(A) En face view of immunostained lungs from lineage-traced Kit^CreER; Rosa^tdT/+ mice, demonstrating a decrease in Cap1 EC number in hyperoxia relative to room air. Hyperoxia-treated lungs also exhibited a stark increase in the proportion of tdT⁺ cells that express CAR4 (yellow arrowheads), suggesting increased conversion from Cap1 to Cap2 in hyperoxia. Boxed regions are shown at a higher magnification to the right. (B) Top: Quantification of tdT⁺ Cap1 ECs in room air and hyperoxia, revealing a significant decrease in lineage-traced Cap1 ECs (Student’s t test). Bottom: Quantification of the proportion of Car4⁺tdT⁺ cells of total tdT⁺ cells in room air and hyperoxia, confirming a significant increase in conversion from lineage-traced Cap1 ECs to Cap2 in hyperoxia (Student’s t test). (C) En face view of immunostained lungs from lineage-traced Car4^CreER; Rosa^tdT/+ mice. Hyperoxia exposure resulted in a reduction in tdT⁺ Cap2 cells, representing Cap2 ECs present before treatment (magenta arrowheads). Some remaining tdT⁺ cells showed a loss in CAR4 expression in hyperoxia (open arrowheads), while tdT^– Cap2 cells (CAR4⁺) also appeared in hyperoxia, mostly representing new Cap2 cells converted from Cap1 (yellow arrowheads). (D) Quantification of tdT⁺ Cap2 ECs in room air and hyperoxia, showing a downward trend in lineage-traced Cap2 ECs (Student’s t test). (E) En face view of immunostained lungs showing individual tdT-labeled Cap2 cells in room air and hyperoxia, demonstrating the loss of the expansive, net-like morphology of Cap2 cells upon sustained hyperoxic injury. Boxed regions are shown at a higher magnification in insets. Images are representative of at least 3 littermate pairs. For quantification, each symbol represents the average of 3 distinct regions imaged within 1 mouse lung. m, macrophage; v, large vessel. TAM, 300 μg tamoxifen administered at P0. Scale bars: 10 μm.