| Literature DB >> 30565679 |
Mohammad Javad Saeedi Borujeni1, Ebrahim Esfandiary1, Azar Baradaran2, Ali Valiani1, Mustafa Ghanadian3, Pilar Codoñer-Franch4, Reyhane Basirat5, Eulalia Alonso-Iglesias6, Hamed Mirzaei7, Amid Yazdani8.
Abstract
Metabolic syndrome is known as a frequent precursor of type 2 diabetes mellitus (T2D). This disease could affect 8% of the people worldwide. Given that pancreatic β-cell dysfunction and loss have central roles in the initiation and progression of the disease, the understanding of cellular and molecular pathways associated with pancreatic β-cell dysfunction can provide more information about the underlying pathways involved in T2D. Multiple lines evidence indicated that oxidative stress, microRNA, and long noncoding RNA play significant roles in various steps of diseases. Oxidative stress is one of the important factors involved in T2D pathogenesis. This could affect the function and survival of the β cell via activation or inhibition of several processes and targets, such as receptor-signal transduction, enzyme activity, gene expression, ion channel transport, and apoptosis. Besides oxidative stress, microRNAs and noncoding RNAs have emerged as epigenetic regulators that could affect pancreatic β-cell dysfunction. These molecules exert their effects via targeting a variety of cellular and molecular pathways involved in T2D pathogenesis. Here, we summarized the molecular aspects of pancreatic β-cell dysfunction. Moreover, we highlighted the roles of oxidative stress, microRNAs, and noncoding RNAs in pancreatic β-cell dysfunction.Entities:
Keywords: microRNAs; noncoding RNAs; oxidative stress; pancreatic β-cell dysfunction; type 2 diabetes mellitus
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Year: 2018 PMID: 30565679 DOI: 10.1002/jcp.27755
Source DB: PubMed Journal: J Cell Physiol ISSN: 0021-9541 Impact factor: 6.384