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MicroRNAs emerging coordinate with placental mammals alter pathways in endometrial epithelia important for endometrial function

We tested the hypothesis that conserved placental mammal-specific microRNAs and their targets facilitate endometrial receptivity to implantation. Expression of miR-340-5p, -542-3p, and -671-5p was regulated by exposure of endometrial epithelial cells to progesterone (10 μg/ml) for 24 h coordinate wi...

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Autores principales: Hume, Laura, Edge, Jessica C., Tinning, Haidee, Wang, Dapeng, Taylor, Alysha S., Ovchinnikov, Vladimir, Geijer-Simpson, Annika V., Vrljicak, Pavle, Brosens, Jan J., Lucas, Emma S., Simpson, Nigel A.B., Shillito, Jayne, Forbes, Karen, O’Connell, Mary J., Forde, Niamh
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10034127/
https://www.ncbi.nlm.nih.gov/pubmed/36968081
http://dx.doi.org/10.1016/j.isci.2023.106339
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author Hume, Laura
Edge, Jessica C.
Tinning, Haidee
Wang, Dapeng
Taylor, Alysha S.
Ovchinnikov, Vladimir
Geijer-Simpson, Annika V.
Vrljicak, Pavle
Brosens, Jan J.
Lucas, Emma S.
Simpson, Nigel A.B.
Shillito, Jayne
Forbes, Karen
O’Connell, Mary J.
Forde, Niamh
author_facet Hume, Laura
Edge, Jessica C.
Tinning, Haidee
Wang, Dapeng
Taylor, Alysha S.
Ovchinnikov, Vladimir
Geijer-Simpson, Annika V.
Vrljicak, Pavle
Brosens, Jan J.
Lucas, Emma S.
Simpson, Nigel A.B.
Shillito, Jayne
Forbes, Karen
O’Connell, Mary J.
Forde, Niamh
author_sort Hume, Laura
collection PubMed
description We tested the hypothesis that conserved placental mammal-specific microRNAs and their targets facilitate endometrial receptivity to implantation. Expression of miR-340-5p, -542-3p, and -671-5p was regulated by exposure of endometrial epithelial cells to progesterone (10 μg/ml) for 24 h coordinate with 1,713 of their predicted targets. Proteomic analysis of cells transfected with miRNA mimic/inhibitor (48 h: n = 3) revealed 1,745 proteins altered by miR-340-5p (mimic; 1,369, inhibitor; 376) of which 171 were predicted targets and P4-regulated. MiR-542-3p altered 2,353 (mimic; 1,378, inhibitor; 975) 100 which were mirDB predicted, including 46 P4-regulated. MiR-671-5p altered 1,744 proteins (mimic; 1,252, inhibitor; 492) 95 of which were predicted targets and 46 P4-regulated. All miRNAs were detected in luteal phase endometrial biopsies, irrespective of pregnancy outcomes. miR-340-5p expression increased in biopsies from individuals suffering previous and subsequent miscarriage compared to those with subsequent live birth. Dysfunction of these miRNAs and their targets contribute to endometrial-derived recurrent pregnancy loss.
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spelling pubmed-100341272023-03-24 MicroRNAs emerging coordinate with placental mammals alter pathways in endometrial epithelia important for endometrial function Hume, Laura Edge, Jessica C. Tinning, Haidee Wang, Dapeng Taylor, Alysha S. Ovchinnikov, Vladimir Geijer-Simpson, Annika V. Vrljicak, Pavle Brosens, Jan J. Lucas, Emma S. Simpson, Nigel A.B. Shillito, Jayne Forbes, Karen O’Connell, Mary J. Forde, Niamh iScience Article We tested the hypothesis that conserved placental mammal-specific microRNAs and their targets facilitate endometrial receptivity to implantation. Expression of miR-340-5p, -542-3p, and -671-5p was regulated by exposure of endometrial epithelial cells to progesterone (10 μg/ml) for 24 h coordinate with 1,713 of their predicted targets. Proteomic analysis of cells transfected with miRNA mimic/inhibitor (48 h: n = 3) revealed 1,745 proteins altered by miR-340-5p (mimic; 1,369, inhibitor; 376) of which 171 were predicted targets and P4-regulated. MiR-542-3p altered 2,353 (mimic; 1,378, inhibitor; 975) 100 which were mirDB predicted, including 46 P4-regulated. MiR-671-5p altered 1,744 proteins (mimic; 1,252, inhibitor; 492) 95 of which were predicted targets and 46 P4-regulated. All miRNAs were detected in luteal phase endometrial biopsies, irrespective of pregnancy outcomes. miR-340-5p expression increased in biopsies from individuals suffering previous and subsequent miscarriage compared to those with subsequent live birth. Dysfunction of these miRNAs and their targets contribute to endometrial-derived recurrent pregnancy loss. Elsevier 2023-03-04 /pmc/articles/PMC10034127/ /pubmed/36968081 http://dx.doi.org/10.1016/j.isci.2023.106339 Text en © 2023 The Author(s) https://creativecommons.org/licenses/by/4.0/This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Hume, Laura
Edge, Jessica C.
Tinning, Haidee
Wang, Dapeng
Taylor, Alysha S.
Ovchinnikov, Vladimir
Geijer-Simpson, Annika V.
Vrljicak, Pavle
Brosens, Jan J.
Lucas, Emma S.
Simpson, Nigel A.B.
Shillito, Jayne
Forbes, Karen
O’Connell, Mary J.
Forde, Niamh
MicroRNAs emerging coordinate with placental mammals alter pathways in endometrial epithelia important for endometrial function
title MicroRNAs emerging coordinate with placental mammals alter pathways in endometrial epithelia important for endometrial function
title_full MicroRNAs emerging coordinate with placental mammals alter pathways in endometrial epithelia important for endometrial function
title_fullStr MicroRNAs emerging coordinate with placental mammals alter pathways in endometrial epithelia important for endometrial function
title_full_unstemmed MicroRNAs emerging coordinate with placental mammals alter pathways in endometrial epithelia important for endometrial function
title_short MicroRNAs emerging coordinate with placental mammals alter pathways in endometrial epithelia important for endometrial function
title_sort micrornas emerging coordinate with placental mammals alter pathways in endometrial epithelia important for endometrial function
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10034127/
https://www.ncbi.nlm.nih.gov/pubmed/36968081
http://dx.doi.org/10.1016/j.isci.2023.106339
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