Transplant rejection

Transplant rejection
Classification and external resources
ICD-10 T86.
MedlinePlus 000815
MeSH D006084

Transplant rejection occurs when a transplanted organ or tissue is not accepted by the body of the transplant recipient. This is explained by the concept that the immune system of the recipient attacks the transplanted organ or tissue. This is expected to happen, because the immune system's purpose is to distinguish foreign material within the body and attempt to destroy it, just as it attempts to destroy infecting organisms such as bacteria and viruses. When possible, transplant rejection can be reduced through serotyping to determine the most appropriate donor-recipient match and through the use of immunosuppressant drugs.[1]

Contents

Types of rejection

Hyperacute rejection

Hyperacute rejection is a complement-mediated response in recipients with pre-existing antibodies to the donor (for example, ABO blood type antibodies). Hyperacute rejection occurs within minutes and the transplant must be immediately removed to prevent a severe systemic inflammatory response. Rapid agglutination of the blood occurs. This is a particular risk in kidney transplants, and so a prospective cytotoxic crossmatch is performed prior to kidney transplantation to ensure that antibodies to the donor are not present. Hyperacute rejection is analogous to a blood transfusion reaction as it is a humoral-mediated immune response. For other organs, hyperacute rejection is prevented by transplanting only ABO-compatible grafts. Hyperacute rejection is not significant in liver allografts and cellular transplants because these tissues have remarkable regenerative abilities. Hyperacute rejection is the outcome of xenotransplanted organ in non-immunosuppressed recipients.

Acute rejection

Acute rejection usually begins one week after transplantation (as opposed to hyperacute rejection, which is immediate). The risk of acute rejection is highest in the first three months after transplantation. However, acute rejection can also occur months to years after transplantation. A single episode of acute rejection is not a cause for concern if recognized and treated promptly, and rarely leads to organ failure. But recurrent episodes are associated with chronic rejection (see below).

Acute rejection occurs to some degree in all transplants (except those between identical twins). It is caused by mismatched HLA, which are present on all cells of the body. There are a large number of different alleles of each HLA, so a perfect match between all HLA in the donor tissue and the recipient's body is extremely rare.

Tissues such as the kidney or the liver which are highly vascularized (rich in blood vessels), are often the earliest victims of acute rejection. In fact, episodes of acute rejection occur in around 10-30% of all kidney transplants, and 50 to 60% of liver transplants. Damage to the endothelial lining of blood vessels is an early predictor of irreversible acute transplant rejection.

The reason that acute rejection usually begins one week after transplantation is that T-cells are involved in the rejection mechanism. These T-cells must differentiate before rejection begins. The T-cells cause cells in the transplanted tissue to lyse, or produce cytokines that cause necrosis of the transplanted tissue.

The first successful organ transplant, performed in 1954 by Dr. Joseph Murray, was successful because the donor and recipient were identical twins, and therefore no T-cell-mediated responses could be generated against the transplanted organ.

The diagnosis of acute rejection relies on clinical data, including patient signs and symptoms, laboratory testing and ultimately a tissue biopsy. The biopsy is interpreted by a pathologist who notes changes in the tissue that suggest rejection. Generally the pathologist looks for three main histological features. First, the presence of T-cells infiltrating the transplanted tissue; these may be accompanied by a heterogeneous collection of other cell types including eosinophils, plasma cells and neutrophils. (The proportions of these cell types may be helpful in diagnosing the exact type of rejection.) Secondly, evidence of structural injury to the transplanted tissue; the characteristics of this injury will depend on the type of tissue being transplanted. Lastly, injury to the blood vessels in the transplanted tissue.

Chronic rejection

The term "chronic rejection" was initially a term used to describe a long-term loss of function in transplanted organs, associated with fibrosis of the internal blood vessels of the transplanted tissue. But this pathology is now termed chronic allograft vasculopathy. The term chronic rejection is reserved for cases of transplant rejection where the rejection is due to a poorly understood chronic inflammatory and immune response against the transplanted tissue.

Chronic rejection of the lungs

Chronic rejection after lung transplantation is the leading cause of long-term morbidity and mortality in lung transplant patients.[2][3] The median survival of lung-transplant patients is approximately 4.7 years—about half that of other major transplanted organ recipients.[4] Histopathologically, the condition is known as bronchiolitis obliterans. Clinically, patients present with progressive airflow obstruction often associated with dyspnea and coughing. Ultimately these patients succumb to pulmonary insufficiency or secondary infection. Bronchiolitis obliterans syndrome (BOS) is used to describe patients with airflow obstruction that cannot be ascribed to any other specific cause. This diagnosis is confirmed by a persistent drop (three or more weeks) in forced expiratory volume (FEV1) of at least 20%.[5] Unfortunately, BOS is common in patients after lung transplant and presents in at least 50% of patients by 5 years and over 80% by ten years post-transplant.

The progression of disease is unpredictable and heterogeneous. In some cases, patients may develop a sudden drop in lung function which then stabilizes for years. In other instances, the progression is rapid leading to death within a few months. Although the onset of chronic lung rejection is unknown, risk factors include prior acute cellular rejection episodes, gastroesophageal reflux disease, infection (viral and bacterial), age of transplant recipient, HLA mis-matching, lymphocytic bronchiolitis and graft dysfunction (e.g. airway ischemia).[6]

Allo Graft: Transplantation of Cells tissue or organ from Genetically non-identical member of the same species as the recipient.

Xeno Graft: Transplantation of Cells tissue or organ from one species to another.

Auto Graft: Transplantation of organs,tissue from one part of body to another in same individual.

Iso Graft: Graft of tissue between two individual who are genetically identical.

Rejection is a recipient response to a foreign antigen with the antigen being the transplanted organ or allograft. Histologically, lymphocytic infiltrates are first noted and this is followed by epithelial cell injury (at least within the lungs). The associated inflammatory reaction results in recruitment and proliferation of fibroblasts and myofibroblasts which leads to airway lesions and scarring.[7] The condition is often patchy and heterogeneous and thus a bronchial biopsy in early disease may miss the formation of the granulation tissue that ultimately can lead to obliteration of airways.

Rejection mechanisms

Rejection is an adaptive immune response and is mediated through both T cell mediated and humoral immune (antibodies) mechanisms. The number of mismatched alleles determines the speed and magnitude of the rejection response. Different mechanisms tend to act against different grafts.

Organ/tissue Mechanism
Blood Antibodies (isohaemagglutinins)
Kidney Antibodies, CMI
Heart Antibodies, CMI
Skin CMI
Bonemarrow CMI
Cornea Usually accepted unless vascularised, CMI

CMI=Cell mediated immunity

Treatment of rejection

Chronic transplant rejection is irreversible and cannot be treated effectively. Treatments with inhaled cyclosporin are being investigated as a means to delay or prevent chronic rejection of the lungs. At present the only definitive treatment is re-transplantation, if patients can be re-allocated and if donors are available.

Acute transplant rejection can be treated using chemotherapeutic drugs designed to suppress the immune system (see list below). Acute rejection is normally treated initially with a short course of high-dose corticosteroids, which is usually sufficient to treat successfully. If this is not enough, the course can be repeated or a triple therapy regimen can be used, consisting of a corticosteroid plus a calcineurin inhibitor and an anti-proliferative agent. Antibodies against specific components of the immune system can be added to this regimen, especially for high-risk patients. mTOR inhibitors can be used in selected patients, where calcineurin inhibitors or steroids are contraindicated. Acute rejection refractory to these treatments may require blood transfusions to remove antibodies against the transplant.

If a bone marrow transplant can be performed, the transplant recipient's immune system can be replaced with the donor's immune system, thus enabling the recipient's body to accept the new organ without risk of rejection. This requires that the bone marrow, which produces the immune cells, be from the same person as the organ donation (or an identical twin or a clone). There is a risk of graft versus host disease (GVHD) in which the lymphoid cells co-injected with the bone marrow transplant recognize the host tissues as foreign and attack and destroy them accordingly.

Immunosuppressive drugs used to treat transplant rejection

The monoclonal anti-T cell antibody OKT3 was formerly used in the prevention of rejection, and is occasionally used in treatment of severe acute rejection, but has fallen out of common use due to the severe cytokine release syndrome and late post-transplant lymphoproliferative disorder, which are both commonly associated with use of OKT3; in the United Kingdom it is available on a named-patient use basis only.

Demi-Lee Brennan

Demi-Lee Brennan is an Australian citizen whose body, after a liver transplant, changed blood type and adopted the immune system of her donor. The result of this is that her body no longer attempts to reject the transplanted liver and she therefore does not need immunosuppressant medication.[8][9]

Her case is described as unique in that there are no other recorded instances of this happening in the history of human organ transplanting. Scientists are now interested in finding out how this occurred in hopes of duplicating the process, as this may be a solution to the problem of transplant rejection.[8][9]

References

  1. Christoph Frohn, Lutz Fricke, Jan-Christoph Puchta, and Holger Kirchner. The effect of HLA-C matching on acute renal transplant rejection. Nephrol. Dial. Transplant. 16: 355-360. http://ndt.oxfordjournals.org/cgi/content/full/16/2/355
  2. Pediatr Transplant. 2005 Feb;9(1):84-93
  3. Eur Respir J Suppl. 2003 Nov;47:57s-64s
  4. www.optn.org
  5. Am J Respir Crit Care Med. 2007 Jun 1;175(11):1192-8
  6. Proc Am Thorac Soc. 2009 6(1):108-21
  7. Proc Am Thorac Soc. 2006 3: 444-49
  8. 8.0 8.1 Demi-Lee Brennan has changed blood types and immune system Kate Sikora, Daily Telegraph, January 25, 2008
  9. 9.0 9.1 Aust doctors hail teen's transplant 'miracle' Sean Rubinsztein-Dunlop, ABC News (Australia), January 24, 2008

External links

Organ transplantation
Types
Autotransplantation · Allotransplantation · Xenotransplantation
Organs and tissues
Bone · Bone marrow · Corneal · Face · Hand · Head · Heart · Heart-lung · Kidney · Liver · Lung · Pancreas · Penis · Skin · Spleen · Uterus
Related topics
Biomedical tissue · Edmonton protocol · Eye bank · Graft-versus-host disease · Immunosuppressive drugs · Islet cell transplantation · Living donor liver transplantation · Lung allocation score · Machine perfusion · Medical grafting · Non-heart beating donation · Organ donation · Organ harvesting · Organ trade · Post-transplant lymphoproliferative disorder · Total body irradiation · Transplant rejection · Transplantation medicine
Organizations
Halachic Organ Donor Society · Human Tissue Authority · National Marrow Donor Program · United Network for Organ Sharing · DKMS Americas
Countries
Organ transplantation in the People's Republic of China  · Organ transplantation in Israel · Organ transplantation in Japan  · Organ theft in Kosovo  · Organ transplantation in different countries · Gurgaon kidney scandal
People
Christiaan Barnard · Michael Woodruff · Alexis Carrel · Norman Shumway · Jean-Michel Dubernard · List of notable organ transplant donors and recipients
Immune disorders: hypersensitivity and autoimmune diseases (279.5-6)
Type I/allergy/atopy
(IgE)
Foreign
Atopic dermatitis · Allergic urticaria · Hay fever · Allergic asthma · Anaphylaxis · Food allergy (Milk, Egg, Peanut, Tree nut, Seafood, Soy, Wheat), Penicillin allergy
Autoimmune
none
Type II/ADCC
(IgM, IgG)
Foreign
Pernicious anemia · Hemolytic disease of the newborn
Autoimmune
Cytotoxic
Autoimmune hemolytic anemia · Idiopathic thrombocytopenic purpura  · Bullous pemphigoid  · Pemphigus vulgaris · Rheumatic fever · Goodpasture's syndrome
Type III
(Immune complex)
Foreign
Henoch–Schönlein purpura · Hypersensitivity vasculitis · Reactive arthritis · Rheumatoid arthritis · Farmer's lung · Post-streptococcal glomerulonephritis · Serum sickness · Arthus reaction
Autoimmune
Systemic lupus erythematosus · Subacute bacterial endocarditis
Type IV/cell-mediated
(T-cells)
Foreign
Allergic contact dermatitis · Mantoux test
Autoimmune
GVHD
Transfusion-associated graft versus host disease
Unknown/
multiple
Foreign
Hypersensitivity pneumonitis (Allergic bronchopulmonary aspergillosis) · Transplant rejection · Latex allergy (I+IV)
Autoimmune
Sjögren's syndrome · Autoimmune hepatitis · Autoimmune polyendocrine syndrome (APS1, APS2) · Autoimmune adrenalitis · Systemic autoimmune disease

: LMC

cell/phys/auag/auab/comp,imrc,tcrp

imdf/ipig/hyps/tumr

proc, drug(/4)