In Vitro Modeling of Atherosclerosis Using iPSC-Derived Blood Vessel Organoids
- Abstract
- As modeling of atherosclerosis requires recapitulating complex interactions with vasculature and immune cells, previous in vitro models have limitations due to their insufficient 3D vascular structures. However, induced pluripotent stem cell-derived blood vessel organoids (BVOs) are applicable for modeling vascular diseases, containing multiple cell types, including endothelial and vascular smooth muscle cells self-assembled into a blood vessel structure. Atherosclerotic BVOs with a microenvironment associated with atherogenesis, such as shear stress, low-density lipoprotein, pro-inflammatory cytokine, and monocyte co-culture are successfully developed. In atherosclerotic BVOs, representative atherosclerotic phenotypes, including endothelial dysfunction, inflammatory responses, formation of foam cells and fibrous plaque, and moreover, calcification of the plaques are observed. To verify the drug response in this model, it is treated with clinically used lovastatin and confirm phenotype attenuation. Furthermore, the therapeutic efficacy of nano-sized graphene oxides (NGOs) is evaluated on atherosclerosis. Due to their anti-inflammatory effects, NGOs effectively alleviate the pathologic lesions in atherosclerotic BVOs by promoting macrophage polarization toward M2. These results suggest that atherosclerotic BVOs a
- Author(s)
- 김다현; 공다솜; 김재철; 신나리; 이승은; 김남교; 김희영; 김민지; 최정주; 강경선
- Issued Date
- 2025-01-03
- Type
- Article
- Keyword
- 세포병리
- DOI
- 10.1002/adhm.202400919
- URI
- http://repository.sungshin.ac.kr/handle/2025.oak/8664
- Publisher
- WILEY
- ISSN
- 2192-2640
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Appears in Collections:
- 바이오신약의과학부 > 학술논문
- 공개 및 라이선스
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