed with the technique until they work out how to prevent dyskinesias. “Unless we resolve this, it will have a tremendous negative impact on this and other issues in stem-cell research,” Olanow says.

After Freed's study, scientists thought that the dyskinesias were caused by overactive neurons. But Olanow found hints that the opposite is true — poorly functioning transplants could be the cause. Olanow and others say that it is crucial to define what makes the transplants function well. Work with neurons grown from stem cells could offer clues, they add, because such lab-derived cells would contain fewer impurities than fetal tissue.

Another question raised by the latest trial is whether the transplants are being inactivated by the immune system. Olanow's team found some evidence to suggest that an immunological reaction is destroying or disabling the tissue grafts. Such evidence had not been found in previous trials.

Neurologist Olle Lindvall of the University of Lund in Sweden, who is leading a 15-year study of fetal transplants for Parkinson's disease, remains strongly supportive of the transplant idea. But he agrees that the trials raise a number of questions that must be answered by lab work before further clinical trials are done.

“Everyone agrees that we don't yet have a method that would make fetal cell transplants competitive as a clinical treatment,” he says.