Altered folate binding protein expression and folate delivery are associated with congenital hydrocephalus in the hydrocephalic Texas rat

Jimenez, Alicia Requena; Naz, Naila; Miyan, Jaleel

doi:10.1177/0271678x18776226

Cited by 14 publications

(19 citation statements)

References 66 publications

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“…Abnormal folate transport to the brain has been proposed to contribute to aqueduct obstruction in the hydrocephalic Texas (H-Tx) rat (23,24). Interestingly, however, hydrocephalus is not commonly described among neurological signs associated with the very low levels of folate in CSF that occur in hereditary folate malabsorption, caused by mutations in SLC46A1 (proton-coupled folate transporter; PCFT) or cerebral folate deficiency, caused by mutations in FOLR1 (folate receptor α; FRα) (25-27).…”

Section: Resultsmentioning

confidence: 99%

Impaired folate 1-carbon metabolism causes formate-preventable hydrocephalus in glycine decarboxylase–deficient mice

Santos¹,

Pai²,

Mahmood³

et al. 2020

Journal of Clinical Investigation

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Section: Resultsmentioning

confidence: 99%

Impaired folate 1-carbon metabolism causes formate-preventable hydrocephalus in glycine decarboxylase–deficient mice

Santos¹,

Pai²,

Mahmood³

et al. 2020

Journal of Clinical Investigation

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“…Interestingly, decreased levels of ALDH1L1 in cerebrospinal fluid were linked to neonatal hydrocephalus in a rat model (Cains et al, 2009). Further studies of this model suggested a role for the enzyme in cerebral folate transport and regulation of folate availability in the brain (Naz et al, 2016; Jimenez et al, 2019). In line with such function, it has been also demonstrated that ALDH1L1 protects folate from degradation in zebrafish embryos, which is a defense mechanism against oxidative stress (Chang et al, 2014; Hsiao et al, 2014).…”

Section: Aldh1l1 Folate Regulatory Enzymementioning

confidence: 98%

The Role of Single-Nucleotide Polymorphisms in the Function of Candidate Tumor Suppressor ALDH1L1

Krupenko

Horita

2019

Front. Genet.

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Folate (vitamin B9) is a common name for a group of coenzymes that function as carriers of chemical moieties called one-carbon groups in numerous biochemical reactions. The combination of these folate-dependent reactions constitutes one-carbon metabolism, the name synonymous to folate metabolism. Folate coenzymes and associated metabolic pathways are vital for cellular homeostasis due to their key roles in nucleic acid biosynthesis, DNA repair, methylation processes, amino acid biogenesis, and energy balance. Folate is an essential nutrient because humans are unable to synthesize this coenzyme and must obtain it from the diet. Insufficient folate intake can ultimately increase risk of certain diseases, most notably neural tube defects. More than 20 enzymes are known to participate in folate metabolism. Single-nucleotide polymorphisms (SNPs) in genes encoding for folate enzymes are associated with altered metabolism, changes in DNA methylation and modified risk for the development of human pathologies including cardiovascular diseases, birth defects, and cancer. ALDH1L1, one of the folate-metabolizing enzymes, serves a regulatory function in folate metabolism restricting the flux of one-carbon groups through biosynthetic processes. Numerous studies have established that ALDH1L1 is often silenced or strongly down-regulated in cancers. The loss of ALDH1L1 protein positively correlates with the occurrence of malignant tumors and tumor aggressiveness, hence the enzyme is viewed as a candidate tumor suppressor. ALDH1L1 has much higher frequency of non-synonymous exonic SNPs than most other genes for folate enzymes. Common SNPs at the polymorphic loci rs3796191, rs2886059, rs9282691, rs2276724, rs1127717, and rs4646750 in ALDH1L1 exons characterize more than 97% of Europeans while additional common variants are found in other ethnic populations. The effects of these SNPs on the enzyme is not clear but studies indicate that some coding and non-coding ALDH1L1 SNPs are associated with altered risk of certain cancer types and it is also likely that specific haplotypes define the metabolic response to dietary folate. This review discusses the role of ALDH1L1 in folate metabolism and etiology of diseases with the focus on non-synonymous coding ALDH1L1 SNPs and their effects on the enzyme structure/function, metabolic role and association with cancer.

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“…The ventricles of these rats remained enlarged, even after the blood pressure was lowered by captopril 89 . Current studies have found that choroid plexus cell death, ependymal injury, impaired glymphatic transport, hemorrhage, and other factors may be involved in the development of hydrocephalus in spontaneously hypertensive rats 17,87,90,91 . Therefore, minocycline is a promising drug for the treatment of hydrocephalus and related tissue damage.…”

Section: Anti‐iron Overload Treatment For Hydrocephalusmentioning

confidence: 99%

“…To unveil the pathogenesis of brain damage in hydrocephalus and develop more effective nonsurgical treatments, researchers have developed different animal models such as intraventricular injection of blood or kaolin to induce hydrocephalus in rats 14,15 . At the same time, some congenital hydrocephalus models characterized by aqueduct stenosis, ependymal stripping, and astrocytes activation have also been applied 16,17 . Although animal models cannot fully simulate human body condition, they still play important roles in hydrocephalus research.…”

Section: Introductionmentioning

confidence: 99%

Novel therapeutics for hydrocephalus: Insights from animal models

Wang

Tan

et al. 2021

CNS Neurosci Ther

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Hydrocephalus is a cerebrospinal fluid physiological disorder that causes ventricular dilation with normal or high intracranial pressure. The current regular treatment for hydrocephalus is cerebrospinal fluid shunting, which is frequently related to failure and complications. Meanwhile, considering that the current nonsurgical treatments of hydrocephalus can only relieve the symptoms but cannot eliminate this complication caused by primary brain injuries, the exploration of more effective therapies has become the focus for many researchers. In this article, the current research status and progress of nonsurgical treatment in animal models of hydrocephalus are reviewed to provide new orientations for animal research and clinical practice.

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Altered folate binding protein expression and folate delivery are associated with congenital hydrocephalus in the hydrocephalic Texas rat

Cited by 14 publications

References 66 publications

Impaired folate 1-carbon metabolism causes formate-preventable hydrocephalus in glycine decarboxylase–deficient mice

Impaired folate 1-carbon metabolism causes formate-preventable hydrocephalus in glycine decarboxylase–deficient mice

The Role of Single-Nucleotide Polymorphisms in the Function of Candidate Tumor Suppressor ALDH1L1

Novel therapeutics for hydrocephalus: Insights from animal models

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