Sevoflurane promotes the apoptosis of laryngeal squamous cell carcinoma in-vitro and inhibits its malignant progression via miR-26a/FOXO1 axis

Sevoflurane promotes the apoptosis of laryngeal squamous cell carcinoma in-vitro and inhibits its malignant progression via miR-26a/FOXO1 axis

Laryngeal squamous cell carcinoma (LSCC) is a laryngeal malignancy with a high mortality rates, and its treatment remains difficult. Sevoflurane is a surgical anesthesia which has anti-tumor effect. This investigation assessed the effects of LSCC cells treatment with Sevoflurane in vitro and in vivo...

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Main Authors: Dan Liu, Lang Wan, Hao Gong, Shiming Chen, Yonggang Kong, Bokui Xiao
Format: Article
Language:English
Published: Taylor & Francis Group 2021-01-01
Series:Bioengineered
Subjects:
sevoflurane
mir-26a
foxo1
laryngeal squamous cell carcinoma
Online Access:http://dx.doi.org/10.1080/21655979.2021.1962684
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spelling doaj-dbd836f1beab474d88cab999f24a5a512021-09-20T13:17:21ZengTaylor & Francis GroupBioengineered2165-59792165-59872021-01-011216364637610.1080/21655979.2021.19626841962684Sevoflurane promotes the apoptosis of laryngeal squamous cell carcinoma in-vitro and inhibits its malignant progression via miR-26a/FOXO1 axisDan Liu0Lang Wan1Hao Gong2Shiming Chen3Yonggang Kong4Bokui Xiao5Huangshi Central Hospital Of Edong Healthcare Group, Hubei Polytechnic UniversityHuangshi Central Hospital Of Edong Healthcare Group, Hubei Polytechnic UniversityHuangshi Maternity And Children’s Health HospitalRenmin Hospital Of Wuhan UniversityRenmin Hospital Of Wuhan UniversityWuhan University School Of MedicineLaryngeal squamous cell carcinoma (LSCC) is a laryngeal malignancy with a high mortality rates, and its treatment remains difficult. Sevoflurane is a surgical anesthesia which has anti-tumor effect. This investigation assessed the effects of LSCC cells treatment with Sevoflurane in vitro and in vivo. Hep-2 and Tu177 cells, human LSCC samples and BALB/C nude mice were used for result assessments. Cell viability, proliferation, migration and invasion were assessed via Cell Count Kit-8, wound healing assay and transwell invasion assay respectively. MiR-26a and FOXO1 expressions was examined by qRT-PCR. FOXO1, E-cadherin, N-cadherin and vimentin activities were examined by Western blotting. Moreover, animal experiments were performed to verify our findings in vitro. Lastly, miR-26a and FOXO1 expression levels in clinical samples were analyzed. According to the results, Sevoflurane decreased LSCC cells’ viability and even stimulated their apoptosis in vitro and in vivo. Moreover, it could reduce the migration, invasion and EMT. Mechanistically, sevoflurane could downregulate miR-26a expression and that miR-26a could negatively modulate FOXO1 activity. Thus, sevoflurane could increase FOXO1 activity. In the clinical samples, miR-26a expression was significantly upregulated, but FOXO1 was remarkably down-regulated and miR-26a expression in LSCC was linked with better prognosis. In conclusion, MiR-26a is increased and FOXO1 is reduced in human LSCC, Sevoflurane inhibits proliferation and mediates apoptosis of LSCC cells. Further, MiR-26a binds FOXO1 directly, and FOXO1 expression is down-regulated by Sevoflurane. Finally, Sevoflurane triggers LSCC cells apoptosis in vivo. Sevoflurane use to target miR-26a/FOXO1 may be a novel alternative for LSCC therapy.http://dx.doi.org/10.1080/21655979.2021.1962684sevofluranemir-26afoxo1laryngeal squamous cell carcinoma
collection DOAJ
language English
format Article
sources DOAJ
author Dan Liu
Lang Wan
Hao Gong
Shiming Chen
Yonggang Kong
Bokui Xiao
spellingShingle Dan Liu
Lang Wan
Hao Gong
Shiming Chen
Yonggang Kong
Bokui Xiao
Sevoflurane promotes the apoptosis of laryngeal squamous cell carcinoma in-vitro and inhibits its malignant progression via miR-26a/FOXO1 axis
Bioengineered
sevoflurane
mir-26a
foxo1
laryngeal squamous cell carcinoma
author_facet Dan Liu
Lang Wan
Hao Gong
Shiming Chen
Yonggang Kong
Bokui Xiao
author_sort Dan Liu
title Sevoflurane promotes the apoptosis of laryngeal squamous cell carcinoma in-vitro and inhibits its malignant progression via miR-26a/FOXO1 axis
title_short Sevoflurane promotes the apoptosis of laryngeal squamous cell carcinoma in-vitro and inhibits its malignant progression via miR-26a/FOXO1 axis
title_full Sevoflurane promotes the apoptosis of laryngeal squamous cell carcinoma in-vitro and inhibits its malignant progression via miR-26a/FOXO1 axis
title_fullStr Sevoflurane promotes the apoptosis of laryngeal squamous cell carcinoma in-vitro and inhibits its malignant progression via miR-26a/FOXO1 axis
title_full_unstemmed Sevoflurane promotes the apoptosis of laryngeal squamous cell carcinoma in-vitro and inhibits its malignant progression via miR-26a/FOXO1 axis
title_sort sevoflurane promotes the apoptosis of laryngeal squamous cell carcinoma in-vitro and inhibits its malignant progression via mir-26a/foxo1 axis
publisher Taylor & Francis Group
series Bioengineered
issn 2165-5979
2165-5987
publishDate 2021-01-01
description Laryngeal squamous cell carcinoma (LSCC) is a laryngeal malignancy with a high mortality rates, and its treatment remains difficult. Sevoflurane is a surgical anesthesia which has anti-tumor effect. This investigation assessed the effects of LSCC cells treatment with Sevoflurane in vitro and in vivo. Hep-2 and Tu177 cells, human LSCC samples and BALB/C nude mice were used for result assessments. Cell viability, proliferation, migration and invasion were assessed via Cell Count Kit-8, wound healing assay and transwell invasion assay respectively. MiR-26a and FOXO1 expressions was examined by qRT-PCR. FOXO1, E-cadherin, N-cadherin and vimentin activities were examined by Western blotting. Moreover, animal experiments were performed to verify our findings in vitro. Lastly, miR-26a and FOXO1 expression levels in clinical samples were analyzed. According to the results, Sevoflurane decreased LSCC cells’ viability and even stimulated their apoptosis in vitro and in vivo. Moreover, it could reduce the migration, invasion and EMT. Mechanistically, sevoflurane could downregulate miR-26a expression and that miR-26a could negatively modulate FOXO1 activity. Thus, sevoflurane could increase FOXO1 activity. In the clinical samples, miR-26a expression was significantly upregulated, but FOXO1 was remarkably down-regulated and miR-26a expression in LSCC was linked with better prognosis. In conclusion, MiR-26a is increased and FOXO1 is reduced in human LSCC, Sevoflurane inhibits proliferation and mediates apoptosis of LSCC cells. Further, MiR-26a binds FOXO1 directly, and FOXO1 expression is down-regulated by Sevoflurane. Finally, Sevoflurane triggers LSCC cells apoptosis in vivo. Sevoflurane use to target miR-26a/FOXO1 may be a novel alternative for LSCC therapy.
topic sevoflurane
mir-26a
foxo1
laryngeal squamous cell carcinoma
url http://dx.doi.org/10.1080/21655979.2021.1962684
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AT langwan sevofluranepromotestheapoptosisoflaryngealsquamouscellcarcinomainvitroandinhibitsitsmalignantprogressionviamir26afoxo1axis
AT haogong sevofluranepromotestheapoptosisoflaryngealsquamouscellcarcinomainvitroandinhibitsitsmalignantprogressionviamir26afoxo1axis
AT shimingchen sevofluranepromotestheapoptosisoflaryngealsquamouscellcarcinomainvitroandinhibitsitsmalignantprogressionviamir26afoxo1axis
AT yonggangkong sevofluranepromotestheapoptosisoflaryngealsquamouscellcarcinomainvitroandinhibitsitsmalignantprogressionviamir26afoxo1axis
AT bokuixiao sevofluranepromotestheapoptosisoflaryngealsquamouscellcarcinomainvitroandinhibitsitsmalignantprogressionviamir26afoxo1axis
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