critical care of organ transplant. transplantation treatment of choice for many patients with...
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Critical Care of Organ
Transplant
Transplantation
Treatment of choice for many patients with end-stage failure of
kidneys, endocrine pancreas, heart, lungs, liver, and small bowel
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GENERAL PRINCIPLES
The increased number of organ transplants :
1-The availability antilymphocyte antibody preparations to prevent and treat rejection episodes
2- Immunosuppressant agent
3-Improvements in organ preservation
4-preoperative patient screening.
5-Increasing sophistication in postoperative intensive care
6-Availability of potent, yet nontoxic antibacterial, antifungal, and antiviral agents
7-Refinements in surgical techniques 3Dr.yekehfallah-phd of nursing201504/21/23
Current absolute contraindications to transplantation - Malignancy (untreated, metastatic, or at high
risk for recurrence)
-Uncontrolled infection -Medical-surgical contraindications to undergo
-Inability to recover from, major surgery
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The gap between available organs and patients awaiting
transplantation is widening. As a result, transplant wait list
mortality is increasing
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THE ORGAN DONOR SHORTAGE POTENTIAL SOLUTIONS
1- Live donors (kidney ,liver, small bowel, pancreas, and lung )
2- Deceased organ donors , Brain-dead donors
3- Unconventional donor organ
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ORGAN-SPECIFIC CONSIDERATIONS
Kidney transplantation:
1/Treatment of choice for nearly all patients of all ages with advanced chronic kidney failure and end-stage renal disease
2/Kidney transplants do not only improve quality of life, but also prolong life
3/Less expensive from a socioeconomic standpoint than chronic hemodialysis
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ORGAN-SPECIFIC CONSIDERATIONS
Liver transplantation: 1/Treatment of choice for patients
with acute and chronic end-stage liver disease.
2/Dramatic improvement in graft survival after introduction of cyclosporine in the late 1970s.
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ORGAN-SPECIFIC CONSIDERATIONSPancreas and islet transplantation1/Indications: Most pancreas transplants are done for selected,
medically suitable patients with type I diabetes who have developed significant secondary diabetic complications or have poor quality of life
2/At present, pancreas transplantation is the only effective option to consistently restore normal glucose homeostasis and normalize glycosylated hemoglobin (HbA1c) levels.
3/Successful pancreas transplants significantly improve quality of life and decrease incidence and severity of secondary diabetic complications.
4/Most pancreas transplants are performed simultaneously with a kidney transplant in preuremic patients with significant renal dysfunction, or in uremic patients with end-stage diabetic nephropathy.
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ORGAN-SPECIFIC CONSIDERATIONSSmall bowel transplantation:1/Indications: Congenital or acquired short bowel
syndrome, especially if liver dysfunction occurs because of long-term parenteral nutrition or if establishing or maintaining central venous access becomes difficult.
2/In patients who have also advanced liver disease, a combined liver &small bowel transplant may be indicated.
3/With refinement of surgical techniques, more specific immunosuppression, and better postoperative monitoring for rejection, graft survival has considerably improved over the past decade and approaches that of other solid organ grafts (e.g., lung transplants).
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ORGAN-SPECIFIC CONSIDERATIONSHeart transplantation:1/Treatment of choice for patients with end-stage
congenital and acquired parenchymal and vascular diseases of the heart after exhaustion of all conventional medical and surgical options.
2/Considerably improved results since introduction of cyclosporine in the early 1980s and refinements in diagnosing and treating rejection episodes.
3/Mechanical devices (e.g., total artificial heart, ventricular assist device) can serve as a temporary bridge between heart failure and transplant.
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ORGAN-SPECIFIC CONSIDERATIONSHeart-lung and lung transplantation:1/Effective treatment for patients with advanced pulmonary
parenchymal or vascular disease with or without primary or secondary cardiac involvement.
2/Increase in lung transplants (most frequently done as single or bilateral single lung transplants) is in large part due to technical improvements, resulting in fewer surgical complications, and to advances in perioperative and postoperative care.
3/Mechanical ventilation or extracorporeal membrane oxygenation (ECMO) can be a temporary bridge to transplant.
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FUTURE CHALLENGES IN ORGAN TRANSPLANTATION Increase number of available donor organs. Minimize rates of chronic graft failure (e.g.,
secondary to chronic rejection, graft atherosclerosis).
Develop immunosuppressive drugs and protocols that have fewer side effects and further improve long-term graft survival.
Develop tolerance-promoting protocols, which would obviate need for chronic immunosuppression beyond the induction phase.
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Rejection, Infection, and Malignancy in Solid Organ
Transplant Recipients
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GENERAL PRINCIPLES
Immunosuppressive therapy must be balanced to prevent
transplant rejection and minimize risk of infection and
malignancy
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REJECTION
The alloimmune response :1/Highly polymorphic human leukocyte
antigens (HLA) are expressed on cell surfaces in different individuals.
2/Foreign HLA molecules expressed on transplants are recognized by recipient helper and cytotoxic T lymphocytes, B lymphocytes, and natural killer cells.
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REJECTION
3/T lymphocytes are central to alloimmunity as well as immunity to viruses and malignant cells.
4/B lymphocytes produce antiâ donor HLA antibodies. Sensitization to donor HLA may occur in recipients with repeated exposures from previous transplant, multiple blood transfusions, or multiple pregnancies.
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REJECTION5/ Immunosuppression targets T lymphocytes. Dual or
triple maintenance therapy permits lower drug doses while providing synergy:
a- Corticosteroids inhibit lymphocyte activation and are
cytolytic at high doses b- Antimetabolites (azathioprine, mycophenolate
mofetil) inhibit lymphocyte proliferationc- Calcineurin inhibitors (cyclosporine, tacrolimus) inhibit production of interleukin-2 (IL-2), a critical
signal for T lymphocyte activation
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Acute RejectionGeneral: Transplant dysfunction is the most common presentation, but often
subclinical rejection is identified on biopsy.
Systemic inflammatory symptoms are less common.
Acute cellular rejection is characterized histologically by lymphocytic cellular infiltrate with active parenchymal injury.
Humoral rejection is characterized by vascular endothelial cell injury with intravascular antibody deposition, fibrin formation, and complement activation.
Biopsy is essential to confirm presence and severity of rejection.
Therapy with high-dose corticosteroids or antilymphocyte antibody is required.
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Acute Rejection
Kidney: Acute rise of serum creatinine. Rule out
drug nephrotoxicity, pyelonephritis, systemic infection, urologic obstruction,
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Acute Rejection
Liver: Acute rise in serum transaminases. Rule
out recurrent disease, biliary complications, hepatic artery thrombosis, and drug toxicity.
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Acute Rejection
Heart:
Acute decrease in left ventricular ejection fraction, or rejection identified on routine endomyocardial biopsy. Rule out infection
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Acute Rejection
Pancreas: Acute serum amylase elevation and decreased
urinary amylase excretion .Hyperglycemia is a late manifestation. Rule out arterial graft thrombosis, impaired exocrine drainage, drug toxicity, or infection.
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Acute Rejection
Lung: Acute decrease in ventilation and
oxygenation, or rejection identified on routine bronchoscopic biopsy. Rule out infection, airway or vascular anastomotic complications, malignancy, and recurrent disease.
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Chronic Rejection
Chronic rejection occurs as coronary artery disease in heart, bronchiolitis obliterans in lung, or ischemia and fibrosis in kidney, pancreas, and liver grafts.
Immunologic and nonimmunologic risk factors are important, including frequency and severity of acute rejection, recurrence of original disease, drug toxicity, and infection.
Therapy includes increased immunosuppression, avoidance of drug toxicity, or treatment of recurrent disease.
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INFECTION
General :
1/Because immunosuppression targets T lymphocytes, risk of opportunistic infection by pathogens controlled by T cell immunity is increased
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INFECTION
General :2/Risk decreases over time with immunosuppression
intensity:
a-Peritransplant infection due to nosocomial infection as in other postoperative patients.
b-Opportunistic infection most common 3 to 6 months after transplant.
c-Later infection generally community-acquired or persistent opportunistic infection.
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INFECTION
General :
3/Antimicrobial prophylaxis and empiric therapy are guided by time after transplant and level of immunosuppression, but a wide differential diagnosis and rapid identification of pathogens are always required.
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INFECTION
Bacterial:1/Peritransplant nosocomial infection: pneumonia,
catheter infection, superficial or deep wound infection, or urinary tract infection.
2/Community-acquired respiratory and urologic tract pathogens predominate later.
3/Consider Legionella in pneumonia.4/Consider Listeria in acute meningitis.5/Tuberculosis may occur at any time and often
presents as disseminated disease.
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INFECTION
Viral:Cytomegalovirus (CMV)
Active infection occurs by reactivation of latent virus
Highest incidence in the first 6 months: pneumonitis, esophagitis, gastritis, colitis, hepatitis, nephritis, bone marrow infection, or febrile syndrome. Diagnosis is confirmed by presence of viremia or biopsy.
Prophylaxis with oral ganciclovir or valganciclovir is maintained for at least 3 months, especially in high-risk recipients.
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INFECTION
Viral:Epstein-Barr virus (EBV) is associated with
posttransplant lymphoproliferative disease (PTLD). It may cause acute hepatitis or infectious mononucleosis.
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INFECTION
Viral:Pneumonitis due to adenovirus, respiratory
syncytial virus, and influenza virus requires rapid bronchoscopic diagnosis and specific antiviral therapy.
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INFECTION
Viral:Hepatitis B and C viruses are most commonly
acquired before transplant.
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INFECTION
Fungal: Pneumocystis pneumonia presents as acute
pneumonitis in the first 6 months after transplant. Prophylaxis with trimethoprim-sulfamethoxazole is highly effective.
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INFECTION
Fungal:
Aspergillosis is often disseminated and associated with high mortality.
Cryptococcosis must be considered in meningitis
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INFECTION
Fungal:Coccidiomycosis, histoplasmosis, &
blastomycosis should be considered after careful demographic evaluation to determine exposure risk. Meningitis, pneumonitis, and dermatitis are common presentations.
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INFECTION
Fungal:Candidiasis may present as disseminated
infection, urinary tract infection, or intraabdominal abscess.
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INFECTION
Parasitic:Parasitic infection should be
suspected in the setting of eosinophilia
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INFECTION
Parasitic:
Toxoplasmosis may present in the first 2 months with systemic inflammation, meningoencephalitis, pneumonitis, pericarditis, myocarditis, or retinitis. Prophylaxis with trimethoprim-sulfamethoxazole is effective.
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MALIGNANCY
Skin cancer is the most common malignancy in all transplant recipients. Risk increases with levels of sun exposure and immunosuppression. Squamous cell carcinoma is most common. Melanoma may present as metastatic disease with an unidentified primary lesion. Kaposi's sarcoma is common in patients of Mediterranean origin.
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MALIGNANCY
Solid organ cancers:1-Recurrent disease is possible, especially colon,
breast, and melanoma.
2-May present as metastatic disease, but a primary lesion is commonly identified.
3-Risk is increased approximately threefold over that for the general population.
4-Risk factors are similar to those for nonimmunosuppressed patients
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MALIGNANCY
Post transplant lymphoproliferative disease: Presents typically as polymorphic non-Hodgkin B
cell lymphoma, commonly associated with EBV infection. The primary lesion may arise in the small bowel, central nervous system, or allograft. Lymphadenopathy is easily identified on physical examination or radiologic imaging.
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MALIGNANCY
Post transplant lymphoproliferative disease:
PTLD usually presents within 1 year after transplant but may also occur later. Risk is 2% for renal transplant recipients to 10% for heart and lung recipients.
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MALIGNANCY Post transplant lymphoproliferative disease:Therapy1-Reduce or discontinue immunosuppression.
2-Cytotoxic chemotherapy or therapy with anti-CD20 antibody (rituximab) targeting B lymphocytes.
3-Antiviral (anti-EBV) therapy with acyclovir or ganciclovir (limited evidence-based support).
4-Consider surgical resection in cases with isolated, limited involvement (e.g., allograft, gastrointestinal lymphoma).
5-Radiation most effective for central nervous system PTLD.
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