Neonatal Oxidative Stress Impairs Cortical Synapse Formation and GABA Homeostasis in Parvalbumin-Expressing Interneurons

Scheuer, Till; Endesfelder, Stefanie; Brinke, Elena auf dem; Bührer, Christoph; Schmitz, Thomas

doi:10.1155/2022/8469756

Cited by 14 publications

(7 citation statements)

References 80 publications

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“…Oxidative stress, especially during the most sensitive and early stages of brain development, has an adverse impact on brain neurodevelopment [50] and is proposed as a common factor in neurodevelopmental disorders such as schizophrenia and autism [51]. Our study found an increase in DCFH and protein carbonylation, indicating oxidative stress in DI patients, without changes in antioxidant defenses.…”

Section: Discussionmentioning

confidence: 45%

Serum Biomarkers to Mild Cognitive Deficits in Children and Adolescents

Tuon,

Tramontin,

Custódio

et al. 2023

Mol Neurobiol

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Introduction: Intellectual Disability (ID) is a condition characterized by signi cant limitations in both cognitive development and adaptive behavior. The diagnosis is made through clinical assessment, standardized tests, and intelligence quotient (IQ). Genetic, in ammation, oxidative stress, and diet, have been suggested to contribute to ID, and biomarkers could potentially aid in diagnosis and treatment.Methods: Study included children and adolescents aged 6-16 years. The ID group (n=16), and the control group (n=18) underwent the Wechsler Intelligence Scale for Children (WISC-IV) test, and blood samples were collected. Correlations between biomarker levels and WISC-IV test scores were analyzed.Results: The ID group had an IQ score below 75, and the values of four domains (IQ, IOP, IMO, and IVP) were lower compared to the control group. Serum levels of FKN, NGF-β, and Vitamin B12 were decreased in the ID group, while DCFH and nitrite levels were increased. Positive correlations were found between FKN and the QIT and IOP domains, NGF and the QIT and IMO domains, and Vitamin B12 and the ICV domain. TNF-α showed a negative correlation with the ICV domain.Discussion: Our study identi ed FKN, NGF-β, and Vitamin B12 as potential biomarkers speci c to ID, which could aid in the diagnosis and treatment of ID. TNF-α and oxidative stress biomarkers suggest that ID has a complex etiology, and further research is needed to better understand this condition and develop effective treatments. Future studies could explore the potential implications of these biomarkers and develop targeted interventions based on their ndings.

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Section: Discussionmentioning

confidence: 45%

Serum Biomarkers to Mild Cognitive Deficits in Children and Adolescents

Tuon,

Tramontin,

Custódio

et al. 2023

Mol Neurobiol

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“…Preterm birth may cause brain injury because newborns are prone to environmental stress, producing an excess of ROS, primarily due to the exposure to high‐oxygen condition compared to fetal life, with a marked increase of arterial oxygen tension. Thus, the preterm brain is exposed to hyperoxia, which induces oxidative stress and impairs neuronal cell development 36 . In particular, lipid peroxidation with reactive ROS leads to MDA production that can be used as a marker of the endogenous peroxidation of polyunsaturated fatty acids 8,9 .…”

Section: Discussionmentioning

confidence: 99%

“…Thus, the preterm brain is exposed to hyperoxia, which induces oxidative stress and impairs neuronal cell development. 36 In particular, lipid peroxidation with reactive ROS leads to MDA production that can be used as a marker of the endogenous peroxidation of polyunsaturated fatty acids. 8,9 It is also known that the preterm newborn's immature enzymatic oxidative stress defense system is incompetent to neutralize the increased formation of reactive ROS.…”

Section: Sepsis Amentioning

confidence: 99%

Fate of melatonin orally administered in preterm newborns: Antioxidant performance and basis for neuroprotection

Garofoli,

Franco,

Accorsi

et al. 2023

Journal of Pineal Research

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Preterm infants cannot counteract excessive reactive oxygen species (ROS) production due to preterm birth, leading to an excess of lipid peroxidation with malondialdehyde (MDA) production, capable of contributing to brain damage. Melatonin (ME), an endogenous brain hormone, and its metabolites, act as a free radical scavenger against ROS. Unfortunately, preterms have an impaired antioxidant system, resulting in the inability to produce and release ME. This prospective, multicenter, parallel groups, randomized, double‐blind, placebo‐controlled trial aimed to assess: (i) the endogenous production of ME in very preterm infants (gestational age ≤ 29 + 6 WE, 28 infants in the ME and 26 in the placebo group); (ii) the exogenous hormone availability and its metabolization to the main metabolite, 6‐OH‐ME after 15 days of ME oral treatment; (iii) difference of MDA plasma concentration, as peroxidation marker, after treatment. Blood was collected before the first administration (T1) and after 15 days of administration (T2). ME and 6‐OH‐ME were detected by liquid chromatography tandem mass spectrometry, MDA was measured by liquid chromatograph with fluorescence detection. ME and 6‐OH‐ME were not detectable in the placebo group at any study time‐point. ME was absent in the active group at T1. In contrast, after oral administration, ME and 6‐OH‐ME resulted highly detectable and the difference between concentrations T2 versus T1 was statistically significant, as well as the difference between treated and placebo groups at T2. MDA levels seemed stable during the 15 days of treatment in both groups. Nevertheless, a trend in the percentage of neonates with reduced MDA concentration at T2/T1 was 48.1% in the ME group versus 38.5% in the placebo group. We demonstrated that very preterm infants are not able to produce endogenous detectable plasma levels of ME during their first days of life. Still, following ME oral administration, appreciable amounts of ME and 6‐OH‐ME were available. The trend of MDA reduction in the active group requires further clinical trials to fix the dosage, the length of ME therapy and to identify more appropriate indexes to demonstrate, at biological and clinical levels, the antioxidant activity and consequent neuroprotectant potential of ME in very preterm newborns.

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“…The pathogenesis of AD is still not elucidated clearly but oxidative stress is one of the key hypotheses. Related studies showed that oxidative stress is a driving force for synapse dysfunction [ [56] , [57] , [58] ]. Withaferin A is a natural drug with neuroprotective effects, such as anti-inflammatory and antioxidation effects.…”

Section: Discussionmentioning

confidence: 99%