Embryonic Hyperglycemia Disrupts Myocardial Growth, Morphological Development, and Cellular Organization: An In Vivo Experimental Study

Ricardo Jaime-Cruz; Concepción Sánchez-Gómez; Laura Villavicencio-Guzmán; Roberto Lazzarini-Lechuga; Carlos César Patiño-Morales; Mario García-Lorenzana; Tania Cristina Ramírez-Fuentes; Marcela Salazar-García

doi:10.3390/life13030768

Embryonic Hyperglycemia Disrupts Myocardial Growth, Morphological Development, and Cellular Organization: An In Vivo Experimental Study

Life (Basel). 2023 Mar 13;13(3):768. doi: 10.3390/life13030768.

Affiliations

¹ Posgrado en Biología Experimental, Departamento de Ciencias de la Salud, Universidad Autónoma Metropolitana-Iztapalapa, Mexico City 09340, Mexico.
² Research Laboratory of Developmental Biology and Experimental Teratogenesis, Children's Hospital of México Federico Gomez, Mexico City 06720, Mexico.
³ Departamento de Ciencias de la Salud, Universidad Tecnológica de México-UNITEC México-Campus Sur, Mexico City 09810, Mexico.
⁴ Departamento de Biología de la Reproducción, División de Ciencias Biológicas y de la Salud, Universidad Autónoma Metropolitana-Iztapalapa, Mexico City 09340, Mexico.
⁵ Laboratorio de Biología Celular, Universidad Autónoma Metropolitana-Cuajimalpa, Mexico City 05348, Mexico.
⁶ Sección de Estudios de Posgrado e Investigación de Escuela Superior de Medicina, Instituto Politécnico Nacional, Mexico City 11340, Mexico.
⁷ Facultad de Medicina, Universidad Nacional Autónoma de México, Mexico City 04360, Mexico.

Abstract

Hyperglycemia during gestation can disrupt fetal heart development and increase postnatal cardiovascular disease risk. It is therefore imperative to identify early biomarkers of hyperglycemia during gestation-induced fetal heart damage and elucidate the underlying molecular pathomechanisms. Clinical investigations of diabetic adults with heart dysfunction and transgenic mouse studies have revealed that overexpression or increased expression of TNNI3K, a heart-specific kinase that binds troponin cardiac I, may contribute to abnormal cardiac remodeling, ventricular hypertrophy, and heart failure. Optimal heart function also depends on the precise organization of contractile and excitable tissues conferred by intercellular occlusive, adherent, and communicating junctions. The current study evaluated changes in embryonic heart development and the expression levels of sarcomeric proteins (troponin I, desmin, and TNNI3K), junctional proteins, glucose transporter-1, and Ki-67 under fetal hyperglycemia. Stage 22HH Gallus domesticus embryos were randomly divided into two groups: a hyperglycemia (HG) group, in which individual embryos were injected with 30 mmol/L glucose solution every 24 h for 10 days, and a no-treatment (NT) control group, in which individual embryos were injected with physiological saline every 24 h for 10 days (stage 36HH). Embryonic blood glucose, height, and weight, as well as heart size, were measured periodically during treatment, followed by histopathological analysis and estimation of sarcomeric and junctional protein expression by western blotting and immunostaining. Hyperglycemic embryos demonstrated delayed heart maturation, with histopathological analysis revealing reduced left and right ventricular wall thickness (-39% and -35% vs. NT). Immunoexpression levels of TNNI3K and troponin 1 increased (by 37% and 39%, respectively), and desmin immunofluorescence reduced (by 23%). Embryo-fetal hyperglycemia may trigger an increase in the expression levels of TNNI3K and troponin I, as well as dysfunction of occlusive and adherent junctions, ultimately inducing abnormal cardiac remodeling.

Keywords: cardiomyopathies; heart development; hyperglycemia; myocardial growth.

Embryonic Hyperglycemia Disrupts Myocardial Growth, Morphological Development, and Cellular Organization: An In Vivo Experimental Study

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Abstract

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