Spina bifida pathophysiology

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Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: , Mohamadmostafa Jahansouz M.D.[2]

Overview

Spina bifida is a congenital malformation in which the spinal column is split (bifid) as a result of failed closure of the embryonic neural tube, during the fourth week post-fertilization. In normal infants, the neural tube closes by the end of the 4 week of conception, but in patients with spina bifida, some parts of the neural tube fails to develop or close that causes defects in the spinal cord and in the vertebral bones. Spina bifida also may be classified according to the tyoe of the vertebrate defect into 2 subtypes: Spina bifida occulta: In this type of spina bifida, the defect of vertebrate is covered by skin ("Occulta" means "hidden"). The spinal cord does not stick out through the skin, although the skin over the lower spine may have a patch of hair, a birthmark, or a dimple above the groove between the buttocks. Spina ifida aperta: In this type of spina bifida , the defect is widely open and is sub classified into 2 types: Meningocele and Myelomeningocele. Spina bifida may be caused by the increase of cerebrospinal fluid (CSF) volume in the central nervous system during the first weeks of embryogenesis. Venous insufficiency is the main cause of the increase of cerebrospinal fluid and it may be caused by any disease that reduces space for venous volume. The development of spina bifida may be the result of multiple genetically defect in the genes important in the metabolism of: Folic acid, glucose, retinoids, apoptosis, genes that regulate transcription in early embryogenesis, methionine Cycle genes, methylation genes, glucose Homeostasis genes, cell Recognition and Migration genes, DNA Repair genes and transcription Factors genes. Conditions associated with spina bifida include: Hydrocephalus, chiari II Malformation, paralysis, urination and deification incontinences, atex Allergy, learning Disabilities, sexual problems, emotional problems, obesity and vision problems.

Pathophysiology

Spina bifida is a congenital malformation in which the spinal column is split (bifid) as a result of failed closure of the embryonic neural tube, during the fourth week post-fertilization.^[1]
In normal infants, the neural tube closes by the end of the 4 week of conception, but in patients with spina bifida, some parts of the neural tube fails to develop or close that causes defects in the spinal cord and in the vertebral bones.
Spina bifida also may be classified according to the tyoe of the vertebrate defect into 2 subtypes:
- Spina bifida occulta: In this type of spina bifida, the defect of vertebrate is covered by skin ("Occulta" means "hidden"). The spinal cord does not stick out through the skin, although the skin over the lower spine may have a patch of hair, a birthmark, or a dimple above the groove between the buttocks.^[1]
- Spina ifida aperta: In this type of spina bifida , the defect is widely open and is sub classified into 2 types: Meningocele and Myelomeningocele.^[1]

Pathogenesis

Spina bifida may be caused by the increase of cerebrospinal fluid (CSF) volume in the central nervous system during the first weeks of embryogenesis.^[2]
Venous insufficiency is the main cause of the increase of cerebrospinal fluid and it may be caused by any disease that reduces space for venous volume.^[2]

Genetics

The development of spina bifida may be the result of multiple genetically defect in the genes important in the metabolism of:^[3]

Other genes which may be contributed in the development of the spina bifida include:

Genes important in apoptosis
Genes that regulate transcription in early embryogenesis
Methionine Cycle genes
Methylation genes
Glucose Homeostasis genes
Cell Recognition and Migration genes
DNA Repair genes
Transcription Factors genes such as:^[4]
1. HOXs
2. PAXs
3. MSX2
4. T brachyury
5. TFAP2a
6. ZICs
7. BRCA1
8. CITED2
9. TP53
10. SLUG

Associated Conditions

Conditions associated with spina bifida include:^[5]^[6]^[7]^[8]^[9]^[10]

Hydrocephalus
Chiari II Malformation
Paralysis
Urination and deification incontinences
Latex Allergy
Learning Disabilities
Sexual problems
Emotional problems
Obesity
Vision problems

References

↑ ^1.0 ^1.1 ^1.2 Kenworthy ME (July 1966). "Introducing the American Orthopsychiatric Association's president for 1966-67: Norman V. Lourie". Am J Orthopsychiatry. 36 (4): 587–9. PMID 5327787.
↑ ^2.0 ^2.1 Williams H (April 2008). "A unifying hypothesis for hydrocephalus, Chiari malformation, syringomyelia, anencephaly and spina bifida". Cerebrospinal Fluid Res. 5: 7. doi:10.1186/1743-8454-5-7. PMC 2365936. PMID 18405364.
↑ Schmoldt A, Benthe HF, Haberland G, Holder AA, Wootton JC, Baron AJ, Chambers GK, Fincham JR, Alekseeva IG, Lapina GP, Tulovskaia ZD, Izmaĭlova VN (September 1975). "Digitoxin metabolism by rat liver microsomes". Biochem. Pharmacol. 24 (17): 1639–41. PMC 5922622. PMID 10.
↑ Nordman H, Keskinen H, Alanko K (1988). "[The changing spectrum of occupational diseases of the lung]". Duodecim (in Finnish). 104 (6): 473–9. PMID 3053142.
↑ Jenkinson MD, Campbell S, Hayhurst C, Clark S, Kandasamy J, Lee MK, Flynn A, Murphy P, Mallucci CL (June 2011). "Cognitive and functional outcome in spina bifida-Chiari II malformation". Childs Nerv Syst. 27 (6): 967–74. doi:10.1007/s00381-010-1368-7. PMID 21193992.
↑ Behe MJ, Beasty AM (1991). "Co-polymer tracts in eukaryotic, prokaryotic, and organellar DNA". DNA Seq. 1 (5): 291–302. PMID 1799681.
↑ Temin HM, Mizutani S (June 1970). "RNA-dependent DNA polymerase in virions of Rous sarcoma virus". Nature. 226 (5252): 1211–3. PMID 4316301.
↑ Brochard C, Peyronnet B, Dariel A, Ménard H, Manunta A, Ropert A, Neunlist M, Bouguen G, Siproudhis L (November 2017). "Bowel Dysfunction Related to Spina Bifida: Keep It Simple". Dis. Colon Rectum. 60 (11): 1209–1214. doi:10.1097/DCR.0000000000000892. PMID 28991086.
↑ Bernardini R, Novembre E, Lombardi E, Mezzetti P, Cianferoni A, Danti DA, Mercurella A, Vierucci A (May 1999). "Risk factors for latex allergy in patients with spina bifida and latex sensitization". Clin. Exp. Allergy. 29 (5): 681–6. PMID 10231329.
↑ Gaston H (1991). "Ophthalmic complications of spina bifida and hydrocephalus". Eye (Lond). 5 ( Pt 3): 279–90. doi:10.1038/eye.1991.44. PMID 1955048.

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[pmid5327787-1] 1.0 ^1.1 ^1.2 Kenworthy ME (July 1966). "Introducing the American Orthopsychiatric Association's president for 1966-67: Norman V. Lourie". Am J Orthopsychiatry. 36 (4): 587–9. PMID 5327787.

[pmid18405364-2] 2.0 ^2.1 Williams H (April 2008). "A unifying hypothesis for hydrocephalus, Chiari malformation, syringomyelia, anencephaly and spina bifida". Cerebrospinal Fluid Res. 5: 7. doi:10.1186/1743-8454-5-7. PMC 2365936. PMID 18405364.

[3] Schmoldt A, Benthe HF, Haberland G, Holder AA, Wootton JC, Baron AJ, Chambers GK, Fincham JR, Alekseeva IG, Lapina GP, Tulovskaia ZD, Izmaĭlova VN (September 1975). "Digitoxin metabolism by rat liver microsomes". Biochem. Pharmacol. 24 (17): 1639–41. PMC 5922622. PMID 10.

[pmid3053142-4] Nordman H, Keskinen H, Alanko K (1988). "[The changing spectrum of occupational diseases of the lung]". Duodecim (in Finnish). 104 (6): 473–9. PMID 3053142.

[pmid21193992-5] Jenkinson MD, Campbell S, Hayhurst C, Clark S, Kandasamy J, Lee MK, Flynn A, Murphy P, Mallucci CL (June 2011). "Cognitive and functional outcome in spina bifida-Chiari II malformation". Childs Nerv Syst. 27 (6): 967–74. doi:10.1007/s00381-010-1368-7. PMID 21193992.

[pmid1799681-6] Behe MJ, Beasty AM (1991). "Co-polymer tracts in eukaryotic, prokaryotic, and organellar DNA". DNA Seq. 1 (5): 291–302. PMID 1799681.

[pmid4316301-7] Temin HM, Mizutani S (June 1970). "RNA-dependent DNA polymerase in virions of Rous sarcoma virus". Nature. 226 (5252): 1211–3. PMID 4316301.

[pmid28991086-8] Brochard C, Peyronnet B, Dariel A, Ménard H, Manunta A, Ropert A, Neunlist M, Bouguen G, Siproudhis L (November 2017). "Bowel Dysfunction Related to Spina Bifida: Keep It Simple". Dis. Colon Rectum. 60 (11): 1209–1214. doi:10.1097/DCR.0000000000000892. PMID 28991086.

[pmid10231329-9] Bernardini R, Novembre E, Lombardi E, Mezzetti P, Cianferoni A, Danti DA, Mercurella A, Vierucci A (May 1999). "Risk factors for latex allergy in patients with spina bifida and latex sensitization". Clin. Exp. Allergy. 29 (5): 681–6. PMID 10231329.

[pmid1955048-10] Gaston H (1991). "Ophthalmic complications of spina bifida and hydrocephalus". Eye (Lond). 5 ( Pt 3): 279–90. doi:10.1038/eye.1991.44. PMID 1955048.

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