| Literature DB >> 28348914 |
Romain Vial1, Christine Zandotti2, Sophie Alain3, Alexandre Decourt1, Noémie Jourde-Chiche1, Raj Purgus4, Charleric Bornet5, Laurent Daniel6, Valérie Moal1, Tristan Legris4.
Abstract
Background. Cytomegalovirus (CMV) antiviral drug resistance constitutes an increasing challenge in transplantation. Foscarnet is usually proposed when resistance for ganciclovir is suspected, but its use is limited by its nephrotoxicity. Case Presentation. We report a case of multiresistant CMV disease in a kidney transplant recipient. Foscarnet was prescribed after ganciclovir treatment failure in a patient with two mutations in the UL97 viral gene. Foscarnet induced biopsy-proven kidney crystal precipitation that resulted in severe acute transplant failure and nephrotic syndrome. Despite a large decrease in immunosuppression, CMV disease was not controlled and a salvage therapy with Brincidofovir (BCV), which is an oral lipid conjugate of cidofovir with limited nephrotoxicity, was attempted. Clinical and virological remission was observed after a 21-day course of BCV, despite mild and reversible liver toxicity. However, a new relapse could not be effectively cured by BCV due to a new mutation in the UL54 gene, which is known to confer resistance to cidofovir. A new course of foscarnet finally resulted in prolonged CMV remission. Herein, we present a review of foscarnet nephropathy cases in solid-organ transplanted patients. Conclusions. This unique case highlights the potential benefit of BCV use during resistant CMV infection, although mutations in the UL54 gene may limit its therapeutic efficacy. These findings need to be confirmed in clinical trials.Entities:
Year: 2017 PMID: 28348914 PMCID: PMC5350387 DOI: 10.1155/2017/3624146
Source DB: PubMed Journal: Case Rep Transplant ISSN: 2090-6951
Figure 1Foscarnet nephropathy in the kidney transplant. (a) Masson's trichrome staining (×200) showed intraglomerular crystalline precipitation obstructing the capillaries and crushing the mesangium together with fibrinoid thrombi. (b) Jones methenamine silver staining (×400) also revealed FOS crystals within the glomerular capillaries. (c) Masson's trichrome staining (×200) showed crystals that resembled short sticks with angular edges in the tubular lumen. (d) Jones methenamine silver staining (×400) also revealed FOS crystals within the tubular lumen.
Figure 2Course of multiresistant CMV disease. (a) Evolution of CMV antigenemia (red line) and kidney transplant function (serum creatinine level, blue line) together with antiviral therapies and genotypic mutations. PC: positive cells/200000 polymorphonuclear leukocytes. GCV: ganciclovir. CDV: cidofovir. (b) Evolution of blood ciclosporin levels (black line) and lymphocytes counts (blue line).
Summary of cases of biopsy-proven foscarnet nephropathy during CMV infection in solid organ transplantation.
| Reference | Type of transplant | Indication of FOS | Time to nephropathy after FOS initiation | Peak serum creatinine | Proteinuria | Biopsy results | Outcome |
|---|---|---|---|---|---|---|---|
| [ | Kidney | CMV syndrome | 30 days (single treatment) | 387 | 7 g/d | Birefringent crystal precipitation surrounded by macrophages in glomeruli and tubules. Fibrinoid thrombi. | FOS withdrawn after 27 days. |
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| [ | Lung | CMV bronchiolitis | 35 days (second treatment; first treatment of 4 weeks) | 475 | NR | Autopsy: birefringent short crystals with angular edges in glomeruli (with rupture of capillaries and Bowman's capsule) and in tubules with tubular necrosis and granulomas. | No FOS withdrawal. |
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| [ | Kidney | Asymptomatic reactivation of GCV resistant strain despite prophylactic valganciclovir | 21 days (single treatment) | Anuria, hemodialysis | NR | Crystals in tubules and in one-third of glomeruli with rupture of the basement membrane, tubular necrosis, and macrophages. | Multiorgan (kidney, pancreas, and myocardium) damage due to FOS crystal precipitation. |
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| [ | Kidney | CMV hepatitis and retinitis | After 14 days (single treatment) | 157 | NR | Birefringent crystals in the tubular lumens. | FOS withdrawal. |
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| PR | Kidney | CMV gastritis | 6 days (second treatment; first treatment of 14 days) | 450 | 4.5 g/g of creatininuria | Crystals in glomeruli and tubules. | FOS withdrawal followed by Brincidofovir. |
CMV, cytomegalovirus; FOS, foscarnet; GCV, ganciclovir; NR, not reported; PCR, polymerase chain reaction; PR, present report.