Cardiac and placental mitochondrial characterization in a rabbit model of intrauterine growth restriction

M. Guitart-Mampel; A. Gonzalez-Tendero; S. Niñerola; C. Morén; M. Catalán-Garcia; I. González-Casacuberta; D. L. Juárez-Flores; O. Ugarteburu; L. Matalonga; M. V. Cascajo; F. Tort; A. Cortés; E. Tobias; J. C. Milisenda; J. M. Grau; F. Crispi; E. Gratacós; G. Garrabou; F. Cardellach

doi:10.1016/j.bbagen.2018.02.006

Cardiac and placental mitochondrial characterization in a rabbit model of intrauterine growth restriction

M. Guitart-Mampel
, A. Gonzalez-Tendero
, S. Niñerola
, C. Morén
, M. Catalán-Garcia
, I. González-Casacuberta
, D. L. Juárez-Flores
, O. Ugarteburu
, L. Matalonga
, M. V. Cascajo
, F. Tort
, A. Cortés
, E. Tobias
, J. C. Milisenda
, J. M. Grau
, F. Crispi
, E. Gratacós
, G. Garrabou^*
, F. Cardellach

^*Autor correspondiente de este trabajo

Universidad Pablo de Olavide

Producción científica: Contribución a una revista › Artículo › revisión exhaustiva

16 Citas (Scopus)

Resumen

Background: Intrauterine growth restriction (IUGR) is associated with cardiovascular remodeling persisting into adulthood. Mitochondrial bioenergetics, essential for embryonic development and cardiovascular function, are regulated by nuclear effectors as sirtuins. A rabbit model of IUGR and cardiovascular remodeling was generated, in which heart mitochondrial alterations were observed by microscopic and transcriptomic analysis. We aimed to evaluate if such alterations are translated at a functional mitochondrial level to establish the etiopathology and potential therapeutic targets for this obstetric complication. Methods: Hearts and placentas from 16 IUGR-offspring and 14 controls were included to characterize mitochondrial function. Results: Enzymatic activities of complexes II, IV and II + III in IUGR-hearts (−11.96 ± 3.16%; −15.58 ± 5.32%; −14.73 ± 4.37%; p < 0.05) and II and II + III in IUGR-placentas (−17.22 ± 3.46%; p < 0.005 and −29.64 ± 4.43%; p < 0.001) significantly decreased. This was accompanied by a not significant reduction in CI-stimulated oxygen consumption and significantly decreased complex II SDHB subunit expression in placenta (−44.12 ± 5.88%; p < 0.001). Levels of mitochondrial content, Coenzyme Q and cellular ATP were conserved. Lipid peroxidation significantly decreased in IUGR-hearts (−39.02 ± 4.35%; p < 0.001), but not significantly increased in IUGR-placentas. Sirtuin3 protein expression significantly increased in IUGR-hearts (84.21 ± 31.58%; p < 0.05) despite conserved anti-oxidant SOD2 protein expression and activity in both tissues. Conclusions: IUGR is associated with cardiac and placental mitochondrial CII dysfunction. Up-regulated expression of Sirtuin3 may explain attenuation of cardiac oxidative damage and preserved ATP levels under CII deficiency. General significance: These findings may allow the design of dietary interventions to modulate Sirtuin3 expression and consequent regulation of mitochondrial imbalance associated with IUGR and derived cardiovascular remodeling.

Idioma original	Inglés
Páginas (desde-hasta)	1157-1167
Número de páginas	11
Publicación	Biochimica et Biophysica Acta - General Subjects
Volumen	1862
N.º	5
DOI	https://doi.org/10.1016/j.bbagen.2018.02.006
Estado	Publicada - may 2018
Publicado de forma externa	Sí

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ODS 3: Salud y bienestar

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10.1016/j.bbagen.2018.02.006

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Guitart-Mampel, M., Gonzalez-Tendero, A., Niñerola, S., Morén, C., Catalán-Garcia, M., González-Casacuberta, I., Juárez-Flores, D. L., Ugarteburu, O., Matalonga, L., Cascajo, M. V., Tort, F., Cortés, A., Tobias, E., Milisenda, J. C., Grau, J. M., Crispi, F., Gratacós, E., Garrabou, G., & Cardellach, F. (2018). Cardiac and placental mitochondrial characterization in a rabbit model of intrauterine growth restriction. Biochimica et Biophysica Acta - General Subjects, 1862(5), 1157-1167. https://doi.org/10.1016/j.bbagen.2018.02.006

@article{899e242772ba41b5930dcebac1865c9c,

title = "Cardiac and placental mitochondrial characterization in a rabbit model of intrauterine growth restriction",

abstract = "Background: Intrauterine growth restriction (IUGR) is associated with cardiovascular remodeling persisting into adulthood. Mitochondrial bioenergetics, essential for embryonic development and cardiovascular function, are regulated by nuclear effectors as sirtuins. A rabbit model of IUGR and cardiovascular remodeling was generated, in which heart mitochondrial alterations were observed by microscopic and transcriptomic analysis. We aimed to evaluate if such alterations are translated at a functional mitochondrial level to establish the etiopathology and potential therapeutic targets for this obstetric complication. Methods: Hearts and placentas from 16 IUGR-offspring and 14 controls were included to characterize mitochondrial function. Results: Enzymatic activities of complexes II, IV and II + III in IUGR-hearts (−11.96 ± 3.16\%; −15.58 ± 5.32\%; −14.73 ± 4.37\%; p < 0.05) and II and II + III in IUGR-placentas (−17.22 ± 3.46\%; p < 0.005 and −29.64 ± 4.43\%; p < 0.001) significantly decreased. This was accompanied by a not significant reduction in CI-stimulated oxygen consumption and significantly decreased complex II SDHB subunit expression in placenta (−44.12 ± 5.88\%; p < 0.001). Levels of mitochondrial content, Coenzyme Q and cellular ATP were conserved. Lipid peroxidation significantly decreased in IUGR-hearts (−39.02 ± 4.35\%; p < 0.001), but not significantly increased in IUGR-placentas. Sirtuin3 protein expression significantly increased in IUGR-hearts (84.21 ± 31.58\%; p < 0.05) despite conserved anti-oxidant SOD2 protein expression and activity in both tissues. Conclusions: IUGR is associated with cardiac and placental mitochondrial CII dysfunction. Up-regulated expression of Sirtuin3 may explain attenuation of cardiac oxidative damage and preserved ATP levels under CII deficiency. General significance: These findings may allow the design of dietary interventions to modulate Sirtuin3 expression and consequent regulation of mitochondrial imbalance associated with IUGR and derived cardiovascular remodeling.",

keywords = "Cardiovascular function, Fetal growth, Mitochondrial complex II, Mitochondrial dysfunction, Rabbit animal model, Sirtuin3",

author = "M. Guitart-Mampel and A. Gonzalez-Tendero and S. Ni{\~n}erola and C. Mor{\'e}n and M. Catal{\'a}n-Garcia and I. Gonz{\'a}lez-Casacuberta and Ju{\'a}rez-Flores, \{D. L.\} and O. Ugarteburu and L. Matalonga and Cascajo, \{M. V.\} and F. Tort and A. Cort{\'e}s and E. Tobias and Milisenda, \{J. C.\} and Grau, \{J. M.\} and F. Crispi and E. Gratac{\'o}s and G. Garrabou and F. Cardellach",

note = "Publisher Copyright: {\textcopyright} 2018 Elsevier B.V.",

year = "2018",

month = may,

doi = "10.1016/j.bbagen.2018.02.006",

language = "English",

volume = "1862",

pages = "1157--1167",

journal = "Biochimica et Biophysica Acta - General Subjects",

issn = "0304-4165",

publisher = "Elsevier",

number = "5",

}

Guitart-Mampel, M, Gonzalez-Tendero, A, Niñerola, S, Morén, C, Catalán-Garcia, M, González-Casacuberta, I, Juárez-Flores, DL, Ugarteburu, O, Matalonga, L, Cascajo, MV, Tort, F, Cortés, A, Tobias, E, Milisenda, JC, Grau, JM, Crispi, F, Gratacós, E, Garrabou, G & Cardellach, F 2018, 'Cardiac and placental mitochondrial characterization in a rabbit model of intrauterine growth restriction', Biochimica et Biophysica Acta - General Subjects, vol. 1862, n.º 5, pp. 1157-1167. https://doi.org/10.1016/j.bbagen.2018.02.006

TY - JOUR

T1 - Cardiac and placental mitochondrial characterization in a rabbit model of intrauterine growth restriction

AU - Guitart-Mampel, M.

AU - Gonzalez-Tendero, A.

AU - Niñerola, S.

AU - Morén, C.

AU - Catalán-Garcia, M.

AU - González-Casacuberta, I.

AU - Juárez-Flores, D. L.

AU - Ugarteburu, O.

AU - Matalonga, L.

AU - Cascajo, M. V.

AU - Tort, F.

AU - Cortés, A.

AU - Tobias, E.

AU - Milisenda, J. C.

AU - Grau, J. M.

AU - Crispi, F.

AU - Gratacós, E.

AU - Garrabou, G.

AU - Cardellach, F.

PY - 2018/5

Y1 - 2018/5

N2 - Background: Intrauterine growth restriction (IUGR) is associated with cardiovascular remodeling persisting into adulthood. Mitochondrial bioenergetics, essential for embryonic development and cardiovascular function, are regulated by nuclear effectors as sirtuins. A rabbit model of IUGR and cardiovascular remodeling was generated, in which heart mitochondrial alterations were observed by microscopic and transcriptomic analysis. We aimed to evaluate if such alterations are translated at a functional mitochondrial level to establish the etiopathology and potential therapeutic targets for this obstetric complication. Methods: Hearts and placentas from 16 IUGR-offspring and 14 controls were included to characterize mitochondrial function. Results: Enzymatic activities of complexes II, IV and II + III in IUGR-hearts (−11.96 ± 3.16%; −15.58 ± 5.32%; −14.73 ± 4.37%; p < 0.05) and II and II + III in IUGR-placentas (−17.22 ± 3.46%; p < 0.005 and −29.64 ± 4.43%; p < 0.001) significantly decreased. This was accompanied by a not significant reduction in CI-stimulated oxygen consumption and significantly decreased complex II SDHB subunit expression in placenta (−44.12 ± 5.88%; p < 0.001). Levels of mitochondrial content, Coenzyme Q and cellular ATP were conserved. Lipid peroxidation significantly decreased in IUGR-hearts (−39.02 ± 4.35%; p < 0.001), but not significantly increased in IUGR-placentas. Sirtuin3 protein expression significantly increased in IUGR-hearts (84.21 ± 31.58%; p < 0.05) despite conserved anti-oxidant SOD2 protein expression and activity in both tissues. Conclusions: IUGR is associated with cardiac and placental mitochondrial CII dysfunction. Up-regulated expression of Sirtuin3 may explain attenuation of cardiac oxidative damage and preserved ATP levels under CII deficiency. General significance: These findings may allow the design of dietary interventions to modulate Sirtuin3 expression and consequent regulation of mitochondrial imbalance associated with IUGR and derived cardiovascular remodeling.

AB - Background: Intrauterine growth restriction (IUGR) is associated with cardiovascular remodeling persisting into adulthood. Mitochondrial bioenergetics, essential for embryonic development and cardiovascular function, are regulated by nuclear effectors as sirtuins. A rabbit model of IUGR and cardiovascular remodeling was generated, in which heart mitochondrial alterations were observed by microscopic and transcriptomic analysis. We aimed to evaluate if such alterations are translated at a functional mitochondrial level to establish the etiopathology and potential therapeutic targets for this obstetric complication. Methods: Hearts and placentas from 16 IUGR-offspring and 14 controls were included to characterize mitochondrial function. Results: Enzymatic activities of complexes II, IV and II + III in IUGR-hearts (−11.96 ± 3.16%; −15.58 ± 5.32%; −14.73 ± 4.37%; p < 0.05) and II and II + III in IUGR-placentas (−17.22 ± 3.46%; p < 0.005 and −29.64 ± 4.43%; p < 0.001) significantly decreased. This was accompanied by a not significant reduction in CI-stimulated oxygen consumption and significantly decreased complex II SDHB subunit expression in placenta (−44.12 ± 5.88%; p < 0.001). Levels of mitochondrial content, Coenzyme Q and cellular ATP were conserved. Lipid peroxidation significantly decreased in IUGR-hearts (−39.02 ± 4.35%; p < 0.001), but not significantly increased in IUGR-placentas. Sirtuin3 protein expression significantly increased in IUGR-hearts (84.21 ± 31.58%; p < 0.05) despite conserved anti-oxidant SOD2 protein expression and activity in both tissues. Conclusions: IUGR is associated with cardiac and placental mitochondrial CII dysfunction. Up-regulated expression of Sirtuin3 may explain attenuation of cardiac oxidative damage and preserved ATP levels under CII deficiency. General significance: These findings may allow the design of dietary interventions to modulate Sirtuin3 expression and consequent regulation of mitochondrial imbalance associated with IUGR and derived cardiovascular remodeling.

KW - Cardiovascular function

KW - Fetal growth

KW - Mitochondrial complex II

KW - Mitochondrial dysfunction

KW - Rabbit animal model

KW - Sirtuin3

UR - https://www.scopus.com/pages/publications/85042286936

U2 - 10.1016/j.bbagen.2018.02.006

DO - 10.1016/j.bbagen.2018.02.006

M3 - Article

C2 - 29452236

AN - SCOPUS:85042286936

SN - 0304-4165

VL - 1862

SP - 1157

EP - 1167

JO - Biochimica et Biophysica Acta - General Subjects

JF - Biochimica et Biophysica Acta - General Subjects

IS - 5

ER -

Cardiac and placental mitochondrial characterization in a rabbit model of intrauterine growth restriction

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