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8p23.1 duplication syndrome

August 31, 2023

8p23.1 duplication syndrome is a rare genetic disorder caused by a duplication of a region from human chromosome 8.[1] This duplication syndrome has an estimated prevalence of 1 in 64,000 births [1] and is the reciprocal of the 8p23.1 deletion syndrome. The 8p23.1 duplication is associated with a variable phenotype including one or more of speech delay, developmental delay, mild dysmorphism, with prominent forehead and arched eyebrows, and congenital heart disease (CHD).[2][3]

8p23.1 duplication syndrome
Other namesDup(8)(p23.1p23.1), Trisomy 8p23.1
Chromosome 8 is associated with this condition

Presentation Edit

The phenotypic data on 11 patients indicated that cases are not always ascertained for CHD but that CHD was the most common single feature found in 6 out of 11 individuals.[1] Developmental delay and/or learning difficulties were found in 5 out of 11 cases, but one prenatal case was developing normally at 15 months of age (Case 1,[3]). Three other prenatal cases could not yet be reliably assessed. A variable degree of facial dysmorphism was present in 5 out of 11 individuals. Partial toe syndactyly has been found in one mother and son diad and adrenal anomalies in two probands but not in the duplicated mother of one of them. The phenotype is compatible with independent adult life with varying degrees of support. Duplication of the GATA4 transcription factor (OMIM: 600576) is believed to underlie the congenital heart disease and other genes, common to the duplication and deletion syndromes, can be regarded as candidates for the 8p23.1 duplication syndrome. These include the SOX7 transcription factor (OMIM: 612202) for both CHD[4] and developmental delay [5] and the TNKS gene (OMIM: 603303) for behavioural difficulties. The diaphragmatic hernia found in the 8p23.1 deletion syndrome has not been found in the 8p23.1 duplication syndrome to date. The duplication may be associated with copy number changes of the adjacent olfactory receptor/defensin repeats (ORDRs) that predispose to the 8p23.1 deletion and duplication syndromes. High total copy numbers of these repeats have been associated with predisposition to psoriasis[6] and low copy number with predisposition to Crohn's disease.[7]

Genetics Edit

The duplication includes ~3.75 Mb between the distal and proximal ORDRs at either end of band 8p23.1. The copy number of the adjacent repeats may also be altered. The 8p23.1 duplication syndrome cannot be distinguished using conventional cytogenetics from high level copy number variation of the repeats themselves.[1][2]

Both de novo cases and families with transmitted duplications from parents of both sex are known. The duplication is believed to arise de novo as a result of non-allelic homologous recombination (NAHR) between the proximal and distal ORDRs. NAHR is also thought to give rise to the reciprocal microdeletion syndrome, the polymorphic inversion between the ORDRs and a variety of other large scale abnormalities involving the short arm of chromosome 8.[6]

Diagnosis Edit

Phenotypes Edit

Primary Secondary Tertiary
NEUROLOGY MENTAL, COGNITIVE FUNCTION, general abnormalities intellectual disability/developmental delay
VOICE Voice, general abnormalities Speech delay

See also Edit

References Edit

  1. ^ a b c d Barber JC, Bunyan D, Curtis M, et al. (2010). "8p23.1 duplication syndrome differentiated from copy number variation of the defensin cluster at prenatal diagnosis in four new families". Mol Cytogenet. 3: 3. doi:10.1186/1755-8166-3-3. PMC 2846957. PMID 20167067.
  2. ^ a b Barber JC, Maloney V, Hollox EJ, et al. (October 2005). "Duplications and copy number variants of 8p23.1 are cytogenetically indistinguishable but distinct at the molecular level". Eur. J. Hum. Genet. 13 (10): 1131–6. doi:10.1038/sj.ejhg.5201475. PMID 16077733.
  3. ^ a b Barber JC, Maloney VK, Huang S, et al. (January 2008). "8p23.1 duplication syndrome; a novel genomic condition with unexpected complexity revealed by array CGH". Eur. J. Hum. Genet. 16 (1): 18–27. doi:10.1038/sj.ejhg.5201932. PMID 17940555. S2CID 11077778.
  4. ^ Wat MJ, Shchelochkov OA, Holder AM, et al. (August 2009). "Chromosome 8p23.1 Deletions as a Cause of Complex Congenital Heart Defects and Diaphragmatic Hernia". Am. J. Med. Genet. A. 149A (8): 1661–77. doi:10.1002/ajmg.a.32896. PMC 2765374. PMID 19606479.
  5. ^ Páez MT, Yamamoto T, Hayashi K, et al. (May 2008). "Two patients with atypical interstitial deletions of 8p23.1: mapping of phenotypical traits". Am. J. Med. Genet. A. 146A (9): 1158–65. doi:10.1002/ajmg.a.32205. PMID 18393291. S2CID 205309084.
  6. ^ a b Hollox EJ, Barber JC, Brookes AJ, Armour JA (2008). "Defensins and the dynamic genome: what we can learn from structural variation at human chromosome band 8p23.1". Genome Res. 18 (11): 1686–97. doi:10.1101/gr.080945.108. PMID 18974263.
  7. ^ Fellermann K, Stange DE, Schaeffeler E, Schmalzl H, Wehkamp J, Bevins CL, Reinisch W, Teml A, Schwab M, Lichter P, Radlwimmer B, Stange EF (2006). "A Chromosome 8 Gene-Cluster Polymorphism with Low Human Beta-Defensin 2 Gene Copy Number Predisposes to Crohn Disease of the Colon". Am J Hum Genet. 79 (3): 439–48. doi:10.1086/505915. PMC 1559531. PMID 16909382.

External links Edit

  • DECIPHER database description

August 31, 2023
8p23, duplication, syndrome, rare, genetic, disorder, caused, duplication, region, from, human, chromosome, this, duplication, syndrome, estimated, prevalence, births, reciprocal, 8p23, deletion, syndrome, 8p23, duplication, associated, with, variable, phenoty. 8p23 1 duplication syndrome is a rare genetic disorder caused by a duplication of a region from human chromosome 8 1 This duplication syndrome has an estimated prevalence of 1 in 64 000 births 1 and is the reciprocal of the 8p23 1 deletion syndrome The 8p23 1 duplication is associated with a variable phenotype including one or more of speech delay developmental delay mild dysmorphism with prominent forehead and arched eyebrows and congenital heart disease CHD 2 3 8p23 1 duplication syndromeOther namesDup 8 p23 1p23 1 Trisomy 8p23 1Chromosome 8 is associated with this condition Contents 1 Presentation 2 Genetics 3 Diagnosis 3 1 Phenotypes 4 See also 5 References 6 External linksPresentation EditThe phenotypic data on 11 patients indicated that cases are not always ascertained for CHD but that CHD was the most common single feature found in 6 out of 11 individuals 1 Developmental delay and or learning difficulties were found in 5 out of 11 cases but one prenatal case was developing normally at 15 months of age Case 1 3 Three other prenatal cases could not yet be reliably assessed A variable degree of facial dysmorphism was present in 5 out of 11 individuals Partial toe syndactyly has been found in one mother and son diad and adrenal anomalies in two probands but not in the duplicated mother of one of them The phenotype is compatible with independent adult life with varying degrees of support Duplication of the GATA4 transcription factor OMIM 600576 is believed to underlie the congenital heart disease and other genes common to the duplication and deletion syndromes can be regarded as candidates for the 8p23 1 duplication syndrome These include the SOX7 transcription factor OMIM 612202 for both CHD 4 and developmental delay 5 and the TNKS gene OMIM 603303 for behavioural difficulties The diaphragmatic hernia found in the 8p23 1 deletion syndrome has not been found in the 8p23 1 duplication syndrome to date The duplication may be associated with copy number changes of the adjacent olfactory receptor defensin repeats ORDRs that predispose to the 8p23 1 deletion and duplication syndromes High total copy numbers of these repeats have been associated with predisposition to psoriasis 6 and low copy number with predisposition to Crohn s disease 7 Genetics EditThe duplication includes 3 75 Mb between the distal and proximal ORDRs at either end of band 8p23 1 The copy number of the adjacent repeats may also be altered The 8p23 1 duplication syndrome cannot be distinguished using conventional cytogenetics from high level copy number variation of the repeats themselves 1 2 Both de novo cases and families with transmitted duplications from parents of both sex are known The duplication is believed to arise de novo as a result of non allelic homologous recombination NAHR between the proximal and distal ORDRs NAHR is also thought to give rise to the reciprocal microdeletion syndrome the polymorphic inversion between the ORDRs and a variety of other large scale abnormalities involving the short arm of chromosome 8 6 Diagnosis EditPhenotypes Edit Primary Secondary TertiaryNEUROLOGY MENTAL COGNITIVE FUNCTION general abnormalities intellectual disability developmental delayVOICE Voice general abnormalities Speech delaySee also EditChromosome 8 human References Edit a b c d Barber JC Bunyan D Curtis M et al 2010 8p23 1 duplication syndrome differentiated from copy number variation of the defensin cluster at prenatal diagnosis in four new families Mol Cytogenet 3 3 doi 10 1186 1755 8166 3 3 PMC 2846957 PMID 20167067 a b Barber JC Maloney V Hollox EJ et al October 2005 Duplications and copy number variants of 8p23 1 are cytogenetically indistinguishable but distinct at the molecular level Eur J Hum Genet 13 10 1131 6 doi 10 1038 sj ejhg 5201475 PMID 16077733 a b Barber JC Maloney VK Huang S et al January 2008 8p23 1 duplication syndrome a novel genomic condition with unexpected complexity revealed by array CGH Eur J Hum Genet 16 1 18 27 doi 10 1038 sj ejhg 5201932 PMID 17940555 S2CID 11077778 Wat MJ Shchelochkov OA Holder AM et al August 2009 Chromosome 8p23 1 Deletions as a Cause of Complex Congenital Heart Defects and Diaphragmatic Hernia Am J Med Genet A 149A 8 1661 77 doi 10 1002 ajmg a 32896 PMC 2765374 PMID 19606479 Paez MT Yamamoto T Hayashi K et al May 2008 Two patients with atypical interstitial deletions of 8p23 1 mapping of phenotypical traits Am J Med Genet A 146A 9 1158 65 doi 10 1002 ajmg a 32205 PMID 18393291 S2CID 205309084 a b Hollox EJ Barber JC Brookes AJ Armour JA 2008 Defensins and the dynamic genome what we can learn from structural variation at human chromosome band 8p23 1 Genome Res 18 11 1686 97 doi 10 1101 gr 080945 108 PMID 18974263 Fellermann K Stange DE Schaeffeler E Schmalzl H Wehkamp J Bevins CL Reinisch W Teml A Schwab M Lichter P Radlwimmer B Stange EF 2006 A Chromosome 8 Gene Cluster Polymorphism with Low Human Beta Defensin 2 Gene Copy Number Predisposes to Crohn Disease of the Colon Am J Hum Genet 79 3 439 48 doi 10 1086 505915 PMC 1559531 PMID 16909382 External links EditDECIPHER database description Retrieved from https en wikipedia org w index php title 8p23 1 duplication syndrome amp oldid 1089835415, wikipedia, wiki, book, books, library,

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