With global air pollution massively on the rise, chronic obstructive pulmonary disease (COPD) with accompanying emphysema is a huge and growing health burden (HL-131). Worldwide, COPD affects 330 Mio people, is the third-leading cause of death with a rapidly rising toll in developing countries and an estimated cost of $2.1 trillion. COPD is a slowly progressive incurable disease of distal airways and lung parenchyma, eventually leading to respiratory failure and death. Chronic bronchitis with airway narrowing and alveolar wall destruction are pathologic hallmarks. Symptoms are mostly therapy-resistant. Airway epithelial cells and innate immune cells are key components of the pathogenesis of COPD, and emerging targets for urgently needed new therapies. Yet our understanding of how this specialized barrier epithelium is regulated is limited. Thus, it is paramount to identify new critical regulators of this tissue. Few airway mouse models of COPD exist and mostly focus on inflammatory regulators and proteases. The p73 gene, a relative of the p53 tumor suppressor with developmental roles in brain and germ cells, encodes two classes of isoforms called TAp73 (transcription factors with a transcriptional activation domain) and DeltaNp73 (DNp73, lacking the N-terminal TA domain and often a dominant-negative inhibitor of the p53/TAp63/TAp73). We discovered strong in vivo evidence for p73 in governing differentiation, integrity and renewal of airway (but not alveolar) epithelium. We find p73 expressed in human and mouse airway epithelium under differentiating conditions, in homeostasis and repair. Notably, p73-deficient mice exhibit severe airway defects and spontaneously develop progressive COPD followed by secondary emphysema. Thus, they are a powerful new genetic model for the epithelial airway component of the disease. Based on separable phenotypes in global (missing all p73 isoforms) and isoform-specific knockout (KO) mice, we identified three distinct functions of p73 isoforms within the airway epithelium. TAp73 appears to be a master regulator of motile multiciliogenesis in ciliated human and mouse cells, while DNp73 appears critical for airway epithelial cohesion and lifelong maintenance of basal stem/progenitor pools for regeneration and repair. Linking COPD to a gene of the p53 family are completely novel and exciting findings. They carry a high potential to greatly extend our understanding of normal airway biology and the pathophysiology of COPD. This proposal aims to firmly establish p73 as a major novel regulator, with the long-term goal of using this knowledge to develop innovative therapeutic strategies for chronic airway disease.
Aim 1 will test the hypothesis that TAp73 is a master regulator of multiciliogenesis, using transcriptional and functional analyses in mouse and human primary organotypic cultures and in frog embryo skin.
Aim 2 will test the hypothesis that DNp73 mediates cell-cell and cell-matrix cohesion within airway epithelium by exploiting a clever isoform- specific DNp73KO/reporter mouse.
Aim 3 will use lineage tracing in mice and clonal tracheosphere assays to determine if DNp73 is an essential regulator of basal stem cells in homeostasis and repair.

Public Health Relevance

With global air pollution and smoking on the rise, chronic obstructive pulmonary disease (COPD) is a huge and growing public health burden for which there is no cure and little symptomatic relief, eventually leading to respiratory failure and death COPD's hallmarks are chronic airway inflammation with narrowing and destruction of gas-exchanging lung tissue. The specialized epithelial cells lining the conducting airways play a key role in disease development and are emerging targets for new therapies. However, our understanding of how this tissue is regulated is limited. Our new studies unexpectedly have shown strong evidence that the p73 gene, a relative of the p53 tumor suppressor, governs differentiation, integrity and self-renewal of airway epithelium. This proposal aims to firmly establish p73 as a major regulator of the biology of airway epithelium, with the long-term goal of using this knowledge to improve therapeutic and diagnostic strategies for chronic airway disease.

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL129223-03
Application #
9288222
Study Section
Lung Cellular, Molecular, and Immunobiology Study Section (LCMI)
Program Officer
Postow, Lisa
Project Start
2015-09-01
Project End
2019-05-31
Budget Start
2017-06-01
Budget End
2018-05-31
Support Year
3
Fiscal Year
2017
Total Cost
$494,753
Indirect Cost
$181,618
Name
State University New York Stony Brook
Department
Pathology
Type
Schools of Medicine
DUNS #
804878247
City
Stony Brook
State
NY
Country
United States
Zip Code
11794
Nemajerova, Alice; Amelio, Ivano; Gebel, Jakob et al. (2018) Non-oncogenic roles of TAp73: from multiciliogenesis to metabolism. Cell Death Differ 25:144-153
Nemajerova, Alice; Kramer, Daniela; Siller, Saul S et al. (2016) TAp73 is a central transcriptional regulator of airway multiciliogenesis. Genes Dev 30:1300-12