Abstract
Cystic (CE) and alveolar (AE) echinococcosis are chronic, neglected parasitic diseases burdened by high morbidity and, for AE, by high mortality, if left untreated. CE and AE have a widespread distribution, including Europe. Albendazole (ABZ), a broad-spectrum benzimidazole drug widely used to treat parasitic infections, is the drug of choice for the management of CE and AE, and is parasitostatic on echinococcal metacestodes. In Europe, ABZ is licensed for interrupted “cyclic” treatment, for a maximum of 3 cycles. However, better efficacy with no increased side effects has been shown when the drug is administered continuously and for longer periods. Current international recommendations, on the basis of clinical, pharmacological, and biological studies, recommend continuous administration of ABZ for months to years for the treatment of CE and AE, and this schedule has been widely in use for the past 20 years. However, in Europe this internationally recommended schedule, with the exception of France, is technically “off-label”, and, as such, requires an informed consent by the patient and, in some countries, even precludes the reimbursement of the drug cost. Adding to the very high cost of the drug, frequent “out-of-stock” situation, and packaging format impractical for long therapies, these conditions put patients with CE and AE regularly at risk of treatment discontinuation and disease progression. European regulations envisage variations to marketing authorization, but postauthorization studies should be carried out by the holder of the license of the drug, in the form of randomized controlled trials. While such studies do not seem feasible and would probably not be ethically justified for CE and AE, European regulations envisage other possibilities in particular situations, which apply to CE and AE, but there is limited interest to invest in this perspective. We urge a coordination between stakeholders to find effective and feasible ways to take action to revise the benzimidazole dosage regimens for CE and AE and to ensure a fair, regular, and easy access to the appropriate treatment to those suffering from these serious diseases.
Highlights
Albendazole (ABZ) and mebendazole (MBZ) are broad-spectrum anthelmintic drugs, included in the World Health Organization (WHO) list of essential medicines, and are used in the treatment of several, mainly metazoan, parasitic infections [1]
We urge a coordination between stakeholders to find effective and feasible ways to take action to revise the benzimidazole dosage regimens for cystic echinococcosis (CE) and alveolar echinococcosis (AE) and to ensure a fair, regular, and easy access to the appropriate treatment to those suffering from these serious diseases
Despite the impossibility of rigorously comparing these studies due to the differences of the populations, cyst characteristics, and overall length of therapy, these results suggest a better efficacy of the continuous administration for the treatment of CE
Summary
Albendazole (ABZ) and mebendazole (MBZ) are broad-spectrum anthelmintic drugs, included in the World Health Organization (WHO) list of essential medicines, and are used in the treatment of several, mainly metazoan, parasitic infections [1]. When ABZ was registered for the treatment of echinococcosis, the interrupted “cyclic” regimen was chosen as a precaution because only limited data on the long-term toxicity were available.
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
