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      Potency of the novel PolC DNA polymerase inhibitor CRS0540 in a disseminated Listeria monocytogenes intracellular hollow-fibre model

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          Abstract

          Background

          Listeriosis is an orphan disease, which is nevertheless fatal in immunocompromised people. CRS0540 is a novel PolC DNA polymerase inhibitor that has demonstrated good in vitro and in vivo activity against Listeria monocytogenes.

          Methods

          Rodent-to-human allometry projection-based human population pharmacokinetics of CRS0540 were used for all studies. CRS0540 pharmacokinetics/pharmacodynamics studies in an intracellular hollow-fibre system model of disseminated listeriosis (HFS-Lister) examined the effect of eight treatment doses, administered daily over 7 days, in duplicate units. Total bacterial burden versus AUC/MIC exposures on each day were modelled using the inhibitory sigmoid E max model, while CRS0540-resistant bacterial burden was modelled using a quadratic function. Ten thousand-subject Monte Carlo simulations were used to predict an optimal clinical dose for treatment.

          Results

          The mean CRS0540 intracellular/extracellular AUC 0–24 ratio was 34.07 (standard error: 15.70) as measured in the HFS-Lister. CRS0540 demonstrated exposure-dependent bactericidal activity in the HFS-Lister, with the highest exposure killing approximately 5.0 log 10 cfu/mL. The free drug AUC 0–24/MIC associated with 80% of maximal kill (EC 80) was 36.4. Resistance emergence versus AUC/MIC was described by a quadratic function, with resistance amplification at an AUC/MIC of 54.8 and resistance suppression at an AUC/MIC of 119. Monte Carlo simulations demonstrated that for the EC 80 target, IV CRS0540 doses of 100 mg/kg achieved PTAs of >90% at MICs up to 1.0 mg/L.

          Conclusions

          CRS0540 is a promising orphan drug candidate for listeriosis. Future PK/PD studies comparing it with penicillin, the standard of care, could lead to this drug as a new treatment in immunocompromised patients.

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          Most cited references34

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          Listeria monocytogenes contamination of ready‐to‐eat foods and the risk for human health in the EU

          Abstract Food safety criteria for Listeria monocytogenes in ready‐to‐eat (RTE) foods have been applied from 2006 onwards (Commission Regulation (EC) 2073/2005). Still, human invasive listeriosis was reported to increase over the period 2009–2013 in the European Union and European Economic Area (EU/EEA). Time series analysis for the 2008–2015 period in the EU/EEA indicated an increasing trend of the monthly notified incidence rate of confirmed human invasive listeriosis of the over 75 age groups and female age group between 25 and 44 years old (probably related to pregnancies). A conceptual model was used to identify factors in the food chain as potential drivers for L. monocytogenes contamination of RTE foods and listeriosis. Factors were related to the host (i. population size of the elderly and/or susceptible people; ii. underlying condition rate), the food (iii. L. monocytogenes prevalence in RTE food at retail; iv. L. monocytogenes concentration in RTE food at retail; v. storage conditions after retail; vi. consumption), the national surveillance systems (vii. improved surveillance), and/or the bacterium (viii. virulence). Factors considered likely to be responsible for the increasing trend in cases are the increased population size of the elderly and susceptible population except for the 25–44 female age group. For the increased incidence rates and cases, the likely factor is the increased proportion of susceptible persons in the age groups over 45 years old for both genders. Quantitative modelling suggests that more than 90% of invasive listeriosis is caused by ingestion of RTE food containing > 2,000 colony forming units (CFU)/g, and that one‐third of cases are due to growth in the consumer phase. Awareness should be increased among stakeholders, especially in relation to susceptible risk groups. Innovative methodologies including whole genome sequencing (WGS) for strain identification and monitoring of trends are recommended.
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            Pasteurized milk as a vehicle of infection in an outbreak of listeriosis.

            Between June 30th and August 30th, 1983, 49 patients in Massachusetts acquired listeriosis. Seven cases occurred in fetuses or infants and 42 in immunosuppressed adults; 14 patients (29 per cent) died. Of 40 Listeria monocytogenes isolates available for testing, 32 were serotype 4b. Two case-control studies, one matching for neighborhood of residence and the other for underlying disease, revealed that the illness was strongly associated with drinking a specific brand of pasteurized whole or 2 per cent milk (odds ratio = 9, P less than 0.01 for the neighborhood-matched study; odds ratio = 11.5, P less than 0.001 for the illness-matched study). The association with milk was further substantiated by four additional analyses that suggested the presence of a dose-response effect, demonstrated a protective effect of skim milk, associated cases with the same product in an independent study in another state, and linked a specific phage type with the disease associated with milk. The milk associated with disease came from a group of farms on which listeriosis in dairy cows was known to have occurred at the time of the outbreak. Multiple serotypes of L. monocytogenes were isolated from raw milk obtained from these farms after the outbreak. At the plant where the milk was processed, inspections revealed no evidence of improper pasteurization. These results support the hypothesis that human listeriosis can be a foodborne disease and raise questions about the ability of pasteurization to eradicate a large inoculum of L. monocytogenes from contaminated raw milk.
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              A disease of rabbits characterised by a large mononuclear leucocytosis, caused by a hitherto undescribed bacillusBacterium monocytogenes (n.sp.)

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                Author and article information

                Contributors
                Journal
                J Antimicrob Chemother
                J Antimicrob Chemother
                jac
                Journal of Antimicrobial Chemotherapy
                Oxford University Press (US )
                0305-7453
                1460-2091
                October 2022
                05 August 2022
                05 August 2022
                : 77
                : 10
                : 2876-2885
                Affiliations
                Hollow Fiber System & Experimental Therapeutics Laboratories, Praedicare Inc. , Dallas, TX, USA
                Hollow Fiber System & Experimental Therapeutics Laboratories, Praedicare Inc. , Dallas, TX, USA
                Crestone, Inc. , Boulder, CO, USA
                Crestone, Inc. , Boulder, CO, USA
                Hollow Fiber System & Experimental Therapeutics Laboratories, Praedicare Inc. , Dallas, TX, USA
                Crestone, Inc. , Boulder, CO, USA
                Crestone, Inc. , Boulder, CO, USA
                Crestone, Inc. , Boulder, CO, USA
                Crestone, Inc. , Boulder, CO, USA
                Crestone, Inc. , Boulder, CO, USA
                Crestone, Inc. , Boulder, CO, USA
                Hollow Fiber System & Experimental Therapeutics Laboratories, Praedicare Inc. , Dallas, TX, USA
                Quantitative Preclinical & Clinical Sciences Department, Praedicare Inc. , Dallas, TX, USA
                Hollow Fiber System & Experimental Therapeutics Laboratories, Praedicare Inc. , Dallas, TX, USA
                Quantitative Preclinical & Clinical Sciences Department, Praedicare Inc. , Dallas, TX, USA
                Author notes
                Corresponding author. E-mail: rozvi1@ 123456praedicareinc.com
                Author information
                https://orcid.org/0000-0001-7592-8012
                Article
                dkac269
                10.1093/jac/dkac269
                9525089
                35929190
                2124e8ba-8a53-4113-a258-7bad916af914
                © The Author(s) 2022. Published by Oxford University Press on behalf of British Society for Antimicrobial Chemotherapy.

                This is an Open Access article distributed under the terms of the Creative Commons Attribution-NonCommercial License ( https://creativecommons.org/licenses/by-nc/4.0/), which permits non-commercial re-use, distribution, and reproduction in any medium, provided the original work is properly cited. For commercial re-use, please contact journals.permissions@oup.com

                History
                : 19 February 2022
                : 15 July 2022
                Page count
                Pages: 10
                Funding
                Funded by: Crestone, Inc.;
                Categories
                Original Research
                AcademicSubjects/MED00740
                AcademicSubjects/MED00290
                AcademicSubjects/MED00230

                Oncology & Radiotherapy
                Oncology & Radiotherapy

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