Melatonin decreases M1 polarization via attenuating mitochondrial oxidative damage depending on UCP2 pathway in prorenin-treated microglia.

Melatonin decreases M1 polarization via attenuating mitochondrial oxidative damage depending on UCP2 pathway in prorenin-treated microglia.

Accumulating evidence suggests that neuroinflammation and oxidative stress in cardiovascular center contribute to the pathological processes underlying hypertension. Microglia activation triggers the inflammation and oxidative stress. Melatonin is a documented potent anti-inflammatory regent and ant...

Full description

Bibliographic Details
Main Authors: Li Hu, Shutian Zhang, Haoyu Wen, Tianfeng Liu, Jian Cai, Dongshu Du, Danian Zhu, Fuxue Chen, Chunmei Xia
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2019-01-01
Series:PLoS ONE
Online Access:https://doi.org/10.1371/journal.pone.0212138
id doaj-a572339c050d4a6fa383802871f20532
record_format Article
spelling doaj-a572339c050d4a6fa383802871f205322021-03-03T20:53:36ZengPublic Library of Science (PLoS)PLoS ONE1932-62032019-01-01142e021213810.1371/journal.pone.0212138Melatonin decreases M1 polarization via attenuating mitochondrial oxidative damage depending on UCP2 pathway in prorenin-treated microglia.Li HuShutian ZhangHaoyu WenTianfeng LiuJian CaiDongshu DuDanian ZhuFuxue ChenChunmei XiaAccumulating evidence suggests that neuroinflammation and oxidative stress in cardiovascular center contribute to the pathological processes underlying hypertension. Microglia activation triggers the inflammation and oxidative stress. Melatonin is a documented potent anti-inflammatory regent and antioxidant, the underlying roles of melatonin in regulating microglia activation via mitochondria remain unclear. In present study, we investigated the protective role of melatonin in decreasing M1 phenotype switching via attenuating mitochondrial oxidative damage in dependence on uncoupling protein 2 (UCP2) pathway in microglia. Prorenin (20 nmol/L; 24 hr) was used to induce inflammation in cultured microglia. Mitochondrial morphology was detected by transmission electron microscope. The reactive oxygen species (ROS) production by using DCFH-DA fluorescence imaging and mitochondrial membrane potential (MMP, ΔΨm) was evaluated by JC-1 staining. The indicator of the redox status as the ratio of the amount of total NADP+ to total NADPH, and the expression of 6 subunits of NADPH oxidase is measured. The pro-inflammatory cytokines releasing was measured by qPCR. UCP2 and activated AMPKα (p-AMPKα) expression were examined by immunoblot. Melatonin (100 μM) markedly alleviated the M1 microglia phenotype shifting and abnormal mitochondria morphology. Melatonin attenuated prorenin-induced ΔΨm increasing and ROS overproduction. Melatonin decreased the redox ratio (NADP+/NADPH) and the p47phox and gp91phox subunits of NADPH oxidase expression in prorenin-treated microglia. These effects were reversed in the presence of UCP2 siRNA. Our results suggested that the protective effect of melatonin against prorenin-induced M1 phenotype switching via attenuating mitochondrial oxidative damage depending on UCP2 upregulation in prorenin-treated microglia.https://doi.org/10.1371/journal.pone.0212138
collection DOAJ
language English
format Article
sources DOAJ
author Li Hu
Shutian Zhang
Haoyu Wen
Tianfeng Liu
Jian Cai
Dongshu Du
Danian Zhu
Fuxue Chen
Chunmei Xia
spellingShingle Li Hu
Shutian Zhang
Haoyu Wen
Tianfeng Liu
Jian Cai
Dongshu Du
Danian Zhu
Fuxue Chen
Chunmei Xia
Melatonin decreases M1 polarization via attenuating mitochondrial oxidative damage depending on UCP2 pathway in prorenin-treated microglia.
PLoS ONE
author_facet Li Hu
Shutian Zhang
Haoyu Wen
Tianfeng Liu
Jian Cai
Dongshu Du
Danian Zhu
Fuxue Chen
Chunmei Xia
author_sort Li Hu
title Melatonin decreases M1 polarization via attenuating mitochondrial oxidative damage depending on UCP2 pathway in prorenin-treated microglia.
title_short Melatonin decreases M1 polarization via attenuating mitochondrial oxidative damage depending on UCP2 pathway in prorenin-treated microglia.
title_full Melatonin decreases M1 polarization via attenuating mitochondrial oxidative damage depending on UCP2 pathway in prorenin-treated microglia.
title_fullStr Melatonin decreases M1 polarization via attenuating mitochondrial oxidative damage depending on UCP2 pathway in prorenin-treated microglia.
title_full_unstemmed Melatonin decreases M1 polarization via attenuating mitochondrial oxidative damage depending on UCP2 pathway in prorenin-treated microglia.
title_sort melatonin decreases m1 polarization via attenuating mitochondrial oxidative damage depending on ucp2 pathway in prorenin-treated microglia.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2019-01-01
description Accumulating evidence suggests that neuroinflammation and oxidative stress in cardiovascular center contribute to the pathological processes underlying hypertension. Microglia activation triggers the inflammation and oxidative stress. Melatonin is a documented potent anti-inflammatory regent and antioxidant, the underlying roles of melatonin in regulating microglia activation via mitochondria remain unclear. In present study, we investigated the protective role of melatonin in decreasing M1 phenotype switching via attenuating mitochondrial oxidative damage in dependence on uncoupling protein 2 (UCP2) pathway in microglia. Prorenin (20 nmol/L; 24 hr) was used to induce inflammation in cultured microglia. Mitochondrial morphology was detected by transmission electron microscope. The reactive oxygen species (ROS) production by using DCFH-DA fluorescence imaging and mitochondrial membrane potential (MMP, ΔΨm) was evaluated by JC-1 staining. The indicator of the redox status as the ratio of the amount of total NADP+ to total NADPH, and the expression of 6 subunits of NADPH oxidase is measured. The pro-inflammatory cytokines releasing was measured by qPCR. UCP2 and activated AMPKα (p-AMPKα) expression were examined by immunoblot. Melatonin (100 μM) markedly alleviated the M1 microglia phenotype shifting and abnormal mitochondria morphology. Melatonin attenuated prorenin-induced ΔΨm increasing and ROS overproduction. Melatonin decreased the redox ratio (NADP+/NADPH) and the p47phox and gp91phox subunits of NADPH oxidase expression in prorenin-treated microglia. These effects were reversed in the presence of UCP2 siRNA. Our results suggested that the protective effect of melatonin against prorenin-induced M1 phenotype switching via attenuating mitochondrial oxidative damage depending on UCP2 upregulation in prorenin-treated microglia.
url https://doi.org/10.1371/journal.pone.0212138
work_keys_str_mv AT lihu melatonindecreasesm1polarizationviaattenuatingmitochondrialoxidativedamagedependingonucp2pathwayinprorenintreatedmicroglia
AT shutianzhang melatonindecreasesm1polarizationviaattenuatingmitochondrialoxidativedamagedependingonucp2pathwayinprorenintreatedmicroglia
AT haoyuwen melatonindecreasesm1polarizationviaattenuatingmitochondrialoxidativedamagedependingonucp2pathwayinprorenintreatedmicroglia
AT tianfengliu melatonindecreasesm1polarizationviaattenuatingmitochondrialoxidativedamagedependingonucp2pathwayinprorenintreatedmicroglia
AT jiancai melatonindecreasesm1polarizationviaattenuatingmitochondrialoxidativedamagedependingonucp2pathwayinprorenintreatedmicroglia
AT dongshudu melatonindecreasesm1polarizationviaattenuatingmitochondrialoxidativedamagedependingonucp2pathwayinprorenintreatedmicroglia
AT danianzhu melatonindecreasesm1polarizationviaattenuatingmitochondrialoxidativedamagedependingonucp2pathwayinprorenintreatedmicroglia
AT fuxuechen melatonindecreasesm1polarizationviaattenuatingmitochondrialoxidativedamagedependingonucp2pathwayinprorenintreatedmicroglia
AT chunmeixia melatonindecreasesm1polarizationviaattenuatingmitochondrialoxidativedamagedependingonucp2pathwayinprorenintreatedmicroglia
_version_ 1714819921873993728

Similar Items