Literature DB >> 32417359

Simvastatin ameliorates altered mechanotransduction in uterine leiomyoma cells.

Sadia Afrin1, Md Soriful Islam1, Kristin Patzkowsky1, Minnie Malik2, William H Catherino2, James H Segars1, Mostafa A Borahay3.   

Abstract

BACKGROUND: Uterine leiomyomas, the most common tumors of the female reproductive system, are characterized by excessive deposition of disordered stiff extracellular matrix and fundamental alteration in the mechanical signaling pathways. Specifically, these alterations affect the normal dynamic state of responsiveness to mechanical cues in the extracellular environment. These mechanical cues are converted through integrins, cell membrane receptors, to biochemical signals including cytoskeletal signaling pathways to maintain mechanical homeostasis. Leiomyoma cells overexpress β1 integrin and other downstream mechanical signaling proteins. We previously reported that simvastatin, an antihyperlipidemic drug, has antileiomyoma effects through cellular, animal model, and epidemiologic studies.
OBJECTIVE: This study aimed to examine the hypothesis that simvastatin might influence altered mechanotransduction in leiomyoma cells. STUDY
DESIGN: This is a laboratory-based experimental study. Primary leiomyoma cells were isolated from 5 patients who underwent hysterectomy at the Department of Gynecology and Obstetrics of the Johns Hopkins University Hospital. Primary and immortalized human uterine leiomyoma cells were treated with simvastatin at increasing concentrations (0.001, 0.01, 0.1, and 1 μM, or control) for 48 hours. Protein and mRNA levels of β1 integrin and extracellular matrix components involved in mechanical signaling were quantified by quantitative real-time polymerase chain reaction, western blotting, and immunofluorescence. In addition, we examined the effect of simvastatin on the activity of Ras homolog family member A using pull-down assay and gel contraction.
RESULTS: We found that simvastatin significantly reduced the protein expression of β1 integrin by 44% and type I collagen by 60% compared with untreated leiomyoma cells. Simvastatin-treated cells reduced phosphorylation of focal adhesion kinase down to 26%-60% of control, whereas it increased total focal adhesion kinase protein expression. Using a Ras homolog family member A pull-down activation assay, we observed reduced levels of active Ras homolog family member A in simvastatin-treated cells by 45%-85% compared with control. Consistent with impaired Ras homolog family member A activation, simvastatin treatment reduced tumor gel contraction where gel area was 122%-153% larger than control. Furthermore, simvastatin treatment led to reduced levels of mechanical signaling proteins involved in β1 integrin downstream signaling, such as A-kinase anchor protein 13, Rho-associated protein kinase 1, myosin light-chain kinase, and cyclin D1.
CONCLUSION: The results of this study suggest a possible therapeutic role of simvastatin in restoring the altered state of mechanotransduction signaling in leiomyoma. Collectively, these findings are aligned with previous epidemiologic studies and other reports and support the need for clinical trials.
Copyright © 2020 Elsevier Inc. All rights reserved.

Entities:  

Keywords:  AKAP13; FAK; MLCK; ROCK1; activated RhoA; cyclin D1; extracellular matrix; leiomyoma; mechanotransduction; simvastatin; type I collagen; β1 integrin

Year:  2020        PMID: 32417359     DOI: 10.1016/j.ajog.2020.05.012

Source DB:  PubMed          Journal:  Am J Obstet Gynecol        ISSN: 0002-9378            Impact factor:   8.661


  12 in total

Review 1.  Uterine Fibroids: Hiding in Plain Sight.

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2.  Simvastatin modulates estrogen signaling in uterine leiomyoma via regulating receptor palmitoylation, trafficking and degradation.

Authors:  Sadia Afrin; Malak El Sabeh; Md Soriful Islam; Mariko Miyashita-Ishiwata; Minnie Malik; William H Catherino; Askar M Akimzhanov; Darren Boehning; Qiwei Yang; Ayman Al-Hendy; James H Segars; Mostafa A Borahay
Journal:  Pharmacol Res       Date:  2021-08-28       Impact factor: 10.334

3.  Fast Forward: Fibroid Management in 2042.

Authors:  Malak El Sabeh; Mostafa Borahay
Journal:  F S Sci       Date:  2021-02-17

Review 4.  Role of inflammation in benign gynecologic disorders: from pathogenesis to novel therapies†.

Authors:  Abdelrahman AlAshqar; Lauren Reschke; Gregory W Kirschen; Mostafa A Borahay
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5.  Differential response to hypoxia in leiomyoma and myometrial cells.

Authors:  Mariko Miyashita-Ishiwata; Malak El Sabeh; Lauren D Reschke; Sadia Afrin; Mostafa A Borahay
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Review 6.  Vascular biology of uterine fibroids: connecting fibroids and vascular disorders.

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Review 7.  Wnt/β-catenin signaling pathway in uterine leiomyoma: role in tumor biology and targeting opportunities.

Authors:  Malak El Sabeh; Subbroto Kumar Saha; Sadia Afrin; Md Soriful Islam; Mostafa A Borahay
Journal:  Mol Cell Biochem       Date:  2021-05-17       Impact factor: 3.842

8.  Extracellular matrix and Hippo signaling as therapeutic targets of antifibrotic compounds for uterine fibroids.

Authors:  Md Soriful Islam; Sadia Afrin; Bhuchitra Singh; Friederike L Jayes; Joshua T Brennan; Mostafa A Borahay; Phyllis C Leppert; James H Segars
Journal:  Clin Transl Med       Date:  2021-07

Review 9.  Diet and Nutrition in Gynecological Disorders: A Focus on Clinical Studies.

Authors:  Sadia Afrin; Abdelrahman AlAshqar; Malak El Sabeh; Mariko Miyashita-Ishiwata; Lauren Reschke; Joshua T Brennan; Amanda Fader; Mostafa A Borahay
Journal:  Nutrients       Date:  2021-05-21       Impact factor: 5.717

Review 10.  Uterine Stem Cells and Benign Gynecological Disorders: Role in Pathobiology and Therapeutic Implications.

Authors:  Malak El Sabeh; Sadia Afrin; Bhuchitra Singh; Mariko Miyashita-Ishiwata; Mostafa Borahay
Journal:  Stem Cell Rev Rep       Date:  2020-11-05       Impact factor: 6.692

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