Although the vaccine was designed to target HPV-16/18, end-of-study data from the 4-year PATRICIA trial demonstrated efficacy against non-vaccine HPV types [10], and an overall VE against CIN3+ lesions of 93% irrespective of HPV type in the lesion in the HPV-naïve1 TVC cohort [9]. We have applied these data to the currently observed disease burden in all WHO reported countries to estimate the additional health benefits of vaccination that accrue from protection against HPV types other than HPV-16/18.

When protection irrespective of HPV types was considered, the number of CC cases and deaths potentially prevented by vaccination was at least 18% larger than when only HPV-16/18 were considered. The increased potential benefit was seen across all five WHO continents, and was particularly pronounced in Africa, where non-HPV-16/18 cases account

selleck chemicals for 17,125 cases prevented at 70% vaccination coverage representing an additional 34% cases potentially prevented, compared with 272 cases additionally prevented in Oceania, representing an additional 18% cases potentially prevented. HPV vaccination also has the potential to reduce the morbidity associated with precancerous lesions. Management of precancerous lesions detected by screening may require surgical procedures, such as conisation. In countries with absent or poorly developed cervical RGFP966 ic50 screening programmes, few precancerous lesions will be detected and the health impact will mainly be observed when undetected lesions progress to symptomatic cancer. Conversely, in countries with well-developed and effective screening programmes, many precancerous lesions are detected at an early stage and are usually treated before they progress to cancer, so the health ALOX15 burden will tend to shift away

from CC treatment towards precancerous lesion treatment. In some industrialised countries, the economic burden of precancerous lesions may exceed or approach the economic burden of CC. For example, a study of patients in a health maintenance plan in the USA found that treatment of CC accounted for 10% of healthcare expenditure on HPV-related cervical disease and treatment of precancerous lesions accounted for 17% [22]. In Belgium, the total annual cost of CC treatment to the healthcare payer was estimated at Euro 6.5 million and the annual cost of precancerous lesions at Euro 1.97 million in a retrospective study [23]. Other morbidities associated with treatment of precancerous lesions of the cervix avoidable by vaccination such as increased risk of perinatal death and pre-term births should also be considered [24] and [25]. To our knowledge, this is the first estimate of the potential impact of HPV vaccination on CC cases and deaths to apply the recent data on VE irrespective of HPV type causing the lesion reported from the end-of-study data in the PATRICIA trial [9] and [10].