Decoding the association of polycystic ovary syndrome with metabolic-associated fatty liver: insights into CK18 and LC3II/ATG7/P62 autophagy axis and adjunct therapeutics of metformin and levothyroxine

Sameeah Mejbel Hamad Algenabi; Anwar Nather Seiwan; Maha Hussein Hashem Sabra; Doaa I. Mohamed; Lobna Fouad Abd ElAziz Bassyouni; Dalia Alaa El-Din Aly El-Waseef; Samar F. Ezzat; Omnyah A. El-Kharashi; Hanaa F. Abd El-Kareem; Hyfa A. Alzahrani; Fawzyah Obeedallah Albaldi; Ahmed Shokry Elharoun; Mansour Altayyar; Amal Fahmy Dawood; Hebatallah H. Abo Nahas; Ahmed Abdel-Salam M. Elmelegy

doi:10.1039/D5MD00819K

Decoding the association of polycystic ovary syndrome with metabolic-associated fatty liver: insights into CK18 and LC3II/ATG7/P62 autophagy axis and adjunct therapeutics of metformin and levothyroxine

Sameeah Mejbel Hamad Algenabi,

^a Anwar Nather Seiwan,

^b Maha Hussein Hashem Sabra,^c Doaa I. Mohamed,^c Lobna Fouad Abd ElAziz Bassyouni,^c Dalia Alaa El-Din Aly El-Waseef,

^d Samar F. Ezzat,^d Omnyah A. El-Kharashi,^ce Hanaa F. Abd El-Kareem,

^f Hyfa A. Alzahrani,^g Fawzyah Obeedallah Albaldi,^g Ahmed Shokry Elharoun,^h Mansour Altayyar,^h Amal Fahmy Dawood,ⁱ Hebatallah H. Abo Nahas

*^j and Ahmed Abdel-Salam M. Elmelegy

^c

Author affiliations

* Corresponding authors

^a Department of Human Anatomy, College of Medicine, University of Anbar, Ramadi city, Anbar, Iraq
E-mail: med.samieaalgenabi@uoanbar.edu.iq

^b Department of Biology, College of Science, University of Basrah, Basrah, Iraq
E-mail: anwar.sewan@uobasrah.edu.iq

^c Department of Clinical Pharmacology and Therapeutics, Faculty of Medicine, Ain Shams University, Cairo, Egypt
E-mail: maha_hussein@med.asu.edu.eg, Doaapharma@med.asu.edu.eg, lobna_fouad@med.asu.edu.eg, omnyah_aly@med.asu.edu.eg, ahmedelmelgy@yahoo.com

^d Department of Histology and Cell Biology, Faculty of Medicine, Ain Shams University, Cairo, Egypt
E-mail: daliaalaaelwaseef@med.asu.edu.eg, Samarezzat@med.asu.edu.eg

^e Department of Clinical Pharmacology and Therapeutics, Faculty of Medicine, Misr University for Science and Technology, Cairo, Egypt
E-mail: omnyah_aly@med.asu.edu.eg

^f Zoology Department, Faculty of Science, Ain Shams University, Cairo, Egypt
E-mail: Hanaafathy@sci.asu.edu.eg

^g Department of Biology Faculty of Science, Al-Baha University, Alaqiq, Saudi Arabia
E-mail: halzhrani@bu.edu.sa, falbeladi@bu.edu.sa

^h Department of Basic Medical Sciences, College of Medicine, University of Jeddah, Jeddah, Saudi Arabia
E-mail: elharounahmed@yahoo.com, maaltayyar@uj.edu.sa

ⁱ Department of Basic Medical Sciences, College of Medicine, Princess Nourah bint Abdulrahman University, P.O. Box 84428, Riyadh 11671, Saudi Arabia
E-mail: Afdawood@pnu.edu.sa

^j Physiology Biochemistry Division Zoology Department, Faculty of Science, Port Said University, 23rd of December St., El Gomhoureya, Port Said, Egypt
E-mail: heba.hassan@sci.psu.edu.eg
Tel: +20 100 152 5588

Abstract

Background: polycystic ovary syndrome (PCOS) is a common endocrine-metabolic disorder often associated with insulin resistance and metabolic-associated fatty liver disease (MAFLD), both linked to impaired autophagy. This study evaluates the effects of metformin and levothyroxine on autophagy regulation in a PCOS-induced MAFLD rat model. Materials and methods: PCOS was induced in female Wistar rats by testosterone enanthate (7.5 mg, E16–19). Post-weaning, rats were assigned to control, model, metformin (300 mg kg⁻¹ per day), levothyroxine (50 μg kg⁻¹ per day), or combination groups. Body/liver weight, serum markers (ALT, AST, TSH, lipid profile, testosterone, LH, estradiol), insulin sensitivity, autophagy-related proteins (LC3II, ATG7, p62, CK18), and histology were assessed. Network pharmacology, protein–protein interaction, KEGG enrichment, and molecular docking were performed. Results: combination therapy reduced body weight (10.29%) and liver weight (37.08%) and lowered ALT (26.17%), AST (42.69%), TSH (77.9%), cholesterol (41.32%), triglycerides (32.37%), and LDL (43.42%). Testosterone and LH declined (37.25%, 14.43%), while estradiol rose (37.4%). HOMA-IR decreased by 51.85%. Autophagy markers (CK18, LC3II, P62, ATG7) were suppressed, with improved hepatic and ovarian histology. Network analysis identified NOS2, KRT18, MAP1LC3B, ATG7, and SQSTM1 as key targets, with KEGG pathways implicated in autophagy, mitophagy, ferroptosis, and apelin signaling. Docking analysis showed stronger binding of levothyroxine to LC3II and ATG7, suggesting a direct modulatory role. Conclusion: metformin and levothyroxine synergistically improve PCOS-related MAFLD by restoring autophagy and metabolic-endocrine balance. System-level and docking analyses support autophagy regulation as a key therapeutic mechanism, highlighting the potential role of levothyroxine in modulating autophagy.

RSC Medicinal Chemistry

Decoding the association of polycystic ovary syndrome with metabolic-associated fatty liver: insights into CK18 and LC3II/ATG7/P62 autophagy axis and adjunct therapeutics of metformin and levothyroxine

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Decoding the association of polycystic ovary syndrome with metabolic-associated fatty liver: insights into CK18 and LC3II/ATG7/P62 autophagy axis and adjunct therapeutics of metformin and levothyroxine

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