Ethanol (E) Impairs Fetal Brain GSH Homeostasis by Inhibiting Excitatory Amino-Acid Carrier 1 (EAAC1)-Mediated Cysteine Transport

Patel, Dhyanesh A.; Mahimainathan, Lenin; Narasimhan, Madhusudhanan; Rathinam, Marylatha; Henderson, George I.

doi:10.3390/ijms18122596

Cited by 4 publications

(7 citation statements)

References 82 publications

(127 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…In a setting of reduced Cys availability as shown by us earlier [ 26 ] with increased accumulation of cystathionine levels (in the current study), we next determined whether this might be caused by an altered expression of CSE, a rate-limiting enzyme that metabolizes cystathionine to Cys. Immunoblotting experiments for CSE revealed that CSE protein was reduced with the treatment of E in fetal PCNs by 36%, 53% ( p < 0.05), and 64% ( p < 0.05) at 6, 12, and 24 h, respectively.…”

Section: Resultsmentioning

confidence: 71%

“…Consistent with this concept, we observed that alcohol caused a significant accumulation of cystathionine levels in the PCNs that was also replicated in the 2nd trimester equivalent in utero binge alcohol model and the 3rd trimester equivalent postnatal day (PN7) ethanol model as indicated by HPLC analysis. The resultant downstream impact of cystathionine accumulation on Cys and GSH levels were recently demonstrated by us [ 26 ]. Notably, previous reports in humans have shown that mutations of Cse gene causes an accumulation of cystathionine in liver, kidney, brain, and cerebrospinal fluid, leading to cystathionuria and decreased plasma cysteine concentration.…”

Section: Discussionmentioning

confidence: 93%

“…Earlier we have shown that E exposure decreases Cys and GSH content in both PCNs and binge alcohol model [ 26 ]. To gain a better understanding of the E-induced GSH loss and the role of transulfuration pathway (TSP), we first assessed the levels of cystathionine, an intermediate of TSP and an immediate precursor of Cys.…”

Section: Resultsmentioning

confidence: 99%

“…Further, alcohol treatment decreased the expression of CSE protein in fetal brain cortices of binge alcohol exposed prenatal animals and PCNs exposed to alcohol without a change in the CBS expression, which supplies the CSE with cystathionine with serine and homocysteine condensation. A decreased CSE expression in the TSP could explain previously observed reductions of Cys and subsequent GSH synthesis with E exposure [ 26 ]. Consistent with this concept, we observed that alcohol caused a significant accumulation of cystathionine levels in the PCNs that was also replicated in the 2nd trimester equivalent in utero binge alcohol model and the 3rd trimester equivalent postnatal day (PN7) ethanol model as indicated by HPLC analysis.…”

Section: Discussionmentioning

confidence: 98%

See 3 more Smart Citations

Role for Cystathionine γ Lyase (CSE) in an Ethanol (E)-Induced Lesion in Fetal Brain GSH Homeostasis

Patel

Rathinam

Jarvis

et al. 2018

IJMS

Self Cite

View full text Add to dashboard Cite

Earlier, we reported that gestational ethanol (E) can dysregulate neuron glutathione (GSH) homeostasis partially via impairing the EAAC1-mediated inward transport of Cysteine (Cys) and this can affect fetal brain development. In this study, we investigated if there is a role for the transulfuration pathway (TSP), a critical bio-synthetic point to supply Cys in E-induced dysregulation of GSH homeostasis. These studies utilized an in utero E binge model where the pregnant Sprague–Dawley (SD) rat dams received five doses of E at 3.5 g/kg by gastric intubation beginning embryonic day (ED) 17 until ED19 separated by 12 h. The postnatal day 7 (PN7) alcohol model employed an oral dosing of 4 g/kg body weight split into 2 feedings at 2 h interval and an iso-caloric and iso-volumic equivalent maltose-dextrin milk solution served as controls. The in vitro model consisted of cerebral cortical neuron cultures from embryonic day (ED) 16–17 fetus from SD rats and differentiated neurons from ED18 rat cerebral cortical neuroblasts. E concentrations were 4 mg/mL. E induced an accumulation of cystathionine in primary cortical neurons (PCNs), 2nd trimester equivalent in utero binge, and 3rd trimester equivalent PN7 model suggesting that breakdown of cystathionine, a required process for Cys supply is impaired. This was associated with a significant reduction in cystathionine γ-lyase (CSE) protein expression in PCN (p < 0.05) and in fetal cerebral cortex in utero (53%, p < 0.05) without a change in the expression of cystathionine β-synthase (CBS). Concomitantly, E decreased Cse mRNA expression in PCNs (by 32% within 6 h of exposure, p < 0.05) and in fetal brain (33%, p < 0.05). In parallel, knock down of CSE in differentiated rat cortical neuroblasts exaggerated the E-induced ROS, GSH loss with a pronounced caspase-3 activation and cell death. These studies illustrate the importance of TSP in CSE-related maintenance of GSH and the downstream events via Cys synthesis in neurons and fetal brain.

show abstract

Section: Resultsmentioning

confidence: 71%

Section: Discussionmentioning

confidence: 93%

Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 98%

See 2 more Smart Citations

Role for Cystathionine γ Lyase (CSE) in an Ethanol (E)-Induced Lesion in Fetal Brain GSH Homeostasis

Patel

Rathinam

Jarvis

et al. 2018

IJMS

Self Cite

View full text Add to dashboard Cite

show abstract

“…Furthermore, experiments using ethanol in neurons, which impairs the expression of EAAC1 by 60-70%, revealed that the level of GSH and cysteine was reduced by up to 50% in primary cerebral cortical neurons. This effect was reversed by administration of NAC [22]. To increase the synthesis of GSH, EAAC1 is translocated to the plasma membrane and transports cysteine and glutamate into the neuron.…”

Section: Eaac1 and Glutathionementioning

confidence: 99%

Role of Excitatory Amino Acid Carrier 1 (EAAC1) in Neuronal Death and Neurogenesis After Ischemic Stroke

Lee

Hong

et al. 2020

IJMS

View full text Add to dashboard Cite

Although there have been substantial advances in knowledge regarding the mechanisms of neuron death after stroke, effective therapeutic measures for stroke are still insufficient. Excitatory amino acid carrier 1 (EAAC1) is a type of neuronal glutamate transporter and considered to have an additional action involving the neuronal uptake of cysteine, which acts as a crucial substrate for glutathione synthesis. Previously, our lab demonstrated that genetic deletion of EAAC1 leads to decreased neuronal glutathione synthesis, increased oxidative stress, and subsequent cognitive impairment. Therefore, we hypothesized that reduced neuronal transport of cysteine due to deletion of the EAAC1 gene might exacerbate neuronal injury and impair adult neurogenesis in the hippocampus after transient cerebral ischemia. EAAC1 gene deletion profoundly increased ischemia-induced neuronal death by decreasing the antioxidant capacity. In addition, genetic deletion of EAAC1 also decreased the overall neurogenesis processes, such as cell proliferation, differentiation, and survival, after cerebral ischemia. These studies strongly support our hypothesis that EAAC1 is crucial for the survival of newly generated neurons, as well as mature neurons, in both physiological and pathological conditions. Here, we present a comprehensive review of the role of EAAC1 in neuronal death and neurogenesis induced by ischemic stroke, focusing on its potential cellular and molecular mechanisms.

show abstract

Ethanol inhibition of undifferentiated rat neural progenitor cell replication can be prevented by chlorogenic acid via the NFATc4/CSE signaling pathway

Shanmugam

Patel

Rodriguez

et al. 2023

Alcohol: Clinical and Experimental Research

Self Cite

View full text Add to dashboard Cite

BackgroundPrenatal ethanol exposure hinders oxidative stress‐mediated neuroblast/neural progenitor cell proliferation by inhibiting G1‐S transition, a process vital to neocortical development. We previously showed that ethanol elicits this redox imbalance by repressing cystathionine γ‐lyase (CSE), the rate‐limiting enzyme in the transsulfuration pathway in fetal brain and cultured cerebral cortical neurons. However, the mechanism by which ethanol impacts the CSE pathway in proliferating neuroblasts is not known. We conducted experiments to define the effects of ethanol on CSE regulation and the molecular signaling events that control this vital pathway. This enabled us to develop an intervention to prevent the ethanol‐associated cytostasis.MethodsSpontaneously immortalized undifferentiated E18 rat neuroblasts from brain cerebral cortex were exposed to ethanol to mimic an acute consumption pattern in humans. We performed loss‐ and gain‐of‐function studies to evaluate whether NFATc4 is a transcriptional regulator of CSE. The neuroprotective effects of chlorogenic acid (CGA) against the effects of ethanol were assessed using ROS and GSH/GSSG assays as measures of oxidative stress, transcriptional activation of NFATc4, and expression of NFATc4 and CSE by qRT‐PCR and immunoblotting.ResultsEthanol treatment of E18‐neuroblast cells elicited oxidative stress and significantly reduced CSE expression with a concomitant decrease in NFATc4 transcriptional activation and expression. In parallel, inhibition of the calcineurin/NFAT pathway by FK506 exaggerated ethanol‐induced CSE loss. In contrast, NFATc4 overexpression prevented loss of ethanol‐induced CSE. CGA increased and activated NFATc4, amplified CSE expression, rescued ethanol‐induced oxidative stress, and averted the cytostasis of neuroblasts by rescuing cyclin D1 expression.ConclusionsThese findings demonstrate that ethanol can perturb CSE‐dependent redox homeostasis by impairing the NFATc4 signaling pathway in neuroblasts. Notably, ethanol‐associated impairments were rescued by genetic or pharmacological activation of NFATc4. Furthermore, we found a potential role for CGA in mitigating the ethanol‐related neuroblast toxicity with a compelling connection to the NFATc4/CSE pathway.

show abstract

Ethanol (E) Impairs Fetal Brain GSH Homeostasis by Inhibiting Excitatory Amino-Acid Carrier 1 (EAAC1)-Mediated Cysteine Transport

Cited by 4 publications

References 82 publications

Role for Cystathionine γ Lyase (CSE) in an Ethanol (E)-Induced Lesion in Fetal Brain GSH Homeostasis

Role for Cystathionine γ Lyase (CSE) in an Ethanol (E)-Induced Lesion in Fetal Brain GSH Homeostasis

Role of Excitatory Amino Acid Carrier 1 (EAAC1) in Neuronal Death and Neurogenesis After Ischemic Stroke

Ethanol inhibition of undifferentiated rat neural progenitor cell replication can be prevented by chlorogenic acid via the NFATc4/CSE signaling pathway

Contact Info

Product

Resources

About