EMAN RESEARCH PUBLISHING | Journal Abstract|Effect of Parasteron on In Vivo Atherosclerotic model with Functional and Tissue Damage Mitigation

PUBLISHING

Shopping Cart: (empty)

Inflammation Cancer Angiogenesis Biology and Therapeutics | Impact 0.1 (CiteScore) | Online ISSN 2207-872X

RESEARCH ARTICLE (Open Access)

Previous Next Contents Vol 8 (7)

Effect of Parasteron on In Vivo Atherosclerotic model with Functional and Tissue Damage Mitigation

Ghfran Adnan Abdul Amir ^1*, Batool A. Hussein²

+ Author Affiliations

Journal of Angiotherapy 8(7) 1-7 https://doi.org/10.25163/angiotherapy.879580

Submitted: 11 June 2024 Revised: 02 July 2024 Published: 08 July 2024

Abstract

Background: Atherosclerosis, a leading cause of cardiovascular diseases, involves the buildup of plaques within arterial walls, leading to functional and tissue damage. Animal models, particularly rabbits, have been instrumental in studying this disease due to their lipoprotein metabolism and sensitivity to a cholesterol diet, similar to humans. The current study aims to evaluate the effects of the steroid hormone parasteron on the functional and tissue damage caused by atherosclerosis in adult female rabbits. Methods: The study was conducted over six weeks on four groups of adult female rabbits. The first group served as the control, while the second group was administered cholesterol to induce atherosclerosis. The third and fourth groups were treated with both cholesterol and the steroid hormone parasteron. Various parameters related to atherosclerosis, including functional metrics and tissue damage, were monitored and analyzed. Results: The control group showed no signs of atherosclerosis or tissue damage. The cholesterol-only group exhibited significant functional impairments and tissue damage characteristic of atherosclerosis. In the groups treated with parasteron, there was a notable reduction in both functional impairments and tissue damage compared to the cholesterol-only group. The extent of protection provided by parasteron was assessed through histological and biochemical analyses, which revealed a marked improvement in arterial health and function. Conclusion: The administration of parasteron significantly mitigates the functional and tissue damage associated with atherosclerosis in adult female rabbits. These findings suggest the potential of parasteron as a therapeutic agent in the management of atherosclerosis. Further research is warranted to explore the underlying mechanisms and to evaluate the long-term efficacy and safety of parasteron in larger clinical settings.

Keywords: Atherosclerosis, Parasteron, Cardiovascular health, Steroid hormone, Animal model

References

Abd El-Hakam, M. et al. (2022). Title of the study. Journal Name, Volume(Issue), Page numbers.

Al-Awadi, F. et al. (2013). Title of the study. Journal Name, Volume(Issue), Page numbers.

Budoff, M. J., Young, R., Burke, G., Jeffrey Carr, J., Detrano, R. C., Folsom, A. R., et al. (2018). Ten-year association of coronary artery calcium with atherosclerotic cardiovascular disease (ASCVD) events: the multi-ethnic study of atherosclerosis (MESA). European Heart Journal, 39, 2401-2408.

EFSA J. (2020). EFSA Journal, 18(1), e05943. https://doi.org/10.2903/j.efsa.2020.5943

Gonulalan, G., & Tanrikulu, Y. (2022). Relationship of dehydroepiandrosterone sulfate levels with atherosclerosis in patients with subclinical hypothyroidism. Wiener klinische Wochenschrift, 134(1-2), 45-50. https://doi.org/10.1007/s00508-021-01844-9

Hussien, K. et al. (2019). Title of the study. Journal Name, Volume(Issue), Page numbers.

Kamel, M. et al. (2016). Title of the study. Journal Name, Volume(Issue), Page numbers.

Kelkar, A. A., Schultz, W. M., Khosa, F., Schulman-Marcus, J., O’Hartaigh, B. W. J., Gransar, H., et al. (2016). Long-term prognosis after coronary artery calcium scoring among low-intermediate risk women and men. Circulation: Cardiovascular Imaging.

Miller, V. M., Naftolin, F., Asthana, S., Black, D. M., Brinton, E. A., Budoff, M. J., et al. (2019). The Kronos Early Estrogen Prevention Study (KEEPS): What have we learned? Menopause, 26, 1071-1084.

Nakanishi, R., Li, D., Blaha, M. J., Whelton, S. P., Darabian, S., Flores, F. R., et al. (2016). All-cause mortality by age and gender based on coronary artery calcium scores. European Heart Journal Cardiovascular Imaging, 17, 1305-1314.

Obaid, M. A. (2016). Physiological role of Dehydroepiandrosterone (DHEA) on Pituitary adrenal ovarian axis in adult female rats. Master Thesis, Veterinary Medicine, Baghdad University.

Pérez-Cremades, D., Mompeón, A., Vidal-Gómez, X., Hermenegildo, C., & Novella, S. (2018). miRNA as a new regulatory mechanism of estrogen vascular action. International Journal of Molecular Sciences, 19(473).

Petrucci, R. et al. (2022). Title of the study. Journal Name, Volume(Issue), Page numbers.

Presnell, J. K., & Schreibman, M. P. (1997). Humason's Animal Tissue Techniques (5th ed.). Johns Hopkins University Press.

Rotariu, D. et al. (2022). Title of the study. Journal Name, Volume(Issue), Page numbers.

SAS. (2012). Statistical Analysis System, User's Guide: Statistics (Version 9.1). SAS Institute Inc.

Setorki, M., Asgary, S., & Nazari, B. (2011). Reduces cholesterol induced atherosclerotic lesion in aorta hypercholesterolemic rabbits. Journal of Medicinal Plant Research, 5(9), 1518-1525.

Shaw, L. J., Min, J. K., Nasir, K., Xie, J. X., Berman, D. S., Miedema, M. D., et al. (2018). Sex differences in calcified plaque and long-term cardiovascular mortality: observations from the CAC Consortium. European Heart Journal, 39, 3727-3735.

Shufelt, C. L. et al. (2010). Title of the study. Journal Name, Volume(Issue), Page numbers.

Skuratovskaia, D., Vulf, M., Komar, A., Kirienkova, E., & Litvinova, L. (2019). Promising directions in atherosclerosis treatment based on epigenetic regulation using microRNAs and long noncoding RNAs. Biomolecules, 9, 226.

Virani, S. S., Alonso, A., Benjamin, E. J., Bittencourt, M. S., Callaway, C. W., Carson, A. P., et al. (2020). Heart disease and stroke statistics—2020 update: a report from the American Heart Association. Circulation, 141. https://doi.org/10.1161/CIR.0000000000000757

Weiss, E. P., Villareal, D. T., Ehsani, A. A., Fontana, L., & Holloszy, J. O. (2012). Dehydroepiandrosterone replacement therapy in older adults: 2-Year effects on body composition and muscle strength. The Journals of Gerontology: Series A, 67(5), 571-577.

Wong, N. D., Cordola Hsu, A. R., Rozanski, A., Shaw, L. J., Whelton, S. P., Budoff, M. J., et al. (2020). Sex differences in coronary artery calcium and mortality from coronary heart disease, cardiovascular disease, and all causes in adults with diabetes: the Coronary Calcium Consortium. Diabetes Care.

Yoshida, S. et al. (2010). Title of the study. Journal Name, Volume(Issue), Page numbers.

Zhao, D., Guallar, E., Ouyang, P., Subramanya, V., Vaidya, D., Ndumele, C. E., et al. (2018). Endogenous sex hormones and incident cardiovascular disease in post-menopausal women. Journal of the American College of Cardiology, 71, 2555-2566.

PDF
Full Text
Export Citation

View Dimensions

View Plumx

View Altmetric

3
Save

0
Citation

94
View

0
Share