Table 2.
Opportunistic infection prophylaxis for HIV-infected transplant recipients
| Opportunistic infection |
Preferred agent | Primary prophylaxis * | Secondary prophylaxis ** |
|---|---|---|---|
|
| |||
| Pneumocystis jiroveci | Trimethoprim-Sufamethoxazole | Indicated for life; initiate immediately post-transplant | Indicated for life; initiate immediately post-transplant |
| Alternatives: dapsone if not G6PD deficient, atovaquone | |||
|
| |||
| Toxoplasmosis | Trimethoprim-Sulfamethoxazole | Toxoplasmosis IgG-positive patients with CD4 T-cell count ≤200 cells/mm3 | CD4 T-cell count <200 cells/mm3 |
| Alternatives: atovaquine, sufadiazine + pyrimethamine + leucovorin | Discontinue when CD4+ T-cell count is >200 cells/mm3 for 3–6 months† | ||
|
| |||
| Mycobacterium avium complex | Azithromycin | CD4+ T-cell count ≤50 cells/mm3 | CD4+ T-cell count <50 cells/mm3 |
| Alternatives: clarithromycin | Discontinue when CD4+ T-cell count >100 cells/mm3 for 3–6 months | Discontinue when CD4+ T-cell count is >100 cells/mm3 for 3–6 months† | |
|
| |||
| Cytomegalovirus | Valganciclovir | No HIV specific indication | CD4 T-cell count <75–100 cells/mm3 |
| Alternatives: foscarnet, cidofovir | Discontinue when CD4+ T-cell count is >100–200 cells/mm3 for 3–6 months† | ||
|
| |||
| Cryptococcosis, extrapulmonary | Fluconazole | No HIV specific indication | CD4 T-cell count <200 cells/mm3 |
| Discontinue when CD4+ T-cell count is >200 cells/mm3 for 3–6 months† | |||
*
No history of infection
**
Prior history of the infection
†
Secondary prophylaxis should also be reinstituted immediately post-transplant for 1 month and during the treatment of acute rejection for 1 month following completion of acute rejection therapy. If the CD4+ T-cell count is suppressed, continuation should be guided by the CD4+ T-cell count.