ABSTRACT:. The overarching long-term objective of this project is to identify principal genetic regulators of alveogenesis. Alveolar defects underlie many neonatal and adult lung diseases. Their arrested development is found in infants with BPD (BronchoPulmonary Dysplasia), while their destruction is characteristic of emphysematous lungs in adults. Despite significant clinical relevance, alveogenesis remains the least understood phase of lung development! We have developed 2 parallel, postnatal genetically-based models to analyze the molecular basis of alveogenesis. In Tgfβr1/2Gli mice, conditional postnatal inactivation of both Alk5 & Tβr2 in secondary crest myofibroblasts, SCMF blocks alveogenesis & disrupts epithelial morphogenesis. Similar strategy in the PdgfrαGli model also yields a nearly identical phenotype. We reasoned that due to nearly identical phenotypes, the two models must share in common some genetic elements whose role in alveogenesis is indispensable. Preliminary data using RNAseq/bioinformatics identified “pathway-specific” differentially expressed genes (DEG) for TGFβ and PDGFA/PDGFRα mutant models. Most importantly, as predicted, we identified a cluster of “common” genes which we propose contains a cluster of conserved core alveogenesis regulatory genes. These preliminary data, justify a more comprehensive and expanded analysis of DEG to improve the reliability of the RNAseq data (Specific Aim 1). In Specific Aim 2, we will validate and functionally characterize the common genes. A notable gene in the initial cluster is Igf1, which encodes the ligand for the IGF1 signaling pathway. We have selected IGF1 for further functional analyses (Specific Aims 3 and 4). HYPOTHESIS: TGFβ, PDGFA/PDGFRa & IGF1 form major sub-circuits of a complex signaling network in SCMF that controls alveogenesis via a cluster of downstream “alveogenesis regulatory genes”. This cluster is uniquely conserved & can be identified by comparative differential gene expression analysis using mutations in each of the three pathways & identifying the common DEG. The Specific Aims are: Specific Aim 1:. Identify Conserved SCMF Regulatory Genes That Control Alveogenesis Thru Analysis of Differentially Expressed Genes in PdgfrαGli1 & Tgfβr1/2Gli1 Lungs. Specific Aim 2:. Validate and Functionally Analyze Candidate Genes from Specific Aim 1. Specific Aim 3:. Develop Conditional, Cell-Targeted Genetic Model of IGF1 Signaling to Interrogate This Pathway as a Key Highly Conserved Regulatory Node in Alveolar Assembly & Epithelial Morphogenesis. Specific aim 4:. To Use Recombinant IGF1 to Identify Candidate IGF1-Regulated Alveogenesis Regulatory Genes via Rescue of Tgfβr1/2Gli1 Lungs. Impact: The alveolus is the functional unit of respiration. Its proper assembly requires coordinated function amongst endodermal, mesodermal, endothelial & perhaps immune cells. Elucidation of the mechanisms not only has an impact, but is necessary for understanding both neonatal (e.g. BPD, CD...