The origin of trisomy 13

Hall, Heather E.; Chan, E. Ricky; Collins, Andrew; Judis, LuAnn; Shirley, Sofia; Surti, Urvashi; Hoffner, Lori; Cockwell, Annette E.; Jacobs, Patricia A.; Hassold, Terry

doi:10.1002/ajmg.a.31913

Cited by 31 publications

(28 citation statements)

References 18 publications

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“…Under the condition that such oocytes are developing slowly, survive in primordial follicles and become recruited for resumption of maturation only late in the reproductive period according to a production line [5] they could contribute to increases in numbers of aneuploid oocytes in older females. In normal diploid oocytes the absence of exchanges or placement, and the numbers of crossing overs that are established in the embryonic ovary, may also relate to the relative risk of each individual chromosome undergoing nondisjunction or facilitating normal distribution after resumption of maturation in the cytoplasm of an aged oocyte [11][12][13]. This means that there is a link between early and late events in oogenesis.…”

Section: Events In the Embryonal Ovary Prior To Birthmentioning

confidence: 99%

“…Lastly, there are different hypotheses on constitutive and age-related alterations in the hormonal homoeostasis, and in oocytes and follicles, which are believed to correlate with increased failures in faithful and sequential segregation of homologues and sister chromatids at meiosis I and II in oocytes [9]. In Figure 1 Stages of oogenesis that are susceptible to disturbances and events leading synergistically to high risks for errors in chromosome segregation in oocytes at advanced maternal age (A) Events in the embryonic ovary, including presence of trisomic cell line of oogonia [10], failure to recombine and/or numbers and placement of exchanges on homologous chromosomes [8,[11][12][13]. (B) Events during long meiotic arrest of dictyate stage-arrested oocyte in the primordial follicle post-birth, including accumulation of insult by environment, life style/nutrition and ROS, loss of cohesion during chronological ageing and reduction of follicle pool (physiological ageing) by continuous recruitment and atresia of follicles [5][6][7][16][17][18][19][20][21][22].…”

Section: Introductionmentioning

confidence: 99%

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Chromosomal and cytoplasmic context determines predisposition to maternal age-related aneuploidy: brief overview and update on MCAK in mammalian oocytes

Eichenlaub-Ritter

Staubach

Trapphoff

2010

Biochemical Society Transactions

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It has been known for more than half a century that the risk of conceiving a child with trisomy increases with advanced maternal age. However, the origin of the high susceptibility to nondisjunction of whole chromosomes and precocious separation of sister chromatids, leading to aneuploidy in aged oocytes and embryos derived from them, cannot be traced back to a single disturbance and mechanism. Instead, analysis of recombination patterns of meiotic chromosomes of spread oocytes from embryonal ovary, and of origins and exchange patterns of extra chromosomes in trisomies, as well as morphological and molecular studies of oocytes and somatic cells from young and aged females, show chromosome-specific risk patterns and cellular aberrations related to the chronological age of the female. In addition, analysis of the function of meiotic- and cell-cycle-regulating genes in oogenesis, and the study of the spindle and chromosomal status of maturing oocytes, suggest that several events contribute synergistically to errors in chromosome segregation in aged oocytes in a chromosome-specific fashion. For instance, loss of cohesion may differentially predispose chromosomes with distal or pericentromeric chiasmata to nondisjunction. Studies on expression in young and aged oocytes from human or model organisms, like the mouse, indicate that the presence and functionality/activity of gene products involved in cell-cycle regulation, spindle formation and organelle integrity may be altered in aged oocytes, thus contributing to a high risk of error in chromosome segregation in meiosis I and II. Genes that are often altered in aged mouse oocytes include MCAK (mitotic-centromere-associated protein), a microtubule depolymerase, and AURKB (Aurora kinase B), a protein of the chromosomal passenger complex that has many targets and can also phosphorylate and regulate MCAK localization and activity. Therefore we explored the role of MCAK in maturing mouse oocytes by immunofluorescence, overexpression of a MCAK-EGFP (enhanced green fluorescent protein) fusion protein, knockdown of MCAK by RNAi (RNA interference) and inhibition of AURKB. The observations suggest that MCAK is involved in spindle regulation, chromosome congression and cell-cycle control, and that reductions in mRNA and protein in a context of permissive SAC (spindle assembly checkpoint) predispose to aneuploidy. Failure to recruit MCAK to centromeres and low expression patterns, as well as disturbances in regulation of enzyme localization and activity, e.g. due to alterations in activity of AURKB, may therefore contribute to maternal age-related rises in aneuploidy in mammalian oocytes.

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Section: Events In the Embryonal Ovary Prior To Birthmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Chromosomal and cytoplasmic context determines predisposition to maternal age-related aneuploidy: brief overview and update on MCAK in mammalian oocytes

Eichenlaub-Ritter

Staubach

Trapphoff

2010

Biochemical Society Transactions

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“…The majority of trisomy 13q cases (>90%) are from maternal origin (Hall et al, 2007), typically due to errors in meiosis I, as in other autosomal trisomies. Many cases are from parental balanced translocations, typically as pericentric inversions.…”

Section: Discussionmentioning

confidence: 99%

“…It has been described as having a variable phenotypic expression. It may result from parental reciprocal translocations, parental pericentric inversions (Chen et al, 2005b) or de novo direct duplications (Hall et al, 2007).…”

Section: Introductionmentioning

confidence: 99%

Prenatal diagnosis of a partial trisomy 13q (q14→qter): phenotype, cytogenetics and molecular characterization by spectral karyotyping and array comparative genomic hybridization

Machado¹,

Heinrich²,

Campanhol³

et al. 2010

Genet. Mol. Res.

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ABSTRACT. Partial trisomy 13q is an uncommon chromosomal abnormality with variable phenotypic expression. We report prenatal diagnosis of partial trisomy 13q in a fetus with partial agenesis of the cerebellar vermis, partial agenesis of the corpus callosum, hydrops and polyhydramnios. G-banding karyotyping, spectral karyotyping and array comparative genomic hybridization (aCGH) analysis of fetal blood were performed. Cytogenetic analysis of fetal blood displayed 46,XX,add(4) (q28). The parental karyotypes were normal. A girl was delivered at 34 weeks gestation; she died within 2 h. Autopsy confirmed all the prenatal findings and also showed agenesis of the diaphragm. Spectral karyotyping identified the additional material's origin as chromosome 13. aCGH was carried out and showed amplification of distal regions of the long arm of chromosome 13 from region 13q14 to qter. This is the first report of a fetus with molecular characterization of a partial trisomy 13q (q14→qter), present as a de novo unbalanced translocation at chromosome 4q. This case demonstrates the usefulness of molecular characterization of malformed fetuses for prenatal diagnosis and counseling.

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“…Klinički se ovaj sindrom karakteriše vrlo teškim malformacijama mozga (arinencefalija), očiju (mikroftalmija ili anoftalmija), rascepima usne, vilice i nepca (heliognatopalatoshiza), polidaktilijom (veći broj prstiju), anomalijama srca (defekti septuma), bubrega (cistični bubrezi, potkovičasti bubrezi) i digestivnog PRIKAZI SLUČAJA trakta (malrotacije creva) 4,5,6 . Preživljavanje preko nekoliko nedelja je veoma retko, a 50% dece umire u prva tri dana života.…”

Section: Diskusijaunclassified

Trisomy 13 (Sy Patau)

Hajrović¹,

Preljevic²,

Hajrovic³

et al. 2014

Mat Med

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Trisomy 13 (Sy Patau) is a clinically severe entity. 85% of the patients do not survive beyond one year, and most children die before completing six months of age. We report a female child, 30 day old, white, the third child of a non-consanguineous couple, who presented trisomy 13. The child was born at term, from a vaginal delivery, weighing 3200 g. The second day of life the development of respiratory distress translated ino KBC Kragujevac (release list no.29623). The initial clinical examination detected shisis primariy and secunday palate, ASD, stenosis rami AP, polidactily pedis dextri, microcornea and microftalmia. After 27 days of hospitalization in KBC Kragujevac, transferred to the Institute for mother and child New Belgrade, where he died after three days of receipt. During hospitalization blood samples were taken for determination of kariotip. Parents are advised that in case of subsequent pregnancies occur in the genetic counseling of the Institute for prenatal diagnosis. ApstraktTrizomija 13 (Patau sindrom) je ozbiljan klinički entitet. 85% pacijenata ne preživi duže od godinu dana, a većina umire pre nego što napuni šest meseci. Mi prikazujemo žensko novorođenče, uzrasta 30 dana, treće dete iz kontrolisane trudnoće, koje je imalo trizomiju 13. hromozoma. Dete je rođeno u terminu, vaginalnim putem, težine 3200 grama. Drugi dan života razvija respiratorni distres, pa je prevedeno u KBC Kragujevac. Na prvom kliničkom pregledu konstatovan je rascep primarnog i sekundarnog nepca, ASD, stenoza rami AP, polidaktilija desnog stopala, microcornea i microftalmia. Posle 27 dana hospitalizacije u KBC Kragujevac, prebačeno je u Institut za majku i dete Novi Beograd, gde je umrlo posle tri dana od dana prijema. Tokom hospitalizacije uzet je uzorak krvi za određivanje kariotipa. Roditeljima je savetovano da u slučaju ponovnih trudnoća dođu u genetičko savetovalište Instituta za prenatalnu dijagnostiku.Ključne reči: Patau syndrom, trizomija 13, hromozomopatija, novorođenče. UvodTrizomijа 13 (tаkođe poznаtа kao Pаtаu sindrom) je genetski poremećаj u kome osobа imа tri kopije genetskog mаterijаlа na hromosomu 13, umesto uobičаjenih dvа primerkа. Retko, ekstrа mаterijаl može biti vezаn zа drugi hromozom (trаnslokаcija) 1 .Sindrom je otkrio i opisao prvi put Klaus Patau (Klaus Patau) 1960. godine. Označava se 47 XX+13 ili 47 XY+13, u zavisnosti od pola 1 . Učestalost sindroma je oko 1:8000 -12000 zivorođenčadi. Specifičan etiološki faktora za nastanaka ovog sindroma nije nađen, ali postoji značajna povezanost sa starošću porodilja. U normalnim somatskim ćelijama čoveka broj hromozoma je 46, a u malom broju slučajeva, oko 5%, može se javiti i tzv. mozaicizam, pri kome postoje dve ćelijske linije: jedna sa normalnim brojem hromozoma, a druga sa trizomijom hromozoma 13. Obično su ovakve osobe sa blažim simptomima i lakšim oblikom bolesti 2,3 .Poremećaj se manifestuje multiplim anomalijama: rascep usne, vilice i nepca (heliognatopalatoshiza), mentalna retardacija, polidaktilija, pupčana i preponska kila, mala gla...

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The origin of trisomy 13

Cited by 31 publications

References 18 publications

Chromosomal and cytoplasmic context determines predisposition to maternal age-related aneuploidy: brief overview and update on MCAK in mammalian oocytes

Chromosomal and cytoplasmic context determines predisposition to maternal age-related aneuploidy: brief overview and update on MCAK in mammalian oocytes

Prenatal diagnosis of a partial trisomy 13q (q14→qter): phenotype, cytogenetics and molecular characterization by spectral karyotyping and array comparative genomic hybridization

Trisomy 13 (Sy Patau)

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