Searching chromosome mosaicisms in 45,X Turner syndrome: how relevant is it?

Soares, Jéssica Silva; Lago, Renata Maria Rabello da Silva; Toralles, Maria Betânia Pereira; Mota, Laís Ribeiro; Alves, Esmeralda Santos; Carvalho, Acácia Fernandes Lacerda de

doi:10.20945/2359-3997000000403

Cited by 1 publication

(2 citation statements)

References 21 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…We expected that a substantial of X monosomy cases would be reclassified to the "low-frequency" 45,X/46,XX mosaic form by using the FISH method. Our expectation was driven by the findings of previous studies that investigated the role of FISH form buccal smear and proposed that tissue-specific karyotyping may explain the discrepancies between karyotypes and phenotypes of individuals with TS [17,18]. However, the FISH of the cells originating from the three distinct germ layers verified X monosomy in the majority of our patients.…”

Section: Discussionmentioning

confidence: 53%

“…However, this was not confirmed by another recent analysis [15]. In addition, studies that explored the tissue-specific mosaicism revealed substantial karyotype differences and indicated that the use of FISH analyses of buccal smears could potentially help to clarify the phenotypic variability in TS [16-18]. Considering the mechanism by which somatic mosaicism emerges [19], it cannot also be excluded that the phenotype of individuals with TS depends on whether the loss of the X chromosome occurred before or after the formation of all three germ layers.…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Karyotyping of Lymphocytes and Epithelial Cells of Distinct Embryonic Origin Does Not Help to Predict the Turner Syndrome Features

et al. 2022

View full text Add to dashboard Cite

Background: In Turner syndrome (TS), fluorescent in situ hybridization (FISH) karyotyping offers an alternative to classical karyotyping. Objective: We tested the added value of FISH karyotyping from lymphocytes (mesodermal origin), buccal cells (ectodermal origin) and a rear-tongue smear (endodermal origin) to determine the 45,X cell line fraction and its impact on patient phenotype. Design and Patients: Classical karyotyping and three FISH assays were done in 153 girls and women previously diagnosed with TS in four university hospitals. The 45,X cell line fraction was determined for each method and correlated with the major phenotypic signs. Results: Classical karyotyping identified 45,X/46,XX mosaicism in 77/153 subjects (50%), 45,X monosomy in 52/153 (34%), and other karyotypes in 24/153 (16%). FISH from lymphocytes verified 45,X in 47/52 original cases, whereas 4/52 had 45,X/46,XX and 1/52 45,X/47,XYY mosaicism. The 45,X cell line fraction was higher in FISH from lymphocytes compared to classical karyotyping (median 86.4% versus 70.0%; p<0.001), while there was no difference for FISH from buccal or rear-tongue smear cells. The mean 45,X cell line fraction was more abundant in patients with several of the characteristic phenotypic signs compared to patients without them (p<0.01), but the predictive power was insufficient. Conclusion: FISH analysis confirmed the findings of classical karyotyping; only a few 45,X monosomy cases were reclassified as mosaics. The 45,X cell line fraction did not show clinically meaningful prediction of the phenotype. FISH analysis of buccal or rear-tongue epithelial cells may be a non-inferior, less invasive alternative to classical karyotyping.

show abstract

Section: Discussionmentioning

confidence: 53%