Development and validation of a rabbit model of Pseudomonas aeruginosa non-ventilated pneumonia for preclinical drug development

Emmanuelle Gras; Trang T T Vu; Nhu T Q Nguyen; Vuvi G Tran; Yanjie Mao; Nguyen D Tran; Nam H Mai; Oliver X Dong; David H Jung; Natalia L P P Iorio; Helvecio C C Povoa; Marcos Gabriel Pinheiro; Fabio Aguiar-Alves; William J Weiss; Bo Zheng; Lily I Cheng; Charles K Stover; Bret R Sellman; Antonio DiGiandomenico; Laure Gibault; Florent Valour; Binh An Diep

doi:10.3389/fcimb.2023.1297281

Development and validation of a rabbit model of Pseudomonas aeruginosa non-ventilated pneumonia for preclinical drug development

Front Cell Infect Microbiol. 2023 Dec 11:13:1297281. doi: 10.3389/fcimb.2023.1297281. eCollection 2023.

Authors

Emmanuelle Gras^#^{1

2}, Trang T T Vu^#¹, Nhu T Q Nguyen¹, Vuvi G Tran¹, Yanjie Mao^{1

3}, Nguyen D Tran^{1

4}, Nam H Mai¹, Oliver X Dong¹, David H Jung¹, Natalia L P P Iorio^{1

5}, Helvecio C C Povoa^{1

5}, Marcos Gabriel Pinheiro¹, Fabio Aguiar-Alves^{1

6}, William J Weiss⁷, Bo Zheng⁸, Lily I Cheng⁹, Charles K Stover⁹, Bret R Sellman⁹, Antonio DiGiandomenico⁹, Laure Gibault¹⁰, Florent Valour^{1

11

12

13}, Binh An Diep¹

Affiliations

¹ Division of HIV, Infectious Diseases, and Global Medicine, Department of Medicine, University of California San Francisco, San Francisco, CA, United States.
² Université François Rabelais, Tours, France.
³ Department of Orthopaedic Surgery, Shanghai Jiao Tong University Affiliated Sixth People's Hospital, Shanghai, China.
⁴ University of Medicine and Pharmacy, Ho Chi Minh City, Vietnam.
⁵ Department of Basic Science, Fluminense Federal University, Nova Friburgo, Rio de Janeiro, Brazil.
⁶ Pathology Program, Universidade Federal Fluminense, Niterói, Rio de Janeiro, Brazil.
⁷ Pre-Clinical Services at UNT Health Science Center, Fort Worth, TX, United States.
⁸ Clinical Pharmacology & DMPK, AstraZeneca, Gaithersburg, MD, United States.
⁹ Early Vaccines and Immune Therapies, AstraZeneca, Gaithersburg, MD, United States.
¹⁰ Pathology Department, George Pompidou European Hospital, Paris, France.
¹¹ Department of Infectious Diseases, Hospices Civils de Lyon, Lyon, France.
¹² CIRI - Centre International de Recherche en Infectiologie, Inserm, U1111, University of Lyon, Lyon, France.
¹³ Université Claude Bernard Lyon 1, CNRS, UMR5308, Ecole Normale Supérieure de Lyon, University of Lyon, Lyon, France.

^# Contributed equally.

Abstract

Background: New drugs targeting antimicrobial resistant pathogens, including Pseudomonas aeruginosa, have been challenging to evaluate in clinical trials, particularly for the non-ventilated hospital-acquired pneumonia and ventilator-associated pneumonia indications. Development of new antibacterial drugs is facilitated by preclinical animal models that could predict clinical efficacy in patients with these infections.

Methods: We report here an FDA-funded study to develop a rabbit model of non-ventilated pneumonia with Pseudomonas aeruginosa by determining the extent to which the natural history of animal disease reproduced human pathophysiology and conducting validation studies to evaluate whether humanized dosing regimens of two antibiotics, meropenem and tobramycin, can halt or reverse disease progression.

Results: In a rabbit model of non-ventilated pneumonia, endobronchial challenge with live P. aeruginosa strain 6206, but not with UV-killed Pa6206, caused acute respiratory distress syndrome, as evidenced by acute lung inflammation, pulmonary edema, hemorrhage, severe hypoxemia, hyperlactatemia, neutropenia, thrombocytopenia, and hypoglycemia, which preceded respiratory failure and death. Pa6206 increased >100-fold in the lungs and then disseminated from there to infect distal organs, including spleen and kidneys. At 5 h post-infection, 67% of Pa6206-challenged rabbits had PaO₂ <60 mmHg, corresponding to a clinical cut-off when oxygen therapy would be required. When administered at 5 h post-infection, humanized dosing regimens of tobramycin and meropenem reduced mortality to 17-33%, compared to 100% for saline-treated rabbits (P<0.001 by log-rank tests). For meropenem which exhibits time-dependent bactericidal activity, rabbits treated with a humanized meropenem dosing regimen of 80 mg/kg q2h for 24 h achieved 100% T>MIC, resulting in 75% microbiological clearance rate of Pa6206 from the lungs. For tobramycin which exhibits concentration-dependent killing, rabbits treated with a humanized tobramycin dosing regimen of 8 mg/kg q8h for 24 h achieved C_max/MIC of 9.8 ± 1.4 at 60 min post-dose, resulting in 50% lung microbiological clearance rate. In contrast, rabbits treated with a single tobramycin dose of 2.5 mg/kg had C_max/MIC of 7.8 ± 0.8 and 8% (1/12) microbiological clearance rate, indicating that this rabbit model can detect dose-response effects.

Conclusion: The rabbit model may be used to help predict clinical efficacy of new antibacterial drugs for the treatment of non-ventilated P. aeruginosa pneumonia.

Keywords: Pseudomonas aeruginosa; meropenem; non-ventilated pneumonia model; preclinical efficacy model validation; rabbit model; tobramycin.

Publication types

Research Support, N.I.H., Extramural

MeSH terms

Animals
Anti-Bacterial Agents / pharmacology
Anti-Bacterial Agents / therapeutic use
Drug Development
Humans
Meropenem / therapeutic use
Microbial Sensitivity Tests
Pneumonia* / drug therapy
Pseudomonas Infections* / drug therapy
Pseudomonas Infections* / microbiology
Pseudomonas aeruginosa
Rabbits
Tobramycin / pharmacology
Tobramycin / therapeutic use

Substances

Meropenem
Anti-Bacterial Agents
Tobramycin

Grants and funding

FD/FDA HHS/United States