Generation of Anterior Segment of the Eye Cells from hiPSCs in Microfluidic Platforms
Creators
- 1. Izmir Biomed & Genome Ctr, TR-35330 Izmir, Turkiye
- 2. Hacettepe Univ, Fac Pharm, Dept Analyt Chem, TR-06100 Ankara, Turkiye
Description
Ophthalmic diseases affect many people, causing partial or total loss of vision and a reduced quality of life. The anterior segment of the eye accounts for nearly half of all visual impairment that can lead to blindness. Therefore, there is a growing demand for ocular research and regenerative medicine that specifically targets the anterior segment to improve vision quality. This study aims to generate a microfluidic platform for investigating the formation of the anterior segment of the eye derived from human induced pluripotent stem cells (hiPSC) under various spatial-mechanoresponsive conditions. Microfluidic platforms are developed to examine the effects of dynamic conditions on the generation of hiPSCs-derived ocular organoids. The differentiation protocol is validated, and mechanoresponsive genes are identified through transcriptomic analysis. Several culture strategies is implemented for the anterior segment of eye cells in a microfluidic chip. hiPSC-derived cells showed anterior eye cell characteristics in mRNA and protein expression levels under dynamic culture conditions. The expression levels of yes-associated protein and transcriptional coactivator PDZ binding motif (YAP/TAZ) and PIEZO1, varied depending on the differentiation and growth conditions of the cells, as well as the metabolomic profiles under dynamic culture conditions.
The use of microfluidic platforms to study how hiPSCs form the ocular cells under varied conditions reveals the change in mechanoresponsive genes' expression levels and metabolomic profiles. YAP/TAZ and PIEZO1 are found to be expressed more in the organoids grown under dynamic culture conditions in comparison to those initially developed in static culture and are later transferred to dynamic culture. image
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