In emphysema the lung cannot spontaneously regenerate lost alveolar tissue. Treatment with retinoic acid (RA) in rodent models of emphysema induces alveolar regeneration. However some animal studies have failed to show regeneration when using different species and strains. We have previously shown that Dexamethasone (Dex) treatment of newborn TO outbred strain mice permanently disrupts alveolar development. Later RA treatment restores alveolar architecture to normal. To determine whether this model of alveolar regeneration is strain-specific, our protocol was repeated with 2 new outbred mouse strains. ICR and NIHS mice received Dex from postnatal day 4-15 (P4-15). From P46-57 mice received RA (2 mg/kg) or vehicle. An additional ICR group received 5xRA (10 mg/kg) from P46-57. Control groups received vehicle at both treatment points. All mice were sacrificed at P90 and lung morphology analysed. Dex-treated ICR and NIHS mice showed increased mean alveolar chord length (Lm) and reduced alveolar surface area (SA) and SA/lung volume (SA/LV) compared with controls. RA-treated NIHS mice showed return of Lm, SA and SA/LV towards control values, indicating alveolar regeneration. ICR RA group mice did not regenerate, but 5xRA mice showed Lm, SA and SA/LV values consistent with alveolar regeneration. In conclusion, the Dex-treated mouse model of emphysema is robust and repeatable in different strains. RA-induced alveolar regeneration is not a strain-specific phenomenon. RA dose threshold for inducing alveolar regeneration is higher in ICR mice, suggesting a difference in retinoid pharmacokinetics between strains. These results provide a possible explanation for previous failed studies of RA-induced alveolar regeneration.