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Eye on a Chip: Microfluidic In Vitro Model of Blood-Retinal Barrier : 체외 안구모사를 위한 미세유체소자 혈액망막장벽 모델

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dc.contributor.advisor전누리-
dc.contributor.author정민환-
dc.date.accessioned2017-07-13T06:29:10Z-
dc.date.available2017-07-13T06:29:10Z-
dc.date.issued2017-02-
dc.identifier.other000000141414-
dc.identifier.urihttps://hdl.handle.net/10371/118592-
dc.description학위논문 (박사)-- 서울대학교 대학원 : 기계항공공학부, 2017. 2. 전누리.-
dc.description.abstractThe efficiency of drug development process has been continuously decreased during last decades. Recently, micro engineering tech-nology have enabled researchers to develop advanced in vitro drug test platform such as organ-on-chip system that is expected to in-novate current drug discovery process. Although some leading start-up companies are trying to commercialize the organ on chip, the ultimate goal creating simple but precise in vitro model have long way to go.
Despite the importance of blood vessel in various pathogenesis, current organ on chip models have missed the organ-specific blood vessel pathophysiology. In parallel with organ on chip technologies, advanced three-dimensional in vitro blood vessel model have been developed during last decade. Either the blood vessel model and the organ on chip have shed a light to the next generation of drug development process, combining the two technologies would be another step towards the development of innovative in vitro drug test model.
To this end, this thesis first describes the method to create in vivo like blood vessel model by mimicking natural morphogenesis of the human primary endothelial cells. Effect of bio-mechanical stimulus exerted by interstitial flow (IF) on the development pro-cess of the model was studied. A minute rate of IF was introduced simply by hydrostatic pressure and visualized by fluorescence re-covery after photobleaching (FRAP). Series of experiments with various direction and sequence of the applied IF revealed the strong directional bias of the angiogenic sprouting into the opposite direction of the IF, which could be used as angiogenic switch to set the model in angiogenic or non-angiogenic condition.
The blood vessel model could be applied to reconstitute retinal pigment epithelium (RPE) – choroid system of the eye, owing to the morphological similarity of the two system. The device design was modified and optimized to introduce RPE cells to mimic cross sectional structure of the RPE-choroid system. Treatment of pro- and anti- angiogenic factors allowed the in vitro model to quantita-tively simulate pathogenesis and treatment of wet type age related macula degeneration (wet-AMD) which causes blindness in many elderly people.
The blood vessel model has potential to be used for various application, including unveiling the biochemical or biomechanical regulation of angiogenesis and evaluation of anti-angiogenic drug candidates. Moreover, the model would be applied to reconstitute various organ specific endothelial physiology, such as RPE-choroid system as described here, which would help predicting the organ specific pathophysiology in response to the drug can-didates in vitro.
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dc.description.tableofcontentsChapter 1 Introduction 1
1.1. Organ-specific endothelial physiology 3
1.2. Micro-engineered in vitro blood vessel models 7
1.3. Limitations of current in vitro angiogenesis model 13
1.4. Motivation and objectives 14
Chapter 2 Study of Microenvironment Surrounding Blood Vessel 16
2.1. Interstitial Flow Regulates Angiogenic Response and Phenotype of Endothelial Cells in a 3d Culture Model 16
2.2. Materials and Methods 20
2.2.1. Microfluidic device design and fabrication 20
2.2.2. Cell culture 21
2.2.3. Angiogenesis assay under interstitial flow condition 21
2.2.4. Quantitative validation of interstitial flow across 3D ECM 23
2.2.5. Biochemical factor treatment 24
2.2.6. Anti-angiogenic compound treatment 24
2.2.7. Immunostaining 25
2.2.8. Image analysis and statistical analysis 26
2.3. Results 27
2.3.1. Microfluidic model to recreate vascular microenvironment in 3D extracellular matrix 27
2.3.2. Vasculogenic formation and angiogenic remodelling of microvascular networks 34
2.3.3. Synergism of biochemical cues and interstitial flow regulates angiogenic response and phenotype of ECs 43
2.3.4. Interstitial flow controls initiation and sustained growth of angiogenic sprouts 45
2.3.5. Interstitial flow influences endothelial response to extrinsic pro-angiogenic factors 50
2.3.6. Evaluation of anti-angiogenic compounds for their differential inhibitory potential to initiating and elongating sprouts 56
2.4. Discussion 61
Chapter 3 Engineering of Vascularized Eye Model 65
3.1. Reconstituting Outer Blood-Retinal Barrier on Microfluidic Chip 65
3.2. Materials and Methods 67
3.2.1. Microfluidic device design and fabrication 67
3.2.2. Cell culture 68
3.2.3. RPE-choroid model in microfluidic device 68
3.2.4. Immunostaining 70
3.2.5. Quantitative validation of barrier function of RPE-choroid model 71
3.2.6. Detection of secreted VEGF and PEDF 71
3.2.7. Biochemical factor treatment 72
3.2.8. Three dimensional reconstruction and Image analysis 72
3.3. Results 74
3.3.1. Design of microfluidic platform to mimic RPE-choroid layer in vitro 74
3.3.2. RPE layer and choroid vessel exhibited intact barrier function of outer BRB 81
3.3.3. VEGF-PEDF distribution in the RPE-choroid model 88
3.3.4. Excessive angiogenic sprouting in response to exogenous VEGF treatment mimic CNV in vito 92
3.4. Conclusion 97
Chapter 4 Conclusion 99
Bibliography 101
요약 111
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dc.formatapplication/pdf-
dc.format.extent4368857 bytes-
dc.format.mediumapplication/pdf-
dc.language.isoen-
dc.publisher서울대학교 대학원-
dc.subjectMicrofluidic-
dc.subjectOrgan on chip-
dc.subjectAngiogenesis-
dc.subjectInterstitial flow-
dc.subjectBiomechanical stimulus-
dc.subjectRetinal pigment epithelium-
dc.subjectRPE-choroid-
dc.subjectChoroidal neovascularization-
dc.subject.ddc621-
dc.titleEye on a Chip: Microfluidic In Vitro Model of Blood-Retinal Barrier-
dc.title.alternative체외 안구모사를 위한 미세유체소자 혈액망막장벽 모델-
dc.typeThesis-
dc.contributor.AlternativeAuthorMinhwan Chung-
dc.description.degreeDoctor-
dc.citation.pages112-
dc.contributor.affiliation공과대학 기계항공공학부-
dc.date.awarded2017-02-
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