New Human Cell-Produced Treatment for Anaemia From Nancy Klimas, MD 16. marts 2007 [I] would like to comment on the recent email on erythropoietin products. I would appreciate if you would widely disseminate this reply, as I believe CFS patients can be at real risk. [ ... ] If you know of other widely read group mails, feel free to send it on. Erythropoietin warning: As you know there has been a black box warning added to all of the erythropoietin products (Procrit, Epogen, and Aranesp), due to two forms of risk: 1) The potential for products that stimulate red cell production to stimulate tumor growth in patients with breast cancer and head and neck cancer. 2) The need to monitor very carefully when using red cell production stimulants in other conditions (including the anemia induced by cancer, renal failure and HIV medications) due to a risk of blood clots that could lead to stroke, heart attacks, deep vein thrombosis, and pulmonary embolism. The deep vein thrombosis risk and pulmonary embolism risk was also seen in healthy patients receiving the products to control post operative anemia. As you know, the University of Miami CFS research team recently completed a study of erythropoietin, using Procrit, in a phase 2 double blind placebo control study. While we did not have any of these complications in our study, patients were monitored very closely and the drug was titered to very low levels when the red cell expansion exceeded the plasma volume expansion and caused the blood to thicken. This happened very frequently, and doses were dropped in many subjects. Doses anywhere close to the doses suggested in the PDR would be very dangerous and even life threatening. The study's principal investigator, Dr. Barry Hurwitz recently reported the results of this phase 2 study at the 8th International IACFS Conference in Ft Lauderdale. He noted that we were unable to increase the red cell mass to mid-normal levels with erythropoietin and salt alone, restricted by safety concerns. At these lower than projected levels of RBC mass increase, the tilt table test did show a longer time until the onset or orthostatic hypotension. However, the patients' overall function and quality of life was not significantly improved. The results from this phase 2 study are not sufficient to suggest the use of erythropoietin in CFS patients. Should the pharmaceutical world like to review our data, and allow us to design a study that increased the plasma volume in addition to the RBC mass, we would consider another clinical trial. However, I think our data can be viewed in another way, as it would appear the inflammatory cytokines play a role in erythropoiesis suppression. In the future, our studies of immunomodulators that attempt to quiet the inflammatory cytokines will also look at the markers of red cell production. Finally, beware of the new erythropoietin drug, Dynepo, available currently in Europe. My reading of the literature suggests that the problem with the EPO drugs currently on the market is that they do their jobs too well. In the end, it is the act of red blood cell stimulation that induced the tumor growth, or the over production of red cells in relation to the plasma. Anything that pushes that button, should, in theory, hold the same risk. While the new product is derived from human cell lines, I don't see why the inherent risk would be different. As it took many patient years for this risk to become evident with the current products, I would not assume that the lack of vast amounts of safety data is the same as an all out "don't worry this one is safe" reassurance. Just my take on a complicated situation! Sincerely, Nancy Klimas, MD Professor of Medicine and Director CFS/GWI Research Center University of Miami Miller School of Medicine and the Miami VA Medical Center Co-PI NIH RO1 HL65668 (the EPO study)