Alterations of the expression levels of glucose, inflammation, and iron metabolism related miRNAs and their target genes in the hypothalamus of STZ-induced rat diabetes model

Edina Pandur; István Szabó; Edina Hormay; Ramóna Pap; Attila Almási; Katalin Sipos; Viktória Farkas; Zoltán Karádi

doi:10.1186/s13098-022-00919-5

Alterations of the expression levels of glucose, inflammation, and iron metabolism related miRNAs and their target genes in the hypothalamus of STZ-induced rat diabetes model

Diabetol Metab Syndr. 2022 Oct 10;14(1):147. doi: 10.1186/s13098-022-00919-5.

Authors

Edina Pandur¹, István Szabó², Edina Hormay², Ramóna Pap³, Attila Almási⁴, Katalin Sipos³, Viktória Farkas³, Zoltán Karádi²

Affiliations

¹ Department of Pharmaceutical Biology, Faculty of Pharmacy, University of Pécs, Rókus u. 4., 7624, Pécs, Hungary. edina.pandur@aok.pte.hu.
² Institute of Physiology, Medical School, University of Pécs, Szigeti út 12., 7624, Pécs, Hungary.
³ Department of Pharmaceutical Biology, Faculty of Pharmacy, University of Pécs, Rókus u. 4., 7624, Pécs, Hungary.
⁴ Institute of Pharmaceutical Chemistry, Faculty of Pharmacy, University of Pécs, Rókus u. 4., 7624, Pécs, Hungary.

Abstract

Background: The hypothalamus of the central nervous system is implicated in the development of diabetes due to its glucose-sensing function. Dysregulation of the hypothalamic glucose-sensing neurons leads to abnormal glucose metabolism. It has been described that fractalkine (FKN) is involved in the development of hypothalamic inflammation, which may be one of the underlying causes of a diabetic condition. Moreover, iron may play a role in the pathogenesis of diabetes via the regulation of hepcidin, the iron regulatory hormone synthesis. MicroRNAs (miRNAs) are short non-coding molecules working as key regulators of gene expression, usually by inhibiting translation. Hypothalamic miRNAs are supposed to have a role in the control of energy balance by acting as regulators of hypothalamic glucose metabolism via influencing translation.

Methods: Using a miRNA array, we analysed the expression of diabetes, inflammation, and iron metabolism related miRNAs in the hypothalamus of a streptozotocin-induced rat type 1 diabetes model. Determination of the effect of miRNAs altered by STZ treatment on the target genes was carried out at protein level.

Results: We found 18 miRNAs with altered expression levels in the hypothalamus of the STZ-treated animals, which act as the regulators of mRNAs involved in glucose metabolism, pro-inflammatory cytokine synthesis, and iron homeostasis suggesting a link between these processes in diabetes. The alterations in the expression level of these miRNAs could modify hypothalamic glucose sensing, tolerance, uptake, and phosphorylation by affecting the stability of hexokinase-2, insulin receptor, leptin receptor, glucokinase, GLUT4, insulin-like growth factor receptor 1, and phosphoenolpyruvate carboxykinase mRNA molecules. Additional miRNAs were found to be altered resulting in the elevation of FKN protein. The miRNA, mRNA, and protein analyses of the diabetic hypothalamus revealed that the iron import, export, and iron storage were all influenced by miRNAs suggesting the disturbance of hypothalamic iron homeostasis.

Conclusion: It can be supposed that glucose metabolism, inflammation, and iron homeostasis of the hypothalamus are linked via the altered expression of common miRNAs as well as the increased expression of FKN, which contribute to the imbalance of energy homeostasis, the synthesis of pro-inflammatory cytokines, and the iron accumulation of the hypothalamus. The results raise the possibility that FKN could be a potential target of new therapies targeting both inflammation and iron disturbances in diabetic conditions.

Keywords: Diabetes; Fractalkine; Hypothalamus; Inflammation; Iron metabolism; miRNA.

Grants and funding

TKP2021-EGA-17/Thematic Excellence Programme