Determining Protease Substrates Within a Complex Protein Background Using the PROtein TOpography and Migration Analysis Platform (PROTOMAP)

Author(s):  
R. A. Fuhrman-Luck ◽  
L. M. Silva ◽  
M. L. Hastie ◽  
J. J. Gorman ◽  
J. A. Clements
2020 ◽  
Vol 127 (8) ◽  
pp. 997-1022
Author(s):  
Tomáš Vaisar ◽  
Jie H. Hu ◽  
Nathan Airhart ◽  
Kate Fox ◽  
Jay Heinecke ◽  
...  

Rationale: Plaque rupture is the proximate cause of most myocardial infarctions and many strokes. However, the molecular mechanisms that precipitate plaque rupture are unknown. Objective: By applying proteomic and bioinformatic approaches in mouse models of protease-induced plaque rupture and in ruptured human plaques, we aimed to illuminate biochemical pathways through which proteolysis causes plaque rupture and identify substrates that are cleaved in ruptured plaques. Methods and Results: We performed shotgun proteomics analyses of aortas of transgenic mice with macrophage-specific overexpression of urokinase (SR-uPA +/0 mice) and of SR-uPA +/0 bone marrow transplant recipients, and we used bioinformatic tools to evaluate protein abundance and functional category enrichment in these aortas. In parallel, we performed shotgun proteomics and bioinformatics studies on extracts of ruptured and stable areas of freshly harvested human carotid plaques. We also applied a separate protein-analysis method (protein topography and migration analysis platform) to attempt to identify substrates and proteolytic fragments in mouse and human plaque extracts. Approximately 10% of extracted aortic proteins were reproducibly altered in SR-uPA +/0 aortas. Proteases, inflammatory signaling molecules, as well as proteins involved with cell adhesion, the cytoskeleton, and apoptosis, were increased. ECM (Extracellular matrix) proteins, including basement-membrane proteins, were decreased. Approximately 40% of proteins were altered in ruptured versus stable areas of human carotid plaques, including many of the same functional categories that were altered in SR-uPA +/0 aortas. Collagens were minimally altered in SR-uPA +/0 aortas and ruptured human plaques; however, several basement-membrane proteins were reduced in both SR-uPA +/0 aortas and ruptured human plaques. Protein topography and migration analysis platform did not detect robust increases in proteolytic fragments of ECM proteins in either setting. Conclusions: Parallel studies of SR-uPA +/0 mouse aortas and human plaques identify mechanisms that connect proteolysis with plaque rupture, including inflammation, basement-membrane protein loss, and apoptosis. Basement-membrane protein loss is a prominent feature of ruptured human plaques, suggesting a major role for basement-membrane proteins in maintaining plaque stability.


Author(s):  
Gemma Vall-llosera ◽  
Albert Rafel ◽  
Neil Parkin ◽  
Marianna Angelou ◽  
Dimitrios Klonidis ◽  
...  

2020 ◽  
Vol 17 (2) ◽  
pp. 379-398 ◽  
Author(s):  
Ibrahim Sirkeci ◽  
Mustafa Murat Yucesahin

Reactions, measures as well as discourses dealing with the current pandemic vary significantly across the world. While some countries were completely locked down, as was the case in Italy, some had claimed to have very few or no cases, as was the case in Turkey and Indonesia by March 10th, 2020. Nevertheless, the spread of COVID-19 from China has been clearly linked to those travelling from Wuhan in Hubei province in Central China. Therefore, it is important to understand the travel density/volume of passengers carried as well as routes from Wuhan through connected main regional air travel hubs across China. In this study, we developed a model on migration and travel intensity that can explain outbreak and spread COVID-19 since it appeared at the end of 2019. We show that the presence of migrant stock populations of Chinese origin and the immigrant stock in China are useful indicators in the prediction of the spread of the outbreak worldwide in the event of interaction with several other macro factors. We argue that monitoring immigrant stock data and travel volume data based on human mobility corridors (i.e. origins and destinations), countries could have been better prepared and taken early measures to contain the spread of COVID-19.


1975 ◽  
Vol 57 (1) ◽  
pp. 26 ◽  
Author(s):  
A. D. Goddard ◽  
W. T. S. Gould ◽  
F. I. Masser

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