FRI492 Malaria In Pregnancy And Lipopolyssacharide Lead To Sex-specific Changes In The Expression Of Genes Involved In The Placental Metabolism Of Thyroid Hormones

Disclosure: K.N. Fontes: None. V.S. Monteiro: None. C.B. Andrade: None. A.C. Valim: None. V.M. Nascimento: None. D.E. Teixeira: None. A.A. Pinheiro: None. E. Bloise: None. T.M. Ortiga-Carvalho: None. Infection during gestation promotes marked changes in placental physiology, leading to intrauterine...

Descripción completa

Detalles Bibliográficos
Autores principales: Fontes, Klaus N, Siqueira Monteiro, Victoria, Vieira de Andrade, Cherley Borba, Valim, Alessandra C C, de Oliveira Nascimento, Verônica Müller, Teixeira, Douglas E, Student, Master, Pinheiro, Ana A S, Bloise, Enrrico, Maria Ortiga-Carvalho, Tania
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2023
Materias:
Thyroid
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10555239/
http://dx.doi.org/10.1210/jendso/bvad114.1838
_version_ 1785116608583172096
author Fontes, Klaus N
Siqueira Monteiro, Victoria
Vieira de Andrade, Cherley Borba
Valim, Alessandra C C
de Oliveira Nascimento, Verônica Müller
Teixeira, Douglas E
Student, Master
Pinheiro, Ana A S
Bloise, Enrrico
Maria Ortiga-Carvalho, Tania
author_facet Fontes, Klaus N
Siqueira Monteiro, Victoria
Vieira de Andrade, Cherley Borba
Valim, Alessandra C C
de Oliveira Nascimento, Verônica Müller
Teixeira, Douglas E
Student, Master
Pinheiro, Ana A S
Bloise, Enrrico
Maria Ortiga-Carvalho, Tania
author_sort Fontes, Klaus N
collection PubMed
description Disclosure: K.N. Fontes: None. V.S. Monteiro: None. C.B. Andrade: None. A.C. Valim: None. V.M. Nascimento: None. D.E. Teixeira: None. A.A. Pinheiro: None. E. Bloise: None. T.M. Ortiga-Carvalho: None. Infection during gestation promotes marked changes in placental physiology, leading to intrauterine growth restriction (IUGR), preterm labor (PTL) and neurodevelopmental disorders. Infection in pregnant women or mice may impact thyroid hormones’ (TH) metabolism and the importance of TH for the development of the placenta and conceptus is widely described in the literature. Our main aim was to evaluate changes in the expression of specific genes involved in placental TH metabolism triggered by malaria in pregnancy (MiP) or bacterial lipopolyssacharide (LPS), in the male and female placenta. Female C57BL/6 mice (8-10 weeks of age) were mated. In the MiP model, dams were infected ip with Plasmodium Berghei ANKA-infected erythrocytes (PBA; 5x10(5) infected-erythrocytes, n=10) or injected with PBS (contro; n=10) at gestational day (GD)13.5 and sacrificed at GD18.5. In the LPS model, dams were injected ip with LPS (150 µg/kg, n=10) or PBS (control; n=10) at GD17.5 and sacrificed at GD18.5. Maternal blood was collected to evaluate PBA parasitemia. Placental disks were collected from dams delivering at term (GD18.5), and qPCR was performed to evaluate the mRNA expression of genes involved in placental TH metabolism. MiP was confirmed by analysis of parasitemia (15.9%), and resulted in increased maternal spleen weight (P<0.05). As expected, MiP induced PTL (at GD17.5) in 23.1% of dams. Fetal weight and fetal/placental weight ratio were reduced in MiP (at term), compared to control (P<0.05). In the LPS model, 33.3% of dams went into PTL (at GD17.5) and fetal weight was reduced in LPS group (at term), compared to control (P<0.05). In both models, mRNA of the Cxcl1 chemokine (P<0.05) was increased in the male and female placenta at term (P<0.05). Male MiP placentas exhibited a reduction in Slc7a8 (P<0.05) and Dio2 (P<0.05) mRNA expression, whereas female MiP placentas exhibited a reduction in Slc7a8 (P<0.05) and an increase in Slco1c1 and Dio1 (P<0.05) at term. LPS increased Dio1 (P<0.05) mRNA in the male term placenta, and increased Ccl2 (P<0.05) mRNA in the term female placenta. In the present study, MiP was associated with sex-specific changes in the placental expression of TH transporters and deiodinases, while LPS injection promoted a limited effect on placental TH metabolism, but increased the expression of placental inflammatory markers at term. We speculate that these changes may result in reduced TH transport from mother to fetus, leading to IUGR among surviving fetuses, especially in pregnancies threatened by MiP. Presentation: Friday, June 16, 2023
format Online
Article
Text
id pubmed-10555239
institution National Center for Biotechnology Information
language English
publishDate 2023
publisher Oxford University Press
record_format MEDLINE/PubMed
spelling pubmed-105552392023-10-06 FRI492 Malaria In Pregnancy And Lipopolyssacharide Lead To Sex-specific Changes In The Expression Of Genes Involved In The Placental Metabolism Of Thyroid Hormones Fontes, Klaus N Siqueira Monteiro, Victoria Vieira de Andrade, Cherley Borba Valim, Alessandra C C de Oliveira Nascimento, Verônica Müller Teixeira, Douglas E Student, Master Pinheiro, Ana A S Bloise, Enrrico Maria Ortiga-Carvalho, Tania J Endocr Soc Thyroid Disclosure: K.N. Fontes: None. V.S. Monteiro: None. C.B. Andrade: None. A.C. Valim: None. V.M. Nascimento: None. D.E. Teixeira: None. A.A. Pinheiro: None. E. Bloise: None. T.M. Ortiga-Carvalho: None. Infection during gestation promotes marked changes in placental physiology, leading to intrauterine growth restriction (IUGR), preterm labor (PTL) and neurodevelopmental disorders. Infection in pregnant women or mice may impact thyroid hormones’ (TH) metabolism and the importance of TH for the development of the placenta and conceptus is widely described in the literature. Our main aim was to evaluate changes in the expression of specific genes involved in placental TH metabolism triggered by malaria in pregnancy (MiP) or bacterial lipopolyssacharide (LPS), in the male and female placenta. Female C57BL/6 mice (8-10 weeks of age) were mated. In the MiP model, dams were infected ip with Plasmodium Berghei ANKA-infected erythrocytes (PBA; 5x10(5) infected-erythrocytes, n=10) or injected with PBS (contro; n=10) at gestational day (GD)13.5 and sacrificed at GD18.5. In the LPS model, dams were injected ip with LPS (150 µg/kg, n=10) or PBS (control; n=10) at GD17.5 and sacrificed at GD18.5. Maternal blood was collected to evaluate PBA parasitemia. Placental disks were collected from dams delivering at term (GD18.5), and qPCR was performed to evaluate the mRNA expression of genes involved in placental TH metabolism. MiP was confirmed by analysis of parasitemia (15.9%), and resulted in increased maternal spleen weight (P<0.05). As expected, MiP induced PTL (at GD17.5) in 23.1% of dams. Fetal weight and fetal/placental weight ratio were reduced in MiP (at term), compared to control (P<0.05). In the LPS model, 33.3% of dams went into PTL (at GD17.5) and fetal weight was reduced in LPS group (at term), compared to control (P<0.05). In both models, mRNA of the Cxcl1 chemokine (P<0.05) was increased in the male and female placenta at term (P<0.05). Male MiP placentas exhibited a reduction in Slc7a8 (P<0.05) and Dio2 (P<0.05) mRNA expression, whereas female MiP placentas exhibited a reduction in Slc7a8 (P<0.05) and an increase in Slco1c1 and Dio1 (P<0.05) at term. LPS increased Dio1 (P<0.05) mRNA in the male term placenta, and increased Ccl2 (P<0.05) mRNA in the term female placenta. In the present study, MiP was associated with sex-specific changes in the placental expression of TH transporters and deiodinases, while LPS injection promoted a limited effect on placental TH metabolism, but increased the expression of placental inflammatory markers at term. We speculate that these changes may result in reduced TH transport from mother to fetus, leading to IUGR among surviving fetuses, especially in pregnancies threatened by MiP. Presentation: Friday, June 16, 2023 Oxford University Press 2023-10-05 /pmc/articles/PMC10555239/ http://dx.doi.org/10.1210/jendso/bvad114.1838 Text en © The Author(s) 2023. Published by Oxford University Press on behalf of the Endocrine Society. https://creativecommons.org/licenses/by-nc-nd/4.0/This is an Open Access article distributed under the terms of the Creative Commons Attribution-NonCommercial-NoDerivs licence (https://creativecommons.org/licenses/by-nc-nd/4.0/), which permits non-commercial reproduction and distribution of the work, in any medium, provided the original work is not altered or transformed in any way, and that the work is properly cited. For commercial re-use, please contact journals.permissions@oup.com
spellingShingle Thyroid
Fontes, Klaus N
Siqueira Monteiro, Victoria
Vieira de Andrade, Cherley Borba
Valim, Alessandra C C
de Oliveira Nascimento, Verônica Müller
Teixeira, Douglas E
Student, Master
Pinheiro, Ana A S
Bloise, Enrrico
Maria Ortiga-Carvalho, Tania
FRI492 Malaria In Pregnancy And Lipopolyssacharide Lead To Sex-specific Changes In The Expression Of Genes Involved In The Placental Metabolism Of Thyroid Hormones
title FRI492 Malaria In Pregnancy And Lipopolyssacharide Lead To Sex-specific Changes In The Expression Of Genes Involved In The Placental Metabolism Of Thyroid Hormones
title_full FRI492 Malaria In Pregnancy And Lipopolyssacharide Lead To Sex-specific Changes In The Expression Of Genes Involved In The Placental Metabolism Of Thyroid Hormones
title_fullStr FRI492 Malaria In Pregnancy And Lipopolyssacharide Lead To Sex-specific Changes In The Expression Of Genes Involved In The Placental Metabolism Of Thyroid Hormones
title_full_unstemmed FRI492 Malaria In Pregnancy And Lipopolyssacharide Lead To Sex-specific Changes In The Expression Of Genes Involved In The Placental Metabolism Of Thyroid Hormones
title_short FRI492 Malaria In Pregnancy And Lipopolyssacharide Lead To Sex-specific Changes In The Expression Of Genes Involved In The Placental Metabolism Of Thyroid Hormones
title_sort fri492 malaria in pregnancy and lipopolyssacharide lead to sex-specific changes in the expression of genes involved in the placental metabolism of thyroid hormones
topic Thyroid
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10555239/
http://dx.doi.org/10.1210/jendso/bvad114.1838
work_keys_str_mv AT fontesklausn fri492malariainpregnancyandlipopolyssacharideleadtosexspecificchangesintheexpressionofgenesinvolvedintheplacentalmetabolismofthyroidhormones
AT siqueiramonteirovictoria fri492malariainpregnancyandlipopolyssacharideleadtosexspecificchangesintheexpressionofgenesinvolvedintheplacentalmetabolismofthyroidhormones
AT vieiradeandradecherleyborba fri492malariainpregnancyandlipopolyssacharideleadtosexspecificchangesintheexpressionofgenesinvolvedintheplacentalmetabolismofthyroidhormones
AT valimalessandracc fri492malariainpregnancyandlipopolyssacharideleadtosexspecificchangesintheexpressionofgenesinvolvedintheplacentalmetabolismofthyroidhormones
AT deoliveiranascimentoveronicamuller fri492malariainpregnancyandlipopolyssacharideleadtosexspecificchangesintheexpressionofgenesinvolvedintheplacentalmetabolismofthyroidhormones
AT teixeiradouglase fri492malariainpregnancyandlipopolyssacharideleadtosexspecificchangesintheexpressionofgenesinvolvedintheplacentalmetabolismofthyroidhormones
AT studentmaster fri492malariainpregnancyandlipopolyssacharideleadtosexspecificchangesintheexpressionofgenesinvolvedintheplacentalmetabolismofthyroidhormones
AT pinheiroanaas fri492malariainpregnancyandlipopolyssacharideleadtosexspecificchangesintheexpressionofgenesinvolvedintheplacentalmetabolismofthyroidhormones
AT bloiseenrrico fri492malariainpregnancyandlipopolyssacharideleadtosexspecificchangesintheexpressionofgenesinvolvedintheplacentalmetabolismofthyroidhormones
AT mariaortigacarvalhotania fri492malariainpregnancyandlipopolyssacharideleadtosexspecificchangesintheexpressionofgenesinvolvedintheplacentalmetabolismofthyroidhormones

Ejemplares similares