Altered Antibody Boosts Transplants.The immune system immune system Cells, cell products, organs, and structures of the body involved in the detection and destruction of foreign invaders, such as bacteria, viruses, and cancer cells. Immunity is based on the system's ability to launch a defense against such invaders. takes a dim view of transplants. Any tissue or blood that doesn't come from an identical twin counts as foreign matter to be destroyed. Treatment with immune-suppressing drugs can counteract such rejection, but it leaves the individual vulnerable to cancer or other ills. Even with drug treatment, many patients reject transplants. At the core of this reaction is a molecule called CD154. It signals T cells--the immune system's shock troops--to spring into action against transplants. Two studies in rhesus monkeys now show that a drug called hu5C8 can waylay this attack without shutting down the rest of the immune system. The antibody binds to CD154, blocking the chain reaction that would have led to overzealous manufacture of T cells T cells A type of white blood cell produced in the thymus gland. T cells are an important part of the immune system. Infants born with an underdeveloped or absent thymus do not have a normal level of T cells in their blood. . In a study described in the June NATURE MEDICINE, scientists gave nine rhesus monkeys kidney transplants from unrelated donors and also intravenous doses of hu5C8, which is made by Biogen in Cambridge, Mass. Previous studies showed that this genetically engineered genetically engineered adjective Recombinant, see there version of a human antibody might block T cell activation (SN: 8/9/97, p. 84). One of the nine treated monkeys died of unrelated causes, but the other eight are thriving with their transplanted kidneys. Five of these animals completed their 5-month regime of antibody treatment about a year ago, says study coauthor Allan D. Kirk, a transplant surgeon at the Naval Medical Research Center in Bethesda, Md. Four other monkeys, which received a transplant but not the antibody, rejected the transplanted kidneys within 8 days. Eleven monkeys getting a combination of the antibody and standard immune-suppressing drugs showed mixed results--some rejected the organs, others didn't. In a separate study, researchers removed the pancreases of six rhesus monkeys and then gave them hu5C8 along with new pancreatic islet cells from unrelated donors. The transplanted cells, placed in the monkeys' livers, weren't rejected, says study coauthor Norma S. Kenyon, a transplant immunologist at the University of Miami This article is about the university in Coral Gables, Florida. For the university in Oxford, Ohio, see Miami University. The University of Miami (also known as Miami of Florida,[2] UM,[3] or just The U School of Medicine. Two monkeys that didn't receive the antibody rejected islet cells. This study, to be published this summer in the PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES The Proceedings of the National Academy of Sciences of the United States of America, usually referred to as PNAS, is the official journal of the United States National Academy of Sciences. , raises hopes for diabetes patients. Islet cells normally make the hormone insulin, and the transplanted cells started producing it immediately. The experiment suggests a means to reverse type 1, or juvenile-onset, diabetes, a condition in which islet cells are destroyed. "I don't want to raise false hopes, but I think this is a very big step forward," Kenyon says. In a study of baboons to be published soon in DIABETES, Kenyon and her colleagues show that hu5C8 also reversed rejection in four baboons that had earlier received islet-cell transplants. "This is an exciting drug," says Mitchell L. Henry, a surgeon at Ohio State University Ohio State University, main campus at Columbus; land-grant and state supported; coeducational; chartered 1870, opened 1873 as Ohio Agricultural and Mechanical College, renamed 1878. There are also campuses at Lima, Mansfield, Marion, and Newark. in Columbus. He's impressed that two types of organ transplants succeeded. In all these experiments, the antibody's precise role remains a mystery. "Our immune system didn't evolve [just] to keep us from getting transplants. It is aimed at infectious pathogens," says endocrinologist David M. Harlan of the Naval Medical Research Center in Bethesda, Md., who participated in all three studies, as did Kirk. Transplant rejection transplant rejection Graft rejection, organ rejection, tissue rejection Immunology The constellation of host immune responses evoked when an allograft tissue is transplanted into a recipient; rejection phenomena may be minimized by optimal matching of MHC antigens may simply be a case of mistaken identity mistaken identity n → erreur f d'identité mistaken identity mistake n → Verwechslung f mistaken identity n , and CD154 may somehow remedy the problem. Evolution may have provided compounds that act as shutoff shut·off n. 1. A device that shuts something off. 2. A stoppage; a cessation. switches each time T cells are produced to mount an attack, Harlan suggests. The antibody hu5C8 may somehow tap into that mechanism, he says. This model could explain why suppression drugs hampered hu5C8's effectiveness in the kidney-transplant experiment. The drugs could be keeping T cells from processing a shutoff signal, Kirk says. "The lesson is that we must choose our signals carefully, not simply block them all," says Polly Matzinger Polly Celine Eveline Matzinger (born 21 July 1947) is an iconoclastic scientist who proposed a novel explanation of how the immune system works, called the danger model. of the National Institute of Allergy and Infectious Diseases infectious diseases: see communicable diseases. in Bethesda, Md., writing in NATURE MEDICINE. |
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