Literature DB >> 31390655

Small Molecule Modulation of the Integrated Stress Response Governs the Keratoconic Phenotype In Vitro.

Uri Simcha Soiberman1, Ahmed Elsayed Mahmoud Shehata2, Michelle Xiaoyi Lu3, Tempest Young3, Yassine J Daoud1, Shukti Chakravarti4, Albert S Jun1, James William Foster1.   

Abstract

Purpose: The degenerative corneal disease keratoconus is a leading indicator for corneal transplant with an unknown etiology. We recently identified the activation of the integrated stress response (ISR) in ex vivo human corneas and in vitro cell culture. Utilizing small molecules to modulate the ISR we sought to investigate the effects of stimulating the ISR in healthy cells to recapitulate aspects of the in vitro keratoconic phenotype and whether relieving the ISR signaling would recover the disease phenotype.
Methods: Corneal fibroblasts were extracted from patients undergoing corneal transplant or unaffected cadaverous donor limbal rings. Cells were exposed to the DNA damage-inducible protein (GADD34) inhibitor SAL003 to stimulate the ISR, or Trans-ISRIB to relieve ISR signaling pathway. Collagen production was assessed through hydroxyproline production, Sirius Red incorporation, or quantitative (q)PCR. Western blotting, hydroxyproline, and qPCR were used to assess components of the ISR pathway and collagen production.
Results: ISR stimulation through SAL003 resulted in significant decrease of hydroxyproline and COL1A1 transcription and eventual apoptosis in normal fibroblasts. Patient (KC) fibroblast production of hydroxyproline was increased in response to ISRIB, while matrix metalloproteinase (MMP)9 production was lowered. The prospective biomarker of keratoconus prolactin-inducible factor was also upregulated in KC fibroblast cultures in response to ISRIB. Inflammatory markers TNFα and IL-1β were unaffected. Conclusions: Activation of the ISR is sufficient to recapitulate many key aspects of the KC phenotype in unaffected cells in vitro. Inhibition of the ISR also relieves many of the hallmarks of KC in affected cells. Therefore, targeting of the ISR through small molecules is a potential therapeutic path for small molecule treatment of keratoconus.

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Year:  2019        PMID: 31390655      PMCID: PMC6686743          DOI: 10.1167/iovs.19-27151

Source DB:  PubMed          Journal:  Invest Ophthalmol Vis Sci        ISSN: 0146-0404            Impact factor:   4.799


  46 in total

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Review 7.  Recurrence or re-emergence of keratoconus--what is the evidence telling us? Literature review and two case reports.

Authors:  Jan P G Bergmanson; John D Goosey; Chirag K Patel; Jessica H Mathew
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Authors:  Huib H Rabouw; Martijn A Langereis; Aditya A Anand; Linda J Visser; Raoul J de Groot; Peter Walter; Frank J M van Kuppeveld
Journal:  Proc Natl Acad Sci U S A       Date:  2019-01-23       Impact factor: 11.205

Review 10.  Pathogenesis of Keratoconus: The intriguing therapeutic potential of Prolactin-inducible protein.

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Review 2.  Endoplasmic reticulum stress: New insights into the pathogenesis and treatment of retinal degenerative diseases.

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3.  Absence of the c.169+50delTAAACAG mutation of SOD1 gene in a sample of keratoconus patients in Brazilian population.

Authors:  Alessandro Garcia Lopes; Gildásio Castello de Almeida Júnior; Ronan Marques Teixeira; Luiz Carlos de Mattos; Cinara Cássia Brandão de Mattos; Lilian Castiglioni
Journal:  BMC Res Notes       Date:  2020-07-09

4.  Induction of the integrated stress response in the rat cornea.

Authors:  C Peterson; Y C Kim; L M Ensign; A S Jun; J Foster
Journal:  Exp Eye Res       Date:  2021-08-08       Impact factor: 3.770

Review 5.  Targeting the integrated stress response in ophthalmology.

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