Melatonin protects against environmental stress-induced fetal growth restriction via suppressing ROS-mediated GCN2/ATF4/BNIP3-dependent mitophagy in placental trophoblasts

Gestational exposure to environmental stress induces fetal growth restriction (FGR), and thereby increasing the risk of infant death and chronic noncommunicable diseases in adults. However, the mechanism by which environmental stress induces FGR remains unclear. Based on case-control study, we found...

Descripción completa

Detalles Bibliográficos
Autores principales: Zhu, Hua-Long, Shi, Xue-Ting, Xu, Xiao-Feng, Zhou, Guo-Xiang, Xiong, Yong-Wei, Yi, Song-Jia, Liu, Wei-Bo, Dai, Li-Min, Cao, Xue-Lin, Xu, De-Xiang, Wang, Hua
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2021
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7811044/
https://www.ncbi.nlm.nih.gov/pubmed/33454563
http://dx.doi.org/10.1016/j.redox.2021.101854
_version_ 1783637428042465280
author Zhu, Hua-Long
Shi, Xue-Ting
Xu, Xiao-Feng
Zhou, Guo-Xiang
Xiong, Yong-Wei
Yi, Song-Jia
Liu, Wei-Bo
Dai, Li-Min
Cao, Xue-Lin
Xu, De-Xiang
Wang, Hua
author_facet Zhu, Hua-Long
Shi, Xue-Ting
Xu, Xiao-Feng
Zhou, Guo-Xiang
Xiong, Yong-Wei
Yi, Song-Jia
Liu, Wei-Bo
Dai, Li-Min
Cao, Xue-Lin
Xu, De-Xiang
Wang, Hua
author_sort Zhu, Hua-Long
collection PubMed
description Gestational exposure to environmental stress induces fetal growth restriction (FGR), and thereby increasing the risk of infant death and chronic noncommunicable diseases in adults. However, the mechanism by which environmental stress induces FGR remains unclear. Based on case-control study, we found that the reduced level of melatonin (MT), a major secretory product from the pineal gland, was observed in placentae of FGR. This work was to investigate the protective effect of MT on environmental stress-caused FGR and its mechanisms. We used cadmium (Cd) as an environmental stressor to stimulate pregnant mice and thereby establishing a FGR model. The data showed that maternal Cd exposure lowered the P4 concentration in maternal sera, placentae and amniotic fluid, and caused FGR. Correspondingly, the expression of CYP11A1, a critical P4 synthase, was markedly downregulated in Cd-treated placentae. Simultaneously, Cd triggered BNIP3-dependent mitophagy in placental trophoblasts, as determined by the degradation of mitochondrial proteins, including HSP60 and COX IV, and the accumulation of puncta representing co-localization of TOM20 with LC3B or BNIP3 with LC3B. Based on our case-control study, we also found that activated BNIP3-dependent mitophagy and P4 synthesis inhibition occurred in SGA placentae. Most importantly, BNIP3 siRNA reversed Cd-induced P4 synthesis suppression in human placental trophoblasts. It is noteworthy that MT alleviated Cd-caused P4 synthesis suppression and FGR via antagonizing BNIP3-dependent mitophagy in placental trophoblasts. Further results confirmed that MT attenuated Cd-triggered BNIP3-dependent mitophagy via blocking GCN2/ATF4 signaling. Amusingly, Cd triggered oxidative stress and then activating GCN2/ATF4 signaling in placental trophoblasts. As expected, MT obviously suppressed Cd-caused reactive oxygen species (ROS) release. In the present study, we propose a neoteric mechanism by which MT protects against environmental stress-impaired P4 synthesis and fetal growth via suppressing ROS-mediated GCN2/ATF4/BNIP3-dependent mitophagy in placental trophoblasts. As above, MT is a potential therapeutic agent antagonizing environmental stress-induced developmental toxicity.
format Online
Article
Text
id pubmed-7811044
institution National Center for Biotechnology Information
language English
publishDate 2021
publisher Elsevier
record_format MEDLINE/PubMed
spelling pubmed-78110442021-01-22 Melatonin protects against environmental stress-induced fetal growth restriction via suppressing ROS-mediated GCN2/ATF4/BNIP3-dependent mitophagy in placental trophoblasts Zhu, Hua-Long Shi, Xue-Ting Xu, Xiao-Feng Zhou, Guo-Xiang Xiong, Yong-Wei Yi, Song-Jia Liu, Wei-Bo Dai, Li-Min Cao, Xue-Lin Xu, De-Xiang Wang, Hua Redox Biol Research Paper Gestational exposure to environmental stress induces fetal growth restriction (FGR), and thereby increasing the risk of infant death and chronic noncommunicable diseases in adults. However, the mechanism by which environmental stress induces FGR remains unclear. Based on case-control study, we found that the reduced level of melatonin (MT), a major secretory product from the pineal gland, was observed in placentae of FGR. This work was to investigate the protective effect of MT on environmental stress-caused FGR and its mechanisms. We used cadmium (Cd) as an environmental stressor to stimulate pregnant mice and thereby establishing a FGR model. The data showed that maternal Cd exposure lowered the P4 concentration in maternal sera, placentae and amniotic fluid, and caused FGR. Correspondingly, the expression of CYP11A1, a critical P4 synthase, was markedly downregulated in Cd-treated placentae. Simultaneously, Cd triggered BNIP3-dependent mitophagy in placental trophoblasts, as determined by the degradation of mitochondrial proteins, including HSP60 and COX IV, and the accumulation of puncta representing co-localization of TOM20 with LC3B or BNIP3 with LC3B. Based on our case-control study, we also found that activated BNIP3-dependent mitophagy and P4 synthesis inhibition occurred in SGA placentae. Most importantly, BNIP3 siRNA reversed Cd-induced P4 synthesis suppression in human placental trophoblasts. It is noteworthy that MT alleviated Cd-caused P4 synthesis suppression and FGR via antagonizing BNIP3-dependent mitophagy in placental trophoblasts. Further results confirmed that MT attenuated Cd-triggered BNIP3-dependent mitophagy via blocking GCN2/ATF4 signaling. Amusingly, Cd triggered oxidative stress and then activating GCN2/ATF4 signaling in placental trophoblasts. As expected, MT obviously suppressed Cd-caused reactive oxygen species (ROS) release. In the present study, we propose a neoteric mechanism by which MT protects against environmental stress-impaired P4 synthesis and fetal growth via suppressing ROS-mediated GCN2/ATF4/BNIP3-dependent mitophagy in placental trophoblasts. As above, MT is a potential therapeutic agent antagonizing environmental stress-induced developmental toxicity. Elsevier 2021-01-06 /pmc/articles/PMC7811044/ /pubmed/33454563 http://dx.doi.org/10.1016/j.redox.2021.101854 Text en © 2021 The Author(s) http://creativecommons.org/licenses/by-nc-nd/4.0/ This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Research Paper
Zhu, Hua-Long
Shi, Xue-Ting
Xu, Xiao-Feng
Zhou, Guo-Xiang
Xiong, Yong-Wei
Yi, Song-Jia
Liu, Wei-Bo
Dai, Li-Min
Cao, Xue-Lin
Xu, De-Xiang
Wang, Hua
Melatonin protects against environmental stress-induced fetal growth restriction via suppressing ROS-mediated GCN2/ATF4/BNIP3-dependent mitophagy in placental trophoblasts
title Melatonin protects against environmental stress-induced fetal growth restriction via suppressing ROS-mediated GCN2/ATF4/BNIP3-dependent mitophagy in placental trophoblasts
title_full Melatonin protects against environmental stress-induced fetal growth restriction via suppressing ROS-mediated GCN2/ATF4/BNIP3-dependent mitophagy in placental trophoblasts
title_fullStr Melatonin protects against environmental stress-induced fetal growth restriction via suppressing ROS-mediated GCN2/ATF4/BNIP3-dependent mitophagy in placental trophoblasts
title_full_unstemmed Melatonin protects against environmental stress-induced fetal growth restriction via suppressing ROS-mediated GCN2/ATF4/BNIP3-dependent mitophagy in placental trophoblasts
title_short Melatonin protects against environmental stress-induced fetal growth restriction via suppressing ROS-mediated GCN2/ATF4/BNIP3-dependent mitophagy in placental trophoblasts
title_sort melatonin protects against environmental stress-induced fetal growth restriction via suppressing ros-mediated gcn2/atf4/bnip3-dependent mitophagy in placental trophoblasts
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7811044/
https://www.ncbi.nlm.nih.gov/pubmed/33454563
http://dx.doi.org/10.1016/j.redox.2021.101854
work_keys_str_mv AT zhuhualong melatoninprotectsagainstenvironmentalstressinducedfetalgrowthrestrictionviasuppressingrosmediatedgcn2atf4bnip3dependentmitophagyinplacentaltrophoblasts
AT shixueting melatoninprotectsagainstenvironmentalstressinducedfetalgrowthrestrictionviasuppressingrosmediatedgcn2atf4bnip3dependentmitophagyinplacentaltrophoblasts
AT xuxiaofeng melatoninprotectsagainstenvironmentalstressinducedfetalgrowthrestrictionviasuppressingrosmediatedgcn2atf4bnip3dependentmitophagyinplacentaltrophoblasts
AT zhouguoxiang melatoninprotectsagainstenvironmentalstressinducedfetalgrowthrestrictionviasuppressingrosmediatedgcn2atf4bnip3dependentmitophagyinplacentaltrophoblasts
AT xiongyongwei melatoninprotectsagainstenvironmentalstressinducedfetalgrowthrestrictionviasuppressingrosmediatedgcn2atf4bnip3dependentmitophagyinplacentaltrophoblasts
AT yisongjia melatoninprotectsagainstenvironmentalstressinducedfetalgrowthrestrictionviasuppressingrosmediatedgcn2atf4bnip3dependentmitophagyinplacentaltrophoblasts
AT liuweibo melatoninprotectsagainstenvironmentalstressinducedfetalgrowthrestrictionviasuppressingrosmediatedgcn2atf4bnip3dependentmitophagyinplacentaltrophoblasts
AT dailimin melatoninprotectsagainstenvironmentalstressinducedfetalgrowthrestrictionviasuppressingrosmediatedgcn2atf4bnip3dependentmitophagyinplacentaltrophoblasts
AT caoxuelin melatoninprotectsagainstenvironmentalstressinducedfetalgrowthrestrictionviasuppressingrosmediatedgcn2atf4bnip3dependentmitophagyinplacentaltrophoblasts
AT xudexiang melatoninprotectsagainstenvironmentalstressinducedfetalgrowthrestrictionviasuppressingrosmediatedgcn2atf4bnip3dependentmitophagyinplacentaltrophoblasts
AT wanghua melatoninprotectsagainstenvironmentalstressinducedfetalgrowthrestrictionviasuppressingrosmediatedgcn2atf4bnip3dependentmitophagyinplacentaltrophoblasts

Ejemplares similares