A-family anti-inflammatory cyclopentenone prostaglandins: A novel class of non-statin inhibitors of HMG-CoA reductase
Lucila Ludmila Paula Gutierrez
1, 2
,
Cláudia Vieira Marques
3
,
Sofia Pizzato Scomazzon
3
,
Helena Trevisan Schroeder
3
,
João Luiz Fernandes
3
,
Juliane Da Silva Rossato
3
,
Paulo Ivo Homem de Bittencourt
3
1
Department of Basic Health Sciences, Federal University of Health Sciences of Porto Alegre (UFCSPA), Porto Alegre, RS, 90050-170, Brazil
|
Publication type: Journal Article
Publication date: 2021-03-01
scimago Q2
wos Q3
SJR: 0.884
CiteScore: 6.0
Impact factor: 3.0
ISSN: 03009084, 61831638, 16386183
PubMed ID:
33412161
Biochemistry
General Medicine
Abstract
Disruption of the intracellular lipid balance leading to cholesterol accumulation is one of the features of cells that participate in the development of atherosclerotic lesions. Evidence form our laboratory indicates that anti-inflammatory cyclopentenone prostaglandins (cyPGs) of A- and J-family deviate lipid metabolism from the synthesis of cholesterol and cholesteryl esters to the synthesis of phospholipids in foam-cell macrophages. cyPGs possessing an α,β-unsaturated cyclopentane ring are highly electrophilic substances able to promptly react with reactive cysteines of intracellular molecules through Michael addition. On the other hand, HMG-CoA reductase (HMGCR), the enzyme responsible for the rate-limiting step in cholesterol biosynthesis, presents critically reactive cysteines at the entry of catalytic domain, particularly Cys561, that could be target of cyPG inhibition. In the present study, we showed that cyPGs (but not other non-α,β-unsaturated PGs) physically interact with HMGCR, in a dithiothreitol- and β-mercaptoethanol-sensitive way, and block the activity of the catalytic subunit of the enzyme (IC50 for PGA2 = 0.17 μM). PGA2 inhibits HMGCR activity in cultured rat and human macrophages/macrophage-foam cells and leads to enhanced expression of HMGCR protein, as observed with statins. In cell culture models, PGA2 effectively inhibits the reductase at non-toxic doses (e.g., 1 μM) that block cell proliferation thus suggesting that part of the well-known antiproliferative effect of PGA2 may be due to its ability of blocking HMGCR activity, as cells cannot proliferate without a robust cholesterogenesis. Therefore, besides the powerfully anti-inflammatory and antiproliferative effects, the anticholesterogenic effects of PGA2 should be exploited in atherosclerosis therapeutics.
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Total citations:
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Citations from 2025:
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Gutierrez L. L. P. et al. A-family anti-inflammatory cyclopentenone prostaglandins: A novel class of non-statin inhibitors of HMG-CoA reductase // Biochimie. 2021. Vol. 182. pp. 37-50.
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Gutierrez L. L. P., Marques C. V., Pizzato Scomazzon S., Schroeder H. T., Fernandes J. L., Da Silva Rossato J., Homem de Bittencourt P. I. A-family anti-inflammatory cyclopentenone prostaglandins: A novel class of non-statin inhibitors of HMG-CoA reductase // Biochimie. 2021. Vol. 182. pp. 37-50.
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TY - JOUR
DO - 10.1016/j.biochi.2020.12.019
UR - https://doi.org/10.1016/j.biochi.2020.12.019
TI - A-family anti-inflammatory cyclopentenone prostaglandins: A novel class of non-statin inhibitors of HMG-CoA reductase
T2 - Biochimie
AU - Gutierrez, Lucila Ludmila Paula
AU - Marques, Cláudia Vieira
AU - Pizzato Scomazzon, Sofia
AU - Schroeder, Helena Trevisan
AU - Fernandes, João Luiz
AU - Da Silva Rossato, Juliane
AU - Homem de Bittencourt, Paulo Ivo
PY - 2021
DA - 2021/03/01
PB - Elsevier
SP - 37-50
VL - 182
PMID - 33412161
SN - 0300-9084
SN - 6183-1638
SN - 1638-6183
ER -
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BibTex (up to 50 authors)
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@article{2021_Gutierrez,
author = {Lucila Ludmila Paula Gutierrez and Cláudia Vieira Marques and Sofia Pizzato Scomazzon and Helena Trevisan Schroeder and João Luiz Fernandes and Juliane Da Silva Rossato and Paulo Ivo Homem de Bittencourt},
title = {A-family anti-inflammatory cyclopentenone prostaglandins: A novel class of non-statin inhibitors of HMG-CoA reductase},
journal = {Biochimie},
year = {2021},
volume = {182},
publisher = {Elsevier},
month = {mar},
url = {https://doi.org/10.1016/j.biochi.2020.12.019},
pages = {37--50},
doi = {10.1016/j.biochi.2020.12.019}
}