8 MTCT was also found to be 42% higher in this female group when compared to HIV positive mothers who were not drug users, in the Ukraine.8 One step towards combating this problem
is the integration of antenatal services with drug treatment LDE225 services.8 So whilst data showing downwards trends is encouraging we need to ensure that all pregnant women living with HIV have safe and simple access to ART, with prime focus on those living in the hardest to reach settings. This refers to both the difficult to reach geographical and social environments (ie. marginalised populations). This, coupled with fragile health care systems heightens the vulnerability of these women and increases the risks that they are exposed to, which in turn, impact upon their children. The answer is multi-faceted R428 mw but requires flexible, practical and innovative solutions. MTCT occurs as a continuum across three time periods; in-utero (10%), perinatal (15%) and postnatally through breastfeeding (10%) [3]. Maternal risk factors include; plasma viral load, CD4 count and the stage of HIV disease. The risk of transmission ranges from 1% with a viral load
of less than 400 to 32% with a viral load of 100,000.9 At delivery risk factors include: mode of delivery, premature delivery, duration of membrane rupture and infection in the birth canal.9 Post natal risk factors include mixed feeding and mastitis.9 Interventions for MTCT can be targeted to these three time periods and can either take a programmatic or individualised approach (Fig. 1). Preventative interventions need to be considered within the context of the environment of the mother–infant pair. In resource poor settings, Bcl-w cessation
of breastfeeding is deemed unsafe as the risks of gastroenteritis and malnutrition from early weaning outweigh the risk of transmission of HIV. Termination of breastfeeding before 6 months of age increases the risk of gastro-enteritis and associated morbidity and mortality as well as increasing the risk of malnutrition in the absence of safe and nutritious feeding alternatives.10 Recent randomised controlled studies have demonstrated the low risk of breast milk transmission where the mother is on ART, or the infant is on pre-exposure prophylaxis.10 and 11 Therefore in such settings PMTCT programmes should be designed around breastfeeding which is the most appropriate way to safely feed infants.10 The combined effect of maternal ART and infant post exposure prophylaxis has been adopted into programmes in Africa to reduce MTCT, and so despite breastfeeding the risk of transmission is 1–2%, this compares to the UK where the risk of transmission is as low as 0.1% with maternal ART and formula feeding.