The dosing and safety issues with newer therapies, such as lopina

The dosing and safety issues with newer therapies, such as lopinavir/ritonavir, are outlined below. It is therefore suggested that neonatal zidovudine monotherapy remains a reasonable approach for infants born to mothers with a HIV VL <50 HIV RNA copies/mL plasma, even if there is a history of zidovudine resistance. Further investigation of the national cohort data to address this question is under way. Where a low transmission-risk mother (see Section 5: Use of antiretroviral therapy in pregnancy) chooses zidovudine

monotherapy plus PLCS, the infant should receive zidovudine monotherapy [1]. There are two situations where triple combination PEP for neonates is advised: Post-delivery infant-only prophylaxis: mother found to be HIV positive after delivery, which is only effective if given CYC202 within 48–72 h of birth. Detectable maternal viraemia (>50 HIV RNA copies/mL) at delivery, mother may be on HAART or not: delivery before complete viral suppression is achieved (e.g. starting HAART late or delivery premature); viral rebound with or without resistance, with or without poor adherence; unplanned NVP-LDE225 delivery ( e.g. premature delivery

before starting ART or late presentation when maternal HIV parameters may be unknown). 8.1.2 Infants <72 h old, born to untreated HIV-positive mothers, should immediately initiate three-drug ART for 4 weeks. Grading: 1C There is one large RCT of combination therapy in neonates born to mothers who did not receive any ART before delivery (n = 1684, in Brazil, Argentina, South Africa and the USA) [18]. Infants were randomly allocated at <48 h of age to: 6 weeks of zidovudine monotherapy; or 6 weeks of zidovudine with three doses of nevirapine in the first week of life; or 6 weeks of zidovudine, with nelfinavir and lamivudine for 2 weeks. Overall, in this

high-risk group, the HIV transmission rate was 8.5%, and in multivariate analysis, only ART arm and maternal VL were significantly associated with transmission. For infants uninfected at birth, transmission Sitaxentan was twofold higher in the zidovudine-alone arm compared to the multiple ART arms (P = 0.034). There was no significant difference in transmission rates between the two multiple ARV arms and neonatal neutropenia was significantly higher in the three-drug arm. In a randomized African study, babies born to mothers presenting at delivery received single-dose nevirapine or single-dose nevirapine and 1 week of zidovudine. Of those HIV negative at birth, 34 (7.7%) who received nevirapine plus zidovudine and 51 (12.1%) who received nevirapine alone were infected (P = 0.03): a protective efficacy of 36% for the dual combination [19]. However, in two other randomized African studies where the mothers received short-course ART, for infants uninfected at birth there was no significant difference in transmission rate at 6 weeks for dual vs. monotherapy short-course regimens to the infant: zidovudine plus lamivudine vs.

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