Differential Ubiquitination of Profilin-1 in Hypoxia-induced Pulmonary Hypertension Open Access

Zhao, Jingru (Spring 2018)

Permanent URL: https://etd.library.emory.edu/concern/etds/cn69m413j?locale=pt-BR%2A
Published

Abstract

Pulmonary hypertension (PH) is a chronic illness characterized by increased pulmonary arterial pressure due to constriction and thickening of the arterial walls. In part, this is due to smooth muscle cell proliferation. Protein ubiquitination is an important regulator of cellular proliferation. Ubiquitin ligases tag target proteins with ubiquitin moieties at lysine (K) residues to alter protein stability and expression. We used mass spectrometry (MS) to screen lung tissue from chronic hypoxia mice exposed to 10% O2 for 3 weeks for changes in ubiquitination. Profilin-1, a mediator of actin-polymerization, had decreased ubiquitination on K54 (fold change -1.86) and K126 (fold change -1.40). Overexpression of profilin-1 is associated with increased wall thickness in aortas of spontaneously hypertensive rats, but its role in PH is not well characterized. Profilin-1 promotes actin polymerization, a process that is known to play a key role in cellular proliferation, cell motility, and muscle contraction and is up-regulated in PH. We hypothesized that hypoxia-induced changes in ubiquitination of profilin-1 changes its regulation of actin polymerization, leading to proliferation of smooth muscle cells. In our hypoxia exposed human pulmonary artery smooth muscle cell (hPASMC) and chronic hypoxia mouse lung models, we found no difference in profilin-1 protein level when compared to normoxia controls. This suggests that ubiquitination of profilin-1 could be a novel mechanism of regulating its activity rather than stability. Knockdown of profilin-1 with siRNA or disrupting actin polymerization using 200nM latrunculin B or 0.25 µM cytochalasin D leads to significant decrease in hPASMC proliferation. Preliminary fractionation results also show an increased association of profilin-1 and G-actin in hypoxia. Together, our results indicate that reduced ubiquitination of profilin-1 may increase actin polymerization and contribute to PH pathogenesis.

Table of Contents

CHAPTER 1. Introduction                                                                                          1

Pulmonary Hypertension                                                                                           2

Models for Hypoxia-induced PH                                                                               10

Ubiquitin and Protein Ubiquitination                                                                      11

Profilin-1                                                                                                                    16

Summary and Hypothesis                                                                                          22       

CHAPTER 2. Methods                                                                                                 24

CHAPTER 3. Results                                                                                                    34

CHAPTER 4. Discussion                                                                                              51

REFERENCES                                                                                                                 58     

About this Honors Thesis

Rights statement
  • Permission granted by the author to include this thesis or dissertation in this repository. All rights reserved by the author. Please contact the author for information regarding the reproduction and use of this thesis or dissertation.
School
Department
Degree
Submission
Language
  • English
Research Field
Keyword
Committee Chair / Thesis Advisor
Committee Members
Last modified

Primary PDF

Thumbnail Title Date Uploaded Actions
Differential Ubiquitination of Profilin-1 in Hypoxia-induced Pulmonary Hypertension () 2018-04-10 11:59:46 -0400

Supplemental Files

Thumbnail Title Date Uploaded Actions