New insights into RAGE/Diaph1 interaction as a modulator of actin cytoskeleton dynamics in peripheral nervous system in long‐term hyperglycaemia

Author:

Zglejc‐Waszak Kamila1ORCID,Pomianowski Andrzej2,Wojtkiewicz Joanna1,Banach Marta3,Juranek Judyta K.1ORCID

Affiliation:

1. Department of Human Physiology and Pathophysiology, Collegium Medicum University of Warmia and Mazury in Olsztyn Olsztyn Poland

2. Department of Internal Diseases with Clinic University of Warmia and Mazury in Olsztyn Olsztyn Poland

3. Department of Neurology, Collegium Medicum Jagiellonian University Cracow Poland

Abstract

AbstractThis review focuses on receptor for advanced glycation endproducts/diaphonous related formin 1 (RAGE/Diaph1) interaction as a modulator of actin cytoskeleton dynamics in peripheral nervous system (PNS) in diabetes. Deciphering the complex molecular interactions between RAGE and Diaph1 is crucial in expanding our understanding of diabetic length dependent neuropathy (DLDN). DLDN is a common neurological disorder in patients with diabetes. It is well known that actin cytoskeletal homeostasis is disturbed during DLDN. Thus, we review the current status of knowledge about RAGE/Diaph1 impact on actin cytoskeletal malfunctions in PNS and DLDN progression in diabetes. We also survey studies about small molecules that may block RAGE/Diaph1 axis and thus inhibit the progression of DLDN. Finally, we explore examples of cytoskeletal long‐non coding RNAs (lncRNAs) currently unrelated to DLDN, to discuss their potential role in this disease. Most recent studies indicated that lncRNAs have a great potential in many research areas, including RAGE/Diaph1 axis as well as DLDN. Altogether, this review is aimed at giving us an insight into the involvement of cytoskeletal lncRNAs in DLDN.

Funder

Narodowe Centrum Nauki

Publisher

Wiley

Subject

General Neuroscience

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