Your search keyword '"Spinal Dysraphism metabolism"' showing total 77 results

1. Parental arsenic exposure and tissue-specific DNA methylation in Bangladeshi infants with spina bifida.

Author

Tindula G, Mukherjee SK, Ekramullah SM, Arman DM, Islam J, Biswas SK, Warf BC, Christiani DC, Lemos B, Liang L, Cardenas A, and Mazumdar M

Subjects

Humans, Male, Female, Bangladesh, Infant, CpG Islands, Nails chemistry, Nails metabolism, Epigenesis, Genetic, Adult, Paternal Exposure adverse effects, Infant, Newborn, DNA Methylation, Arsenic adverse effects, Arsenic toxicity, Spinal Dysraphism genetics, Spinal Dysraphism chemically induced, Spinal Dysraphism metabolism

Abstract

An emerging hypothesis linking arsenic toxicity involves altered epigenetic mechanisms, such as DNA methylation. In this study, we examined the relationship between parents' arsenic exposure and DNA methylation in tissues obtained from 28 infants with spina bifida from Bangladesh. We analyzed arsenic in parents' toenails using inductively coupled plasma mass spectrometry (ICP-MS). DNA methylation was measured in infants' dural tissue, buccal swabs, and whole blood using the Illumina Infinium MethylationEPIC BeadChip. We performed epigenome-wide association analyses (EWAS) and tested differentially methylated regions (DMRs). In EWAS, DNA methylation at cg24039697 in dural tissue was positively associated (β = 0.59, p  = 7.6 × 10 -9 ) with father's toenail arsenic concentrations, adjusting for covariates. We did not identify any CpG sites related to father's arsenic exposure in the other tissues, or any CpG sites related to mother's arsenic exposure. Gene ontology analysis identified many biological pathways of interest, including the Wnt signaling pathways. We identified several DMRs across the tissues related to arsenic exposure that included probes mapping to genes that have previously been identified in studies of neural tube defects. This study emphasizes the potential impact of arsenic exposure in fathers, often understudied in epidemiological studies, on DNA methylation in a unique neurological tissue specific to spina bifida.

Published

2024

2. Altered placental immune cell composition and gene expression with isolated fetal spina bifida.

Author

White M, Abdo H, Grynspan D, Mieghem TV, and Connor KL

Subjects

Pregnancy, Male, Female, Humans, Folic Acid metabolism, Phenotype, Gene Expression, Placenta metabolism, Spinal Dysraphism genetics, Spinal Dysraphism metabolism

Abstract

Problem: Fetal spina bifida (SB) is more common in pregnant people with folate deficiency or anomalies of folate metabolism. It is also known that fetuses with SB have a higher risk of low birthweight, a condition that is typically placental-mediated. We therefore hypothesized that fetal SB would associate with altered expression of key placental folate transporters and an increase in Hofbauer cells (HBCs), which are folate-dependent placental macrophages., Method of Study: Folate receptor-α (FRα), proton coupled folate receptor (PCFT), and reduced folate carrier (RFC) protein localization and expression (immunohistochemistry) and HBC phenotypes (HBC abundance and folate receptor-β [FRβ] expression; RNA in situ hybridization) were assessed in placentae from fetuses with SB (cases; n = 12) and in term (n = 10) and gestational age (GA) - and maternal body mass index - matched (n = 12) controls without congenital anomalies., Results: Cases had a higher proportion of placental villous cells that were HBCs (6.9% vs. 2.4%, p = .0001) and higher average HBC FRβ expression (3.2 mRNA molecules per HBC vs. 2.3, p = .03) than GA-matched controls. HBCs in cases were largely polarized to a regulatory phenotype (median 92.1% of HBCs). In sex-stratified analyses, only male cases had higher HBC levels and HBC FRβ expression than GA-matched controls. There were no differences between groups in the total percent of syncytium and stromal cells that were positive for FRα, PCFT, or RFC protein immunolabeling., Conclusions: HBC abundance and FRβ expression by HBCs are increased in placentae of fetuses with SB, suggesting immune-mediated dysregulation in placental phenotype, and could contribute to SB-associated comorbidities., (© 2024 The Authors. American Journal of Reproductive Immunology published by John Wiley & Sons Ltd.)

Published

2024

3. Fetal spina bifida associates with dysregulation in nutrient-sensitive placental gene networks: Findings from a matched case-control study.

Author

White M, Arif-Pardy J, Van Mieghem T, and Connor KL

Subjects

Humans, Pregnancy, Female, Placenta, Case-Control Studies, Gene Regulatory Networks, Nutrients, Zinc metabolism, Vitamin B Complex metabolism, Spinal Dysraphism epidemiology, Spinal Dysraphism genetics, Spinal Dysraphism metabolism

Abstract

To improve outcomes in fetuses with spina bifida (SB), better understanding is needed of the molecular drivers of SB and its comorbidities. Pregnant people carrying a fetus with isolated SB (cases; n = 12) or a fetus with no congenital anomalies (controls; n = 21) were recruited at Mount Sinai Hospital, Toronto, Ontario, Canada. Clinical data and placental samples were collected. Placental transcriptome was sequenced (Clariom D microarray) and a nutrient-focused gene expression analysis pipeline was applied to determine whether fetal SB associates with placental dysfunction. Of the 391 differentially expressed genes (DEGs) in cases, 11% (n = 42) had at least one nutrient cofactor, including B vitamins (n = 7 genes), iron/heme (n = 6), and zinc (n = 11). Cases had dysregulation in genes not previously known to associate with SB, and in placental genes that have known links to SB but have not been previously identified in the placenta. Cases also had downregulated nutrient transport and upregulated branching angiogenesis and immune/inflammatory processes. Five nutrient-dependent transcription regulators, collectively predicted to target 46% of DEGs in cases, were identified and were most commonly dependent on B vitamins (n = 3) and zinc (n = 2). Placental gene expression changes were most acute in cases with poor growth. Placentae from fetuses with SB have dysregulation in several gene networks, including those that are sensitive to multiple micronutrients beyond the well-known folic acid. An improved understanding of placental phenotype in fetuses with SB may help identify novel mechanisms associated with comorbidities in fetuses with SB, and reveal new targets to improve fetal outcomes in this population., (© 2024 The Authors. Clinical and Translational Science published by Wiley Periodicals LLC on behalf of American Society for Clinical Pharmacology and Therapeutics.)

Published

2024

4. scRNA-Seq of Cultured Human Amniotic Fluid from Fetuses with Spina Bifida Reveals the Origin and Heterogeneity of the Cellular Content.

Author

Dasargyri A, González Rodríguez D, Rehrauer H, Reichmann E, Biedermann T, and Moehrlen U

Subjects

Humans, Amniotic Fluid metabolism, Single-Cell Gene Expression Analysis, Tissue Engineering, Spina Bifida Cystica metabolism, Spinal Dysraphism metabolism

Abstract

Amniotic fluid has been proposed as an easily available source of cells for numerous applications in regenerative medicine and tissue engineering. The use of amniotic fluid cells in biomedical applications necessitates their unequivocal characterization; however, the exact cellular composition of amniotic fluid and the precise tissue origins of these cells remain largely unclear. Using cells cultured from the human amniotic fluid of fetuses with spina bifida aperta and of a healthy fetus, we performed single-cell RNA sequencing to characterize the tissue origin and marker expression of cultured amniotic fluid cells at the single-cell level. Our analysis revealed nine different cell types of stromal, epithelial and immune cell phenotypes, and from various fetal tissue origins, demonstrating the heterogeneity of the cultured amniotic fluid cell population at a single-cell resolution. It also identified cell types of neural origin in amniotic fluid from fetuses with spina bifida aperta. Our data provide a comprehensive list of markers for the characterization of the various progenitor and terminally differentiated cell types in cultured amniotic fluid. This study highlights the relevance of single-cell analysis approaches for the characterization of amniotic fluid cells in order to harness their full potential in biomedical research and clinical applications.

Published

2023

5. Fetal and Perinatal Expression Profiles of Proinflammatory Cytokines in the Neuroplacodes of Rats with Myelomeningoceles: A Contribution to the Understanding of Secondary Spinal Cord Injury in Open Spinal Dysraphism.

Author

Cohrs G, Blumenröther AK, Sürie JP, Synowitz M, Held-Feindt J, and Knerlich-Lukoschus F

Subjects

Animals, Disease Models, Animal, Meningomyelocele pathology, Rats, Rats, Sprague-Dawley, Spinal Cord Injuries metabolism, Spinal Cord Injuries pathology, Spinal Dysraphism metabolism, Spinal Dysraphism pathology, Cytokines metabolism, Meningomyelocele complications, Meningomyelocele metabolism, Spinal Cord Injuries etiology, Spinal Dysraphism etiology

Abstract

The cellular and molecular mechanisms that presumably underlie the progressive functional decline of the myelomeningocele (MMC) placode are not well understood. We previously identified key players in post-traumatic spinal cord injury cascades in human MMC tissues obtained during postnatal repair. In this study, we conducted experiments to further investigate these mediators in the prenatal time course under standardized conditions in a retinoic acid-induced MMC rat model. A retinoic acid MMC model was established using time-dated Sprague-Dawley rats, which were gavage-fed with all-trans retinoic acid (RA; 60 mg/kg) dissolved in olive oil at E10. Control animals received olive oil only. Fetuses from both groups were obtained at E16, E18, and E22. The spinal cords (SCs) of both groups were formalin-fixed or snap-frozen. Tissues were screened by real-time reverse transcription polymerase chain reaction for the expression of cytokines and chemokines known to play a role in the lesion cascades of the central nervous system after trauma. MMC placodes exhibited inflammatory cells and glial activation in the later gestational stages. At the messenger RNA (mRNA) level, interleukin-1 beta, tumor necrosis factor alpha, and tumor necrosis factor receptor type 1 exhibited significant induction at E22. interleukin-1 beta receptor type 1 mRNA was induced significantly at E16 and E22. Double labeling experiments confirmed the co-staining of these cytokines and their receptors with ionized calcium-binding adapter molecule 1 (i.e., inflammatory cells), vimentin, and nestin in different anatomical SC areas and neuronal nuclear protein in ventral horn neurons. C-X-C motif chemokine 12 mRNA was elevated in control and MMC animals at E16 compared with E18 and E22. C-X3-C motif ligand 1 mRNA was lower in MMC tissues than in control tissues on E16. The presented findings contribute to the concept that pathophysiological mechanisms, such as cytokine induction in the neuroplacode, in addition to the "first hit," promote secondary spinal cord injury with functional loss in the late fetal time course. Further, these mediators should be taken into consideration in the development of new therapeutic approaches for open spinal dysraphism.

Published

2021

6. Expression Pattern of 5-HT (Serotonin) Receptors during Normal Development of the Human Spinal Cord and Ganglia and in Fetus with Cervical Spina Bifida.

Author

Punda H, Mardesic S, Filipovic N, Kosovic I, Benzon B, Ogorevc M, Bocina I, Kolic K, Vukojevic K, and Saraga-Babic M

Subjects

Apoptosis physiology, Caspase 3 metabolism, Cell Differentiation physiology, Cell Proliferation physiology, Humans, Ki-67 Antigen metabolism, Sensory Receptor Cells metabolism, Serotonin metabolism, Fetus metabolism, Ganglia metabolism, Ganglia, Spinal metabolism, Receptors, Serotonin metabolism, Spinal Cord metabolism, Spinal Dysraphism metabolism

Abstract

The expression of 5-HT (serotonin) receptors (sr) was analyzed in the spinal cord and ganglia of 15 human conceptuses (5-10-weeks), and in the 9-week fetus with spina bifida. We used immunohistochemical method to detect sr-positive, apoptotic (caspase-3) and proliferating (Ki-67) cells, double immunofluorescence for co-localization with protein gene peptide (pgp) 9.5 and GFAP, as well as semiquantification and statistical measurements. Following the neurulation process, moderate (sr1 and sr2) and mild (sr3) expression characterized neuroblasts in the spinal cord and ganglia. During further development, sr1 expression gradually increased in the motoneurons, autonomic and sensory neurons, while sr2 and sr3 increased strongly in floor and roof plates. In the ganglia, sr3 expression increased during limited developmental period, while sr1 and sr2 increased throughout the investigated period. Co-expression of sr/pgp 9.5 characterized developing neurons, while sr/GFAP co-localized in the roof plate. In the spinal cord and ganglia of malformed fetus, weaker sr1 and sr2 and stronger sr3 expression accompanied morphological abnormalities. Anomalous roof plate morphology showed an excess of apoptotic and proliferating cells and increased sr3 expression. Our results indicate a human-species specific sr expression pattern, and the importance of sr1 in neuronal differentiation, and sr2 and sr3 in the control of the roof plate morphogenesis in normal and disturbed development.

Published

2021

7. The N-terminus of MTRR plays a role in MTR reactivation cycle beyond electron transfer.

Author

Zhang J, Liu GC, Dai XL, Wang J, Jin MH, Mi NN, and Wang SQ

Subjects

5-Methyltetrahydrofolate-Homocysteine S-Methyltransferase chemistry, Amino Acid Sequence, Electron Transport, Exons, Ferredoxin-NADP Reductase chemistry, Ferredoxin-NADP Reductase genetics, Humans, Models, Molecular, Protein Conformation, Sequence Alignment, Sequence Deletion, Spinal Dysraphism genetics, Spinal Dysraphism metabolism, 5-Methyltetrahydrofolate-Homocysteine S-Methyltransferase metabolism, Ferredoxin-NADP Reductase metabolism

Abstract

In eucaryotic cells, methionine synthase reductase (MSR/MTRR) is capable of dominating the folate-homocysteine metabolism as an irreplaceable partner in electron transfer for regeneration of methionine synthase. The N-terminus of MTRR containing a conserved domain of FMN_Red is closely concerned with the oxidation-reduction process. Maternal substitution of I22M in this domain can bring about pregnancy with high risk of spina bifida. A new variation of Arg2del was identified from a female conceiving a fetus with spina bifida cystica. Although the deletion is far from the N-terminal FMN_Red domain, the biochemical features of the variant had been seriously investigated. Curiously, the deletion of arginine(s) of MTRR could not affect the electron relay, if only the FMN_Red domain was intact, but by degrees reduced the ability to promote MTR catalysis in methionine formation. Confirmation of the interaction between the isolated MTRR N-terminal polypeptide and MTR suggested that the native MTRR N-terminus might play an extra role in MTR function. The tandem arginines at the end of MTRR N-terminus conferring high affinity to MTR were indispensable for stimulating methyltransferase activity perhaps via triggering allosteric effect that could be attenuated by removal of the arginine(s). It was concluded that MTRR could also propel MTR enzymatic reaction relying on the tandem arginines at N-terminus more than just only implicated in electron transfer in MTR reactivation cycle. Perturbance of the enzymatic cooperation due to the novel deletion could possibly invite spina bifida in clinics., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2020 Elsevier Inc. All rights reserved.)

Published

2020

8. Non-neural surface ectodermal rosette formation and F-actin dynamics drive mammalian neural tube closure.

Author

Zhou CJ, Ji Y, Reynolds K, McMahon M, Garland MA, Zhang S, Sun B, Gu R, Islam M, Liu Y, Zhao T, Hsu G, and Iwasa J

Subjects

Actins analysis, Animals, DNA-Binding Proteins genetics, Ectoderm abnormalities, Ectoderm metabolism, Ectoderm ultrastructure, Mice, Mutation, Neural Tube abnormalities, Neural Tube metabolism, Neural Tube ultrastructure, Neural Tube Defects genetics, Neural Tube Defects metabolism, Spinal Dysraphism embryology, Spinal Dysraphism genetics, Spinal Dysraphism metabolism, Spine abnormalities, Spine embryology, Spine metabolism, Spine ultrastructure, Transcription Factors genetics, Actins metabolism, Ectoderm embryology, Neural Tube embryology, Neural Tube Defects embryology, Neurulation

Abstract

The mechanisms underlying mammalian neural tube closure remain poorly understood. We report a unique cellular process involving multicellular rosette formation, convergent cellular protrusions, and F-actin cable network of the non-neural surface ectodermal cells encircling the closure site of the posterior neuropore, which are demonstrated by scanning electron microscopy and genetic fate mapping analyses during mouse spinal neurulation. These unique cellular structures are severely disrupted in the surface ectodermal transcription factor Grhl3 mutants that exhibit fully penetrant spina bifida. We propose a novel model of mammalian neural tube closure driven by surface ectodermal dynamics, which is computationally visualized., (Copyright © 2020 Elsevier Inc. All rights reserved.)

Published

2020

9. Melatonin protected against the detrimental effects of microRNA-363 in a rat model of vitamin A-associated congenital spinal deformities: Involvement of Notch signaling.

Author

Li Z, Li X, Bi J, Chan MTV, Wu WKK, and Shen J

Subjects

Animals, Cell Differentiation drug effects, Cell Differentiation genetics, Cell Proliferation drug effects, Cell Proliferation genetics, Disease Models, Animal, Female, Neural Stem Cells metabolism, Neurogenesis drug effects, Neurogenesis genetics, Rats, Rats, Wistar, Receptor, Notch1 metabolism, Signal Transduction drug effects, Spinal Dysraphism etiology, Spinal Dysraphism metabolism, Melatonin pharmacology, MicroRNAs genetics, Neural Stem Cells drug effects, Spinal Dysraphism genetics, Vitamin A Deficiency complications

Abstract

Congenital spinal deformities are a result of defective somitogenesis and are associated with vitamin A deficiency (VAD). However, the molecular mechanisms of VAD-associated congenital spinal deformities remain largely unknown. Increasing number of studies suggested that microRNAs and melatonin played important roles in the development of congenital spinal deformities. In this study, we showed that the whole-embryo expression of miR-363 was upregulated in VAD rats. Furthermore, we demonstrated that miR-363 inhibited the proliferation and neuronal differentiation of primary cultured NSCs, accompanied by downregulation of Notch1. To this end, melatonin suppressed miR-363 expression and rescued the effects of miR-363 on NSC proliferation and neuronal differentiation together with restoration of Notch signaling. The present study provided new insights into the mechanism of VAD-associated spinal deformities and the therapeutic effect of melatonin that may lead to novel understanding of the molecular mechanisms of congenital spinal deformities., (© 2019 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published

2019

10. Generation of integration-free induced pluripotent stem cells from a patient with spina bifida.

Author

Wang H, Zhao S, Finnell RH, George T, and Cooney AJ

Subjects

Female, Humans, Infant, Kruppel-Like Factor 4, Spinal Dysraphism pathology, Induced Pluripotent Stem Cells metabolism, Spinal Dysraphism metabolism

Abstract

A skin biopsy was obtained from a 14-year-old female patient with a history of Myelomeningocele. Dermal fibroblasts were isolated and reprogrammed with Sendai virus (SeV) vectors encoding OCT3/4, SOX2, KLF4, and c-MYC. The generated induced Pluripotent Stem Cell (iPSC) clones NTDi4_09A were free of genomically integrated reprogramming genes, had a stable normal karyotype and expressed pluripotency markers. The iPSCs formed teratomas in mice, which were differentiated towards derivatives of the three germ layers in vivo. This iPSC line offers a useful resource to study a genetic profile of a patient with spina bifida., (Copyright © 2018. Published by Elsevier B.V.)

Published

2018

11. Total energy expenditure and body composition of children with developmental disabilities.

Author

Polfuss M, Sawin KJ, Papanek PE, Bandini L, Forseth B, Moosreiner A, Zvara K, and Schoeller DA

Subjects

Adipose Tissue metabolism, Adolescent, Analysis of Variance, Body Fluid Compartments metabolism, Child, Child, Preschool, Developmental Disabilities complications, Disabled Children, Down Syndrome complications, Energy Intake, Female, Humans, Male, Pilot Projects, Spinal Dysraphism complications, Walking, Wheelchairs, Body Composition, Developmental Disabilities metabolism, Disabled Persons, Down Syndrome metabolism, Energy Metabolism, Obesity etiology, Obesity prevention & control, Spinal Dysraphism metabolism

Abstract

Background: Obesity prevalence is increased in children with developmental disabilities, specifically in children with spina bifida and Down syndrome. Energy expenditure, a critical aspect of weight management, has been extensively studied in the typically developing population, but not adequately studied in children with developmental disabilities., Objective: Determine energy expenditure, fat-free mass and body fat percentile and the impact of these findings on recommended caloric intake in children with spina bifida and Down syndrome., Methods/measures: This pilot study included 36 children, 18 with spina bifida, 9 with Down syndrome and 9 typically developing children. Half of the children with spina bifida were non-ambulatory. Doubly labeled water was used to measure energy expenditure and body composition. Descriptive statistics described the sample and MANOVA and ANOVA methods were used to evaluate differences between groups., Results: Energy expenditure was significantly less for children with spina bifida who primarily used a wheelchair (p = .001) and children with Down syndrome (p = .041) when compared to children without a disability when adjusted for fat-free mass. However, no significant difference was detected in children with spina bifida who ambulated without assistance (p = .072)., Conclusions: Children with spina bifida and Down syndrome have a significantly decreased energy expenditure which directly impacts recommended caloric intake. No significant difference was detected for children with spina bifida who ambulated, although the small sample size of this pilot study may have limited these findings. Validating these results in a larger study is integral to supporting successful weight management of these children., (Copyright © 2017 Elsevier Inc. All rights reserved.)

Published

2018

12. Spina bifida-predisposing heterozygous mutations in Planar Cell Polarity genes and Zic2 reduce bone mass in young mice.

Author

Orriss IR, Lanham S, Savery D, Greene NDE, Stanier P, Oreffo R, Copp AJ, and Galea GL

Subjects

Animals, Bone and Bones metabolism, Heterozygote, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Neural Tube Defects genetics, PAX3 Transcription Factor physiology, Spinal Dysraphism genetics, Spinal Dysraphism metabolism, Bone and Bones pathology, Cell Polarity, Mutation, Nerve Tissue Proteins physiology, Receptors, G-Protein-Coupled physiology, Spinal Dysraphism pathology, Transcription Factors physiology

Abstract

Fractures are a common comorbidity in children with the neural tube defect (NTD) spina bifida. Mutations in the Wnt/planar cell polarity (PCP) pathway contribute to NTDs in humans and mice, but whether this pathway independently determines bone mass is poorly understood. Here, we first confirmed that core Wnt/PCP components are expressed in osteoblasts and osteoclasts in vitro. In vivo, we performed detailed µCT comparisons of bone structure in tibiae from young male mice heterozygous for NTD-associated mutations versus WT littermates. PCP signalling disruption caused by Vangl2 (Vangl2 Lp/+ ) or Celsr1 (Celsr1 Crsh/+ ) mutations significantly reduced trabecular bone mass and distal tibial cortical thickness. NTD-associated mutations in non-PCP transcription factors were also investigated. Pax3 mutation (Pax3 Sp2H/+ ) had minimal effects on bone mass. Zic2 mutation (Zic2 Ku/+ ) significantly altered the position of the tibia/fibula junction and diminished cortical bone in the proximal tibia. Beyond these genes, we bioinformatically documented the known extent of shared genetic networks between NTDs and bone properties. 46 genes involved in neural tube closure are annotated with bone-related ontologies. These findings document shared genetic networks between spina bifida risk and bone structure, including PCP components and Zic2. Genetic variants which predispose to spina bifida may therefore independently diminish bone mass.

Published

2018

13. MARK2/Par1b Insufficiency Attenuates DVL Gene Transcription via Histone Deacetylation in Lumbosacral Spina Bifida.

Author

Chen S, Zhang Q, Bai B, Ouyang S, Bao Y, Li H, and Zhang T

Subjects

Acetylation, Cell Proliferation physiology, Child, Child, Preschool, Dishevelled Proteins metabolism, Female, Humans, Infant, Infant, Newborn, Male, Neural Stem Cells metabolism, Neurogenesis physiology, Phosphorylation, Promoter Regions, Genetic, Protein Serine-Threonine Kinases metabolism, Spinal Dysraphism metabolism, Dishevelled Proteins genetics, Histones metabolism, Protein Serine-Threonine Kinases genetics, Spinal Dysraphism genetics, Transcription, Genetic

Abstract

Dishevelled (DVL/Dvl) genes play roles in canonical and noncanonical Wnt signaling, both of which are essential in neural tube closing and are involved in balancing neural progenitor growth and differentiation, or neuroepithelial cell polarity, respectively. In mouse Dvl haploinsufficiency leads to neural tube defects (NTDs), which represent the second most common birth defects. However, DVL genes' genetic contributions in human NTDs are modest. We sought to explore the molecular impact on such genes in human NTDs in a Han Chinese cohort. In 47 cases with NTDs and 61 matched controls, in brain tissues, the DVL1/2 mRNA levels were correlated with the levels of a serine/threonine protein kinase MARK2, and in 20 cases with lumbosacral spina bifida, the mRNA levels of DVL1 and MARK2 were significantly decreased; by contrast, only an intronic rare variant was found. Moreover, in an extended population, we found merely three novel rare missense variants in 1 % of individuals with NTDs. In cell-based assays, Mark2 depletion indeed reduces Dvl gene expression and interrupts neural stem cell (NSCs) growth and differentiation, which are likely to be mediated through a decrease in class IIa HDAC phosphorylation and reduced H3K4ac and H3K27ac occupancies at the Dvl1/2 promoters. Finally, the detections of folate concentration in human brain tissue and NSCs and MEF cells indicates that folate deficiency contributes to the observed decreases in Mark2 and Dvl1 expression. Our present study raises a potential common pathogenicity mechanism in human lumbosacral spina bifida about DVL genes rather than their genetic pathogenic role.

Published

2017

14. Stage specific requirement of platelet-derived growth factor receptor-α in embryonic development.

Author

Qian C, Wong CWY, Wu Z, He Q, Xia H, Tam PKH, Wong KKY, and Lui VCH

Subjects

Abdominal Wall abnormalities, Abdominal Wall embryology, Abnormalities, Multiple embryology, Abnormalities, Multiple genetics, Abnormalities, Multiple metabolism, Animals, Apoptosis physiology, Cleft Lip embryology, Cleft Lip genetics, Cleft Lip metabolism, Cleft Palate embryology, Cleft Palate genetics, Cleft Palate metabolism, Gene Expression Regulation, Developmental, Gene Knockout Techniques, Hernia, Umbilical embryology, Hernia, Umbilical genetics, Hernia, Umbilical metabolism, Immunohistochemistry, In Situ Nick-End Labeling, Mice, Inbred C57BL, Mice, Transgenic, Receptor, Platelet-Derived Growth Factor alpha genetics, Skeleton abnormalities, Skeleton embryology, Skeleton metabolism, Spinal Dysraphism embryology, Spinal Dysraphism genetics, Spinal Dysraphism metabolism, Tamoxifen, Time Factors, Embryonic Development physiology, Receptor, Platelet-Derived Growth Factor alpha metabolism

Abstract

Background: Platelet-derived growth factor receptor alpha (PDGFRα) is a cell-surface receptor tyrosine kinase for platelet-derived growth factors. Correct timing and level of Pdgfra expression is crucial for embryo development, and deletion of Pdgfra caused developmental defects of multiple endoderm and mesoderm derived structures, resulting in a complex phenotypes including orofacial cleft, spina bifida, rib deformities, and omphalocele in mice. However, it is not clear if deletion of Pdgfra at different embryonic stages differentially affects these structures., Purpose: To address the temporal requirement of Pdgfra in embryonic development., Methods: We have deleted the Pdgfra in Pdgfra-expressing tissues at different embryonic stages in mice, examined and quantified the developmental anomalies., Results: Current study showed that (i) conditional deletion of Pdgfra at different embryonic days (between E7.5 and E10.5) resulted in orofacial cleft, spina bifida, rib cage deformities, and omphalocele, and (ii) the day of Pdgfra deletion influenced the combinations, incidence and severities of these anomalies. Deletion of Pdgfra caused apoptosis of Pdgfra-expressing tissues, and developmental defects of their derivatives., Conclusion: Orofacial cleft, spina bifida and omphalocele are among the commonest skeletal and abdominal wall defects of newborns, but their genetic etiologies are largely unknown. The remarkable resemblance of our conditional Pdgfra knockout embryos to theses human congenital anomalies, suggesting that dysregulated PDGFRA expression could cause these anomalies in human. Future work should aim at defining (a) the regulatory elements for the expression of the human PDGFRA during embryonic development, and (b) if mutations / sequence variations of these regulatory elements cause these anomalies.

Published

2017

15. Neural tube closure and embryonic metabolism.

Author

Yamaguchi Y, Miyazawa H, and Miura M

Subjects

Anencephaly etiology, Anencephaly pathology, Animals, Chorioallantoic Membrane metabolism, Chorioallantoic Membrane pathology, Embryo, Mammalian, Female, Humans, Infant, Newborn, Maternal Exposure adverse effects, Maternal-Fetal Exchange physiology, Metabolome, Neural Tube abnormalities, Neural Tube embryology, Pregnancy, Spinal Dysraphism etiology, Spinal Dysraphism pathology, Anencephaly metabolism, Energy Metabolism physiology, Glucose metabolism, Neural Tube metabolism, Spinal Dysraphism metabolism

Abstract

Neural tube closure (NTC) is an embryonic process during formation of the mammalian central nervous system. Disruption of the dynamic, sequential events of NTC can cause neural tube defects (NTD) leading to spina bifida and anencephaly in the newborn. NTC is affected by inherent factors such as genetic mutation or if the mother is exposed to certain environmental factors such as intake of harmful chemicals, maternal infection, irradiation, malnutrition, and inadequate or excessive intake of specific nutrients. Although effects of these stress factors on NTC have been intensively studied, the metabolic state of a normally developing embryo remains unclear. State-of-the art mass spectrometry techniques have enabled detailed study of embryonic metabolite profiles and their distribution within tissues. This approach has demonstrated that glucose metabolism is altered during NTC stages involving chorioallantoic branching. An understanding of embryonic metabolic rewiring would help reveal the etiology of NTD caused by environmental factors., (© 2017 Japanese Teratology Society.)

Published

2017

16. Medical cost savings in Sakado City and worldwide achieved by preventing disease by folic acid fortification.

Author

Kagawa Y, Hiraoka M, Kageyama M, Kontai Y, Yurimoto M, Nishijima C, and Sakamoto K

Subjects

Adult, Cost-Benefit Analysis, Female, Folic Acid administration & dosage, Folic Acid Deficiency epidemiology, Folic Acid Deficiency metabolism, Folic Acid Deficiency prevention & control, Food, Fortified statistics & numerical data, Humans, Infant, Newborn, Japan epidemiology, Methylenetetrahydrofolate Reductase (NADPH2) genetics, Methylenetetrahydrofolate Reductase (NADPH2) metabolism, Myocardial Infarction epidemiology, Myocardial Infarction metabolism, Myocardial Infarction prevention & control, Polymorphism, Genetic, Pregnancy, Prevalence, Recommended Dietary Allowances, Spinal Dysraphism epidemiology, Spinal Dysraphism metabolism, Spinal Dysraphism prevention & control, Dietary Supplements, Folic Acid metabolism, Folic Acid Deficiency economics, Food, Fortified economics, Myocardial Infarction economics, Spinal Dysraphism economics

Abstract

The introduction of mandatory fortification of grains with folate in 1998 in the United States resulted in 767 fewer spina bifida cases annually and a cost saving of $603 million per year. However, far more significant medical cost savings result from preventing common diseases, including myocardial infarction, stroke, dementia and osteoporosis. A cost-effectiveness analysis showed a gain of 266 649 quality-adjusted life-years and $3.6 billion saved annually, mainly due to the reduction of cardiac infarction. The recommended folate intake in Japan is 240 μg/day whereas it is 400 μg/day internationally. Our Sakado Folate Project targeted individuals with genetic polymorphism of methylenetetrahydrofolate reductase or with hyperhomocysteinemia. Using, for example, folate-fortified rice, resulted in an increase in serum folate and a decrease in serum homocysteine in the participants, and reduced medical costs were achieved by decreasing myocardial infarction, stroke, dementia and fracture. Due to the small population of Sakado City (approximately 101 000) and small number of births (693) in 2015, a decrease in spina bifida could not be confirmed but there was a significant decrease in the number of very low birthweight infants. The genome notification of subjects was effective in motivating intake of folate, but the increase in serum folate (from 17.4 to 22.5 nmol/L, 129%) was less than that observed following compulsory folic acid fortification of cereals in the USA (from 12.1 to 30.2 nmol/L, 149.6%). Mandatory folic acid fortification is cheap in decreasing medical costs and is thus recommended in Japan., (© 2017 The Authors. Congenital Anomalies published by John Wiley & Sons Australia, Ltd on behalf of Japanese Teratology Society.)

Published

2017

17. Clusters of amniotic fluid cells and their associated early neuroepithelial markers in experimental myelomeningocele: Correlation with astrogliosis.

Author

Zieba J, Miller A, Gordiienko O, Smith GM, and Krynska B

Subjects

Actins genetics, Animals, Cadherins genetics, Doublecortin Protein, Fetus, Gliosis diagnosis, Gliosis genetics, Gliosis physiopathology, Humans, Meningomyelocele diagnosis, Meningomyelocele physiopathology, PAX6 Transcription Factor genetics, Prenatal Diagnosis methods, Rats, Spinal Cord metabolism, Spinal Cord physiopathology, Spinal Cord Injuries diagnosis, Spinal Cord Injuries physiopathology, Spinal Dysraphism diagnosis, Spinal Dysraphism genetics, Spinal Dysraphism physiopathology, Stem Cells metabolism, Stem Cells pathology, Zonula Occludens-1 Protein genetics, Amniotic Fluid, Biomarkers, Meningomyelocele genetics, Spinal Cord Injuries genetics, Spinal Dysraphism metabolism

Abstract

Myelomeningocele (MMC) is the most common and severe disabling type of spina bifida resulting in the exposure of vulnerable spinal cord to the hostile intrauterine environment. In this study, we sought to examine the cellular content of fetal amniotic fluid (AF) in MMC and explore a correlation between these cells and pathological development of MMC. MMC was induced in fetal rats by exposing pregnant mothers to all-trans retinoic acid and AF samples were collected before term. Cells were isolated from AF samples and morphologically and phenotypically characterized in short-term cultures. In addition, the spinal cord injury in MMC fetuses was assessed by immunohistochemical examination of astrogliosis. We identified a population of cells from the AF of MMC fetuses (MMC-AF) that formed adherent clusters of tightly packed cells, which were absent from the AF of normal control fetuses (norm-AF). MMC-AF clusters contained cells co-expressing adherens junction associated proteins (ZO-1), N-cadherin and F-actin at sites of cell-cell contacts. In addition, they expressed markers of early neuroepithelial cells such as SOX-1 and Pax-6 along with other stem/progenitor cell markers such as SOX-2 and nestin. Subpopulations of cells in MMC-AF clusters also expressed more advanced differentiation markers such as doublecortin and GFAP. We found that the appearance of cluster forming cells in cultures from MMC-AF correlated with activation of astrogliosis associated with the spinal cord injury in MMC fetuses. In summary, we identified a neuroepithelial cell population in the AF of MMC fetuses that formed adherent clusters in culture and we characterized cellular markers of these cells. Our data suggests that the phase of the disease is a crucial factor in the emergence of these cells into the AF and that these cells may provide a new and important platform for studying the progression of MMC and development of improved strategies for the repair and diagnosis of MMC prenatally.

Published

2017

18. The enteric nervous system and the musculature of the colon are altered in patients with spina bifida and spinal cord injury.

Author

den Braber-Ymker M, Lammens M, van Putten MJ, and Nagtegaal ID

Subjects

Adolescent, Adult, Aged, Biomarkers metabolism, Case-Control Studies, Child, Child, Preschool, Colon metabolism, Colon physiopathology, Enteric Nervous System metabolism, Enteric Nervous System physiopathology, Female, Gastrointestinal Motility, Humans, Immunohistochemistry, Infant, Male, Middle Aged, Muscle, Smooth metabolism, Muscle, Smooth physiopathology, Spinal Cord Injuries metabolism, Spinal Cord Injuries physiopathology, Spinal Dysraphism metabolism, Spinal Dysraphism physiopathology, Young Adult, Colon pathology, Enteric Nervous System pathology, Muscle, Smooth pathology, Spinal Cord Injuries pathology, Spinal Dysraphism pathology

Abstract

Neurogenic bowel dysfunction occurs in a large percentage of adult patients with spina bifida (SB) and spinal cord injury (SCI), significantly affecting their quality of life. Although bowel motility is autonomously regulated by the enteric nervous system (ENS), disruption of the modulation of the ENS by extrinsic innervation as present in many patients with SB and SCI might lead to motility disorders. In order to gain insight in the pathophysiology, we studied histological changes of the neuromuscular structures in the colon of SB and SCI patients. Archival colon tissue blocks from SB (n = 13) and SCI (n = 34) patients were collected nationwide in The Netherlands and compared with control samples (n = 16). Histological (semiquantitative) evaluation of the ENS, the network of interstitial cells of Cajal (ICC), and the muscularis propria was performed using hematoxylin and eosin, periodic acid Schiff, and elastic von Gieson staining, and immunohistochemistry with antibodies against HuC/D, calretinin, S100, CD117, α-smooth muscle actin, and desmin. Compared to controls, SB and SCI patients showed neuronal loss and decreased nerve fiber density in the myenteric plexus. Lower nerve fiber density was significantly more often found in patients with severe bowel dysfunction. Other major findings were loss of ICCs around the myenteric plexus and fibrosis in the longitudinal muscle layer. Altered histology of the ENS may explain abnormal intestinal motility in SB and SCI patients. Furthermore, loss of myenteric nerve fibers (including enteric glial cells) may play a major role in the development of severe motility complaints., Competing Interests: Compliance with ethical standards Funding No funding declared. Conflict of interest The authors declare that they have no conflict of interest. Ethical approval The study has been approved by the institutional research committee (reference number 2014-1256). For this type of study, formal consent is not required.

Published

2017

19. Preliminary investigation of methylation status of microRNA-124a in spinal cords of rat fetuses with congenital spina bifida.

Author

Qin P, Li L, Zhang D, Liu QL, Chen XR, Yang HY, Fan Y, and Wang JX

Subjects

Animals, Biomarkers metabolism, Blotting, Western, Case-Control Studies, Down-Regulation, Female, Immunohistochemistry, Male, Methylation, Rats, Rats, Sprague-Dawley, Real-Time Polymerase Chain Reaction, Spinal Cord metabolism, Spinal Dysraphism metabolism, Gene Expression Regulation, Developmental, MicroRNAs metabolism, Spinal Cord embryology, Spinal Dysraphism embryology, Spinal Dysraphism genetics

Abstract

Objective: We investigated the expression of microRNA-124a and its methylation status in the spinal cords of rats with congenital spina bifida versus rats with normal fetuses., Methods: Real-time quantitative reverse transcription-polymerase chain reaction was used to compare the expression of microRNA-124a in the spinal cords of 42 rats with all-trans retinoic acid induced congenital spina bifida and 42 rats with normal fetuses. The DNA methylation status in the promoter region of miRNA-124a was detected using methylation specific-PCR., Results: Compared with rats with normal fetuses, expression of microRNA-124a was significantly decreased in rats with congenital spina bifida fetuses. The percentages of spinal cords with DNA hypermethylation in the microRNA-124a promoter were 81% and 14% in the congenital spina bifida and normal control groups, respectively. The difference was statistically significant. Further apoptosis testing revealed increased apoptosis cell numbers in the congenital spina bifida samples. Meanwhile, the phosphorylated mitogen-activated protein kinase protein expression level dramatically decreased in the congenital spina bifida samples., Conclusion: Aberrant DNA methylation was responsible for down-regulation of microRNA-124a by regulating the mitogen-activated protein kinase pathway, suggesting that microRNA-124a is a potential diagnostic biomarker in congenital spina bifida.

Published

2017

20. Formate supplementation enhances folate-dependent nucleotide biosynthesis and prevents spina bifida in a mouse model of folic acid-resistant neural tube defects.

Author

Sudiwala S, De Castro SC, Leung KY, Brosnan JT, Brosnan ME, Mills K, Copp AJ, and Greene ND

Subjects

Animals, Disease Models, Animal, Mice, Folic Acid metabolism, Formates pharmacology, Nucleotides biosynthesis, Spinal Dysraphism metabolism, Spinal Dysraphism prevention & control

Abstract

The curly tail mouse provides a model for neural tube defects (spina bifida and exencephaly) that are resistant to prevention by folic acid. The major ct gene, responsible for spina bifida, corresponds to a hypomorphic allele of grainyhead-like 3 (Grhl3) but the frequency of NTDs is strongly influenced by modifiers in the genetic background. Moreover, exencephaly in the curly tail strain is not prevented by reinstatement of Grhl3 expression. In the current study we found that expression of Mthfd1L, encoding a key component of mitochondrial folate one-carbon metabolism (FOCM), is significantly reduced in ct/ct embryos compared to a partially congenic wild-type strain. This expression change is not attributable to regulation by Grhl3 or the genetic background at the Mthfd1L locus. Mitochondrial FOCM provides one-carbon units as formate for FOCM reactions in the cytosol. We found that maternal supplementation with formate prevented NTDs in curly tail embryos and also resulted in increased litter size. Analysis of the folate profile of neurulation-stage embryos showed that formate supplementation resulted in an increased proportion of formyl-THF and THF but a reduction in proportion of 5-methyl THF. In contrast, THF decreased and 5-methyl THF was relatively more abundant in the liver of supplemented dams than in controls. In embryos cultured through the period of spinal neurulation, incorporation of labelled thymidine and adenine into genomic DNA was suppressed by supplemental formate, suggesting that de novo folate-dependent biosynthesis of nucleotides (thymidylate and purines) was enhanced. We hypothesise that reduced Mthfd1L expression may contribute to susceptibility to NTDs in the curly tail strain and that formate acts as a one-carbon donor to prevent NTDs., (Copyright © 2016 The Authors. Published by Elsevier B.V. All rights reserved.)

Published

2016

21. Spina bifida in fetus is associated with an altered pattern of DNA methylation in placenta.

Author

Zhang X, Pei L, Li R, Zhang W, Yang H, Li Y, Guo Y, Tan P, Han JJ, Zheng X, and Ma RZ

Subjects

Animals, CHO Cells, Cricetinae, Cricetulus, DNA-Binding Proteins genetics, Female, Humans, Male, Pregnancy, Spinal Dysraphism genetics, Tripartite Motif Proteins, Ubiquitin-Protein Ligases, DNA Methylation, DNA-Binding Proteins metabolism, Epigenesis, Genetic, Placenta metabolism, Spinal Dysraphism metabolism

Abstract

Failure in closure of neural tube leads to neural tube defects (NTDs), which are among the most common symptoms of human birth defects. Although epigenetic status in placenta is linked to fetal development, the mechanism behind this remains unknown. Because of the importance of DNA methylation in gene function, we set to explore whether or not DNA methylation in human placenta is also linked to fetal NTDs. Here we show for the first time that alteration of DNA methylation in placenta is closely associated with the phenotypes of fetal spina bifida (Sb). We found that patterns of DNA methylation for genes in neurological system process were differentially altered in the Sb placenta. In particular, the transcription regulatory regions of TRIM26 and GANS were kept at the hypomethylation status in Sb placenta alone. Accordingly, the protein levels of TRIM26 and GNAS were significantly elevated only in the Sb placenta but not in the Sb-affected fetuses. In cellular model of CHO cells deficient in Dihydrofolate reductase and treated with 5-aza-2'-deoxycytidine, the protein levels of GNAS and TRIM26 were significantly higher than those in normal control cells. These findings suggested that epigenetic status of genes in placenta have profound impacts on the development of NTDs.

Published

2015

22. Risk of fracture prevention in spina bifida patients: correlation between bone mineral density, vitamin D, and electrolyte values.

Author

Martinelli V, Dell'Atti C, Ausili E, Federici E, Magarelli N, Leone A, Massimi L, Di Rocco C, Bonomo L, and Rendeli C

Subjects

Absorptiometry, Photon, Adolescent, Child, Child, Preschool, Female, Humans, Male, Young Adult, Bone Density physiology, Electrolytes metabolism, Fractures, Bone etiology, Fractures, Bone prevention & control, Spinal Dysraphism complications, Spinal Dysraphism metabolism, Vitamin D metabolism

Abstract

Purpose: The aim of our study was to investigate the relationship between bone mineral density (BMD), vitamin D, and electrolyte blood values in patients with spina bifida, to find a possible therapeutic regimen and an intervention to reduce the risk of fractures in this population., Methods: BMD values were measured in 49 patients (32 females, 17 males; aged 14.1 ± 3.86 years; range 5-20 years) using dual-energy X-ray absorptiometry (DEXA) and were analyzed based on sex, the level of spinal involvement, vitamin D, and electrolyte values, physical activity, body mass index (BMI), and ambulatory status [patients were divided into three subgroups: full-time wheelchair (FTWC), limited ambulator (LA), and full-time ambulator (FTA)]. These data were analyzed considering sex-, age-, and BMD-matched values and compared with those of normal population., Results: BMD was significantly lower in these patients compared with that in the general healthy population (Z-score: -1.2 ± 1.8); in particular, females had Z-score values significantly lower that of the males (Z-score: -2.43 ± 2.02; P < 0.0004). In FTWC subgroup, Z-score was lower than that of the other two subgroups (P < 0.009). Vitamin D values were significantly lower compared with those in the general healthy population (vitamin D spina bifida group: 14.6 ± 8.7 mg/dL; normal subjects: 35 ± 9.8 mg/dL; P < 0.001). Subjects with spina bifida showed hypophosphatemia (<3 mg/dL) because of the lower levels of vitamin D (3.1 ± 0.9 mg/dL; P < 0.001)., Conclusions: Spina bifida patients showed lower BMD, vitamin D, and electrolyte values than the healthy population; hence, they have an increase risk of developing pathological fractures. Vitamin D supplementation for a longer time period could reduce this risk.

Published

2015

23. An integrative computational approach for prioritization of genomic variants.

Author

Dubchak I, Balasubramanian S, Wang S, Cem M, Sulakhe D, Poliakov A, Börnigen D, Xie B, Taylor A, Ma J, Paciorkowski AR, Mirzaa GM, Dave P, Agam G, Xu J, Al-Gazali L, Mason CE, Ross ME, Maltsev N, and Gilliam TC

Subjects

Child, Female, Folic Acid metabolism, Genomics methods, Humans, Models, Molecular, Pregnancy, Protein Conformation, Reduced Folate Carrier Protein chemistry, Reduced Folate Carrier Protein metabolism, Software, Spinal Dysraphism metabolism, Mutation, Reduced Folate Carrier Protein genetics, Spinal Dysraphism genetics

Abstract

An essential step in the discovery of molecular mechanisms contributing to disease phenotypes and efficient experimental planning is the development of weighted hypotheses that estimate the functional effects of sequence variants discovered by high-throughput genomics. With the increasing specialization of the bioinformatics resources, creating analytical workflows that seamlessly integrate data and bioinformatics tools developed by multiple groups becomes inevitable. Here we present a case study of a use of the distributed analytical environment integrating four complementary specialized resources, namely the Lynx platform, VISTA RViewer, the Developmental Brain Disorders Database (DBDB), and the RaptorX server, for the identification of high-confidence candidate genes contributing to pathogenesis of spina bifida. The analysis resulted in prediction and validation of deleterious mutations in the SLC19A placental transporter in mothers of the affected children that causes narrowing of the outlet channel and therefore leads to the reduced folate permeation rate. The described approach also enabled correct identification of several genes, previously shown to contribute to pathogenesis of spina bifida, and suggestion of additional genes for experimental validations. The study demonstrates that the seamless integration of bioinformatics resources enables fast and efficient prioritization and characterization of genomic factors and molecular networks contributing to the phenotypes of interest.

Published

2014

24. Association of neural tube defects in children of mothers with MTHFR 677TT genotype and abnormal carbohydrate metabolism risk: a case-control study.

Author

Cadenas-Benitez NM, Yanes-Sosa F, Gonzalez-Meneses A, Cerrillos L, Acosta D, Praena-Fernandez JM, Neth O, Gomez de Terreros I, and Ybot-González P

Subjects

Adult, Alleles, Case-Control Studies, Female, Genetic Association Studies, Homocysteine blood, Humans, Incidence, Neural Tube Defects epidemiology, Pregnancy, Risk Factors, Spinal Dysraphism epidemiology, Spinal Dysraphism genetics, Spinal Dysraphism metabolism, Young Adult, Carbohydrate Metabolism, Genotype, Methylenetetrahydrofolate Reductase (NADPH2) genetics, Mothers, Neural Tube Defects genetics, Neural Tube Defects metabolism, Polymorphism, Single Nucleotide

Abstract

Abnormalities in maternal folate and carbohydrate metabolism have both been shown to induce neural tube defects (NTD) in humans and animal models. However, the relationship between these two factors in the development of NTDs remains unclear. Data from mothers of children with spina bifida seen at the Unidad de Espina Bífida del Hospital Infantil Virgen del Rocío (case group) were compared to mothers of healthy children with no NTD (control group) who were randomly selected from patients seen at the outpatient ward in the same hospital. There were 25 individuals in the case group and 41 in the control group. Analysis of genotypes for the methylenetetrahydrofolate reductase (MTHFR) 677CT polymorphism in women with or without risk factors for abnormal carbohydrate metabolism revealed that mothers who were homozygous for the MTHFR 677TT polymorphism and at risk of abnormal carbohydrate metabolism were more likely to have offspring with spina bifida and high levels of homocysteine, compared to the control group. The increased incidence of NTDs in mothers homozygous for the MTHFR 677TT polymorphism and at risk of abnormal carbohydrate metabolism stresses the need for careful metabolic screening in pregnant women, and, if necessary, determination of the MTHFR 677CT genotype in those mothers at risk of developing abnormal carbohydrate metabolism.

Published

2014

25. Identification of novel CELSR1 mutations in spina bifida.

Author

Lei Y, Zhu H, Yang W, Ross ME, Shaw GM, and Finnell RH

Subjects

Animals, Base Sequence, Cadherins metabolism, Cell Membrane metabolism, DNA Mutational Analysis, Dogs, HEK293 Cells, Humans, Infant, Intracellular Signaling Peptides and Proteins metabolism, Madin Darby Canine Kidney Cells, Membrane Proteins metabolism, Mice, Protein Transport, Spinal Dysraphism metabolism, Spinal Dysraphism pathology, Cadherins genetics, Mutation, Spinal Dysraphism genetics

Abstract

Spina bifida is one of the most common neural tube defects (NTDs) with a complex etiology. Variants in planar cell polarity (PCP) genes have been associated with NTDs including spina bifida in both animal models and human cohorts. In this study, we sequenced all exons of CELSR1 in 192 spina bifida patients from a California population to determine the contribution of CELSR1 mutations in the studied population. Novel and rare variants identified in these patients were subsequently genotyped in 190 ethnically matched control individuals. Six missense mutations not found in controls were predicted to be deleterious by both SIFT and PolyPhen. Two TG dinucleotide repeat variants were individually detected in 2 spina bifida patients but not detected in controls. In vitro functional analysis showed that the two TG dinucleotide repeat variants not only changed subcellular localization of the CELSR1 protein, but also impaired the physical association between CELSR1 and VANGL2, and thus diminished the ability to recruit VANGL2 for cell-cell contact. In total, 3% of our spina bifida patients carry deleterious or predicted to be deleterious CELSR1 mutations. Our findings suggest that CELSR1 mutations contribute to the risk of spina bifida in a cohort of spina bifida patients from California.

Published

2014

26. Physiological relevance of LL-37 induced bladder inflammation and mast cells.

Author

Oottamasathien S, Jia W, Roundy LM, Zhang J, Wang L, Ye X, Hill AC, Savage J, Lee WY, Hannon AM, Milner S, and Prestwich GD

Subjects

Adolescent, Animals, Antimicrobial Cationic Peptides toxicity, Cell Count, Child, Child, Preschool, Cystitis etiology, Cystitis pathology, Disease Models, Animal, Enzyme-Linked Immunosorbent Assay, Female, Humans, Immunohistochemistry, Infant, Infant, Newborn, Lipopolysaccharides, Male, Mast Cells pathology, Mice, Mice, Inbred C57BL, Spinal Dysraphism complications, Spinal Dysraphism pathology, Urothelium metabolism, Urothelium pathology, Cathelicidins, Antimicrobial Cationic Peptides metabolism, Cystitis metabolism, Mast Cells metabolism, Spinal Dysraphism metabolism

Abstract

Purpose: We established the physiological relevance of LL-37 induced bladder inflammation. We hypothesized that 1) human urinary LL-37 is increased in pediatric patients with spina bifida, 2) LL-37 induced inflammation occurs in our mouse model via urothelial binding and is dose dependent and 3) LL-37 induced inflammation involves mast cells., Materials and Methods: To test our first hypothesis, we obtained urine samples from 56 pediatric patients with spina bifida and 22 normal patients. LL-37 was measured by enzyme-linked immunosorbent assay. Our second hypothesis was tested in C57Bl/6 mice challenged with 7 LL-37 concentrations intravesically for 1 hour. At 24 hours tissues were examined histologically and myeloperoxidase assay was done to quantitate inflammation. In separate experiments fluorescent LL-37 was instilled and tissues were obtained immediately (time = 0) and at 24 hours (time = 24). To test our final hypothesis, we performed immunohistochemistry for mast cell tryptase and evaluated 5 high power fields per bladder to determine the mean number of mast cells per mm(2)., Results: Urinary LL-37 was 89-fold higher in patients with spina bifida. Mouse LL-37 dose escalation experiments revealed increased inflammation at higher LL-37 concentrations. Fluorescent LL-37 demonstrated global urothelial binding at time = 0 but was not visible at time = 24. Immunohistochemistry for tryptase revealed mast cell infiltration in all tissue layers. At higher concentrations the LL-37 challenge led to significantly greater mast cell infiltration., Conclusions: Urinary LL-37 was significantly increased in pediatric patients with spina bifida. To our knowledge we report for the first time that LL-37 can elicit profound, dose dependent bladder inflammation involving the urothelium. Finally, inflammation propagation involves mast cells., (Copyright © 2013 American Urological Association Education and Research, Inc. Published by Elsevier Inc. All rights reserved.)

Published

2013

27. Editorial comment.

Author

Manson SR

Subjects

Animals, Female, Humans, Male, Cathelicidins, Antimicrobial Cationic Peptides metabolism, Cystitis metabolism, Mast Cells metabolism, Spinal Dysraphism metabolism

Published

2013

28. miR-9*- and miR-124a-Mediated switching of chromatin remodelling complexes is altered in rat spina bifida aperta.

Author

Wei X, Li H, Miao J, Liu B, Zhan Y, Wu D, Zhang Y, Wang L, Fan Y, Gu H, Wang W, and Yuan Z

Subjects

Animals, Base Sequence, DNA Primers, Female, Gene Expression Regulation, Male, Pregnancy, Rats, Rats, Wistar, Chromatin Assembly and Disassembly, MicroRNAs physiology, Spinal Dysraphism metabolism

Abstract

Neural tube defects (NTDs) are complex congenital malformations resulting from incomplete neurulation. Our previous work has demonstrated that motor and sensory neurons develop defectively in rat embryos with spina bifida aperta. To identify whether neural development-associated miRNAs play a role in the neurological deficits of NTDs, we screened a panel of neural development-related miRNAs, including miR-9, miR-9*, miR-124a, miR-10a, miR10b, miR-34a, miR-221 and miR-222, in the spinal cords of rats with retinoic acid-induced spina bifida aperta. We discovered that the expression of miR-9, miR-9* and miR-124a was specifically down-regulated compared to spinal cords without spina bifida. To further clarify whether down-regulation of miR-9* and miR-124a contributes to the neurological deficits of NTDs, we investigated the levels of genes involved in switching in the subunit composition of Swi/Snf-like BAF (Brg/Brm associated factor) complexes modulated by miR-9* and miR-124a and neuronal differentiation. In addition to the down-regulation of miR-9* and miR-124a expression, we also observed increased expression of repressor element silencing transcription factor (REST) and BAF53a and decreased expression of BAF53b, Brg1 and NeuroD1. Our results suggest that REST-regulated miR-9*- and the miR-124a-mediated chromatin remodelling regulatory mechanism may participate in the neuronal deficits of spina bifida.

Published

2013

29. The role of amino acids in spina bifida.

Author

Kale A and Kale E

Subjects

Adult, Alanine analysis, Amniocentesis, Cystathionine analysis, Cysteine analysis, Female, Gestational Age, Humans, Phenylalanine analysis, Pregnancy, Pregnancy Trimester, Second, Spinal Dysraphism diagnostic imaging, Spinal Dysraphism etiology, Tryptophan analysis, Tyrosine analysis, Ultrasonography, Prenatal, Amino Acids analysis, Amniotic Fluid chemistry, Spinal Dysraphism metabolism

Abstract

Our objective was to measure amniotic fluid amino acid concentrations in pregnant women diagnosed as having fetuses with spina bifida in the second trimester of pregnancy. Fifteen pregnant women who had fetuses with spina bifida detected by ultrasonography (spina bifida group) in the second trimester and 19 women who had abnormal triple screenings indicating an increased risk for Down's syndrome but had healthy fetuses (control group) were enrolled in the study. Amniotic fluid was obtained by amniocentesis. The chromosomal analysis of the study and control groups was normal. Levels of free amino acids were measured in amniotic fluid samples using EZ: fast kits (EZ: fast GC/FID free (physiological) amino acid kit) by gas chromatography (Focus GC AI 3000 Thermo Finnigan analyzer). The mean levels of alanine, cystathionine, cysteine, phenylalanine, tryptophane, and tyrosine amino acids were found to be significantly higher in fetuses of the control group than in the spina bifida group (p<0.05). The detection of significantly higher amino acid concentrations in the amniotic fluid of healthy fetuses suggests loss of amino acids from the fetus through the spinal cord may contribute to the etiology of spina bifida.

Published

2012

30. Genetic and lifestyle variables associated with homocysteine concentrations and the distribution of folate derivatives in healthy premenopausal women.

Author

Summers CM, Mitchell LE, Stanislawska-Sachadyn A, Baido SF, Blair IA, Von Feldt JM, and Whitehead AS

Subjects

5-Methyltetrahydrofolate-Homocysteine S-Methyltransferase genetics, Adolescent, Adult, Black or African American genetics, Child, Child, Preschool, Dietary Supplements, Erythrocytes chemistry, Female, Genetic Association Studies, Homocysteine genetics, Humans, Infant, Membrane Transport Proteins genetics, Methylenetetrahydrofolate Reductase (NADPH2) genetics, Middle Aged, Polymorphism, Genetic, Pregnancy, Premenopause genetics, Spinal Dysraphism epidemiology, Spinal Dysraphism etiology, Spinal Dysraphism genetics, Spinal Dysraphism metabolism, Tetrahydrofolates analysis, Thymidylate Synthase genetics, Vitamins administration & dosage, White People genetics, Young Adult, Homocysteine blood, Life Style, Premenopause metabolism

Abstract

Background: Low folate and high homocysteine (Hcy) concentrations are associated with pregnancy-related pathologies such as spina bifida. Polymorphisms in folate/Hcy metabolic enzymes may contribute to this potentially pathogenic biochemical phenotype., Methods: The study comprised 26 Caucasian and 23 African-American premenopausal women. Subjects gave fasting blood samples for biochemical phenotyping and genotyping. Total Hcy (tHcy) and both plasma and red blood cell (RBC) folate derivatives (i.e. tetrahydrofolate [THF], 5-methylTHF [5-MTHF], and 5,10-methenylTHF [5,10-MTHF]) were measured using stable isotope dilution liquid chromatography, multiple reaction monitoring, and mass spectrometry. Eleven polymorphisms from nine folate/Hcy pathway genes were genotyped. Tests of association between genetic, lifestyle, and biochemical variables were applied., Results: In African American women, tHcy concentrations were associated (p < 0.05) with total RBC folate, RBC 5-MTHF, B(12), and polymorphisms in methionine synthase (MTR) and thymidylate synthase (TYMS). In Caucasian women, tHcy concentrations were not associated with total folate levels, but were associated (p < 0.05) with RBC THF, ratios of RBC 5-MTHF:THF, and polymorphisms in 5,10-methylenetetrahydrofolate reductase (MTHFR) and MTR. In African Americans, folate derivative levels were associated with smoking, B(12), and polymorphisms in MTR, TYMS, methionine synthase reductase (MTRR), and reduced folate carrier1 (RFC1). In Caucasians, folate derivative levels were associated with vitamin use, B(12), and polymorphisms in MTHFR, TYMS, and RFC1., Conclusions: Polymorphisms in the folate/Hcy pathway are associated with tHcy and folate derivative levels. In African American and Caucasian women, different factors are associated with folate/Hcy phenotypes and may contribute to race-specific differences in the risks of a range of pregnancy-related pathologies.

Published

2010

31. Epidemiologic and genetic aspects of spina bifida and other neural tube defects.

Author

Au KS, Ashley-Koch A, and Northrup H

Subjects

Birth Order, Ethnicity statistics & numerical data, Female, Fever epidemiology, Folic Acid Deficiency epidemiology, Folic Acid Deficiency metabolism, Gene Expression, Genome-Wide Association Study, Genotype, Glucose metabolism, Humans, Meningomyelocele epidemiology, Meningomyelocele genetics, Meningomyelocele metabolism, Neural Tube Defects metabolism, Parents, Phenotype, Pregnancy, Pregnancy Complications epidemiology, Pregnancy Trimester, First, Prenatal Diagnosis, Socioeconomic Factors, Spinal Dysraphism epidemiology, Spinal Dysraphism genetics, Spinal Dysraphism metabolism, Vitamin B 12 Deficiency epidemiology, Vitamin B 12 Deficiency metabolism, Neural Tube Defects epidemiology, Neural Tube Defects genetics

Abstract

The worldwide incidence of neural tube defects (NTDs) ranges from 1.0 to 10.0 per 1,000 births with almost equal frequencies between two major categories: anencephaly and spina bifida (SB). Epidemiological studies have provided valuable insight for (a) researchers to identify nongenetic and genetic factors contributing to etiology, (b) public health officials to design and implement policies to prevent NTD pregnancies, and (c) individuals to take precautions to reduce the chance of having an NTD-affected pregnancy. Despite extensive research, our knowledge of the genetic etiology of human NTDs is limited. Although more than 200 small animal models with NTDs exist, most of these models do not replicate the human disease phenotype. Over a hundred candidate genes have been examined for risk association to human SB. The candidate genes studied include those important in folic acid metabolism, glucose metabolism, retinoid metabolism, and apoptosis. Many genes that regulate transcription in early embryogenesis and maintain planar cell polarity have also been tested as candidates. Additionally, genes identified through mouse models of NTDs have been explored as candidates. We do not know how many genes in the human genome may confer risk for NTDs in human. Less than 20% of the studied candidate genes have been determined to confer even a minor effect on risk association. Many studies have provided conflicting conclusions due to limitations in study design that potentially affect the power of statistical analysis. Future directions such as genomewide association studies (GWAS) and whole exome or even whole genome sequencing are discussed as possible avenues to identify genes that affect risk for human NTDs.

Published

2010

32. Mouse hitchhiker mutants have spina bifida, dorso-ventral patterning defects and polydactyly: identification of Tulp3 as a novel negative regulator of the Sonic hedgehog pathway.

Author

Patterson VL, Damrau C, Paudyal A, Reeve B, Grimes DT, Stewart ME, Williams DJ, Siggers P, Greenfield A, and Murdoch JN

Subjects

Animals, Embryo, Mammalian, Female, Gene Expression Regulation, Developmental, Hedgehog Proteins genetics, Humans, Intercellular Signaling Peptides and Proteins, Intracellular Signaling Peptides and Proteins, Male, Mice, Mice, Inbred C3H, Mice, Inbred C57BL, Mutation, Neural Tube embryology, Neural Tube metabolism, Polydactyly embryology, Polydactyly genetics, Proteins genetics, Spinal Cord embryology, Spinal Cord metabolism, Spinal Dysraphism embryology, Spinal Dysraphism genetics, Body Patterning, Down-Regulation, Hedgehog Proteins metabolism, Polydactyly metabolism, Proteins metabolism, Signal Transduction, Spinal Dysraphism metabolism

Abstract

The mammalian Sonic hedgehog (Shh) signalling pathway is essential for embryonic development and the patterning of multiple organs. Disruption or activation of Shh signalling leads to multiple birth defects, including holoprosencephaly, neural tube defects and polydactyly, and in adults results in tumours of the skin or central nervous system. Genetic approaches with model organisms continue to identify novel components of the pathway, including key molecules that function as positive or negative regulators of Shh signalling. Data presented here define Tulp3 as a novel negative regulator of the Shh pathway. We have identified a new mouse mutant that is a strongly hypomorphic allele of Tulp3 and which exhibits expansion of ventral markers in the caudal spinal cord, as well as neural tube defects and preaxial polydactyly, consistent with increased Shh signalling. We demonstrate that Tulp3 acts genetically downstream of Shh and Smoothened (Smo) in neural tube patterning and exhibits a genetic interaction with Gli3 in limb development. We show that Tulp3 does not appear to alter expression or processing of Gli3, and we demonstrate that transcriptional regulation of other negative regulators (Rab23, Fkbp8, Thm1, Sufu and PKA) is not affected. We discuss the possible mechanism of action of Tulp3 in Shh-mediated signalling in light of these new data.

Published

2009

33. The roles of p53 and p21 in normal development and hyperthermia-induced malformations.

Author

Hosako H, Francisco LE, Martin GS, and Mirkes PE

Subjects

Animals, Cyclin-Dependent Kinase Inhibitor p21 metabolism, Female, Genotype, Mice, Mice, Knockout, Neural Tube Defects etiology, Neural Tube Defects metabolism, Pregnancy, Spinal Dysraphism etiology, Spinal Dysraphism metabolism, Tumor Suppressor Protein p53 metabolism, Cyclin-Dependent Kinase Inhibitor p21 genetics, Embryonic Development genetics, Fever, Gene Expression Regulation, Developmental, Neural Tube Defects genetics, Spinal Dysraphism genetics, Tumor Suppressor Protein p53 genetics

Abstract

Background: Hyperthermia (HS) is a well-studied teratogen that induces serious malformations, including neural tube defects. Our previous studies have shown that HS induces apoptosis by activating the mitochondrial apoptotic pathway. Prior to activation of the mitochondrial apoptotic pathway, HS also activates p53 and its target genes. In the present study, we determine whether p53 and/or p21 play a role as teratogen suppressors or inducers of HS-induced malformations., Methods: Pregnant mice carrying all three p53 or p21 genotype embryos were exposed to HS on day 8.5. Subsequently, fetuses were collected on day 15.5, and genotyped. In addition to genotype, we also determined the number of resorptions and dead fetuses as well as the number and types of external malformations., Results: In the absence of HS exposure, fetuses exhibiting exencephaly and spina bifida were observed in approximately 11% of p53 -/- fetuses, whereas no malformations were observed among p21 -/- fetuses. Exposure to HS resulted in an increase in exencephaly and polydactyly in fetuses of all three p53 genotypes. However, the incidence of these malformations was statistically significantly higher in p53 -/- compared to p53 +/- and p53 +/+ fetuses. Exencephaly was the only malformation observed in p21 fetuses exposed to HS, with an approximately 2-fold increase among p21 +/- and a 3-fold increase among p21 -/- compared to p21 +/+ fetuses., Conclusions: Our study confirms that p53 plays a role in normal development and has shown, for the first time that p53 and p21 function to suppress HS-induced malformations., ((c) 2009 Wiley-Liss, Inc.)

Published

2009

34. Corticosteroids reduce glial fibrillary acidic protein expression in response to spinal cord injury in a fetal rat model of dysraphism.

Author

Melo-Filho AA, Weber Guimarães Barreto M, Capelli Nassr AC, Rogério F, Langone F, Pereira LA, and Sbragia L

Subjects

Animals, Biomarkers metabolism, Disease Models, Animal, Female, Gliosis drug therapy, Gliosis metabolism, Gliosis pathology, Male, Pregnancy, Rats, Rats, Sprague-Dawley, Spinal Cord metabolism, Spinal Cord pathology, Spinal Cord Injuries pathology, Spinal Dysraphism pathology, Adrenal Cortex Hormones pharmacology, Glial Fibrillary Acidic Protein metabolism, Spinal Cord Injuries drug therapy, Spinal Cord Injuries metabolism, Spinal Dysraphism drug therapy, Spinal Dysraphism metabolism

Abstract

Background: Exposure of the spinal cord in myelomeningocele (MM) throughout gestation increases spinal injury. Astrocyte activation evidenced by glial fibrillary acidic proteins (GFAP) indicates the extent of injury. Corticosteroids modulate GFAP synthesis, but their effect in MM is unclear. The purpose of this study was to evaluate the GFAP expression in a fetal rat model of dysraphism and the effect of corticosteroid treatment on this marker and on clinical neurological disabilities., Methods: Dysraphism was surgically created in 2 groups of 48 rat fetuses; group 1: control, and group 2: treated with corticosteroid. Each group was subdivided into fetuses with surgically created MM, controls and shams on day 18.5 of gestation (term = 22 days). Fetuses were harvested on day 21.5, examined for evidence of neurological deficits, and the following clinical parameters were registered: kyphosis, tail deformities, leg deformities, leg paralysis or paresis and pain perception. The fetuses were fixed for GFAP immunostaining., Results: All fetuses with MM in group 1 presented neurological deficits and glial reactions with GFAP expression, as opposed to controls and shams. In group 2, corticosteroid treatment prevented some neurological deficits (18-25%), reducing glial response and GFAP expression., Conclusions: Experimentally induced dysraphism in the rat fetus is related to glial response and increased GFAP expression in the spinal cord. Corticoid treatment clinically improved nerve injury in some fetuses. It reduced glial reaction and GFAP expression., (Copyright 2009 S. Karger AG, Basel.)

Published

2009

35. Spina bifida before and after folic acid fortification in Canada.

Author

De Wals P, Tairou F, Van Allen MI, Lowry RB, Evans JA, Van den Hof MC, Crowley M, Uh SH, Zimmer P, Sibbald B, Fernandez B, Lee NS, and Niyonsenga T

Subjects

Canada epidemiology, Female, Humans, Male, Pregnancy, Prevalence, Retrospective Studies, Spinal Dysraphism metabolism, Spinal Dysraphism prevention & control, Folic Acid administration & dosage, Folic Acid physiology, Food, Fortified, Spinal Dysraphism epidemiology

Abstract

Background: In 1998, fortification of a large variety of cereal products with folic acid became mandatory in Canada. A multicentric study was carried out to assess the impact of this policy on the frequency of NTDs. The present analysis focused on spina bifida., Methods: The study population included approximately 2 million livebirths, stillbirths, and terminations of pregnancies because of fetal anomalies among women residing in seven Canadian provinces, from 1993 to 2002. Spina bifida cases were divided according to the upper limit of the defect: upper (cranial, cervical, or thoracic) and lower (lumbar or sacral) defects. Based on published results of red blood cell folate tests, the study period was divided into prefortification, partial fortification, and full fortification periods., Results: A total of 1,286 spina bifida cases were identified: 51% livebirths, 3% stillbirths, and 46% terminations. Prevalence decreased from 0.86/1,000 in the prefortification to 0.40 in the full fortification period, while the proportion of upper defects decreased from 32% to 13%. Following fortification, regional variations in the prevalence and distribution of sites almost disappeared., Conclusions: Results confirmed the etiologic heterogeneity of spina bifida and the more pronounced effect of folic acid in decreasing the risk of the more severe clinical presentations., ((c) 2008 Wiley-Liss, Inc.)

Published

2008

36. Hyperglycemic condition disturbs the proliferation and cell death of neural progenitors in mouse embryonic spinal cord.

Author

Gao Q and Gao YM

Subjects

Animals, Apoptosis drug effects, Apoptosis physiology, Caspase 3 metabolism, Cell Differentiation drug effects, Cell Differentiation physiology, Cell Proliferation drug effects, Cells, Cultured, Diabetes Complications metabolism, Diabetes Mellitus, Experimental complications, Diabetes Mellitus, Experimental metabolism, Diabetes Mellitus, Experimental physiopathology, Enzyme Activation drug effects, Enzyme Activation physiology, Female, Glucose toxicity, Mice, Nervous System Malformations etiology, Nervous System Malformations metabolism, Nervous System Malformations physiopathology, Neurons drug effects, Neurons metabolism, Pregnancy, Prenatal Exposure Delayed Effects metabolism, Prenatal Exposure Delayed Effects physiopathology, Spinal Cord metabolism, Spinal Dysraphism metabolism, Stem Cells drug effects, Diabetes Complications physiopathology, Hyperglycemia complications, Spinal Cord abnormalities, Spinal Dysraphism etiology, Spinal Dysraphism physiopathology, Stem Cells metabolism

Abstract

Spina bifida, which results from failure of fusion in the spinal region of neural tube, is among the most common birth defects associated with diabetic pregnancy. However, the mechanism underlying maternal diabetes-induced congenital malformations including spina bifida is not fully understood. It was hypothesized that hyperglycemic conditions affect the proliferation and apoptosis of neural progenitor cells in the developing spinal neural tube, leading to abnormal neurodevelopment. In the present study, biological processes such as proliferation and apoptosis were investigated in the neuroepithelial cells of the developing spinal neural tube of embryos from diabetic mice, and in embryonic spinal neural tube derived neural progenitor cell cultures exposed to high glucose in vitro. Maternal diabetes caused decreased proliferation and increased apoptosis of the neuroepithelial cells in the developing spinal cord of embryos from diabetic mouse. Decreased proliferation and increased apoptosis were also found in neural progenitor cells exposed to high glucose. In addition, high glucose-induced apoptosis in neural progenitor cells was associated with activation of caspase-3. Thus, high glucose disturbs both proliferation and cell death of neural progenitors in the developing spinal neural tube. This could provide a cellular mechanism by which maternal hyperglycemia induces spina bifida in embryos from diabetic pregnancy.

Published

2007

37. Variation and expression of dihydrofolate reductase (DHFR) in relation to spina bifida.

Author

van der Linden IJ, Nguyen U, Heil SG, Franke B, Vloet S, Gellekink H, den Heijer M, and Blom HJ

Subjects

5' Untranslated Regions metabolism, Adolescent, Adult, Case-Control Studies, Cell Line, Female, Homocysteine blood, Humans, Male, Middle Aged, Population Groups, Reverse Transcriptase Polymerase Chain Reaction, Risk Factors, Sequence Deletion, Spinal Dysraphism metabolism, Tetrahydrofolate Dehydrogenase metabolism, Genetic Variation, Spinal Dysraphism enzymology, Tetrahydrofolate Dehydrogenase genetics

Abstract

The dihydrofolate reductase (DHFR) enzyme is important for folate availability, folate turnover and DNA synthesis. The 19-bp deletion in intron-1 of DHFR has been associated with the risk of having spina bifida affected offspring, supposedly by changing DHFR gene expression. A 9-bp repeat in exon 1 of the mutS homolog 3 (MSH3) gene was recently demonstrated to be also located in the 5'UTR of DHFR and may possibly affect DHFR gene expression as well. We examined the association between these DHFR variants and spina bifida risk and investigated their effect on DHFR expression. Our study population, consisting of 121 mothers of a spina bifida affected child, 109 spina bifida patients, 292 control women and 234 pediatric controls was screened for the DHFR 19-bp deletion and the DHFR 9-bp repeat. DHFR gene expression was measured in 66 spina bifida patients, using real-time PCR analysis. In this study population, the DHFR 19-bp del/del genotype was not associated with spina bifida risk in mothers and children (OR: 0.8; 95%CI: 0.4-1.5 and OR: 1.2; 95%CI: 0.6-2.2, respectively) and both the WT/del and the del/del genotype did not affect DHFR expression relative to the WT/WT genotype (relative expression=0.89, p=0.46 and relative expression=1.26, p=0.24, respectively). The DHFR 9-bp repeat was not associated with spina bifida risk in mothers and children. DHFR expression of the 6/6 allele was 73% increased compared to the 3/3 allele, although not significantly (relative expression=1.73, p=0.09). We did not find evidence for an effect of the DHFR 19-bp deletion or 9-bp repeat on spina bifida risk in mothers and children. An effect of the 6/6 repeat genotype on DHFR expression cannot be ruled out.

Published

2007

38. Abnormal folate metabolism in foetuses affected by neural tube defects.

Author

Dunlevy LP, Chitty LS, Burren KA, Doudney K, Stojilkovic-Mikic T, Stanier P, Scott R, Copp AJ, and Greene ND

Subjects

Anencephaly embryology, Anencephaly metabolism, Animals, Antimetabolites pharmacology, Deoxyuridine pharmacology, Female, Ferredoxin-NADP Reductase genetics, Fetus drug effects, Fibroblasts metabolism, Folic Acid genetics, Genotype, Humans, Methylation, Mice, NIH 3T3 Cells, Neural Tube Defects embryology, Neural Tube Defects genetics, Polymorphism, Genetic genetics, Pregnancy, S-Adenosylhomocysteine analysis, S-Adenosylmethionine analysis, Spinal Dysraphism embryology, Spinal Dysraphism metabolism, Fetal Diseases metabolism, Fetus metabolism, Folic Acid metabolism, Neural Tube Defects metabolism

Abstract

Folic acid supplementation can prevent many cases of neural tube defects (NTDs), whereas suboptimal maternal folate status is a risk factor, suggesting that folate metabolism is a key determinant of susceptibility to NTDs. Despite extensive genetic analysis of folate cycle enzymes, and quantification of metabolites in maternal blood, neither the protective mechanism nor the relationship between maternal folate status and susceptibility are understood in most cases. In order to investigate potential abnormalities in folate metabolism in the embryo itself, we derived primary fibroblastic cell lines from foetuses affected by NTDs and subjected them to the dU suppression test, a sensitive metabolic test of folate metabolism. Significantly, a subset of NTD cases exhibited low scores in this test, indicative of abnormalities in folate cycling that may be causally linked to the defect. Susceptibility to NTDs may be increased by suppression of the methylation cycle, which is interlinked with the folate cycle. However, reduced efficacy in the dU suppression test was not associated with altered abundance of the methylation cycle intermediates, s-adenosylmethionine and s-adenosylhomocysteine, suggesting that a methylation cycle defect is unlikely to be responsible for the observed abnormality of folate metabolism. Genotyping of samples for known polymorphisms in genes encoding folate-associated enzymes did not reveal any correlation between specific genotypes and the observed abnormalities in folate metabolism. These data suggest that as yet unrecognized genetic variants result in embryonic abnormalities of folate cycling that may be causally related to NTDs.

Published

2007

39. Metabolic syndrome in adolescents with spinal cord dysfunction.

Author

Nelson MD, Widman LM, Abresch RT, Stanhope K, Havel PJ, Styne DM, and McDonald CM

Subjects

Absorptiometry, Photon, Adolescent, Adult, Analysis of Variance, Anthropometry, Blood Glucose, Blood Pressure, Child, Female, Humans, Insulin Resistance, Lipoproteins, HDL metabolism, Male, Metabolic Diseases epidemiology, Metabolic Diseases metabolism, Obesity, Prevalence, Sex Factors, Spinal Cord Injuries epidemiology, Spinal Cord Injuries metabolism, Spinal Dysraphism epidemiology, Spinal Dysraphism metabolism, Triglycerides blood, Metabolic Diseases etiology, Spinal Cord Injuries complications, Spinal Dysraphism complications

Abstract

Objective: The purpose of this study was to determine the prevalence of components of the metabolic syndrome in adolescents with spinal cord injury (SCI) and spina bifida (SB), and their associations with obesity in subjects with and without SCI and SB., Methods: Fifty-four subjects (20 SCI and 34 SB) age 11 to 20 years with mobility impairments from lower extremity paraparesis were recruited from a hospital-based clinic. Sixty able-bodied subjects who were oversampled for obesity served as controls (CTRL). Subjects were categorized as obese if their percent trunk fat measured by dual x-ray absorptiometry (DXA) was > 30.0% for males and > 35.0% for females. Ten SCI, 24 SB, and 19 CTRL subjects were classified as obese. Fasting serum samples were collected to determine serum glucose, insulin, and lipid concentrations. Metabolic syndrome was defined as having > or =3 of the following components: (a) obesity; (b) high-density lipoprotein (HDL) <45 mg/dL for males; <50 mg/dL for females; (c) triglycerides 2100 mg/dL; (d) systolic or diastolic blood pressure > or =95th percentile for age/ height/gender, and (e) insulin resistance determined by either fasting serum glucose 100-125 mg/dL; fasting insulin > or =20 microU /mL; or homeostasis model assessment of insulin resistance > or = 4.0., Results: Metabolic syndrome was identified in 32.4% of the SB group and 55% of the SCI group. Metabolic syndrome occurred at a significantly higher frequency in obese subjects (SB = 45.8%, SCI = 100%, CTRL = 63.2%) than nonobese subjects (SB = 0%, SCI = 10%, CTRL = 2.4%)., Conclusions: The prevalence of metabolic syndrome in adolescents with SB/SCI is quite high, particularly in obese individuals. These findings have important implications due to the known risks of cardiovascular diseases and diabetes mellitus associated with metabolic syndrome in adults, particularly those with spinal cord dysfunction.

Published

2007

40. The methionine synthase reductase 66A>G polymorphism is a maternal risk factor for spina bifida.

Author

van der Linden IJ, den Heijer M, Afman LA, Gellekink H, Vermeulen SH, Kluijtmans LA, and Blom HJ

Subjects

Adolescent, Adult, Aged, Alleles, Case-Control Studies, Child, Child, Preschool, Confidence Intervals, Female, Humans, Male, Methylenetetrahydrofolate Reductase (NADPH2) genetics, Methylmalonic Acid blood, Middle Aged, Odds Ratio, Risk Factors, Spinal Dysraphism metabolism, Ferredoxin-NADP Reductase genetics, Mothers, Polymorphism, Genetic, Spinal Dysraphism genetics

Abstract

The methionine synthase reductase (MTRR) enzyme restores methionine synthase (MTR) enzyme activity and therefore plays an essential role in homocysteine remethylation. In some studies, the 66A>G polymorphism in the MTRR gene was associated with increased neural tube defect (NTD) risk. Using a case-control design, we studied the association between the MTRR 66A>G polymorphism and spina bifida risk in 121 mothers, 109 spina bifida patients, 292 control women, and 234 pediatric controls. Possible interactions between the MTRR 66A>G variant and the MTR 2756A>G polymorphism, the MTHFR 677C>T variant, plasma vitamin B12, and plasma methylmalonic acid (MMA) levels were examined in the 121 mothers and 292 control women. Meta-analyses were conducted to set the results of the case-control study in the context of eligible literature on the relation between the MTRR 66A>G variant and NTD risk. Finally, a transmission disequilibrium test was performed for 82 complete mother-father-child triads to test for preferential transmission of the MTRR risk allele. In our case-control study, the MTRR 66A>G polymorphism had no influence on spina bifida risk in children [odds ratio (OR) 0.6, 95% confidence interval (CI) 0.4-1.1]. The MTRR 66GG genotype increased maternal spina bifida risk by 2.1-fold (OR 2.1, 95% CI 1.3-3.3). This risk became more pronounced in combination with the MTHFR 677TT genotype (OR 4.0, 95% CI 1.3-12.5). Moreover, we demonstrate a possible interaction between the MTRR 66GG genotype and high plasma MMA levels (OR 5.5, 95% CI 2.2-13.5). The meta-analyses demonstrated that the maternal MTRR 66GG genotype was associated with an overall 55% (95% CI 1.04-2.30) increase in NTD risk and that the MTRR 66GG genotype did not increase NTD risk in children (OR 0.96, 95% CI 0.46-2.01). These data show that the MTRR 66GG genotype is a maternal risk factor for spina bifida especially when intracellular vitamin B12 status is low.

Published

2006

41. Effectiveness of an upper extremity exercise device integrated with computer gaming for aerobic training in adolescents with spinal cord dysfunction.

Author

Widman LM, McDonald CM, and Abresch RT

Subjects

Adolescent, Arm, Feasibility Studies, Female, Heart Rate physiology, Humans, Male, Patient Satisfaction, Exercise physiology, Oxygen Consumption physiology, Spinal Dysraphism metabolism, User-Computer Interface, Video Games

Abstract

Background/objective: To determine whether a new upper extremity exercise device integrated with a video game (GameCycle) requires sufficient metabolic demand and effort to induce an aerobic training effect and to explore the feasibility of using this system as an exercise modality in an exercise intervention., Design: Pre-post intervention., Setting: University-based research facility. SUBJECT POPULATION: A referred sample of 8 adolescent subjects with spina bifida (4 girls, 15.5 +/- 0.6 years; 4 boys, 17.5 +/- 0.9 years) was recruited to participate in the project. All subjects had some level of mobility impairment that did not allow them to participate in mainstream sports available to their nondisabled peers. Five subjects used a wheelchair full time, one used a wheelchair occasionally, but walked with forearm crutches, and 2 were fully ambulatory, but had impaired gait., Main Outcome Measures: Peak oxygen uptake, maximum work output, aerobic endurance, peak heart rate, rating of perceived exertion, and user satisfaction., Results: Six of the 8 subjects were able to reach a Vo2 of at least 50% of their Vo2 reserve while using the GameCycle. Seven of the 8 subjects reached a heart rate of at least 50% of their heart rate reserve. One subject did not reach either 50% of Vo2 reserve or 50% of heart rate reserve. Seven of the 8 subjects increased their maximum work capability after training with the GameCycle at least 3 times per week for 16 weeks., Conclusions: The data suggest that the GameCycle seems to be adequate as an exercise device to improve oxygen uptake and maximum work capability in adolescents with lower extremity disability caused by spinal cord dysfunction. The subjects in this study reported that the video game component was enjoyable and provided a motivation to exercise.

Published

2006

42. Primary lumbosacral Wilms tumor associated with diastematomyelia and occult spinal dysraphism. A report of a rare case and a short review of literature.

Author

Sharma MC, Sarat Chandra P, Goel S, Gupta V, and Sarkar C

Subjects

Female, Humans, Immunohistochemistry methods, Infant, Keratins metabolism, Kidney Neoplasms metabolism, Kidney Neoplasms pathology, Lumbosacral Region pathology, Magnetic Resonance Imaging methods, Spina Bifida Occulta metabolism, Spina Bifida Occulta pathology, Spinal Cord Neoplasms metabolism, Spinal Cord Neoplasms pathology, Spinal Dysraphism metabolism, Spinal Dysraphism pathology, Staining and Labeling, Wilms Tumor metabolism, Wilms Tumor pathology, Kidney Neoplasms complications, Spina Bifida Occulta complications, Spinal Cord Neoplasms complications, Spinal Dysraphism complications, Wilms Tumor complications

Abstract

Background: The occurrence of an extrarenal Wilms tumor in the lumbosacral region is an extremely uncommon condition., Case Report: We report a case of Wilms tumor in the lumbosacral region that was associated with diastematomyelia and occult spina bifida. An 18-month-old girl presented with a swelling over the lower back with a tuft of hair on it, which she had had since birth. Imaging of the spine revealed spina bifida, bony diastematomyelia, and tethered cord. Excision of the bony spur and detethering of the cord was done. After a year, she had recurrence of swelling at the same site, weakness of both lower limbs, and incontinence of bladder and bowel. Excision of the mass and bony spur and detethering of the spinal cord were done. Histopathological examination showed features of a Wilms tumor.

Published

2005

43. Spina bifida and genetic factors related to myo-inositol, glucose, and zinc.

Author

Groenen PM, Klootwijk R, Schijvenaars MM, Straatman H, Mariman EC, Franke B, and Steegers-Theunissen RP

Subjects

Alcohol Drinking, Body Mass Index, Case-Control Studies, Child, Preschool, Erythrocytes metabolism, Female, Humans, Infant, Linkage Disequilibrium, Logistic Models, Male, Odds Ratio, Polymorphism, Genetic, Spinal Dysraphism metabolism, Blood Glucose metabolism, Inositol blood, Spinal Dysraphism genetics, Zinc metabolism

Abstract

Background: Myo-inositol, glucose and zinc and related genetic factors are suggested to be implicated in the etiology of spina bifida. We investigated the biochemical concentrations of these nutrients and polymorphisms in the myo-inositol transporter SLC5A11, myo-inositol synthase ISYNA1, and zinc transporter SLC39A4 in association with spina bifida risk., Methods: Seventy-six spina bifida triads only were ascertained. In mothers, fathers, and spina bifida children polymorphisms determined were SLC5A11 (544C > T), ISYNA1 (1029A > G), and SLC39A4 (1069C > T). Serum myo-inositol and glucose, and red blood cell zinc concentrations were determined in mothers and spina bifida children. Transmission disequilibrium tests (TDT) were applied to determine associations between the polymorphisms and spina bifida. Associations between biochemical values and genotypes were studied by one-way analysis of variance (ANOVA). Interactions between alleles, biochemical values, and environmental factors were analyzed by conditional logistic regression., Results: No association between SLC5A11, ISYNA1, and SLC39A4 and spina bifida was shown, chi2SLC5A11=0.016, P=0.90; chi2SYNA1=1.52, P=0.22; chi2SLC39A4=0.016, P=0.90; and degrees of freedom (df)=1. Maternal glucose concentrations were comparable for the SLC5A11 genotypes. Significantly lower myo-inositol concentrations were observed in mothers with SLC5A11 CC-genotype, mean (SD) 14.2 (2.6)micromol/L compared to SLC5A11 TT-genotype, 17.0 (3.4)micromol/L, P <0.05 . No significant associations were observed between ISYNA1 and myo-inositol and glucose, and between SLC39A4 and zinc. A significant interaction was demonstrated between a maternal glucose < 4.5 mmol/L and ISYNA1 1029A > G polymorphism on spina bifida risk., Conclusion: The combination of maternal glucose < 4.5 mmol/L and ISYNA1 1029A > G polymorphism protects against spina bifida offspring. Moreover, maternal SLC5A11 544C > T polymorphism contributes to the serum myo-inositol concentration. Larger studies should confirm these findings.

Published

2004

44. Methylenetetrahydrofolate reductase (MTHFR): incidence of mutations C677T and A1298C in Brazilian population and its correlation with plasma homocysteine levels in spina bifida.

Author

Perez AB, D'Almeida V, Vergani N, de Oliveira AC, de Lima FT, and Brunoni D

Subjects

Brazil epidemiology, Child, Preschool, Female, Gene Frequency, Humans, Infant, Infant, Newborn, Male, Methylenetetrahydrofolate Reductase (NADPH2) genetics, Point Mutation, Spinal Dysraphism genetics, Homocysteine blood, Methylenetetrahydrofolate Reductase (NADPH2) metabolism, Spinal Dysraphism metabolism

Abstract

Homocysteine (Hcy) is converted to cysteine or is remethylated to methionine by methylenetetrahydrofolate reductase (MTHFR). MTHFR plays a central role in the metabolism of folate. Two common polymorphisms in the MTHFR gene (C677T and A1298C) have been described and studies suggest that these polymorphisms are positively associated with the occurrence of spina bifida (SB). Among Brazilians, the incidence of 677T allele homozygosity is 4%. We compared Hcy levels with the genotypes obtained for the mutations C677T and A1298C in the gene MTHFR. Levels of plasma Hcy were higher in children with SB than in controls (average 7.95 vs. 5.55 (micromol/L); P < 0.001). There was no significant difference in the levels of Hcy for these children's mothers and controls (average 7.76 vs. 8.36 (micromol/L); P = 0.27). Eighty one (61.8%) of the affected children were white and 50 (38.2%) were non-white. A similar ratio was observed in the mothers. In the control group, 51 children (40.5%) were white and 75 (59.5%) were non-white, and 52 mothers (41.3%) were white and 74 (58.7%) were non-white. There was no significant difference in the homozygous frequency for the mutated allele 677T among different racial groups. We obtained a prevalence of TT homozygosity of 10/131 (7.64%) in affected children and 13/126 (10.32%) in controls. With respect to the mutation A1298C, the homozygous prevalence for the wild allele was greater among non-white individuals than in white individuals both in case and control groups. Hyperhomocysteinemia is a risk factor for SB. However, in our population, the increase in plasma levels of Hcy is not explained by the presence of the homozygous TT. It is possible that low folic acid intake combined with other genetic factors plays a more important role in the cause of this disease., (Copyright 2003 Wiley-Liss, Inc.)

Published

2003

45. Are myo-inositol, glucose and zinc concentrations in amniotic fluid of fetuses with spina bifida different from controls?

Author

Groenen PM, Wevers RA, Janssen FS, Tuerlings JH, Merkus JM, and Steegers-Theunissen RP

Subjects

Adult, Amniotic Fluid chemistry, Female, Gestational Age, Glucose analysis, Humans, Inositol analysis, Maternal Age, Pregnancy, Pregnancy, High-Risk, Spectrophotometry, Atomic, Spinal Dysraphism etiology, Zinc analysis, Amniotic Fluid metabolism, Glucose metabolism, Inositol metabolism, Spinal Dysraphism metabolism, Zinc metabolism

Abstract

Objective: Associations are reported between myo-inositol, glucose, zinc and the occurrence of spina bifida. To gain more insight into the pathogenesis of spina bifida, the concentrations of myo-inositol, glucose and zinc were determined in amniotic fluids from pregnancies with a spina bifida or unaffected control fetus., Methods: Amniotic fluids of 27 pregnancies complicated by spina bifida and 49 controls were collected at the Department of Obstetrics and Gynecology of the University Medical Center Nijmegen in the Netherlands. Myo-inositol, glucose and zinc concentrations were determined. By indication, the samples were taken at different gestational ages. Therefore, the data were evaluated using multiple linear regression analysis to adjust for gestational age., Results: Amniocentesis was performed at a more advanced gestational age in the spina bifida group than in controls. In the spina bifida group, amniotic fluid myo-inositol, glucose and zinc concentrations gradually declined throughout pregnancy. At a gestational age of 15 weeks, the estimated mean amniotic fluid glucose and zinc concentrations in the spina bifida group were, respectively, significantly lower (p< or =0.5) and higher (p< or =0.5) compared with the control group. At the same gestational age, the estimated mean myo-inositol concentrations were comparable in both groups. At a gestational age of 38 weeks, the estimated mean myo-inositol, glucose and zinc concentrations were not significantly different in the spina bifida compared with the control group., Conclusion: This study may suggest that a derangement in zinc and glucose transfer or metabolism is associated with spina bifida. Since compounds in amniotic fluid are only a very crude marker of the actual fetal condition, studies that focus on the metabolism of these compounds on tissue or even cellular level should be performed to clarify their role in the pathogenesis and future prevention of spina bifida.

Published

2003

46. Spina bifida and folate-related genes: a study of gene-gene interactions.

Author

de Franchis R, Botto LD, Sebastio G, Ricci R, Iolascon A, Capra V, Andria G, and Mastroiacovo P

Subjects

Alleles, Case-Control Studies, Child, Child, Preschool, Cystathionine beta-Synthase metabolism, Humans, Infant, Lod Score, Methylenetetrahydrofolate Reductase (NADPH2), Mutation, Oxidoreductases Acting on CH-NH Group Donors metabolism, Spinal Dysraphism metabolism, Cystathionine beta-Synthase genetics, Folic Acid genetics, Oxidoreductases Acting on CH-NH Group Donors genetics, Spinal Dysraphism genetics

Abstract

Purpose: To assess whether interactions of common alleles of two folate genes contribute to spina bifida risk., Methods: Case-control study, comparing 203 children with spina bifida to 583 controls., Results: Homozygosity for the 677C-T allele of 5,10-methylenetetrahydrofolate reductase (MTHFR) alone was associated with an odds ratio for spina bifida of 1.57 (95% confidence interval [CI], 1.02-2.38). For the 844ins68 allele of cystathionine-beta-synthase alone, the odds ratio was 0.83 (95% CI, 0.39-1.64). For the joint genotype, the odds ratio was 3.69 (95% CI, 1.04-13.50)., Conclusions: Interactions between common alleles of folate genes might contribute to the risk for spina bifida.

Published

2002

47. Cartilage-specific matrix protein, chondromodulin-I (ChM-I), is a strong angio-inhibitor in endochondral ossification of human neonatal vertebral tissues in vivo: relationship with angiogenic factors in the cartilage.

Author

Kusafuka K, Hiraki Y, Shukunami C, Kayano T, and Takemura T

Subjects

Antigens, CD34 biosynthesis, Biomarkers, Cartilage metabolism, Cartilage pathology, Child, Preschool, Humans, Immunohistochemistry, Infant, Infant, Newborn, Spinal Dysraphism metabolism, Spinal Dysraphism pathology, Spine drug effects, Spine pathology, Tissue Embedding, Angiogenesis Inducing Agents physiology, Angiogenesis Inhibitors pharmacology, Cartilage physiology, Intercellular Signaling Peptides and Proteins pharmacology, Membrane Proteins, Osteogenesis drug effects, Spine embryology

Abstract

Although cartilage contains many angiogenic factors during endochondral ossification, it is an avascular tissue. The cartilage-specific non-collagenous matrix protein chondromodulin-I (ChM-I) has been shown to be a strong angio-inhibitor. To elucidate whether ChM-I plays an essential role in angio-inhibition during endochondral ossification in man, we investigated the expression and localization of ChM-I in comparison with those of angiogenic factors and the endothelial cell marker CD34 in human neonatal vertebral tissues. Although invasion of CD34-positive endothelial cells was observed in primary subchondral spongiosa, expression of the marker of endothelial cells, CD34, was not found in neonatal vertebral cartilage matrix. Type II collagen was deposited in all matrices during endochondral ossification, whereas aggrecan was deposited in the matrix of hypertrophic cartilage, especially around lacunae. Vascular endothelial growth factor (VEGF), which is known to be a strong angiogenic factor, was localized in chondrocytes in mature to hypertrophic cartilage and also in bone marrow. Fibroblast growth factor-2 (FGF-2; basic fibroblast growth factor), which is also known to be a strong angiogenic factor, was localized in the cytoplasm of chondrocytes of mature cartilage in human vertebral cartilage tissues. Transforming growth factor (TGF)-beta has been reported to have many functions including angiogenesis, and TGF-beta1 was also localized in mature chondrocytes in endochondral tissues undergoing ossification. On the other hand, the novel cartilage-specific matrix protein ChM-I was localized in interterritorial regions of the matrix in mature to hypertrophic cartilage, especially around lacunae. In conclusion, these observations indicate that ChM-I may serve as a barrier against the angiogenic properties of VEGF, FGF-2 and TGF-beta1 during endochondral ossification, and this matrix molecule may play an essential role in determining the avascular nature of cartilage in vivo.

Published

2002

48. An examination of polymorphic genes and folate metabolism in mothers affected by a spina bifida pregnancy.

Author

Lucock M, Daskalakis I, Hinkins M, and Yates Z

Subjects

Adult, Alleles, England, Erythrocytes enzymology, Erythrocytes metabolism, Female, Folic Acid analogs & derivatives, Folic Acid blood, Gene Frequency, Humans, Methionine biosynthesis, Methionine metabolism, Methylation, Polyglutamic Acid metabolism, Polymorphism, Single Nucleotide genetics, Pregnancy, Pteroylpolyglutamic Acids metabolism, Spinal Dysraphism blood, Spinal Dysraphism enzymology, Vitamin B 12 metabolism, Folic Acid metabolism, Mutation genetics, Polymorphism, Genetic genetics, Spinal Dysraphism genetics, Spinal Dysraphism metabolism

Abstract

The effect of four polymorphic genes of folate-dependent methionine biosynthesis have been investigated in mothers affected by a neural tube defect pregnancy (NTD) and matched controls. The influence of the various genotypes on total red cell 5-methyl-H(4)folate,5,10-methenyl-H(4)folate, and 5-formyl-H(4)folate is reported, as is the effect on homocysteine and radioassay folate in both serum and red cells. All of the single nucleotide polymorphisms studied would seem to contribute to the cellular folate profile in some way. From the data presented, and from the work of others, it is likely that C677T 5,10-methylenetetrahydrofolate reductase is the most important of these polymorphisms. Control mother folate profiles seem reasonably predictive of any given methionine cycle mutation, but profiles in NTD mothers do not. On this basis, it seems likely that some other, as yet unidentified folate lesion is causal for NTD. In NTD-C677T 5,10-methylenetetrahydrofolate reductase in particular, indexes of folate depletion such as high-performance liquid chromatography (HPLC) folate level, oligo-gamma-glutamyl chain length, homocysteine, and radioassay folate values all seem to deteriorate with increased mutant allele carriage. This indicates that this folate polymorphism may provide a critical threshold effect that helps to promote NTD occurrence in the presence of another, as yet unidentified folate-related factor. In more general terms, on a by genotype basis, all 11 genotypes studied give NTD mothers a higher homocysteine compared to controls. Furthermore, a trend that is less universal indicates that NTD mothers have higher 5,10-methenyl-H(4)folate and 5-methyl-H(4)folate levels and lower 5-formyl-H(4)folate and H(4)PteGlu(1) levels than do controls. One of the most consistent, and possibly specific, differences between participant groups is a statistically significant elevation of 5,10-methenyl-H(4)folate in NTD mothers (affects three genotypes). Possible interpretations of this finding are discussed., (Copyright 2001 Academic Press.)

Published

2001

49. Inadequate folic acid intakes are prevalent among young women with neural tube defects.

Author

Gross SM, Caulfield LE, Kinsman SL, and Ireys HT

Subjects

Adolescent, Adult, Baltimore epidemiology, Delaware epidemiology, Dietary Supplements, Female, Folic Acid Deficiency etiology, Food, Fortified, Humans, Nutritional Requirements, Prevalence, Risk Factors, Spinal Dysraphism metabolism, Folic Acid administration & dosage, Folic Acid Deficiency epidemiology, Spinal Dysraphism complications

Published

2001

50. Dissection of inhibitory Smad proteins: both N- and C-terminal domains are necessary for full activities of Xenopus Smad6 and Smad7.

Author

Nakayama T, Berg LK, and Christian JL

Subjects

Animals, Blotting, Western, Bone Morphogenetic Proteins metabolism, DNA-Binding Proteins genetics, Gene Deletion, Models, Genetic, Mutation, Phenotype, Plasmids metabolism, Protein Structure, Tertiary, RNA metabolism, Reverse Transcriptase Polymerase Chain Reaction, Signal Transduction, Smad6 Protein, Smad7 Protein, Spinal Dysraphism metabolism, Structure-Activity Relationship, Time Factors, Trans-Activators genetics, Xenopus, Xenopus Proteins, DNA-Binding Proteins chemistry, DNA-Binding Proteins physiology, Trans-Activators chemistry, Trans-Activators physiology

Abstract

Smad6 and Smad7 comprise a subclass of vertebrate Smads that antagonize, rather than transduce, TGF-beta family signaling. These Anti-Smads can block BMP signaling, as evidenced by their ability to induce a secondary dorsal axis when misexpressed ventrally in Xenopus embryos. Smad7 inhibits additional TGF-beta related pathways, and causes spina bifida when misexpressed dorsally. We have performed structure-function analyses to identify domains of Anti-Smads that are responsible for their shared and unique activities. We find that the C-terminal domain of Smad7 displays strong axis inducing activity but cannot induce spina bifida. The isolated N-terminal domain of Smad7 is inactive but restores the ability of the C-terminus to cause spina bifida when the two are co-expressed. By contrast, the N- and C-terminal domains of Smad6 have weak axis inducing activity when expressed individually, but show full activity when co-expressed. Chimeric analysis demonstrates that the C-terminal domain of Smad7, but not Smad6, can induce spina bifida when fused to the N-terminal domain of either Smad6 or Smad7. Thus, although the C-terminal domain is the primary determinant of the intrinsic activity of Xenopus Anti-Smads, the N-terminal domain is essential for full activity, is interchangeable between Smad6 and 7, and can function in trans.

Published

2001