Partial trisomy 17q22-qter and partial monosomy Xq27-qter in a girl with a de novo unbalanced translocation due to a postzygotic error: Case report and review of the literature on partial trisomy 17qter

Sarri, Catherine; Gyftodimou, Jolanda; Avramopoulos, Dimitris; Grigoriadou, Maria; Pedersen, W; Pandelia, Effie; Pangalos, Constantinos; Abazis, Danai; Kitsos, George; Vassilopoulos, Dimitris; Brøndum‐Nielsen, Karen; Petersen, Michael B.

doi:10.1002/(sici)1096-8628(19970502)70:1<87::aid-ajmg16>3.0.co;2-t

Cited by 22 publications

(24 citation statements)

References 31 publications

(41 reference statements)

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“…The etiology of trisomy 8 therefore seems to differ from that of common autosomal trisomies, even when considering only liveborn mosaic cases, 13,14 and represents a new addition to the expanding category of mitotically derived chromosome abnormalities, as previously described in some cases of homologous Robertsonian translocations and isochromosomes 40,41 and unbalanced de novo translocations. 42,43 An excess of males was observed in the present study (19M:7F) as previously reported from clinical series. 16,20 Looking only at the mitotic cases in our study, the skewed sex ratio persists (15M:5F).…”

Section: Discussionsupporting

confidence: 90%

Origin of nondisjunction in trisomy 8 and trisomy 8 mosaicism

et al. 1998

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Causes of chromosomal nondisjunction is one of the remaining unanswered questions in human genetics. In order to increase our understanding of the mechanisms underlying nondisjunction we have performed a molecular study on trisomy 8 and trisomy 8 mosaicism. We report the results on analyses of 26 probands (and parents) using 19 microsatellite DNA markers mapping along the length of chromosome 8. The 26 cases represented 20 live births, four spontaneous abortions, and two prenatal diagnoses (CVS). The results of the nondisjunction studies show that 20 cases (13 maternal, 7 paternal) were probably due to mitotic (postzygotic) duplication as reduction to homozygosity of all informative markers was observed and as no third allele was ever detected. Only two cases from spontaneous abortions were due to maternal meiotic nondisjunction. In four cases we were not able to detect the extra chromosome due to a low level of mosaicism. These results are in contrast to the common autosomal trisomies (including mosaics), where the majority of cases are due to errors in maternal meiosis.

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Section: Discussionsupporting

confidence: 90%

Origin of nondisjunction in trisomy 8 and trisomy 8 mosaicism

et al. 1998

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“…Hypertrichosis had previously been reported in a case of partial trisomy 17q22-qter associated with a de novo unbalanced translocation [14], suggesting that the distal portion of human chromosome 17q may contain dosage-sensitive genes that contribute to excessive hair growth. Recently, a series of microdeletions were reported on chromosome 17q24.2–q24.3 in three cases of familial congenital generalized hypertrichosis terminalis with gingival hyperplasia (CGHT), as well as a de novo microduplication within this same region in a case of sporadic CGHT [15].…”

Section: Introductionmentioning

confidence: 88%

Trps1 and Its Target Gene Sox9 Regulate Epithelial Proliferation in the Developing Hair Follicle and Are Associated with Hypertrichosis

et al. 2012

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Hereditary hypertrichoses are a group of hair overgrowth syndromes that are extremely rare in humans. We have previously demonstrated that a position effect on TRPS1 is associated with hypertrichosis in humans and mice. To gain insight into the functional role of Trps1, we analyzed the late morphogenesis vibrissae phenotype of Trps1Δgt mutant mice, which is characterized by follicle degeneration after peg downgrowth has been initiated. We found that Trps1 directly represses expression of the hair follicle stem cell regulator Sox9 to control proliferation of the follicle epithelium. Furthermore, we identified a copy number variation upstream of SOX9 in a family with hypertrichosis that significantly decreases expression of the gene in the hair follicle, providing new insights into the long-range regulation of SOX9. Our findings uncover a novel transcriptional hierarchy that regulates epithelial proliferation in the developing hair follicle and contributes to the pathology of hypertrichosis.

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“…Partial trisomy 17q releated to recognizable dysmorphic evidences and psychomotor retardation. 6 Mental and growth retardation, microcephaly, high forehead, frontal bossing, temporal retraction, short and broad nose, broad and flat nasal bridge, large mouth with down-turned corners, thin upper lip, cleft palate, low-set and malformed ears, short and webbed neck, limb shortness and skeletal anomalies, abnormalities of genital, brain, heart and kidney were reported in partial trisomy17q patients. 6,7 Cordier et al first reported a combination of partial trisomy 17q and monosomy 5p in fetus.…”

Section: Discussionmentioning

confidence: 99%

“…Until now, 32 cases of partial trisomy for the distal region of 17q were reported either inherited or de novo. [2][3][4][5][6][7][8] A derivative chromosome 4 due to partial trisomy of chromosome 17q has never been described, to our knowledge. We demonstrated that the fetus was a carrier of a de novo derivative chromosome 4 arising from partial trisomy 17q.…”

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confidence: 99%