Abstract |
Corneal scarring/ fibrosis disturbs normal transparency and curvature of the tissue and thus impairs vision. The lesion is characterized by appearance of myofibroblasts, the key player of the fibrogenic reaction, and excess accumulation of extracellular matrix. Inflammatory/fibrogenic growth factors or cytokines expressed in inflammatory cells that infiltrate into injured tissues play a pivotal role in fibrotic tissue formation. In this article the pathogenesis of fibrosis/ scarring in the corneal stroma is reviewed focusing on the roles of myofibroblast, the key player in corneal stromal wound healing and fibrosis, and cytoplasmic signals activated by the fibrogenic cytokine, transforming growth factor β (TGFβ). Although it is established that TGFβ/Smad signal is essential to the process of keratocyte-myofibroblast transformation in a healing corneal stroma post-injury. This article emphasizes the involvement of non-TGFβ molecular mechanisms in modulating Smad signal. We focus on the roles of matricellular proteins, i.e., osteopontin and tenascin C, and as cellular components, the roles of transient receptor potential ( TRP) cation channel receptors are discussed. Our intent is to draw attention to the possibility of signal transduction cascade modulation (e.g., Smad signal and mitogen-activated protein kinases, by gene transfer and other related technology) as being beneficial in a clinical setting to reduce or even prevent corneal stromal tissue fibrosis/ scarring and inflammation.
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Authors | Shizuya Saika, Osamu Yamanaka, Yuka Okada, Takayoshi Sumioka |
Journal | Experimental eye research
(Exp Eye Res)
Vol. 142
Pg. 40-8
(Jan 2016)
ISSN: 1096-0007 [Electronic] England |
PMID | 26675402
(Publication Type: Journal Article, Research Support, Non-U.S. Gov't, Review)
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Copyright | Copyright © 2014 Elsevier Ltd. All rights reserved. |
Chemical References |
- Extracellular Matrix Proteins
- Smad Proteins
- Transforming Growth Factor beta1
- Mitogen-Activated Protein Kinases
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Topics |
- Cell Differentiation
(physiology)
- Corneal Diseases
(physiopathology)
- Corneal Stroma
(physiopathology)
- Extracellular Matrix Proteins
(physiology)
- Humans
- Macrophages
(metabolism)
- Mitogen-Activated Protein Kinases
(physiology)
- Myofibroblasts
(physiology)
- Signal Transduction
(physiology)
- Smad Proteins
(physiology)
- Transforming Growth Factor beta1
(metabolism)
- Wound Healing
(physiology)
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