# Mechanosensitive mechanism of age-dependent decline in angiogenesis in the lung

> **NIH NIH R21** · MEDICAL COLLEGE OF WISCONSIN · 2020 · $190,000

## Abstract

Project Summary
Age-dependent impairment of lung regeneration and repair contributes to the pathogenesis of aging-
associated chronic lung diseases (CLD). Angiogenesis – the formation of new blood capillaries- plays a key
role in lung regeneration and is impaired in aging animals. Thus, in order to develop more efficient therapies for
aging-associated CLD, we need to understand the mechanisms by which aging impairs angiogenesis in the
lung. In addition to soluble growth factors and signaling molecules, biophysical factors alter angiogenic gene
expression and regulate angiogenesis. We have reported that changes in cell size and geometry control
endothelial cell (EC) growth. It is known that cell size increases during aging in various tissues. However, the
effects of age-dependent increases in EC size on impairment of angiogenesis in the aged lung and the
underlying mechanism have not been explored. The overall goal of this proposal is to characterize the
mechanosensitive mechanism of age-dependent decline in angiogenesis, and to leverage this knowledge to
develop an efficient strategy for CLD. Angiopoietin (Ang)-Tie2 signaling controls angiogenesis and plays
important roles in lung development and regeneration. The mechanosensitive transcriptional co-activator, Yes-
associated protein (YAP1), senses various mechanical forces and controls organ development and
regeneration. YAP1 stimulates angiogenesis through angiopoietin2 (Ang2) signaling and deregulation of YAP1
is involved in the pathogenesis of aging-associated CLD. Our new preliminary data demonstrate that
pulmonary ECs in aged mice are significantly larger than those in young mice. The levels of YAP1 are lower
and EC proliferation is inhibited in ECs isolated from aged mouse lungs compared to those from younger
mouse lungs. YAP1 knockdown decreases Ang2 expression in mouse lung ECs and the levels of Ang2 is
lower in aged mouse lung ECs. When we culture aged lung ECs on single-cell sized fibronectin-coated large
islands comparable in size to aged mouse lung EC, YAP1 is excluded from the nucleus and is inactive, while
reduction of aged EC size restores YAP1 nuclear localization. Vascular network formation is inhibited in the
fibrin gel implanted on the aged mouse lungs. We hypothesize that age-dependent increases in EC size may
suppress aged EC proliferation and angiogenesis in the aged mouse lung through aberrant YAP1-Ang2
signaling. In Aim1, we will investigate the effects of age-dependent changes in EC size on EC proliferation,
apoptosis, and senescence using the microcontact printing system. In Aim2, we will determine whether EC
size-dependent changes in YAP1 signaling mediates impairment of angiogenesis in the aged lung through
Ang2. Our idea to focus on the effects of age-related changes in EC size on angiogenesis is highly unique and
innovative advances. If this study proves that reduction of aged EC size reverses the age-dependent decline in
vascular morphogenesis in the aged lungs thr...

## Key facts

- **NIH application ID:** 9906834
- **Project number:** 5R21AG062893-02
- **Recipient organization:** MEDICAL COLLEGE OF WISCONSIN
- **Principal Investigator:** TADANORI MAMMOTO
- **Activity code:** R21 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2020
- **Award amount:** $190,000
- **Award type:** 5
- **Project period:** 2019-04-15 → 2021-12-31

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/9906834

## Citation

> US National Institutes of Health, RePORTER application 9906834, Mechanosensitive mechanism of age-dependent decline in angiogenesis in the lung (5R21AG062893-02). Retrieved via AI Analytics 2026-05-25 from https://api.ai-analytics.org/grant/nih/9906834. Licensed CC0.

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