Table 2.
Passive immunization preclinical and clinical trials against P. aeruginosa infections.
| Immunogen | Clinical Trial | Immunization Protocol | Results | References | |
|---|---|---|---|---|---|
| Pros | Cons | ||||
| KB001 (anti-PcrV PEGylated mouse Mab) |
Phase 1/2 (NCT00691587): Safety and pharmacokinetics (PK) of KB001 in mechanically ventilated (MV) ICU patients colonized with P. aeruginosa. | Patients (older than 18 years) will receive randomly either placebo, or single low-dose or single high-dose of KB001 intravenously (IV). | Safe and well-tolerated. | No anti-KB001 antibodies were detected. | [64,77] |
| Decrease in the incidence of P. aeruginosa associated pneumonia in patients on MV. | |||||
| Phase 1/2 (NCT00638365): Dose escalation study of KB001 in CF patients colonized with P. aeruginosa. | Patients (older than 12 years) will randomly receive either placebo, single-dose 3 mg/kg or single-dose 10 mg/kg of KB001 IV. | Safe and well-tolerated. | No significant differences between KB001 and the placebo | ||
| Reduced lung inflammation of KB001 vaccinated patients. | group in P. aeruginosa colonization of CF patients. | ||||
| KB001-A | Phase 2 (NCT01695343): Evaluation of the effect of KB001-A on time-to-need for antibiotic treatment of CF patients. | Patients (12–50 years of age) will randomly receive either placebo, KB001-A up to 5× IV at 10 mg/kg to a maximum dose of 800 mg per dose. | Safe and well-tolerated. | Reduced clinical efficacy, being not associated with an increased time to need for antibiotics. | [63] |
| (anti-PcrV PEGylated mouse MAb) | Modest FEV1 benefit and reduction in selected sputum inflammatory markers (IL-8). | ||||
| (One amino acid difference from KB001) | |||||
| V2L2MD | Preclinical | Good prophylactic protection in several mouse models of P. aeruginosa infection. | [66] | ||
| (anti-PcrV Human MAb) | |||||
| MEDI3902 (anti-PcrV and Psl bispecific human MAb) |
Phase 1 (NCT02255760): Safety evaluation, PK, anti-drug antibody (ADA) responses, ex vivo anticytotoxicity and OPK of MEDI3902 in healthy adults | Single IV infusion in healthy adults aged 18–60 years. | The safety and tolerability profile of MEDI3902 was acceptable. | Infusion-related reaction (e.g., skin rash). | [71,78] |
| Dose-escalation study: subjects were randomized in a 3:1 ratio to receive 250, 750, 1500 or 3000 mg of MEDI3902 or placebo. | Anti–P. aeruginosa activity was demonstrated in sera of treated subjects. | ||||
| Subjects followed for 60 days afterwards. | |||||
| Phase 2 (NCT02696902): Evaluation of MEDI3902 efficacy and safety on the prevention of P. aeruginosa nosocomial pneumonia in MV patients | Participants will receive a single IV dose of placebo, MEDI3902 500 mg or MEDI3902 1500 mg. | Some clinical efficacy in ICU patients with lower baseline inflammation. | |||
| Panobacumab or KBPA-101 or AR-101 (IgM/κ isotype directed against the LPS O-polysaccharide moiety of P. aeruginosa serotype O11) |
Phase 2: PK and safety profile of KBPA-101 in healthy volunteers | No adverse effects in healthy volunteers. | [61,69] | ||
| NCT00851435 (phase 2): Safety and PK in patients with hospital acquired pneumonia (HAP) caused by serotype O11 P. aeruginosa | HAP patients (older than 18 years of age) were treated by IV infusion of 1.2 mg/kg KBPA-101, 3 separate doses, every third day. | Improve clinical outcome in a shorter time. | |||
| Passive immunotherapy targeting LPS can be a complementary strategy for the treatment of nosocomial P. aeruginosa pneumonia. | |||||
| Aerucin or AR-105 (Human IgG1 MAb that targets P. aeruginosa alginate) |
NCT02486770 (phase 1): Safety evaluation of Aerucin in healthy individuals. | IV administration up to 20 mg/kg monitored for 84 days in healthy individuals. | Safety up to doses of 20 mg/kg. | [79] | |
| NCT03027609 (phase 2): Efficacy, safety and PK evaluation of Aerucin in combination with standard antibiotic treatment in P. aeruginosa VAP patients. | Placebo controlled, double-blind, randomized trial. | No significant difference between Aerucin and placebo patient groups for treatment of P. aeruginosa VAP patients. | |||
| Single IV infusion of Aerucin 20 mg/kg. | |||||
| PseudIgY | NCT00633191 (phase 2): Study of anti-pseudomonas IgY in prevention of recurrence of P. aeruginosa infections in CF Patients. | Oral administration (gargle solution) of CF patients every night after toothbrushing. | After 12 years of prophylactic anti-Pseudomonas IgY treatment a reduction was observed in the level of infections with P. aeruginosa in the treated CF patients and no decrease in lung function. | [72] | |
| (anti-pseudomonas IgY gargle) | |||||
| PsAer-IgY (anti-pseudomonas IgY gargle) |
NCT01455675 (phase 3): Evaluation of the clinical efficacy and safety of anti-Pseudomonas IgY in prevention of recurrence of P. aeruginosa infection in CF patients | Randomized, double-blind, | IgY antibodies were present in the oral cavity of treated patients for up to 24 h. | Clinical efficacy results were unclear. | [76] |
| placebo-controlled. | No adverse immune or allergic reaction. | ||||
| Oral administration of CF patients (older than 5 years of age), every day with 70 mL gargling solution (contains 50 mg IgY) or placebo. Treatment for 24 months. | |||||