Abstract
Gardasil (Merck’s quadrivalent HPV vaccine) is the first vaccine in history to have been granted the FDA’s accelerated approval and fast track. Using unpublished documents and data, we investigated the impact of US regulators’ choices on the quality of available evidence regarding the vaccine’s efficacy in preventing high-grade cervical lesions, which are precursors of cervical cancer. We found that, as early as 2001, the accelerated approval and fast track procedures prompted FDA advisory committees to make methodological choices such that only weak claims could be made regarding the vaccine’s efficacy and to approve a product whose benefit-to-harm ratio cannot be appropriately assessed. By giving more weight to the HPV vaccine’s hypothetical promises rather than to compliance with best methodological principles, regulatory authorities’ decisions turned out to be more favorable to commercial interests than to public health thereby allowing HPV vaccine manufacturers to escape the usual burden of proof while generating huge profits. Published and unpublished results of pre-marketing trials strongly suggest that introduction of the vaccine will not lead to the expected reduction in the incidence of high-grade cervical lesions, let alone of cervical cancer. The available HPV vaccines do not target all high-risk HPV strains. Consequently, screening must be maintained. The marketing of Gardasil has thus inaugurated a new form of medical overuse in the field of prevention: the introduction of a low-value primary prevention measure (vaccination) whose effectiveness can never be completely assessed since the secondary prevention measure (screening) cannot be removed. Meanwhile, health authorities promote the product and society bears the costs of vaccination campaigns and health risks. This is a concerning outcome. Such over-prevention creates a societal and individual burden of unnecessary medical expansion that undermines science.
Highlights
Gardasil, Merck’s quadrivalent HPV vaccine, has been touted as a significant breakthrough in cervical cancer prevention and women’s health, offering the potential to reduce the incidence and mortality from this disease by at least two-thirds.[1,2] It is the first vaccine for which the U.S Food and Drug Administration (FDA) has granted accelerated approval and fast track
Since Center for Biologics Evaluation and Research (CBER) mentioned in a list of appendices for a clinical study report (CSR) that, in 2005, changes were made to the planned efficacy analysis prior to unblinding,[20] we asked for the different versions of the statistical data analysis plan (DAP)
The FDA states that accelerated approval was instituted to allow “drugs for serious conditions that filled an unmet medical need to be approved based on a surrogate endpoint,” which enables the FDA to “approve these drugs faster.”[24]. As for fast track, it is “a process designed to facilitate the development, and expedite the review of drugs to treat serious conditions and fill an unmet medical need.”[25]. In the fast track context, the FDA defines an unmet medical need as follows: Filling an unmet medical need is defined as providing a therapy where none exists or providing a therapy which may be potentially superior to existing therapy
Summary
Merck’s quadrivalent HPV (human papillomavirus) vaccine, has been touted as a significant breakthrough in cervical cancer prevention and women’s health, offering the potential to reduce the incidence and mortality from this disease by at least two-thirds.[1,2] It is the first vaccine for which the U.S Food and Drug Administration (FDA) has granted accelerated approval and fast track. Gardasil targets two high-risk HPV strains (HPV 16 and HPV 18) that are found in approximately 70% of cervical cancer cases.[3,4,5] According to the International Agency for Research on Cancer, at least 11 other high-risk HPV types can cause cervical cancer.[6] Pre-marketing randomized controlled trials (RCTs) have provided solid evidence that Gardasil is very effective in preventing high-grade cervical lesions (CIN, precursors of cervical cancer) linked to HPV 16 and HPV 18 in women not previously infected.[7] But we still lack strong evidence from RCTs that HPV vaccination leads to an expected reduction in the overall incidence of highgrade CIN and of cervical cancer, this is the most relevant issue in terms of public health.
Sign-in/Register to view highlights & summary Sign-in/Register to access full text options 
Free) 
Talk to us
Join us for a 30 min session where you can share your feedback and ask us any queries you have
Schedule a call
