Publications by authors named "Tania Cristina Ramirez-Fuentes"

Learning alterations in the child population may be linked to gestational diabetes as a causal factor, though this remains an open and highly controversial question. In that sense, it has been reported that maternal hyperglycemia generates a threatening condition that affects hippocampal development in offspring. The pyramidal cells of the CA3 subfield, a key structure in learning and memory processes, are particularly important in cognitive deficiencies.

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Article Synopsis
  • The chorioallantoic membrane (CAM) serves as an efficient research tool for studying tumors, enabling the examination of key processes like migration, invasion, and angiogenesis, as well as evaluating new antitumor drugs.
  • The CAM allows for rapid and cost-effective tumor establishment through xenotransplantation, adhering to the three "R" principles of replacement, reduction, and refinement in research practices.
  • Preclinical models like the CAM are crucial for understanding complex diseases such as neuroblastoma, aiding in the exploration of tumor biology and improving therapeutic strategies for treatment.
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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.

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Despite the extensive information available on the different genetic, epigenetic, and molecular features of cardiogenesis, the origin of congenital heart defects remains unknown. Most genetic and molecular studies have been conducted outside the context of the progressive anatomical and histological changes in the embryonic heart, which is one of the reasons for the limited knowledge of the origins of congenital heart diseases. We integrated the findings of descriptive studies on human embryos and experimental studies on chick, rat, and mouse embryos.

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