Transplantologiya 2016
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Keywords: liver transplantation, fungal infections, antifungal therapy.
The development of fungal infection in patients undergoing liver transplantation is still associated with a poor outcome, despite a number of commercially available anti-fungal drugs. Thus, some authors have reported mortality rates from 30 to 77% among the cases of the invasive candidiasis development, and 65-90% among aspergillosis cases. The delay in administering an antifungal therapy has a negative impact on the outcomes [1-6].
2 The optimal approach to prevention of the antifungal infection has not been standardized yet. A number of studies demonstrated the isolation of resistant Candida strains in patients receiving a prevention therapy with fluconazole [7].
A meta-analysis of published studies on the prevention of fungal infection has shown a decrease in the rates of undiagnosed fungal infection, but the overall mortality rates and the need to administer an empirical therapy for suspected fungal infection have not reduced [8]. Given the lack of accurate data on a clinically beneficial effect of the prevention, its high costs, potential toxicity, and the risk of pathogen resistance development, many transplant centers refrain from administering a universal antifungal prevention therapy nowadays [9].
A so-called targeted approach is the most commonly used, i.e. when prevention therapy is administered in the patients of a high-risk group only.
We should note that the term "high risk patients" has not been defined anyway yet, and the transplant specialists are often guided by various sets of criteria for stratifying the patients with increased risks of fungal infection.
There are a great number of factors making the patients vulnerable to invasive mycoses. The most important of these factors include liver re- transplantation, a fulminant hepatic failure as an indication to transplantation, an acute kidney injury in the postoperative period requiring the use of dialysis techniques, relaparotomy in the early postoperative period, a massive blood loss (requiring more than 20 units of blood components to be transfused for correction during surgery).
Other factors include the surgery duration for more than 12 hours, a disseminated (≥ 2 loci) superficial colonization with Candida spp., and 3 making a hepatico-jejunal anastomosis versus a choledocho-choledochal anastomosis [10-13].
The choice of antifungal drugs for targeted prophylaxis, their dosages, and the duration of prevention therapy course also remain controversial.
Fluconazole and different forms of amphotericin B have been widely used in clinical practice for targeted prophylaxis. Meanwhile, the fluconazole-resistant strains of Candida krusei and Candida glabrata are identified more and more frequently. One should remember that azoles influence the plasma
levels of
the most
commonly used
immunosuppressants: cyclosporine, tacrolimus, and everolimus.
The duration of prevention therapy has not been standardized either, ranging from 5-7 days to 4 weeks or longer post-transplantation [14].
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