Such monitoring is available in Europe, and in many settings outside Europe, allowing ART to be deferred. It is also noted that the evidence basis for these recommendations is weak or very weak, based entirely on cohort data after infancy. Studies expected to publish results soon may shed more light on the subject. We endorse WHO’s recommendation to treat early where the ability to provide monitoring is limited, as well as the call for more research to provide RCT evidence for treatment initiation thresholds
after infancy. PENTA continues to recommend universal treatment in infancy. Given the lack of RCT data showing a benefit of universal treatment in children aged over 12 months, PENTA recommends treatment initiation based
on clinical and CD4 criteria in all children over 12 months, buy Ruxolitinib including those aged 12 to 23 months, in high- and middle-income countries with resources to monitor frequently. “
“Table of Contents 1 Introduction 1.1 Antiretroviral therapy 1.2 The patient pathway 1.3 References 2 Central nervous system opportunistic infections 2.1 Methods 2.2 Introduction 2.3 General overview 2.4 Cryptococcus neoformans 2.4.1 Background and epidemiology 2.4.2 Presentation 2.4.3 Diagnosis 2.4.4 Treatment 2.4.5 Prophylaxis 2.4.6 Impact of HAART 2.5 Toxoplasma gondii 2.5.1 Background and epidemiology 2.5.2 Presentation 2.5.3 Diagnosis 2.5.4 Treatment 2.5.5 Prophylaxis 2.5.6 Impact of HAART 2.6 Progressive multifocal leukoencephalopathy see more (PML) 2.6.1 Background and epidemiology 2.6.2 VAV2 Presentation
2.6.3 Diagnosis 2.6.4 Treatment 2.6.5 Prophylaxis 2.6.6 Impact of HAART 2.7 Cytomegalovirus (CMV) 2.7.1 Background and epidemiology 2.7.2 Presentation 2.7.3 Diagnosis 2.7.4 Treatment 2.7.5 Prophylaxis 2.7.6 Impact of HAART 2.8 References 3 Pulmonary opportunistic infections 3.1 Methods 3.2 Introduction 3.3 General overview 3.4 Pneumocystis jirovecii 3.4.1 Background and epidemiology 3.4.2 Presentation 3.4.3 Diagnosis 3.4.4 Treatment 3.4.5 Prophylaxis 3.4.6 Impact of HAART 3.5 Bacterial pneumonia 3.5.1 Background and epidemiology 3.5.2 Presentation 3.5.3 Treatment 3.5.4 Impact of HAART 3.6 Cryptococcus neoformans 3.6.1 Background and epidemiology (see section 2.4 Cryptococcus neoformans) 3.6.2 Presentation 3.6.3 Diagnosis 3.6.4 Treatment 3.6.5 Prophylaxis 3.6.6 Impact of HAART 3.7 Aspergillosis 3.7.1 Background and epidemiology 3.7.2 Presentation 3.7.3 Diagnosis 3.7.4 Treatment 3.7.5 Prophylaxis 3.7.6 Impact of HAART 3.8 Cytomegalovirus (CMV) 3.8.1 Background and epidemiology 3.8.2 Presentation 3.8.3 Diagnosis 3.8.4 Treatment 3.8.5 Prophylaxis 3.8.6 Impact of HAART 3.9 Influenza A virus (IAV) 3.9.1 Background and clinical presentation 3.9.2 Diagnosis 3.9.3 Treatment 3.9.4 Prevention 3.