國立虎尾科技大學 |

Designing Microfluidic Devices for the Study of Cardiovascular Diseases.

紀錄類型:	書目-語言資料,印刷品 : Monograph/item
正題名/作者:	Designing Microfluidic Devices for the Study of Cardiovascular Diseases./
作者:	Garcia de Herreros, Antoni.
出版者:	Ann Arbor : ProQuest Dissertations & Theses, : 2022,
面頁冊數:	118 p.
附註:	Source: Dissertations Abstracts International, Volume: 84-04, Section: B.
Contained By:	Dissertations Abstracts International84-04B.
標題:	Biomechanics. -
電子資源:	http://pqdd.sinica.edu.tw/twdaoapp/servlet/advanced?query=29255869
ISBN:	9798351430874

Designing Microfluidic Devices for the Study of Cardiovascular Diseases.
Garcia de Herreros, Antoni.

Designing Microfluidic Devices for the Study of Cardiovascular Diseases. - Ann Arbor : ProQuest Dissertations & Theses, 2022 - 118 p.

Source: Dissertations Abstracts International, Volume: 84-04, Section: B.

Thesis (Ph.D.)--University of California, San Diego, 2022.

This item must not be sold to any third party vendors.

Microfluidic devices are an extremely useful tool to explore in vitro the pathophysiology of many different cardiovascular diseases. In this work, we designed two microfabricated platforms, one for the study of RBCs transmigration through the spleen and to characterize three dimensional forces exerted by cells. Red blood cells (RBCs) are cleared from the circulation when they become damaged or display aging signals targeted by macrophages. This process occurs mainly in the spleen, where blood flows through submicrometric constrictions called inter-endothelial slits (IES), subjecting RBCs to large-amplitude deformations. In this work, RBCs are circulated through microfluidic devices containing microchannels that replicate the IES. The cyclic mechanical stresses experienced by the cells affect their biophysical properties and molecular composition, accelerating cell aging. Specifically, RBCs quickly transition to a more spherical, less deformable phenotype that hinders microchannel passage, causing hemolysis. This transition is associated with the release of membrane vesicles, which self-extinguishes as the spacing between membrane-cytoskeleton linkers becomes tighter. Proteomics analysis of the mechanically aged RBCs reveals significant losses of essential proteins involved in antioxidant protection, gas transport, and cell metabolism. Finally, it is shown that these changes make mechanically aged RBCs more susceptible to macrophage phagocytosis. These results provide a comprehensive model explaining how physical stress induces RBC clearance in the spleen. The data also suggest new biomarkers of early "hemodamage" and inflammation preceding hemolysis in RBCs subjected to mechanical stress.Force exertion is an integral part of cellular phenotype regulating important cell functions and fate. In order to quantify mechanical forces at the cellular scale, traction force microscopy has traditionally been considered a standard when quantification of forces at the cell-substrate interface are required. However, quantification of compressive and shear stresses in three dimensions have been elusive due to the lack of experimental and computational techniques appropriate for this sizable challenge. This dissertation presents a novel methodology to produce photo-initiated elastic round microgels that can be functionalized and embedded in three dimensional tissues for force quantification.

ISBN: 9798351430874Subjects--Topical Terms:

565307
Biomechanics.
Subjects--Index Terms:

Microfluidic devices

Designing Microfluidic Devices for the Study of Cardiovascular Diseases.
LDR:03618nam a2200373 4500 001 1104635
005 20230619080107.5
006 m o d
007 cr#unu||||||||
008 230907s2022 ||||||||||||||||| ||eng d
020 $a 9798351430874
035 $a (MiAaPQ)AAI29255869
035 $a AAI29255869
040 $a MiAaPQ $c MiAaPQ
100 1 $a Garcia de Herreros, Antoni. $3 1413536
245 1 0 $a Designing Microfluidic Devices for the Study of Cardiovascular Diseases.
260 1 $a Ann Arbor : $b ProQuest Dissertations & Theses, $c 2022
300 $a 118 p.
500 $a Source: Dissertations Abstracts International, Volume: 84-04, Section: B.
500 $a Advisor: Del Alamo, Juan Carlos;Rangamani, Padmini.
502 $a Thesis (Ph.D.)--University of California, San Diego, 2022.
506 $a This item must not be sold to any third party vendors.
520 $a Microfluidic devices are an extremely useful tool to explore in vitro the pathophysiology of many different cardiovascular diseases. In this work, we designed two microfabricated platforms, one for the study of RBCs transmigration through the spleen and to characterize three dimensional forces exerted by cells. Red blood cells (RBCs) are cleared from the circulation when they become damaged or display aging signals targeted by macrophages. This process occurs mainly in the spleen, where blood flows through submicrometric constrictions called inter-endothelial slits (IES), subjecting RBCs to large-amplitude deformations. In this work, RBCs are circulated through microfluidic devices containing microchannels that replicate the IES. The cyclic mechanical stresses experienced by the cells affect their biophysical properties and molecular composition, accelerating cell aging. Specifically, RBCs quickly transition to a more spherical, less deformable phenotype that hinders microchannel passage, causing hemolysis. This transition is associated with the release of membrane vesicles, which self-extinguishes as the spacing between membrane-cytoskeleton linkers becomes tighter. Proteomics analysis of the mechanically aged RBCs reveals significant losses of essential proteins involved in antioxidant protection, gas transport, and cell metabolism. Finally, it is shown that these changes make mechanically aged RBCs more susceptible to macrophage phagocytosis. These results provide a comprehensive model explaining how physical stress induces RBC clearance in the spleen. The data also suggest new biomarkers of early "hemodamage" and inflammation preceding hemolysis in RBCs subjected to mechanical stress.Force exertion is an integral part of cellular phenotype regulating important cell functions and fate. In order to quantify mechanical forces at the cellular scale, traction force microscopy has traditionally been considered a standard when quantification of forces at the cell-substrate interface are required. However, quantification of compressive and shear stresses in three dimensions have been elusive due to the lack of experimental and computational techniques appropriate for this sizable challenge. This dissertation presents a novel methodology to produce photo-initiated elastic round microgels that can be functionalized and embedded in three dimensional tissues for force quantification.
590 $a School code: 0033.
650 4 $a Biomechanics. $3 565307
650 4 $a Mechanical engineering. $3 557493
650 4 $a Biomedical engineering. $3 588770
653 $a Microfluidic devices
653 $a Pathophysiology
653 $a Cardiovascular diseases
690 $a 0648
690 $a 0548
690 $a 0541
710 2 $a University of California, San Diego. $b Mechanical and Aerospace Engineering. $3 1241242
773 0 $t Dissertations Abstracts International $g 84-04B.
790 $a 0033
791 $a Ph.D.
792 $a 2022
793 $a English
856 4 0 $u http://pqdd.sinica.edu.tw/twdaoapp/servlet/advanced?query=29255869