Ujjini H. Manjunatha, Suresh B. Lakshminarayana, Rajiv S. Jumani, Alexander T. Chao, Joseph M. Young, Jonathan E. Gable, Mark Knapp, Imad Hanna, Jean-Rene Galarneau, John Cantwell, Upendra Kulkarni, Michael Turner, Peichao Lu, Kristen H. Darrell, Lucy C. Watson, Katherine Chan, Debjani Patra, Mulugeta Mamo, Catherine Luu, Carlos Cuellar, Jacob Shaul, Linda Xiao, Ying-Bo Chen, Shannon K. Carney, Jay Lakshman, Colin S. Osborne, Jennifer A. Zambriski, Natasha Aziz, Christopher Sarko, Thierry T. Diagana
{"title":"隐孢子虫 PI(4)K 抑制剂 EDI048 是一种肠道限制性杀寄生虫剂,可用于治疗小儿肠道隐孢子虫病","authors":"Ujjini H. Manjunatha, Suresh B. Lakshminarayana, Rajiv S. Jumani, Alexander T. Chao, Joseph M. Young, Jonathan E. Gable, Mark Knapp, Imad Hanna, Jean-Rene Galarneau, John Cantwell, Upendra Kulkarni, Michael Turner, Peichao Lu, Kristen H. Darrell, Lucy C. Watson, Katherine Chan, Debjani Patra, Mulugeta Mamo, Catherine Luu, Carlos Cuellar, Jacob Shaul, Linda Xiao, Ying-Bo Chen, Shannon K. Carney, Jay Lakshman, Colin S. Osborne, Jennifer A. Zambriski, Natasha Aziz, Christopher Sarko, Thierry T. Diagana","doi":"10.1038/s41564-024-01810-x","DOIUrl":null,"url":null,"abstract":"Diarrhoeal disease caused by Cryptosporidium is a major cause of morbidity and mortality in young and malnourished children from low- and middle-income countries, with no vaccine or effective treatment. Here we describe the discovery of EDI048, a Cryptosporidium PI(4)K inhibitor, designed to be active at the infection site in the gastrointestinal tract and undergo rapid metabolism in the liver. By using mutational analysis and crystal structure, we show that EDI048 binds to highly conserved amino acid residues in the ATP-binding site. EDI048 is orally efficacious in an immunocompromised mouse model despite negligible circulating concentrations, thus demonstrating that gastrointestinal exposure is necessary and sufficient for efficacy. In neonatal calves, a clinical model of cryptosporidiosis, EDI048 treatment resulted in rapid resolution of diarrhoea and significant reduction in faecal oocyst shedding. Safety and pharmacological studies demonstrated predictable metabolism and low systemic exposure of EDI048, providing a substantial safety margin required for a paediatric indication. EDI048 is a promising clinical candidate for the treatment of life-threatening paediatric cryptosporidiosis. EDI048 is a gastrointestinal-targeted Cryptosporidium PI(4)K inhibitor that undergoes a predictable metabolism and limits systemic exposure without compromising its anti-parasitic activity.","PeriodicalId":18992,"journal":{"name":"Nature Microbiology","volume":"9 11","pages":"2817-2835"},"PeriodicalIF":20.5000,"publicationDate":"2024-10-08","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"https://www.nature.com/articles/s41564-024-01810-x.pdf","citationCount":"0","resultStr":"{\"title\":\"Cryptosporidium PI(4)K inhibitor EDI048 is a gut-restricted parasiticidal agent to treat paediatric enteric cryptosporidiosis\",\"authors\":\"Ujjini H. Manjunatha, Suresh B. Lakshminarayana, Rajiv S. Jumani, Alexander T. Chao, Joseph M. Young, Jonathan E. Gable, Mark Knapp, Imad Hanna, Jean-Rene Galarneau, John Cantwell, Upendra Kulkarni, Michael Turner, Peichao Lu, Kristen H. Darrell, Lucy C. Watson, Katherine Chan, Debjani Patra, Mulugeta Mamo, Catherine Luu, Carlos Cuellar, Jacob Shaul, Linda Xiao, Ying-Bo Chen, Shannon K. Carney, Jay Lakshman, Colin S. Osborne, Jennifer A. Zambriski, Natasha Aziz, Christopher Sarko, Thierry T. Diagana\",\"doi\":\"10.1038/s41564-024-01810-x\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"Diarrhoeal disease caused by Cryptosporidium is a major cause of morbidity and mortality in young and malnourished children from low- and middle-income countries, with no vaccine or effective treatment. Here we describe the discovery of EDI048, a Cryptosporidium PI(4)K inhibitor, designed to be active at the infection site in the gastrointestinal tract and undergo rapid metabolism in the liver. By using mutational analysis and crystal structure, we show that EDI048 binds to highly conserved amino acid residues in the ATP-binding site. EDI048 is orally efficacious in an immunocompromised mouse model despite negligible circulating concentrations, thus demonstrating that gastrointestinal exposure is necessary and sufficient for efficacy. In neonatal calves, a clinical model of cryptosporidiosis, EDI048 treatment resulted in rapid resolution of diarrhoea and significant reduction in faecal oocyst shedding. Safety and pharmacological studies demonstrated predictable metabolism and low systemic exposure of EDI048, providing a substantial safety margin required for a paediatric indication. EDI048 is a promising clinical candidate for the treatment of life-threatening paediatric cryptosporidiosis. 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Cryptosporidium PI(4)K inhibitor EDI048 is a gut-restricted parasiticidal agent to treat paediatric enteric cryptosporidiosis
Diarrhoeal disease caused by Cryptosporidium is a major cause of morbidity and mortality in young and malnourished children from low- and middle-income countries, with no vaccine or effective treatment. Here we describe the discovery of EDI048, a Cryptosporidium PI(4)K inhibitor, designed to be active at the infection site in the gastrointestinal tract and undergo rapid metabolism in the liver. By using mutational analysis and crystal structure, we show that EDI048 binds to highly conserved amino acid residues in the ATP-binding site. EDI048 is orally efficacious in an immunocompromised mouse model despite negligible circulating concentrations, thus demonstrating that gastrointestinal exposure is necessary and sufficient for efficacy. In neonatal calves, a clinical model of cryptosporidiosis, EDI048 treatment resulted in rapid resolution of diarrhoea and significant reduction in faecal oocyst shedding. Safety and pharmacological studies demonstrated predictable metabolism and low systemic exposure of EDI048, providing a substantial safety margin required for a paediatric indication. EDI048 is a promising clinical candidate for the treatment of life-threatening paediatric cryptosporidiosis. EDI048 is a gastrointestinal-targeted Cryptosporidium PI(4)K inhibitor that undergoes a predictable metabolism and limits systemic exposure without compromising its anti-parasitic activity.
期刊介绍:
Nature Microbiology aims to cover a comprehensive range of topics related to microorganisms. This includes:
Evolution: The journal is interested in exploring the evolutionary aspects of microorganisms. This may include research on their genetic diversity, adaptation, and speciation over time.
Physiology and cell biology: Nature Microbiology seeks to understand the functions and characteristics of microorganisms at the cellular and physiological levels. This may involve studying their metabolism, growth patterns, and cellular processes.
Interactions: The journal focuses on the interactions microorganisms have with each other, as well as their interactions with hosts or the environment. This encompasses investigations into microbial communities, symbiotic relationships, and microbial responses to different environments.
Societal significance: Nature Microbiology recognizes the societal impact of microorganisms and welcomes studies that explore their practical applications. This may include research on microbial diseases, biotechnology, or environmental remediation.
In summary, Nature Microbiology is interested in research related to the evolution, physiology and cell biology of microorganisms, their interactions, and their societal relevance.