| Literature DB >> 32635780 |
Nieves Martínez-Peinado1, Nuria Cortes-Serra1, Irene Losada-Galvan1, Cristina Alonso-Vega1, Julio A Urbina2, Ana Rodríguez3, John L VandeBerg4, Maria-Jesus Pinazo1, Joaquim Gascon1, Julio Alonso-Padilla1.
Abstract
INTRODUCTION: Chagas disease treatment relies on the lengthy administration of benznidazole and/or nifurtimox, which have frequent toxicity associated. The disease, caused by the parasite Trypanosoma cruzi, is mostly diagnosed at its chronic phase when life-threatening symptomatology manifest in approximately 30% of those infected. Considering that both available drugs have variable efficacy by then, and there are over 6 million people infected, there is a pressing need to find safer, more efficacious drugs. AREAS COVERED: We provide an updated view of the path to achieve the aforementioned goal. From state-of-the-art in vitro and in vivo assays based on genetically engineered parasites that have allowed high throughput screenings of large chemical collections, to the unfulfilled requirement of having treatment-response biomarkers for the clinical evaluation of drugs. In between, we describe the most promising pre-clinical hits and the landscape of clinical trials with new drugs or new regimens of existing ones. Moreover, the use of monkey models to reduce the pre-clinical to clinical attrition rate is discussed. EXPERT OPINION: In addition to the necessary research on new drugs and much awaited biomarkers of treatment efficacy, a key step will be to generalize access to diagnosis and treatment and maximize efforts to impede transmission.Entities:
Keywords: Trypanosoma cruzi ; Benznidazole; Chagas disease; clinical trials; drug discovery; fexinidazole; monkeys; nifurtimox; posaconazole; pre-clinical assays
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Year: 2020 PMID: 32635780 DOI: 10.1080/13543784.2020.1793955
Source DB: PubMed Journal: Expert Opin Investig Drugs ISSN: 1354-3784 Impact factor: 6.206