Maternal thyroid hormones are transcriptionally active during embryo-foetal development: results from a novel transgenic mouse model

Carmelo Nucera; Patrizia Muzzi; Cecilia Tiveron; Antonella Farsetti; Federico La Regina; Benedetta Foglio; Shou-Ching Shih; Fabiola Moretti; Linda Della Pietra; Francesca Mancini; Ada Sacchi; Francesco Trimarchi; Alessandro Vercelli; Alfredo Pontecorvi

doi:10.1111/j.1582-4934.2009.00947.x

Maternal thyroid hormones are transcriptionally active during embryo-foetal development: results from a novel transgenic mouse model

Carmelo Nucera, Patrizia Muzzi, Cecilia Tiveron, Antonella Farsetti, Federico La Regina, Benedetta Foglio, Shou-Ching Shih, Fabiola Moretti, Linda Della Pietra, Francesca Mancini, Ada Sacchi, Francesco Trimarchi, Alessandro Vercelli, Alfredo Pontecorvi

Risultato della ricerca: Contributo in rivista › Articolo in rivista

16 Citazioni (Scopus)

Abstract

Even though several studies highlighted the role of maternal thyroid hormones (THs) during embryo-foetal development, direct evidence of their interaction with embryonic thyroid receptors (TRs) is still lacking. We generated a transgenic mouse model ubiquitously expressing a reporter gene tracing TH action during development. We engineered a construct (TRE2×) containing two TH-responsive elements controlling the expression of the LacZ reporter gene, which encodes β-galactosidase (β-gal). The specificity of the TRE2× activation by TH was evaluated in NIH3T3 cells by cotransfecting TRE2× along with TRs, retinoic or oestrogen receptors in the presence of their specific ligands. TRE2× transgene was microinjected into the zygotes, implanted in pseudopregnant BDF1 (a first-generation (F1) hybrid from a cross of C57BL/6 female and a DBA/2 male) mice and transgenic mouse models were developed. β-gal expression was assayed in tissue sections of transgenic mouse embryos at different stages of development. In vitro, TRE2× transactivation was observed only following physiological T3 stimulation, mediated exclusively by TRs. In vivo, β-gal staining, absent until embryonic day 9.5-10.5 (E9.5-E10.5), was observed as early as E11.5-E12.5 in different primordia (i.e. central nervous system, sense organs, intestine, etc.) of the TRE2× transgenic embryos, while the foetal thyroid function (FTF) was still inactive. Immunohistochemistry for TRs essentially colocalized with β-gal staining. No β-gal staining was detected in embryos of hypothyroid transgenic mice. Importantly, treatment with T3 in hypothyroid TRE2× transgenic mice rescued β-gal expression. Our results provide in vivo direct evidence that during embryonic life and before the onset of FTF, maternal THs are transcriptionally active through the action of embryonic TRs. This model may have clinical relevance and may be employed to design end-point assays for new molecules affecting THs action.

Lingua originale	English
pagine (da-a)	2417-2435
Numero di pagine	19
Rivista	Journal of Cellular and Molecular Medicine
Volume	14
DOI	https://doi.org/10.1111/j.1582-4934.2009.00947.x
Stato di pubblicazione	Pubblicato - 2010

Keywords

Animals
Central Nervous System
Embryonic Development
Female
Gene Expression Regulation, Developmental
Gene Expression Regulation, Enzymologic
Genes, Reporter
Genetic Engineering
Immunohistochemistry
Lac Operon
Male
Mice
Mice, Inbred C57BL
Mice, Inbred DBA
Mice, Transgenic
Pregnancy
Promoter Regions, Genetic
Thyroid Hormones
Transcriptional Activation
Transgenes
beta-Galactosidase

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10.1111/j.1582-4934.2009.00947.x

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Nucera, C., Muzzi, P., Tiveron, C., Farsetti, A., Regina, F. L., Foglio, B., Shih, S.-C., Moretti, F., Pietra, L. D., Mancini, F., Sacchi, A., Trimarchi, F., Vercelli, A., & Pontecorvi, A. (2010). Maternal thyroid hormones are transcriptionally active during embryo-foetal development: results from a novel transgenic mouse model. Journal of Cellular and Molecular Medicine, 14, 2417-2435. https://doi.org/10.1111/j.1582-4934.2009.00947.x

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abstract = "Even though several studies highlighted the role of maternal thyroid hormones (THs) during embryo-foetal development, direct evidence of their interaction with embryonic thyroid receptors (TRs) is still lacking. We generated a transgenic mouse model ubiquitously expressing a reporter gene tracing TH action during development. We engineered a construct (TRE2×) containing two TH-responsive elements controlling the expression of the LacZ reporter gene, which encodes β-galactosidase (β-gal). The specificity of the TRE2× activation by TH was evaluated in NIH3T3 cells by cotransfecting TRE2× along with TRs, retinoic or oestrogen receptors in the presence of their specific ligands. TRE2× transgene was microinjected into the zygotes, implanted in pseudopregnant BDF1 (a first-generation (F1) hybrid from a cross of C57BL/6 female and a DBA/2 male) mice and transgenic mouse models were developed. β-gal expression was assayed in tissue sections of transgenic mouse embryos at different stages of development. In vitro, TRE2× transactivation was observed only following physiological T3 stimulation, mediated exclusively by TRs. In vivo, β-gal staining, absent until embryonic day 9.5-10.5 (E9.5-E10.5), was observed as early as E11.5-E12.5 in different primordia (i.e. central nervous system, sense organs, intestine, etc.) of the TRE2× transgenic embryos, while the foetal thyroid function (FTF) was still inactive. Immunohistochemistry for TRs essentially colocalized with β-gal staining. No β-gal staining was detected in embryos of hypothyroid transgenic mice. Importantly, treatment with T3 in hypothyroid TRE2× transgenic mice rescued β-gal expression. Our results provide in vivo direct evidence that during embryonic life and before the onset of FTF, maternal THs are transcriptionally active through the action of embryonic TRs. This model may have clinical relevance and may be employed to design end-point assays for new molecules affecting THs action.",

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author = "Carmelo Nucera and Patrizia Muzzi and Cecilia Tiveron and Antonella Farsetti and Regina, {Federico La} and Benedetta Foglio and Shou-Ching Shih and Fabiola Moretti and Pietra, {Linda Della} and Francesca Mancini and Ada Sacchi and Francesco Trimarchi and Alessandro Vercelli and Alfredo Pontecorvi",

year = "2010",

doi = "10.1111/j.1582-4934.2009.00947.x",

language = "English",

volume = "14",

pages = "2417--2435",

journal = "Journal of Cellular and Molecular Medicine",

issn = "1582-4934",

publisher = "Wiley-Blackwell Publishing Ltd",

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Nucera, C, Muzzi, P, Tiveron, C, Farsetti, A, Regina, FL, Foglio, B, Shih, S-C, Moretti, F, Pietra, LD, Mancini, F, Sacchi, A, Trimarchi, F, Vercelli, A & Pontecorvi, A 2010, 'Maternal thyroid hormones are transcriptionally active during embryo-foetal development: results from a novel transgenic mouse model', Journal of Cellular and Molecular Medicine, vol. 14, pagg. 2417-2435. https://doi.org/10.1111/j.1582-4934.2009.00947.x

TY - JOUR

T1 - Maternal thyroid hormones are transcriptionally active during embryo-foetal development: results from a novel transgenic mouse model

AU - Nucera, Carmelo

AU - Muzzi, Patrizia

AU - Tiveron, Cecilia

AU - Farsetti, Antonella

AU - Regina, Federico La

AU - Foglio, Benedetta

AU - Shih, Shou-Ching

AU - Moretti, Fabiola

AU - Pietra, Linda Della

AU - Mancini, Francesca

AU - Sacchi, Ada

AU - Trimarchi, Francesco

AU - Vercelli, Alessandro

AU - Pontecorvi, Alfredo

PY - 2010

Y1 - 2010

N2 - Even though several studies highlighted the role of maternal thyroid hormones (THs) during embryo-foetal development, direct evidence of their interaction with embryonic thyroid receptors (TRs) is still lacking. We generated a transgenic mouse model ubiquitously expressing a reporter gene tracing TH action during development. We engineered a construct (TRE2×) containing two TH-responsive elements controlling the expression of the LacZ reporter gene, which encodes β-galactosidase (β-gal). The specificity of the TRE2× activation by TH was evaluated in NIH3T3 cells by cotransfecting TRE2× along with TRs, retinoic or oestrogen receptors in the presence of their specific ligands. TRE2× transgene was microinjected into the zygotes, implanted in pseudopregnant BDF1 (a first-generation (F1) hybrid from a cross of C57BL/6 female and a DBA/2 male) mice and transgenic mouse models were developed. β-gal expression was assayed in tissue sections of transgenic mouse embryos at different stages of development. In vitro, TRE2× transactivation was observed only following physiological T3 stimulation, mediated exclusively by TRs. In vivo, β-gal staining, absent until embryonic day 9.5-10.5 (E9.5-E10.5), was observed as early as E11.5-E12.5 in different primordia (i.e. central nervous system, sense organs, intestine, etc.) of the TRE2× transgenic embryos, while the foetal thyroid function (FTF) was still inactive. Immunohistochemistry for TRs essentially colocalized with β-gal staining. No β-gal staining was detected in embryos of hypothyroid transgenic mice. Importantly, treatment with T3 in hypothyroid TRE2× transgenic mice rescued β-gal expression. Our results provide in vivo direct evidence that during embryonic life and before the onset of FTF, maternal THs are transcriptionally active through the action of embryonic TRs. This model may have clinical relevance and may be employed to design end-point assays for new molecules affecting THs action.

AB - Even though several studies highlighted the role of maternal thyroid hormones (THs) during embryo-foetal development, direct evidence of their interaction with embryonic thyroid receptors (TRs) is still lacking. We generated a transgenic mouse model ubiquitously expressing a reporter gene tracing TH action during development. We engineered a construct (TRE2×) containing two TH-responsive elements controlling the expression of the LacZ reporter gene, which encodes β-galactosidase (β-gal). The specificity of the TRE2× activation by TH was evaluated in NIH3T3 cells by cotransfecting TRE2× along with TRs, retinoic or oestrogen receptors in the presence of their specific ligands. TRE2× transgene was microinjected into the zygotes, implanted in pseudopregnant BDF1 (a first-generation (F1) hybrid from a cross of C57BL/6 female and a DBA/2 male) mice and transgenic mouse models were developed. β-gal expression was assayed in tissue sections of transgenic mouse embryos at different stages of development. In vitro, TRE2× transactivation was observed only following physiological T3 stimulation, mediated exclusively by TRs. In vivo, β-gal staining, absent until embryonic day 9.5-10.5 (E9.5-E10.5), was observed as early as E11.5-E12.5 in different primordia (i.e. central nervous system, sense organs, intestine, etc.) of the TRE2× transgenic embryos, while the foetal thyroid function (FTF) was still inactive. Immunohistochemistry for TRs essentially colocalized with β-gal staining. No β-gal staining was detected in embryos of hypothyroid transgenic mice. Importantly, treatment with T3 in hypothyroid TRE2× transgenic mice rescued β-gal expression. Our results provide in vivo direct evidence that during embryonic life and before the onset of FTF, maternal THs are transcriptionally active through the action of embryonic TRs. This model may have clinical relevance and may be employed to design end-point assays for new molecules affecting THs action.

KW - Animals

KW - Central Nervous System

KW - Embryonic Development

KW - Female

KW - Gene Expression Regulation, Developmental

KW - Gene Expression Regulation, Enzymologic

KW - Genes, Reporter

KW - Genetic Engineering

KW - Immunohistochemistry

KW - Lac Operon

KW - Male

KW - Mice

KW - Mice, Inbred C57BL

KW - Mice, Inbred DBA

KW - Mice, Transgenic

KW - Pregnancy

KW - Promoter Regions, Genetic

KW - Thyroid Hormones

KW - Transcriptional Activation

KW - Transgenes

KW - beta-Galactosidase

KW - Animals

KW - Central Nervous System

KW - Embryonic Development

KW - Female

KW - Gene Expression Regulation, Developmental

KW - Gene Expression Regulation, Enzymologic

KW - Genes, Reporter

KW - Genetic Engineering

KW - Immunohistochemistry

KW - Lac Operon

KW - Male

KW - Mice

KW - Mice, Inbred C57BL

KW - Mice, Inbred DBA

KW - Mice, Transgenic

KW - Pregnancy

KW - Promoter Regions, Genetic

KW - Thyroid Hormones

KW - Transcriptional Activation

KW - Transgenes

KW - beta-Galactosidase

UR - http://hdl.handle.net/10807/12571

U2 - 10.1111/j.1582-4934.2009.00947.x

DO - 10.1111/j.1582-4934.2009.00947.x

M3 - Article

SN - 1582-4934

VL - 14

SP - 2417

EP - 2435

JO - Journal of Cellular and Molecular Medicine

JF - Journal of Cellular and Molecular Medicine

ER -

Maternal thyroid hormones are transcriptionally active during embryo-foetal development: results from a novel transgenic mouse model

Abstract

Keywords

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