Table 3.
Summary of studies of dry powder measles product presented to the expert group for stage II of the CHNRI process
| Reference | Factor for investigation | Results | Conclusions |
|---|---|---|---|
| LiCalsi, C., et al [55] |
Feasibility of dry powder inhalation in measles | Optimal vaccine delivery site – lungs; Particle sizing 1-5μm; Preparation – micronization and jet-milling ;3 Spiros delivery devices designed | Undemonstrable clinical application |
| de Swart, R.L., et al [56] |
Dry powder vaccination in Macaques | Low seroresponse to measles dry powder blend compared to injection or liquid aerosol vaccination | Proof of principle evident by stimulation of weak immune response. Poor device design in macaque model – loss of vaccine at delivery. |
| LiCalsi, C., et al [57] |
Dry powder measles vaccine potency retention | Up to 89% viral potency retention can be achieved with micronization. | |
| Burger, J.L., et al [58] |
Stabilizing dry powder measles formulations | Myo-inositol> trehalose as a sugar stabilizer in dry powder measles vaccinations | Myo-inositol is relatively unhygroscopic, improving its dry powder vaccination credentials |