Prenatal caffeine intake differently affects synaptic proteins during fetal brain development

Mioranzza, Sabrina; Nunes, Fernanda Costa; Marques, Daniela Melo; Fioreze, Gabriela T.; Rocha, Andréia Silva da; Botton, Paulo Henrique S.; Costa, Marcelo Silveira da; Porciúncula, Lisiane O.

doi:10.1016/j.ijdevneu.2014.04.006

Cited by 30 publications

(25 citation statements)

References 69 publications

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“…Well before birth, hippocampal and cortical neurons in the brain express BDNF and TrkB (Behar et al, 1997; Mioranzza et al, 2014). Exogenous BDNF increases the number of primary dendrites in an activity dependent manner through TrkB in specific cortical layers (McAllister et al, 1997; McAllister et al, 1995).…”

Section: Resultsmentioning

confidence: 99%

Kalirin is required for BDNF-TrkB stimulated neurite outgrowth and branching

2016

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Exogenous brain-derived neurotrophic factor (BDNF), acting through TrkB, is known to promote neurite formation and branching. This response to BDNF was eliminated by inhibition of TrkB kinase and by specific inhibition of the GEF1 domain of Kalirin, which activates Rac1. Neurons from Kalrn knockout mice were unable to activate Rac1 in response to BDNF. BDNF-triggered neurite outgrowth was abolished when Kalrn expression was reduced using shRNA that targets all of the major Kalrn isoforms, and reduced in neurons from Kalrn knockout mice. The Kalrn isoforms expressed early in development also include a GEF2 domain that activates RhoA. However, BDNF-stimulated neurite outgrowth in Kalrn knockout neurons was rescued by expression of Kalirin-7, which includes only the GEF1 domain but lacks the GEF2 domain. Dendritic morphogenesis, which requires spatially restricted, coordinated changes in the actin cytoskeleton and in the organization of microtubules, involves essential contributions from multiple Rho GEFs. Since Tiam1, another Rho GEF, is also required for BDNF-stimulated neurite outgrowth, an inhibitory fragment of Tiam1 (PHn-CC-EX) was tested and found to interfere with both Kalirin and Tiam1 GEF activity. The prolonged TrkB activation observed in response to BDNF in Kalrn knockout neurons and the altered time course and extent of ERK, CREB and Akt activation observed in the absence of Kalrn would be expected to alter the response of these neurons to other regulatory factors.

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Section: Resultsmentioning

confidence: 99%

Kalirin is required for BDNF-TrkB stimulated neurite outgrowth and branching

2016

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“…Notably, exposure of immature brain cells to CAF or SADs reduces mRNA and protein levels of BDNF [6,24–26], and altered BDNF expression by CAF or SADs has been implicated in neuroapoptosis [27] and long-term neurodevelopmental impairment [25,28]. In addition, CAF [29] and SADs [27,28] have been shown to downregulate activity of the pro-survival Akt pathway.…”

Section: Discussionmentioning

confidence: 99%

Caffeine combined with sedative/anesthetic drugs triggers widespread neuroapoptosis in a mouse model of prematurity

Cabrera

O’Connor

Swiney

et al. 2016

The Journal of Maternal-Fetal & Neonatal Medicine

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Objectives Caffeine (CAF) and sedative/anesthetic drugs (SADs) are often coadministered to premature infants in the neonatal intensive care unit (NICU). While SAD neurotoxicity in the developing brain is well established, it is not fully clear whether CAF interacts with SADs and whether this interaction is detrimental. Using a mouse model of prematurity, we hypothesized that CAF would increase apoptotic neurotoxicity when coadministered with SADs. Methods Postnatal day 3 mice were treated with vehicle or 80 mg/kg CAF prior to challenge with 6 mg/kg midazolam, 40 mg/kg ketamine, or 40 μg/kg fentanyl. Six hours later, pups were sacrificed for activated caspase 3 (AC3) immunohistochemistry, and number of AC3 positive cells per mm3 throughout neocortex, hippocampus, caudate, thalamus, and colliculi was analyzed. Results CAF caused a statistically significant increase in AC3 positive cells when coadministered with midazolam (p = 0.002), ketamine (p = 0.014), or fentanyl (p <0.001). Our composite dataset suggests that the addition of CAF to these SADs has a supra-additive effect, causing more neurotoxicity than expected. Conclusions CAF may augment the neurotoxic action of SADs indicated for neonatal sedation/anesthesia in the NICU by triggering widespread apoptosis in the developing brains of premature infants.

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“…Importantly also, caffeine actions do not result solely from A 2A R antagonism since caffeine is an antagonist of different adenosine receptor subtypes. However, several studies have indeed shown that gestational exposure to caffeine may alter the normal development of the brain with cognitive consequences to the adult brain (Juárez-Méndez et al 2006;Soellner et al 2009;Silva et al 2013;Mioranzza et al 2014), by delaying migration and insertion of GABAergic neurons into the hippocampal circuitry (Silva et al 2013), by decreasing either BDNF or TrkB receptor levels (Mioranzza et al 2014), by affecting the different adenosine receptors expression during neural Fig. 11 Adenosine A 2A Rs activation increases microtubule dynamics.…”

Section: Adenosine a 2a Receptor Activation Increases Microtubule Dynmentioning

confidence: 99%

Axonal elongation and dendritic branching is enhanced by adenosine A2A receptors activation in cerebral cortical neurons

et al. 2015

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Axon growth and dendrite development are key processes for the establishment of a functional neuronal network. Adenosine, which is released by neurons and glia, is a known modulator of synaptic transmission but its influence over neuronal growth has been much less investigated. We now explored the action of adenosine A2A receptors (A2AR) upon neurite outgrowth, discriminating actions over the axon or dendrites, and the mechanisms involved. Morphometric analysis of primary cultures of cortical neurons from E18 Sprague-Dawley rats demonstrated that an A2AR agonist, CGS 21680, enhances axonal elongation and dendritic branching, being the former prevented by inhibitors of phosphoinositide 3-kinase, mitogen-activated protein kinase and phospholipase C, but not of protein kinase A. By testing the influence of a scavenger of BDNF (brain-derived neurotrophic factor) over the action of the A2AR agonist and the action of a selective A2AR antagonist over the action of BDNF, we could conclude that while the action of A2ARs upon dendritic branching is dependent on the presence of endogenous BDNF, the influence of A2ARs upon axonal elongation is independent of endogenous BDNF. In consonance with the action over axonal elongation, A2AR activation promoted a decrease in microtubule stability and an increase in microtubule growth speed in axonal growth cones. In conclusion, we disclose a facilitatory action of A2ARs upon axonal elongation and microtubule dynamics, providing new insights for A2ARs regulation of neuronal differentiation and axonal regeneration.

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Prenatal caffeine intake differently affects synaptic proteins during fetal brain development

Cited by 30 publications

References 69 publications

Kalirin is required for BDNF-TrkB stimulated neurite outgrowth and branching

Kalirin is required for BDNF-TrkB stimulated neurite outgrowth and branching

Caffeine combined with sedative/anesthetic drugs triggers widespread neuroapoptosis in a mouse model of prematurity

Axonal elongation and dendritic branching is enhanced by adenosine A2A receptors activation in cerebral cortical neurons

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