The strategy

has shown efficacy in HIV-seronegative individuals [71–73], though specific data from HIV-seropositive individuals is more limited. Antiviral therapy should be initiated during the prodrome or early in an attack and aciclovir 200–400 mg orally five times daily for 5 days is recommended [47]. Alternative regimens are aciclovir 400 mg orally three times a day for 5 days; valaciclovir 500 mg orally twice daily for 3–5 days; valaciclovir 1 g orally, twice daily for 5 days; famciclovir 500 mg orally twice daily Inhibitor Library order for 5 days. There is no evidence of clear superiority of the alternative regimens over standard doses of aciclovir. In more immunocompromised HIV-seropositive persons, episodes may be prolonged and more severe, requiring a longer duration of antiviral treatment. In HIV negative individuals, discontinuation of suppressive or episodic antiviral therapy after 12 months is recommended in order to assess the ongoing frequency of recurrences. In an HIV-seropositive individual with a low CD4 cell count, the interruption may be delayed. The timing of this treatment

interruption should be agreed with the patient and they should be given a supply of antiviral therapy to enable prompt administration of episodic treatment if recurrences recur. 6.3.5.3 Non-mucosal (or systemic) herpes. There is limited data on the treatment TSA HDAC cell line of systemic HSV disease in HIV-seropositive individuals. Recommendations

are based on evidence from studies in both immunocompetent and immunocompromised patient populations. Systemic infection should be treated with intravenous aciclovir 5–10 mg/kg every 8 h for 10–21 days. HSV meningitis can be treated with 10 mg/kg every 8 h [74]. For HSV encephalitis, aciclovir 10 mg/kg every 8 h for 14–21 days is recommended [75] and quantitative PCR in the CSF may be helpful in monitoring response to treatment. Mortality and morbidity is high. Joint care with a neurologist is essential and there should be a low threshold for referral to a brain ITU. Patients with HSV keratoconjunctivitis or acute retinal necrosis should be seen urgently by an ophthalmologist and managed jointly. 6.3.5.4 Antiviral-resistant HSV infection. DOK2 In prospective studies, aciclovir-resistant HSV variants have been described in up to 7% of isolates from HIV-seropositive patients [76,77]. The threshold for resistance is a greater than 1–3 mg/mL aciclovir concentration for viral inhibition. This is most usually due to a mutation affecting the gene encoding viral thymidine kinase (TK), the enzyme that phosphorylates aciclovir in HSV-infected cells. TK-deficient strains are of reduced pathogenesis in immunocompetent individuals but cause significant clinical disease in immunosuppressed patients. Although partial resistance can occur, most TK mutants are resistant to aciclovir, valaciclovir and ganciclovir and the majority to famciclovir.