4.7 Article

Peri/Epicellular Thiol Oxidoreductases as Mediators of Extracellular Redox Signaling

期刊

ANTIOXIDANTS & REDOX SIGNALING
卷 33, 期 4, 页码 280-307

出版社

MARY ANN LIEBERT, INC
DOI: 10.1089/ars.2019.8012

关键词

thiol proteins; oxidoreductases; protein disulfide isomerase; thrombosis; vascular remodeling; immunoinflammation

资金

  1. Centros de Pesquisa, Inovacao e Difusao (CEPID) Redoxoma-FAPESP RedoxomaFAPESP (Fundacao de Amparo a Pesquisa do Estado de Sao Paulo) [2013/07937-8, 2018/07230-5, 2019/03617-5]

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Recent Advances: pecTOR redox-modulates several targets including integrins, ECM proteins, surface molecules, and plasma components, although clear-cut documentation of direct effects is lacking in many cases. TOR catalytic pathways, displaying common patterns, culminate in substrate thiol reduction, oxidation, or isomerization. Peroxiredoxins act as redox/peroxide sensors, contrary to PDIs, which are likely substrate-targeted redox modulators. Emerging evidence suggests important pecTOR roles in patho(physio)logical processes, including blood coagulation, vascular remodeling, mechanosensing, endothelial function, immune responses, and inflammation. Critical Issues: Effects of pecPDIs supporting thrombosis/platelet activation have been well documented and reached the clinical arena. Roles of pecPDIA1 in vascular remodeling/mechanosensing are also emerging. Extracellular thioredoxin and pecPDIs redox-regulate immunoinflammation. Routes of TOR externalization remain elusive and appear to involve Golgi-independent routes. pecTORs are particularly accessible drug targets. Future Directions: Further understanding mechanisms of thiol redox reactions and developing assays for assessing pecTOR redox activities remain important research avenues. Also, addressing pecTORs as disease markers and achieving more efficient/specific drugs for pecTOR modulation are major perspectives for diagnostic/therapeutic improvements.

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