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Sodium glucose transporter 2 inhibitor Dapagliflozin Regulates kisspeptin and GABA receptors mRNA expression in hypothalamic arcuate nucleus in polycystic ovary rat model, Can it

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Last updated: 03 Jan 2025

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Abstract

Background: Polycystic ovary syndrome (PCOS) is a reproductive disease that causes metabolic, endocrine and cardiovascular effects. Dapagliflozin (DAPA) is a sodium glucose transporter 2 (SGLT-2) inhibitors that control glucose level, and improve insulin sensitivity, DAPA improved sex hormones profile and ovulation rate in obese mouse model. Objective: The study aimed to detect if there is a role of DAPA on ovarian function in estradiol-induced PCOS rats. Material and methods: Thirty rats were divided into 2 groups. Group Ι (control) were given 0.5 ml saline intramuscular (IM) once, after 60 days, they were given. 0.9% saline by gastric gavage. Group II (PCOS-induced group) where rats were administered 4 mg/kg of estradiol valerate by single IM injection, 60 days later. PCO group was subdivided into subgroup IIa where rats were given 0.9% saline. Subgroup IIb included rats that were given DAPA 5 mg/kg/day. Both subgroups were administered by gastric gavage for 4 weeks. At end of experiment, serum sex hormones profile, insulin, glucose, ovarian oxidative stress and inflammatory markers, ovarian histopathology, transforming growth factor B1 (TGF-Β1) immunohistochemistry, hypothalamic kisspeptin and GABA B receptor gene expression were estimated. Results: In PCO group IIa, value of kisspeptin expression was increased significantly (p <0.01), value of GABA B receptor expression was decreased significantly (P < 0.01), compared to Dapagliflozin-treated PCO group IIb. The same opposing results when both compared to normal control group I (P< 0.001). Moreover, there was a significant increase in kisspeptin expression (P<0.05) and significant decrease in GABA B receptor expression (P< 0.01) in Dapagliflozin-treated PCO group IIa compared to normal control group I. Conclusion: DAPA improved inflammatory status, oxidative stress markers, hormonal profile, ovarian histological structure and decreased TGF-Β1 immunoreactivity and kisspeptin and increased GABA B receptor gene expression. DAPA can be used as a therapeutic target for PCOS.  

DOI

10.21608/ejhm.2024.341817

Keywords

polycystic ovary syndrome, estradiol, Dapagliflozin, Glucose transporter 2 inhibitors

Volume

94

Article Issue

1

Related Issue

45268

Issue Date

2024-01-01

Receive Date

2024-02-17

Publish Date

2024-01-01

Page Start

621

Page End

629

Print ISSN

1687-2002

Online ISSN

2090-7125

Article File

EJHM_Volume 94_Issue 1_Pages 621-629.pdf

PDF . 767.3kB

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https://ejhm.journals.ekb.eg/article_341817.html

Detail API

https://ejhm.journals.ekb.eg/service?article_code=341817

Order

91

Type

Original Article

Type Code

606

Publication Type

Journal

Publication Title

The Egyptian Journal of Hospital Medicine

Publication Link

https://ejhm.journals.ekb.eg/

MainTitle

Sodium glucose transporter 2 inhibitor Dapagliflozin Regulates kisspeptin and GABA receptors mRNA expression in hypothalamic arcuate nucleus in polycystic ovary rat model, Can it

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Type

Article

Created At

24 Dec 2024