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Merck
  • Activation of RhoA-ROCK-BMP signaling reprograms adult human corneal endothelial cells.

Activation of RhoA-ROCK-BMP signaling reprograms adult human corneal endothelial cells.

The Journal of cell biology (2014-09-10)
Ying-Ting Zhu, Fu Li, Bo Han, Sean Tighe, Suzhen Zhang, Szu-Yu Chen, Xin Liu, Scheffer C G Tseng
摘要

Currently there are limited treatment options for corneal blindness caused by dysfunctional corneal endothelial cells. The primary treatment involves transplantation of healthy donor human corneal endothelial cells, but a global shortage of donor corneas necessitates other options. Conventional tissue approaches for corneal endothelial cells are based on EDTA-trypsin treatment and run the risk of irreversible endothelial mesenchymal transition by activating canonical Wingless-related integration site (Wnt) and TGF-β signaling. Herein, we demonstrate an alternative strategy that avoids disruption of cell-cell junctions and instead activates Ras homologue gene family A (RhoA)-Rho-associated protein kinase (ROCK)-canonical bone morphogenic protein signaling to reprogram adult human corneal endothelial cells to neural crest-like progenitors via activation of the miR302b-Oct4-Sox2-Nanog network. This approach allowed us to engineer eight human corneal endothelial monolayers of transplantable size, with a normal density and phenotype from one corneoscleral rim. Given that a similar signal network also exists in the retinal pigment epithelium, this partial reprogramming approach may have widespread relevance and potential for treating degenerative diseases.

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MISSION® esiRNA, targeting human ROCK2