Your search keyword '"sex chromosome aneuploidy"' showing total 364 results

51. Medical Reasons for Pregnancy Interruption: Chromosomal and Genetic Abnormalities

Author

Dungan, Jeffrey S., Paley Galst, Joann, editor, and Verp, Marion S., editor

Published

2015

52. Experiences of social interaction in young women with Turner syndrome: A qualitative study.

Author

Wolstencroft, Jeanne, Mandy, William, and Skuse, David

Subjects

*COGNITION, *COMMUNICATION, *HEARING disorders, *INTERVIEWING, *RESEARCH methodology, *PARENTS, *QUESTIONNAIRES, *SELF-perception, *SOCIAL adjustment, *SOCIAL skills, *SOCIAL skills education, *TURNER'S syndrome, *QUALITATIVE research, *THEMATIC analysis, *PROMPTS (Psychology)

Abstract

Background: Turner Syndrome (TS; 45,X) is a sex chromosome aneuploidy associated with deficits in social interaction, for which clinical care guidelines have recently recommended trialling a social skills training intervention. The present study aimed to gather preliminary evidence to support a training programme for young women. Methods: Semi‐structured interviews and psychometric questionnaires about social ability were administered to young women with TS aged 16 to 25 years old (n=17) and their parents (n=20). Interview transcripts were analysed using thematic analysis. Results: Although young women with TS experienced a "wide range of social competencies," they attributed social challenges to "personal and contextual factors." The magnitude of these challenges to social integration intensified during adolescence. They felt increasingly "out of sync" with their peers. They also considered their social abilities to be better than their parents did; on a scale of autistic traits (rated by parents), half had mild to severe autistic traits. Most expressed interest in taking part in a social skills programme. Conclusion: Young women with TS are aware they experience difficulties in social communication, and they express interest in improving their social skills. Accordingly, social skills training during adolescence would be welcomed by them and their families. Any intervention should take account of their feelings of social dislocation arising from hearing difficulties together with limited recognition, and slow processing, of social cues. [ABSTRACT FROM AUTHOR]

Published

2020

53. Emotion regulation in adults with Klinefelter syndrome (47,XXY): Neurocognitive underpinnings and associations with mental health problems.

Author

Rijn, Sophie and Swaab, Hanna

Subjects

*KLINEFELTER'S syndrome, *ASSOCIATION of ideas, *MENTAL health, *EMOTIONS, *HOSTILITY, *ADULTS

Abstract

Objectives: The aim of this study is to evaluate if language and executive functioning deficits in individuals with the 47,XXY chromosomal pattern contribute to emotion regulation problems and related symptoms of psychopathology. Methods: A group of 26 adult men with 47,XXY completed measures of cognitive emotion regulation strategies, neurocognitive functioning, and symptoms of psychopathology. Results: Atypical emotion regulation strategies were found in the XXY group, with increased expression of emotions (69%), avoiding (65%), distraction seeking (54%), and passive coping (54%). More difficulties in mental flexibility and attention regulation, and speeded responding were associated with more pronounced emotion expression (emotional outbursts). Emotion regulation problems were associated with symptoms of anxiety, depression, thought problems, and hostility. Conclusion: This study has identified emotion regulation as a potential target for treatment and intervention, with a specific focus on executive functions in the management of emotions in individuals with 47,XXY. [ABSTRACT FROM AUTHOR]

Published

2020

54. Testosterone Treatment in Infants With 47,XXY: Effects on Body Composition.

Author

Davis, Shanlee M, Reynolds, Regina M, Dabelea, Dana M, Zeitler, Philip S, and Tartaglia, Nicole R

Subjects

TESTOSTERONE, KLINEFELTER'S syndrome in children, BODY composition

Abstract

Context Boys with XXY have greater adiposity and a higher risk of cardiovascular disease. Infants with XXY have lower testosterone concentrations than typical boys, but no studies have evaluated adiposity in infants with XXY or the physiologic effects of giving testosterone replacement. Objective To determine the effect of testosterone on body composition in infants with XXY. Design Prospective, randomized trial. Setting Tertiary care pediatric referral center. Participants 20 infants 6 to 15 weeks of age with 47,XXY. Intervention Testosterone cypionate 25 mg intramuscularly monthly for three doses vs no treatment. Main Outcome Measures Difference in change in adiposity (percent fat mass z scores); other body composition measures, penile length, and safety outcomes between treated and untreated infants; and comparison with typical infants. Results The increase in percent fat mass (%FM) z scores was greater in the untreated group than in the treated group (+0.92 ± 0.62 vs −0.12 ± 0.65, P = 0.004). Increases in secondary outcomes were greater in the testosterone-treated group for total mass, fat-free mass, length z score, stretched penile length, and growth velocity (P < 0.002 for all). At 5 months of age, adiposity in untreated infants with XXY was 26.7% compared with 23.2% in healthy male infants of the same age (P = 0.0037); there was no difference in %FM between the treated XXY boys and controls. Reported side effects were minimal and self-limited; no serious adverse events occurred. Conclusions Adiposity of untreated infants was 15% greater than that of male controls by 5 months of age. Testosterone treatment for infants with XXY resulted in positive changes in body composition. [ABSTRACT FROM AUTHOR]

Published

2019

55. CHK1-CENP B/MAD2 is associated with mild oxidative damage-induced sex chromosome aneuploidy of male mouse embryos during in vitro fertilization.

Author

Huang, Yue, Ha, Siyao, Li, Zhiling, Li, Jiena, and Xiao, Wanfen

Subjects

*Y chromosome, *FERTILIZATION in vitro, *SEX chromosomes, *MITOSIS, *HUMAN chromosomes, *CHROMOSOME abnormalities

Abstract

A high incidence of aneuploidy is observed in vitro fertilization (IVF)-derived embryos, but the formation and repair mechanisms are unknown. Here, we investigated the effects of slightly increased reactive oxygen species (ROS) produced by in vitro culture conditions on embryo aneuploidy and the roles of the spindle assembly checkpoint (SAC) protein, mitotic arrest-deficient 2 (MAD2), and the DNA damage response (DDR) protein, checkpoint kinase 1 (CHK1), in aneuploidy repair. By assessing chromosome abnormalities via DAPI staining, karyotype analysis and next-generation sequencing technology, we demonstrated that mild oxidative damage mainly increased the risk of sex chromosome aneuploidy in male mouse embryos (41,XXY,+X and 41,XYY,+Y) through chromosome mis-segregation during the first mitosis. Isobaric tags for relative and absolute quantitation technology revealed that mild oxidative damage inhibited the expression of male reproduction-related proteins, including a kinase anchor protein 4 (AKAP4), whose gene is located on mouse/human Chromosome X. Under mild oxidative damage, abrogation of MAD2 by MAD2 inhibitor-1 (M2I-1) or CHK1 by siRNA microinjection increased sex chromosome mosaicism rate and reduced mitosis-promoting factor (MPF) activity. CHK1 inhibition also reduced kinetochore localization of centromere protein B (CENP B) and MAD2. These findings show that DDR and SAC are responsible for repair of sex chromosome mosaicism via the pCHK1 (S345)-CENP B/MAD2-MPF pathway; further, IVF may have negative effects on male offspring's reproduction ability, which ultimately depends on their continued repair capability. Therefore, we suggest that antioxidants, especially those targeting improved CHK1-MAD2 function, may be a promising therapeutic strategy to reduce aneuploidy formation of IVF-derived embryos and to maintain genome integrity of embryo and offspring. Image 1 • ROS increases sex chromosome aneuploidy of IVF male embryos during first mitosis. • ROS inhibits the expression of male reproduction-related proteins. • CHK1-CENP B/MAD2 is responsible for repair of ROS-induced sex chromosome mosaicism. • High levels of MAD2 after first mitosis continue to repair abnormal sex chromosomes. • Male offspring's reproduction ability is dependent on ROS damage and continuous repair. [ABSTRACT FROM AUTHOR]

Published

2019

56. Patterns of psychopathology and cognition in sex chromosome aneuploidy

Author

Ethan T. Whitman, Srishti Rau, Kimberly Schauder, Lauren Kenworthy, Nancy Raitano Lee, Nikhita Gogate, and Armin Raznahan

Subjects

Adult, Adolescent, Psychopathology, Cognitive Neuroscience, Mental Disorders, Sex chromosomes, Cognition, Neurosciences. Biological psychiatry. Neuropsychiatry, Aneuploidy, Pathology and Forensic Medicine, Neurogenetic conditions, Sex chromosome aneuploidy, Pediatrics, Perinatology and Child Health, Humans, Neurology (clinical), Child, Psychology, Sex Chromosome Aberrations, Clinical psychology, RC321-571

Abstract

Background Sex chromosome aneuploidies (SCAs) are a collectively common family of genetic disorders that increase the risk for neuropsychiatric and cognitive impairment. Beyond being important medical disorders in their own right, SCAs also offer a unique naturally occurring model for studying X- and Y-chromosome influences on the human brain. However, it remains unclear if (i) different SCAs are associated with different profiles of psychopathology and (ii) the notable interindividual variation in psychopathology is related to co-occurring variation in cognitive ability. Methods We examined scores for 11 dimensions of psychopathology [Child/Adult Behavior Checklist (CBCL)] and general cognitive ability [full-scale IQ (FSIQ) from Wechsler tests] in 110 youth with varying SCAs (XXY = 41, XYY = 22, XXX = 27, XXYY = 20) and 131 typically developing controls (XX = 59, XY = 72). Results All SCAs were associated with elevated CBCL scores across several dimensions of psychopathology (two-sample t tests comparing the euploidic and aneuploidic groups [all |T| > 9, and p < 0.001]). Social and attentional functioning were particularly sensitive to the carriage of a supernumerary Y-chromosome. In particular, the XYY group evidenced significantly more social problems than both extra-X groups (Cohen’s d effect size > 0.5, Bonferroni corrected p < .05). There was marked variability in CBCL scores within each SCA group, which generally correlated negatively with IQ, but most strongly so for social and attentional difficulties (standardized β, − 0.3). These correlations showed subtle differences as a function of the SCA group and CBCL scale. Conclusions There is domain-specific variation in psychopathology across SCA groups and domain-specific correlation between psychopathology and IQ within SCAs. These findings (i) help to tailor clinical assessment of this common and impactful family of genetic disorders and (ii) suggest that dosage abnormalities of X- and Y-linked genes impart somewhat distinct profiles of neuropsychiatric risk.

Published

2021

57. Executive Dysfunction in Klinefelter Syndrome: Associations With Brain Activation and Testicular Failure.

Author

Foland-Ross LC, Ghasemi E, Lozano Wun V, Aye T, Kowal K, Ross J, and Reiss AL

Subjects

Male, Adolescent, Humans, Child, Brain pathology, Testosterone, Executive Function, Klinefelter Syndrome genetics, Cognitive Dysfunction etiology

Abstract

Context: Executive dysfunction is a well-recognized component of the cognitive phenotype of Klinefelter syndrome (KS), yet the neural basis of KS-associated cognitive weaknesses, and their association with testicular failure is unknown., Objective: We investigated executive function, brain activation, and pubertal development in adolescents with and without KS., Methods: Forty-three adolescents with KS (mean age 12.3 ± 2.3 years) and 41 typically developing boys (mean age 11.9 ± 1.8 years) underwent pubertal evaluation, behavioral assessment, and completed functional magnetic resonance imaging (fMRI) as they performed an executive function task, the go/no-go task. Group differences in activation were examined. Associations among activation, executive function, and pubertal development measures were tested in secondary analyses., Results: Boys with KS exhibited reduced executive function, as well as lower activation in brain regions subserving executive function, including the inferior frontal gyrus, anterior insula, dorsal anterior cingulate cortex, and caudate nucleus. Secondary analyses indicated that the magnitude of activation differences in boys with KS was associated with severity of pubertal developmental delay, as indexed by lower testosterone (t(36) = 2.285; P = .028) and lower testes volume (t(36) = 2.238; P = .031). Greater parent-reported attention difficulties were additionally associated with lower testicular volume (t(36) = -2.028; P = .050)., Conclusion: These findings indicate a neural basis for executive dysfunction in KS and suggest alterations in pubertal development may contribute to increased severity of this cognitive weakness. Future studies that examine whether these patterns change with testosterone replacement therapy are warranted., (© The Author(s) 2023. Published by Oxford University Press on behalf of the Endocrine Society. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com.)

Published

2023

58. Non-Invasive Prenatal Testing for Sex Chromosome Aneuploidy in Routine Clinical Practice.

Author

Kornman, Louise, Palma-Dias, Ricardo, Nisbet, Debbie, Scott, Fergus, Menezes, Melody, da Silva Costa, Fabricio, and McLennan, andrew

Subjects

*ANEUPLOIDY, *SEX chromosomes, *PRENATAL diagnosis, *Y chromosome, *X chromosome, *SEX chromosome abnormalities

Abstract

Objectives: To assess the accuracy of non-invasive prenatal testing (NIPT) for sex chromosome aneuploidy (SCA) in routine clinical practice and to review counselling and sonographic issues arising in SCA cases.Methods: Three specialist Australian obstetric ultrasound and prenatal diagnosis practices offering NIPT after 10 weeks' gestation participated in this study. NIPT was reported for chromosomes 21, 18, 13, X, and Y.Results: NIPT screening was performed in 5,267 singleton pregnancies. The odds of being affected given a positive screening result (OAPR) was lowest for SCAs, most notably for monosomy X (20%). Fewer women underwent invasive prenatal testing when counselled regarding a high risk for SCA (65.5%) compared with those who had a high risk for another aneuploidy (85%). The positive screening rate of NIPT including SCA was 2.3%, but 1.2% if only the autosomal trisomies were included in the panel.Conclusion: The addition of SCA testing to NIPT doubles the positive screening rate. The OAPR for SCAs (most notably for monosomy X) is reduced compared with the autosomal trisomies. Clinicians need a more extensive discussion with women prior to the inclusion of the X and Y chromosomes in the NIPT panel, given the complexity in counselling regarding further management and the additional anxiety that these abnormal results may cause. A benefit of sex chromosome analysis is an improvement in antenatal diagnosis of some disorders of sexual development. [ABSTRACT FROM AUTHOR]

Published

2018

59. Mammalian X Chromosome Dosage Compensation: Perspectives From the Germ Line.

Author

Sangrithi, Mahesh N. and Turner, James M. A.

Subjects

*X chromosome, *MAMMALS, *GERM cells, *DIMORPHISM in animals, *NUCLEOTIDE sequencing

Abstract

Sex chromosomes are advantageous to mammals, allowing them to adopt a genetic rather than environmental sex determination system. However, sex chromosome evolution also carries a burden, because it results in an imbalance in gene dosage between females (XX) and males (XY). This imbalance is resolved by X dosage compensation, which comprises both X chromosome inactivation and X chromosome upregulation. X dosage compensation has been well characterized in the soma, but not in the germ line. Germ cells face a special challenge, because genome wide reprogramming erases epigenetic marks responsible for maintaining the X dosage compensated state. Here we explain how evolution has influenced the gene content and germ line specialization of the mammalian sex chromosomes. We discuss new research uncovering unusual X dosage compensation states in germ cells, which we postulate influence sexual dimorphisms in germ line development and cause infertility in individuals with sex chromosome aneuploidy. [ABSTRACT FROM AUTHOR]

Published

2018

60. Sleep Problems and Life Satisfaction as Predictors of Health in Men with Sex Chromosome Aneuploidies.

Author

Fjermestad, Krister W. and Stokke, Simen

Subjects

*ANEUPLOIDY, *EMOTIONS, *HEALTH status indicators, *HEALTH surveys, *MEDICAL care, *PAIN, *PATIENTS, *QUESTIONNAIRES, *REGRESSION analysis, *SATISFACTION, *SELF-evaluation, *SEX chromosomes, *SLEEP disorders, *WELL-being

Abstract

More knowledge is needed about men with sex chromosome aneuploidies (SCA). We present self-reported data from 53 men with SCA (Mage = 36.8 years, SD = 12.3, range 19-67). The Health Survey-Short Form (SF-36) measured eight health domains (physical functioning, role-physical, role-emotional, vitality, emotional health, social functioning, pain, general health). The Pittsburgh Sleep Quality Index measured sleep problems. The Personal Wellbeing Index measured satisfaction with eight life domains. Compared to norms, SCA reported poorer health (mean d = −0.80) and more sleep problems (mean d = −0.85). Differences between SCA and norms on personal well-being were small, except lower health satisfaction in SCA (d = −1.06). Seven of eight regression models predicting the SF-36 domains from life satisfaction and sleep problems were significant (explained variance 12.2% to 46.2%), except physical functioning (ns). Clinical assessment/intervention for a broad range of health and sleep problems is indicated for men with SCA. [ABSTRACT FROM AUTHOR]

Published

2018

61. International investigation of neurocognitive and behavioral phenotype in 47,XXY (Klinefelter syndrome): Predicting individual differences.

Author

Samango‐Sprouse, Carole, Stapleton, Emily, Chea, Selena, Lawson, Patrick, Sadeghin, Teresa, Cappello, Chris, de Sonneville, Leo, and van Rijn, Sophie

Abstract

47,XXY (KS) occurs in 1:650 male births, though less than 25% are ever identified. We assessed stability of neurocognitive features across diverse populations and quantified factors mediating outcome. Forty‐four boys from the Netherlands (NL) and 54 boys from the United States (US) participated. The Wechsler Intelligence Scales assessed intellectual functioning; the ANT program evaluated cognitive function; and the CBCL assessed behavioral functioning. ANOVA was used for group comparisons. Hierarchical regressions assessed variance explained by each independent variable: parental education, timing of diagnosis, testosterone, age, and nationality. Parental education, timing of diagnosis, and hormonal treatment all played an important role in neurocognitive performance. The observed higher IQ and better attention regulation in the US group as compared to the NL group was observed with decreased levels of behavioral problems in the US group. Cognitive measures that were different between the NL and US groups, i.e., attention regulation and IQ scores, were also significantly influenced by external factors including timing of diagnosis, testosterone treatment, and parental education. On the ANT, a cognitive phenotype of 47,XXY was observed, with similar scores on 9 out of the 10 ANT subtests for the NL and US groups. This study lays additional features to the foundation for an algorithm linking external variables to outcome on various neurodevelopmental measures. [ABSTRACT FROM AUTHOR]

Published

2018

62. The effect of early life stress on the cognitive phenotype of children with an extra X chromosome (47,XXY/47,XXX).

Author

van Rijn, Sophie, Barneveld, Petra, Descheemaeker, Mie-Jef, Giltay, Jacques, and Swaab, Hanna

Subjects

*STRESS in children, *HUMAN phenotype, *KLINEFELTER'S syndrome in children, *GENOTYPE-environment interaction, *COGNITIVE ability

Abstract

Studies on gene-environment interactions suggest that some individuals may be more susceptible to life adversities than others due to their genetic profile. This study assesses whether or not children with an extra X chromosome are more vulnerable to the negative impact of early life stress on cognitive functioning than typically-developing children. A total of 50 children with an extra X chromosome and 103 non-clinical controls aged 9 to 18 years participated in the study. Cognitive functioning in domains of language, social cognition and executive functioning were assessed. Early life stress was measured with the Questionnaire of Life Events. High levels of early life stress were found to be associated with compromised executive functioning in the areas of mental flexibility and inhibitory control, irrespective of group membership. In contrast, the children with an extra X chromosome were found to be disproportionally vulnerable to deficits in social cognition on top of executive dysfunction, as compared to typically-developing children. Within the extra X group the number of negative life events is significantly correlated with more problems in inhibition, mental flexibility and social cognition. It is concluded that children with an extra X chromosome are vulnerable to adverse life events, with social cognition being particularly impacted in addition to the negative effects on executive functioning. The findings that developmental outcome is codependent on early environmental factors in genetically vulnerable children also underscores opportunities for training and support to positively influence the course of development. [ABSTRACT FROM AUTHOR]

Published

2018

63. False Low-Risk Single Nucleotide Polymorphism–Based Noninvasive Prenatal Screening in Pentasomy 49,XXXXY

Author

Manesha Putra, Melissa A. Hicks, and Jacques S. Abramowicz

Subjects

sex chromosome aneuploidy, nipt, prenatal diagnosis, screening, Gynecology and obstetrics, RG1-991

Abstract

Introduction Pentasomy 49,XXXXY is a sex chromosome anomaly difficult to be diagnosed prenatally. We describe a patient of pentasomy 49,XXXXY with false low-risk results using a noninvasive prenatal screening (NIPS). A 30-year-old G1P0 woman presented at 336/7 weeks, secondary to sonographic fetal anomalies. She had low-risk NIPS at 136/7 weeks. Anatomy survey showed bilateral clubfeet, clinodactyly of the left fifth digit, micropenis, and echogenic bowel. Cytogenetics analysis revealed pentasomy 49,XXXXY syndrome. We report third-trimester sonographic features of a fetus with pentasomy 49,XXXXY and the importance of thorough pre- and posttest counseling for NIPS.

Published

2018

64. 49, XXXXY syndrome: An infant presenting with ambiguous genitalia

Author

Rajendra B Nerli, Prasad V Magdum, Amit M Mungarwadi, Shridhar C Ghagane, and Murigendra B Hiremath

Subjects

49 XXXXY syndrome, ambiguous genitalia, intrauterine growth restriction, sex chromosome aneuploidy, Medicine

Abstract

Presences of normal genes on the Y chromosome are essential for normal sex determination and sex differentiation of male genitalia. Several genes on the X chromosome and other autosomes have been shown to be anti-testes and have a detrimental effect on the development process of normal male genital system. The addition of X chromosomes to the 46, XY karyotype results in seminiferous tubules dysgenesis, hypogonadism, and malformed genitalia. We report an infant male with 49, XXXXY syndrome presenting with ambiguous genitalia and multiple extra-gonadal anomalies.

Published

2016

65. Parental decisions following prenatal diagnosis of sex chromosome aneuploidy in Hong Kong.

Author

So, Po Lam, Cheng, Kwun Yue Yvonne, Cheuk, Kwan Yiu, Chiu, Wan Kam, Mak, Shui Lam, Mok, Sau Lan, Lo, Tsz Kin, Yung, Wai Kuen, Lo, Fai Man, Chung, Hon Yin Brian, Kan, Sik Yau Anita, Lee, Chin Peng, and Tang, Hoi Yin Mary

Subjects

*SEX chromosome abnormalities, *ABORTION, *ANEUPLOIDY, *COUNSELING, *DECISION making, *DEMOGRAPHY, *FETAL ultrasonic imaging, *LONGITUDINAL method, *MOSAICISM, *MULTIVARIATE analysis, *PRENATAL diagnosis, *REGRESSION analysis, *STATISTICS, *RETROSPECTIVE studies, *ODDS ratio, *PREGNANCY, *DIAGNOSIS

Abstract

Aim According to the published work, pregnancy termination rates due to prenatal diagnosis of fetal sex chromosome aneuploidies (SCA) vary widely. Some potentially modifiable and non-modifiable factors have been reported to be associated with parental decision. This study aimed to evaluate the rate of pregnancy termination for fetal SCA and the factors influencing parents' decisions in Hong Kong. Methods This was a 21-year retrospective cohort study of parents' decisions following prenatal diagnosis of SCA. Univariate and multivariate analyses for the association between demographic factors, prenatal factors, or counseling provided and decision-making were conducted. Results The study included 399 pregnancies with prenatal diagnosis of SCA and the overall termination rate was 55.6% (91.7%, 48.0%, 23.4%, 4.8%, and 22.7% for 45,X, 47,XXY, 47,XXX, 47,XYY, and mosaicism, respectively). Pregnancies with ultrasound abnormalities were associated with higher termination rates than pregnancies with normal ultrasound findings (91.3% vs 28.3%, P < 0.0001). From multivariate regression analysis on 226 pregnancies with normal ultrasound examination, a higher likelihood to terminate was found in pregnancies affected by 45,X and 47,XXY (adjusted odds ratio, 4.72, P < 0.0001). Increased maternal age and history of infertility were associated with lower likelihood to terminate (adjusted odds ratio, 0.9, P = 0.012; and 5.12, P = 0.038, respectively). The pregnancy termination rate declined over time. Conclusion A significant correlation was found between the termination of SCA-affected pregnancy and the presence of fetal sonographic abnormalities, type of SCA, maternal age, and presence of infertility. [ABSTRACT FROM AUTHOR]

Published

2017

66. Analysis of cell-free DNA in maternal blood in screening for aneuploidies: updated meta-analysis.

Author

Gil, M. M., Accurti, V., Santacruz, B., Plana, M. N., and Nicolaides, K. H.

Subjects

*ANEUPLOIDY, *BLOOD testing, *DNA analysis, *MEDICAL screening, *TRISOMY, *FETAL abnormalities

Abstract

Objectives: To review clinical validation or implementation studies of maternal blood cell-free (cf) DNA analysis and define the performance of screening for fetal trisomies 21, 18 and 13 and sex chromosome aneuploidies (SCA).Methods: Searches of PubMed, EMBASE and The Cochrane Library were performed to identify all peer-reviewed articles on cfDNA testing in screening for aneuploidies between January 2011, when the first such study was published, and 31 December 2016. The inclusion criteria were peer-reviewed study reporting on clinical validation or implementation of maternal cfDNA testing in screening for aneuploidies, in which data on pregnancy outcome were provided for more than 85% of the study population. We excluded case-control studies, proof-of-principle articles and studies in which the laboratory scientists carrying out the tests were aware of fetal karyotype or pregnancy outcome. Pooled detection rates (DRs) and false-positive rates (FPRs) were calculated using bivariate random-effects regression models.Results: In total, 35 relevant studies were identified and these were used for the meta-analysis on the performance of cfDNA testing in screening for aneuploidies. These studies reported cfDNA results in relation to fetal karyotype from invasive testing or clinical outcome. In the combined total of 1963 cases of trisomy 21 and 223 932 non-trisomy 21 singleton pregnancies, the weighted pooled DR and FPR were 99.7% (95% CI, 99.1-99.9%) and 0.04% (95% CI, 0.02-0.07%), respectively. In a total of 563 cases of trisomy 18 and 222 013 non-trisomy 18 singleton pregnancies, the weighted pooled DR and FPR were 97.9% (95% CI, 94.9-99.1%) and 0.04% (95% CI, 0.03-0.07%), respectively. In a total of 119 cases of trisomy 13 and 212 883 non-trisomy 13 singleton pregnancies, the weighted pooled DR and FPR were 99.0% (95% CI, 65.8-100%) and 0.04% (95% CI, 0.02-0.07%), respectively. In a total of 36 cases of monosomy X and 7676 unaffected singleton pregnancies, the weighted pooled DR and FPR were 95.8% (95% CI, 70.3-99.5%) and 0.14% (95% CI, 0.05-0.38%), respectively. In a combined total of 17 cases of SCA other than monosomy X and 5400 unaffected singleton pregnancies, the weighted pooled DR and FPR were 100% (95% CI, 83.6-100%) and 0.004% (95% CI, 0.0-0.08%), respectively. For twin pregnancies, in a total of 24 cases of trisomy 21 and 1111 non-trisomy 21 cases, the DR was 100% (95% CI, 95.2-100%) and FPR was 0.0% (95% CI, 0.0-0.003%), respectively.Conclusions: Screening by analysis of cfDNA in maternal blood in singleton pregnancies could detect > 99% of fetuses with trisomy 21, 98% of trisomy 18 and 99% of trisomy 13 at a combined FPR of 0.13%. The number of reported cases of SCA is too small for accurate assessment of performance of screening. In twin pregnancies, performance of screening for trisomy 21 is encouraging but the number of cases reported is small. Copyright © 2017 ISUOG. Published by John Wiley & Sons Ltd. [ABSTRACT FROM AUTHOR]

Published

2017

67. The Impact of Living with Klinefelter Syndrome: A Qualitative Exploration of Adolescents and Adults.

Author

Turriff, Amy, Macnamara, Ellen, Levy, Howard, and Biesecker, Barbara

Abstract

Klinefelter syndrome (XXY) is a common yet significantly underdiagnosed condition with considerable medical, psychological and social implications. Many health care providers lack familiarity with XXY, resulting in medical management challenges and a limited understanding of the personal impact of the condition. Genetic counselors benefit from understanding the challenges adolescents and men with XXY face to effectively address their medical and psychosocial needs. The purpose of this study was to understand the impact of living with XXY as an adolescent or an adult. Individuals aged 14 to 75 years with self-reported XXY were recruited from online support networks to complete a web-based survey that included open-ended questions. Open-ended responses were coded and analyzed thematically ( n = 169 to 210 for each open-ended question). Over half of respondents to the open-ended questions reported challenges in finding health care providers who are knowledgeable about XXY, with many describing an extensive diagnostic odyssey and relief when receiving a diagnosis. Individuals sought support coping with the challenges they face and acknowledgement of the positive aspects of XXY. Recommendations are made for how genetic counseling can enhance quality of life for individuals living with XXY. [ABSTRACT FROM AUTHOR]

Published

2017

68. Health professionals' involvement and information provision in genetic counseling following prenatal diagnosis of sex chromosome aneuploidy in Hong Kong.

Author

So, Po Lam, Cheng, Yvonne Kwun Yue, Cheuk, Kwan Yiu, Chiu, Wan Kam, Mak, Shui Lam, Mok, Sau Lan, Lo, Tsz Kin, Yung, Wai Kuen, Lo, Fai Man, Chung, Brian Hon Yin, Kan, Anita Sik Yau, Lee, Chin Peng, and Tang, Mary Hoi Yin

Subjects

*PRENATAL diagnosis, *GENETIC counseling, *SEX chromosomes, *ANEUPLOIDY, *OBSTETRICIANS, *COUNSELING, *OBSTETRICS, *RETROSPECTIVE studies

Abstract

This study supports training in genetic counseling for obstetricians and adoption of a multidisciplinary approach in the counseling process following prenatal diagnosis of sex chromosome aneuploidy. [ABSTRACT FROM AUTHOR]

Published

2019

69. Noninvasive prenatal testing for assessing foetal sex chromosome aneuploidy: a retrospective study of 45,773 cases

Author

Jiansheng Zhu, Keting Tong, Xinran Lu, Junxiang Tang, Chaohong Wang, and Yuxiu Sun

Subjects

medicine.medical_specialty, Positive predictive value, lcsh:QH426-470, Genetic counseling, Prenatal diagnosis, Noninvasive prenatal testing, Advanced maternal age, Biochemistry, Genetics, medicine, Risk factor, Molecular Biology, Genetics (clinical), Pregnancy, Fetus, High-throughput sequencing, Obstetrics, business.industry, Research, Biochemistry (medical), Retrospective cohort study, Prenatal screening, medicine.disease, lcsh:Genetics, Sex chromosome aneuploidy, Molecular Medicine, Anxiety, medicine.symptom, business

Abstract

Objective To assess the positive predictive value (PPV) of noninvasive prenatal testing (NIPT) as a screening test for sex chromosome aneuploidy (SCA) with different maternal characteristics and prenatal decisions in positive cases. Materials and methods We retrospectively analysed 45,773 singleton pregnancies with different characteristics that were subjected to NIPT in the Maternity and Child Health Hospital of Anhui Province. The results were validated by karyotyping. Clinical data, diagnostic results, and data on pregnancy outcomes were collected. Results In total, 314 cases were SCA positive by NIPT; among those, 143 underwent invasive prenatal diagnostic testing, and 58 were true-positive. Overall, the PPVs for 45,X, 47,XXX, 47,XXY and 47,XYY were 12.5%, 51.72%, 66.67% and 83.33%, respectively. Interestingly, when only pregnant women of advanced maternal age (AMA) were screened, the PPVs for 45,X, 47,XXX, 47,XXY and 47,XYY were 23.81%, 53.33%, 78.95%, and 66.67%, respectively. The frequency of SCA was significantly higher in the AMA group than in the non-AMA group. The frequencies of 47,XXX and 47,XXY were significantly correlated with maternal age. Conclusion NIPT performed better in predicting sex chromosome trisomies than monosomy X, and patients with 45,X positive foetuses were more eager to terminate pregnancy than those with 47,XXX and 47,XYY. AMA may be a risk factor of having a foetus with SCA. Our findings may assist in genetic counselling of AMA pregnant women. Our pre- and posttest counselling are essential for familiarizing pregnant women with the benefits and limitations of NIPT, which may ease their anxiety and enable them to make informed choices for further diagnosis and pregnancy decisions.

Published

2021

70. Rare sex chromosome variation 48,<scp>XXYY</scp>: An integrative review

Author

Kristy K. Martyn, Amy Talboy, Sharron Close, and Amy Blumling

Subjects

Male, education.field_of_study, Sex Chromosomes, Adolescent, Population, Aneuploidy, Sex chromosome aneuploidy, Klinefelter Syndrome, Variation (linguistics), Chromosome (genetic algorithm), Inclusion and exclusion criteria, Genetics, Humans, Child, education, Psychology, Psychosocial, Neurocognitive, Sex Chromosome Aberrations, Genetics (clinical), Brain function, Clinical psychology

Abstract

While the most common Sex Chromosome Aneuploidy (SCA) is 47,XXY, other variations, such as 48,XXYY, are less studied, perhaps due to its rarity. 48,XXYY occurs with an estimated prevalence of 1:18,000-40,000 male births. This SCA is associated with a variety of complex physical, psychological, and neuroanatomical findings. The purpose of this integrative review is to summarize the available evidence related to 48,XXYY and identify gaps in the literature. This study utilized integrative review and PRISMA-guided methodology to search six databases for information pertaining to 48,XXYY. There were no exclusion criteria related to design methodology, given the paucity of available research. Among 397 articles reviewed for potential inclusion, 30 articles remained after inclusion and exclusion criteria were applied. Seven of these articles concentrated solely on participants with 48,XXYY. Literature was summarized into categories of physical phenotype, psychosocial, behavioral, neurocognitive, and brain function. Clinical description of 48,XXYY has evolved over time to develop a deeper understanding of this complex disorder. Large gaps remain, especially a lack of experimental studies, clinical guidelines, and treatments. Additionally, few studies explore methodologies such as interviews or self-report surveys in this population. 48,XXYY presents with a wide spectrum of physical, psychological, and neurocognitive symptoms, and frequently requires complex interdisciplinary care. In order to better understand this disorder and to appropriately treat the individuals affected by it, future research should focus on experimental studies and research that utilizes a variety of methods, including participant interviews and patient-report surveys.

Published

2020

71. Sex chromosome aneuploidy alters the relationship between neuroanatomy and cognition

Author

Siyuan Liu, Francois Lalonde, Jonathan D. Blumenthal, Ethan T. Whitman, Kathleen Wilson, Allysa Warling, Liv S. Clasen, and Armin Raznahan

Subjects

Male, Biology, Article, Cohort Studies, Sex chromosome aneuploidy, Cognition, Genetics, medicine, Humans, Supernumerary, Sex Chromosome Aberrations, Genetics (clinical), Sex Chromosomes, Brain, Wechsler Adult Intelligence Scale, Aneuploidy, Brain Cortical Thickness, Magnetic Resonance Imaging, Phenotype, Neuroanatomy, medicine.anatomical_structure, Karyotyping, Cohort, Female

Abstract

Sex chromosome aneuploidy (SCA) increases the risk for cognitive deficits, and confers changes in regional cortical thickness (CT) and surface area (SA). Neuroanatomical correlates of inter-individual variation in cognitive ability have been described in health, but are not well-characterized in SCA. Here, we modeled relationships between general cognitive ability (estimated using full-scale IQ [FSIQ] from Wechsler scales) and regional estimates of SA and CT (from structural MRI scans) in both aneuploid (28 XXX, 55 XXY, 22 XYY, 19 XXYY) and typically-developing euploid (79 XX, 85 XY) individuals. Results indicated widespread decoupling of normative anatomical–cognitive relationships in SCA: we found five regions where SCA significantly altered SA–FSIQ relationships, and five regions where SCA significantly altered CT–FSIQ relationships. The majority of areas were characterized by the presence of positive anatomy-IQ relationships in health, but no or slightly negative anatomy-IQ relationships in SCA. Disrupted anatomical–cognitive relationships generalized from the full cohort to karyotypically defined subcohorts (i.e., XX-XXX; XY-XYY; XY-XXY), demonstrating continuity across multiple supernumerary SCA conditions. As the first direct evidence of altered regional neuroanatomical–cognitive relationships in supernumerary SCA, our findings shed light on potential genetic and structural correlates of the cognitive phenotype in SCA, and may have implications for other neurogenetic disorders.

Published

2020

72. Impact of early diagnosis and noninvasive prenatal testing (NIPT): Knowledge, attitudes, and experiences of parents of children with sex chromosome aneuploidies (SCAs)

Author

Andrea L. Gropman, Carole A. Samango-Sprouse, Teresa Sadeghin, Patricia C. Lasutschinkow, Selena L. Tran, and Grace F. Porter

Subjects

Male, Parents, 0301 basic medicine, Health Knowledge, Attitudes, Practice, medicine.medical_specialty, Prenatal counseling, Noninvasive Prenatal Testing, Psychological intervention, MEDLINE, Sex Chromosome Disorders, 030105 genetics & heredity, 03 medical and health sciences, Sex chromosome aneuploidy, Klinefelter Syndrome, 0302 clinical medicine, Prenatal Diagnosis, XYY Karyotype, Health care, medicine, Humans, Sex Chromosome Aberrations, Genetics (clinical), Multiple choice, 030219 obstetrics & reproductive medicine, business.industry, Obstetrics and Gynecology, Expectant mothers, Early Diagnosis, Family medicine, Female, Personal experience, business

Abstract

Objective To investigate the attitudes of parents of children with a sex chromosome aneuploidy (SCA) regarding the impact of an early diagnosis and noninvasive prenatal testing (NIPT). Method A survey consisting of multiple choice and long response formatted questions was completed by parents of children with SCA(s). Results Fifty-five participants responded to the survey. A total of 88.1% of participants who received an early diagnosis expressed that it had a positive impact on their child's life. Of the 23 participants who utilized NIPT, 95.7% believed it was a decisive factor in their life because they could research the disorders prior to the birth of their child (35.3%), pinpoint valuable resources and interventions (38.2%), and determine possible risk factors of neurodevelopmental delays to be considered after delivery (20.6%). Conclusion This study documented parental perspectives on the impact of an early SCA diagnosis and attitudes towards NIPT use for identifying those at risk for SCAs. These informative and insightful results provide personal experiences that health care providers may want to consider when providing prenatal counseling on NIPT for expectant mothers. As this analysis is the first of its kind, ascertainment is limited, and future research should aim to expand these findings by investigating the different factors influencing attitudes towards NIPT.

Published

2020

73. Cell-Free DNA Screening for Sex Chromosome Abnormalities and Pregnancy Outcomes, 2018-2020: A Retrospective Analysis

Author

Yanmei Lu, Shihao Zhou, Siyuan Linpeng, Siyi Ding, Shihong Li, Yujiao Li, Liangcheng Shi, Jun He, and Yalan Liu

Subjects

prenatal diagnosis, non-invasive prenatal screening (NIPT), Medicine (miscellaneous), Medicine, sex chromosome aneuploidy, the termination of pregnancy (TOP), sex chromosome abnormality, Article

Abstract

To evaluate the efficacy of non-invasive prenatal screening (NIPT) for detecting fetal sex chromosome abnormalities, a total of 639 women carrying sex chromosome abnormalities were selected from 222,107 pregnant women who participated in free NIPT from April 2018 to December 2020. The clinical data, prenatal diagnosis results, and follow-up pregnancy outcomes of participants were collected. The positive predictive value (PPV) was used to analyze the performance of NIPT. Around 235 cases were confirmed with sex chromosome abnormalities, including 229 cases with sex chromosome aneuploidy (45, X (n = 37), 47, XXX (n = 37), 47, XXY (n = 110), 47, XYY (n = 42)) and 6 cases with structural abnormalities. The total incidence rate was 0.11% (235/222,107). The PPV of NIPT was 45.37% (235/518). NIPT accuracy for detecting sex chromosome polysomes was higher than that for sex chromosome monomers. The termination of pregnancy rate for fetal diagnosis of 45, X, and 47, XXY was higher than that of 47, XXX, and 47, XYY. The detection rate of fetal sex chromosome abnormalities was higher in 2018–2020 than in 2010–2012 (χ2 = 69.708, P < 2.2 × 10−16), indicating that NIPT is greatly efficient to detect fetal sex chromosome abnormalities.

Published

2021

74. Development and Validation of a Computable Phenotype for Turner Syndrome Utilizing Electronic Health Records from a National Pediatric Network.

Author

Huang SD, Bamba V, Bothwell S, Fechner PY, Furniss A, Ikomi C, Nahata L, Nokoff NJ, Pyle L, Seyoum H, and Davis SM

Abstract

Turner syndrome (TS) is a genetic condition occurring in ~1 in 2,000 females characterized by the complete or partial absence of the second sex chromosome. TS research faces similar challenges to many other pediatric rare disease conditions, with homogenous, single-center, underpowered studies. Secondary data analyses utilizing Electronic Health Record (EHR) have the potential to address these limitations, however, an algorithm to accurately identify TS cases in EHR data is needed. We developed a computable phenotype to identify patients with TS using PEDSnet, a pediatric research network. This computable phenotype was validated through chart review; true positives and negatives and false positives and negatives were used to assess accuracy at both primary and external validation sites. The optimal algorithm consisted of the following criteria: female sex, ≥1 outpatient encounter, and ≥3 encounters with a diagnosis code that maps to TS, yielding average sensitivity 0.97, specificity 0.88, and C-statistic 0.93 across all sites. The accuracy of any estradiol prescriptions yielded an average C-statistic of 0.91 across sites and 0.80 for transdermal and oral formulations separately. PEDSnet and computable phenotyping are powerful tools in providing large, diverse samples to pragmatically study rare pediatric conditions like TS., Competing Interests: CONFLICT OF INTEREST STATEMENT SMD and PYF are site investigators for a clinical trial of growth hormone in Turner syndrome sponsored by Ascendis Pharma. NJN is a consultant for Neurocrine Biosciences, Inc. and Ionis Pharmaceuticals. CI is a site investigator for clinical trial of growth hormone in children with growth hormone deficiency and Turner syndrome sponsored by Novo Nordisk, and treatment of type 2 diabetes in children sponsored by Eli Lilly. All other authors have no conflicts of interest to declare.

Published

2023

75. The Clinical Application and Accuracy Evaluation of Noninvasive Prenatal Testing for Common Trisomy and Sex Chromosome Aneuploidy.

Author

Wang Y, Shao Y, and Yu J

Subjects

Child, Female, Pregnancy, Humans, Sex Chromosome Aberrations, Prenatal Diagnosis methods, Aneuploidy, Trisomy 13 Syndrome diagnosis, Trisomy 13 Syndrome genetics, Sex Chromosomes genetics, Trisomy diagnosis, Trisomy genetics, Noninvasive Prenatal Testing

Abstract

Background: Noninvasive prenatal testing (NIPT) has been widely adopted in prenatal examination for fetal chromosomal aneuploidy. The present study aimed to evaluate the clinical features of NIPT for both common trisomy and sex chromosome aneuploidy (SCA)., Methods: A total of 24,164 pregnant women with NIPT testing from July 2020 to June 2022 were recruited at the Linping Maternity and Child Health Care Hospital., Results: Ninety cases showed high risk of trisomy 21/18/13 with karyotype results available, and the sensitivity, specificity, and positive predictive value (PPV) were 98.41%, 99.88% and 68.89%, respectively. The three most important reasons for screening were advanced maternal age (AMA, 28.06%), intermediate risk of prenatal screening (20.34%) and Multiple of medium (MoM) abnormality of prenatal screening (17.38%). High risk of NIPT results with Z-score ≥15 have a higher PPV when compared to those with 3 ≤ Z-score < 10, and 10 ≤ Z-score < 15. Meanwhile, 97 pregnant women received positive results for fetal sex chromosome aneuploidy (SCA) in NIPT. In addition, the rate for further diagnostics of SCA was 64.95% and the PPV of SCA was 50.79%., Conclusions: Our data show that NIPT has a promising future in prenatal screening for genetic abnormalities of the fetus, and that the accuracy of NIPT is closely related to Z-score., Competing Interests: The authors declare no conflict of interest., (© 2023 The Author(s). Published by Discovery Medicine.)

Published

2023

76. Noninvasive Prenatal DNA Testing: The Vanguard of Genomic Medicine.

Author

Hui, Lisa and Bianchi, Diana W.

Abstract

Noninvasive prenatal DNA testing is the vanguard of genomic medicine. In only four years, this screening test has revolutionized prenatal care globally and opened up new prospects for personalized medicine for the fetus. There are widespread implications for increasing the scope of human genetic variation that can be detected before birth, and for discovering more about maternofetal and placental biology. These include an urgent need to develop pretest education for all pregnant women and consistent post-test management recommendations for those with discordant test results. The reduction in invasive testing has had downstream effects on specialist training and caused many countries to re-examine their national approaches to prenatal screening. Finally, the accumulating datasets of genomic information on pregnant women and their fetuses raise ethical issues regarding consent for future data mining and intellectual property. [ABSTRACT FROM AUTHOR]

Published

2017

77. Gonadal function is associated with cardiometabolic health in pre-pubertal boys with Klinefelter syndrome.

Author

Davis, S., Lahlou, N., Bardsley, M., Temple, M.‐C., Kowal, K., Pyle, L., Zeitler, P., and Ross, J.

Abstract

The most common sex chromosome aneuploidy, Klinefelter syndrome (KS), is associated with primary gonadal failure and increased morbidity and mortality from cardiometabolic disorders in adulthood. Children with KS also have a high prevalence of metabolic syndrome (MetS) features. To assess the relationship of gonadal and cardiometabolic function in children with KS, we evaluated serum hormones [gonadotropins, inhibin B (INHB), anti-mullerian hormone (AMH), total testosterone (TT)], and features of MetS (waist circumference, fasting lipid panel, fasting blood glucose (FBG), and blood pressure) in 93 pre-pubertal boys with KS age 4–12 years (mean 7.7 ± 2.5 years). The cohort was grouped by age and tanner stage, and biomarkers were compared to normal ranges. A total of 80% of this pre-pubertal cohort had ≥1 feature of metabolic syndrome (MetS) and 11% had ≥3 features of MetS. Risk of MetS was independent of age and body mass index. Sertoli cell dysfunction was common with 18% having an INHB below the normal range. A low INHB was associated with higher FBG, triglycerides, LDL, and lower HDL (p < 0.05). An INHB <50 ng/dL yielded a sensitivity of 83% and a specificity of 79% for having ≥3 features of MetS. INHB and AMH positively correlated with each other (p < 0.001), and high AMH was protective of MetS. TT was below the lower limit of normal in 49% of subjects, with mean values significantly lower than expected (3.3 ng/dL vs. 4.9 ng/dL, p < 0.0001), however, no convincing relationship between TT and MetS was seen. In conclusion, gonadal and cardiometabolic dysfunction are prevalent in pre-pubertal boys with KS. Although the relationship of testosterone deficiency and MetS is well-known, this study is the first to report an association between impaired Sertoli cell function and cardiometabolic risk. [ABSTRACT FROM AUTHOR]

Published

2016

78. The Effects of Turner Syndrome, 45,X on Obstetric and Neonatal Outcomes: A Retrospective Cohort Evaluation.

Author

Dotters-Katz, Sarah K., Humphrey, Whitney M., Senz, Kayli L., Lee, Vanessa R., Shaffer, Brian L., and Caughey, Aaron B.

Subjects

*BIRTH size, *CESAREAN section, *CONGENITAL heart disease, *PREMATURE infants, *INFANT death, *LONGITUDINAL method, *EVALUATION of medical care, *MULTIVARIATE analysis, *NOSOLOGY, *PERINATAL death, *PREECLAMPSIA, *PREGNANCY, *PREGNANCY complications, *PRENATAL diagnosis, *STATISTICS, *RETROSPECTIVE studies, *TURNER'S syndrome, *DISEASE complications, *DIAGNOSIS

Abstract

Objective This study aims to evaluate the perinatal and neonatal outcomes associated with prenatal diagnosis of 45,X, both with and without fetal cardiac anomalies. Study Design A retrospective cohort of singleton pregnancies in California, 2005 to 2008, using vital statistics and International Classification of Diseases, Ninth Revision data, identifying prenatally diagnosed 45,X. Outcomes included preterm delivery, preeclampsia, intrauterine fetal demise (IUFD), cesarean section, small for gestational age (SGA), neonatal death, and infant death. Bivariate and multivariate analyses were used to compare pregnancies and neonates with and without 45,X. Prenatally diagnosed cardiac anomalies were also considered. Results Of the 2,029,000 deliveries, 138 had prenatally diagnosed 45,X. Out of these 138 deliveries, 22 had a prenatally diagnosed cardiac anomaly. Compared with unaffected pregnancies, those with fetal 45,X had higher rates of preterm delivery (19.5 vs. 9.9%, p = 0.001), cesarean section (44.2 vs. 30.2%, p < 0.0001), and SGA (21.5 vs. 6.3%, p < 0.0001). The affected cohort had no IUFDs. Neonatal death was 14.5 times higher in the 45,X cohort (p < 0.0001). Of only infants with cardiac anomalies, neonatal death was significantly more likely in those with 45,X (p = 0.005). In adjusted analysis, risk of SGA (< 3rd percentile), neonatal death, and infant death remained increased for infants with 45,X while controlling for fetal cardiac anomalies. Conclusion Prenatally diagnosed 45,X was associated with increased risk of cesarean section, and adverse neonatal outcomes, including mortality. [ABSTRACT FROM AUTHOR]

Published

2016

79. Advances in the Interdisciplinary Care of Children with Klinefelter Syndrome.

Author

Davis, Shanlee, Howell, Susan, Wilson, Rebecca, Tanda, Tanea, Ross, Judy, Zeitler, Philip, and Tartaglia, Nicole

Published

2016

80. Aplastic Anemia in Two Patients with Sex Chromosome Aneuploidies.

Author

Rush, Eric T., Schaefer, G. Bradley, Sanger, Warren G., and Coccia, Peter F.

Subjects

*SEX chromosomes, *APLASTIC anemia, *ANEUPLOIDY, *TRISOMY, *LYMPHOPENIA

Abstract

Sex chromosome aneuploidies range in incidence from rather common to exceedingly rare and have a variable phenotype. We report 2 patients with sex chromosome aneuploidies who developed severe aplastic anemia requiring treatment. The first patient had tetrasomy X (48,XXXX) and presented at 9 years of age, and the second patient had trisomy X (47,XXX) and presented at 5 years of age. Although aplastic anemia has been associated with other chromosomal abnormalities, sex chromosome abnormalities have not been traditionally considered a risk factor for this condition. A review of the literature reveals that at least one other patient with a sex chromosome aneuploidy (45,X) has suffered from aplastic anemia and that other autosomal chromosomal anomalies have been described. Despite the uncommon nature of each condition, it is possible that the apparent association is coincidental. A better understanding of the genetic causes of aplastic anemia remains important. © 2015 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published

2016

81. The human inactive X chromosome modulates expression of the active X chromosome

Author

Brown, Dutra, Godfrey, Buscetta, Lasutschinkow, Blanton, Samango-Sprouse, Tartaglia, Davis, Banks, Phou, Skaletsky, Bellott, Hughes, Muenke, Groff, Keen, Kruszka, Pak, and San Roman

Subjects

Genetics, Sex chromosome aneuploidy, Dosage compensation, microRNA, Disease, Ploidy, Biology, Y chromosome, Gene, X chromosome

Abstract

Dosage compensation in humans – ensuring the viability and fitness of females, with two X chromosomes, and males, with one – is thought to be achieved chromosome-wide by heterochromatinization of one X chromosome during female development. We reassessed this through quantitative gene-by-gene analyses of expression in individuals with one to four X chromosomes, tolerance for loss-of-function mutations, regulation by miRNAs, allele-specific expression, and the presence of homologous genes on the Y chromosome. We found a mosaic of dosage compensation strategies on the human X chromosome reflecting gene-by-gene differences in multiple dimensions, including sensitivity to under- or over-expression. These insights enrich our understanding of Turner, Klinefelter, and other sex chromosome aneuploidy syndromes, and of sex-chromosome-mediated effects on health and disease in euploid males and females. One-Sentence Summary The human X chromosome displays several modes of dosage compensation, tailored to the qualities of individual genes.

Published

2021

82. Non-invasive prenatal testing in detecting sex chromosome aneuploidy: A large-scale study in Xuzhou area of China.

Author

Suo, Feng, Wang, Chuangxia, Liu, Tianya, Fang, Yuan, Wu, Qin, Gu, Maosheng, and Gou, Lingshan

Subjects

*PRENATAL genetic testing, *SEX chromosomes, *ANEUPLOIDY, *KARYOTYPES

Abstract

Background Cell-free fetal DNA are widely used in the prenatal genetic testing during recent years. In the present study, we tried to investigate the clinical practical feasibility of non-invasive prenatal testing (NIPT) for prenatal sex chromosome aneuploidy (SCA) analysis among pregnancies in Xuzhou area of China. Methods Among a cohort of 8384 pregnancies, maternal plasma samples from our prenatal diagnosis center was subject to the analysis for SCA using NIPT detection. The cases with positive screening results by NIPT detection were validated on karyotyping analysis. Results From 8384 clinical pregnancies, 64 cases exhibited abnormal results detected by NIPT, in which 34 cases were false positive verified by amniotic fluid puncture and chromosome karyotyping analysis. Twelve positive Turner syndrome (monosomy X) cases in NIPT was confirmed to be sex chromosome abnormal by karyotyping analysis, in which included 9 cases of monosomy X, 1 case of mosaic (45X/47XXX), and 2 cases of mosaic with 45X/45XY karyotype. Of those 9 cases with 47XXX, 5 cases were found to be true positive. Among the ten cases of Klinefelter's syndrome (47XXY) indicated by NIPT, 6 cases (60%) were true positive. Lastly, NIPT indicated 47XYY in 9 cases. Karyotyping analysis found six cases were 47XYY, and one case was mosaic (46XY/47XYY). Conclusion Our findings showed that the true positive rate for monosomy X was lower by NIPT detection, while prediction of other SCA was relatively accurate. Therefore, NIPT could be a potential method for SCA screening, while this technique needed to be further investigated. [ABSTRACT FROM AUTHOR]

Published

2018

83. An adolescent with 48,xxyy syndrome with hypergonadotrophic hypogonadism, attention deficit hyperactive disorder and renal malformations

Author

Prasad Katulanda, J. Rasika D. K. Rajapakse, Jayani Kariyawasam, Rohan Jayasekara, and Vajira H. W. Dissanayake

Subjects

48, XXYY syndrome, hypergonadotrophic hypogonadism, sex chromosome aneuploidy, Diseases of the endocrine glands. Clinical endocrinology, RC648-665, Diseases of the digestive system. Gastroenterology, RC799-869

Abstract

48,XXYY is a rare sex chromosome aneuploidy affecting 1 in 18,000 to 50,000 male births. They present with developmental delay, hypogonadism, gynecomastia, intention tremors, and a spectrum of neurodevelopmental and psychiatric disorders. At one time this condition was considered a variant of Klinefelter syndrome. In clinically suspected cases, 48,XXYY syndrome can be diagnosed by chromosome culture and karyotyping. This patient presented with hypergonadotrophic hypogonadism, attention deficit hyperactive disorder, and renal malformatons. Klinefelter syndrome was clinically suspected. The karyotype confirmed the diagnosis of 48,XXYY syndrome. This is the first reported case of 48,XXYY syndrome from Sri Lanka.

Published

2012

84. Testosterone Treatment in Infants With 47,XXY: Effects on Body Composition

Author

Regina M. Reynolds, Dana Dabelea, Nicole Tartaglia, Philip Zeitler, and Shanlee M Davis

Subjects

0301 basic medicine, Endocrinology, Diabetes and Metabolism, Physiology, Context (language use), 030105 genetics & heredity, Tertiary care, law.invention, Growth velocity, 03 medical and health sciences, Randomized controlled trial, law, Reproductive Biology and Sex-Based Medicine, Testosterone treatment, XXY, Medicine, Adverse effect, Klinefelter syndrome, Testosterone, Clinical Research Articles, adiposity, business.industry, sex chromosome aneuploidy, medicine.disease, 3. Good health, mini-puberty, 030104 developmental biology, testosterone, business

Abstract

Context Boys with XXY have greater adiposity and a higher risk of cardiovascular disease. Infants with XXY have lower testosterone concentrations than typical boys, but no studies have evaluated adiposity in infants with XXY or the physiologic effects of giving testosterone replacement. Objective To determine the effect of testosterone on body composition in infants with XXY. Design Prospective, randomized trial. Setting Tertiary care pediatric referral center. Participants 20 infants 6 to 15 weeks of age with 47,XXY. Intervention Testosterone cypionate 25 mg intramuscularly monthly for three doses vs no treatment. Main Outcome Measures Difference in change in adiposity (percent fat mass z scores); other body composition measures, penile length, and safety outcomes between treated and untreated infants; and comparison with typical infants. Results The increase in percent fat mass (%FM) z scores was greater in the untreated group than in the treated group (+0.92 ± 0.62 vs −0.12 ± 0.65, P = 0.004). Increases in secondary outcomes were greater in the testosterone-treated group for total mass, fat-free mass, length z score, stretched penile length, and growth velocity (P < 0.002 for all). At 5 months of age, adiposity in untreated infants with XXY was 26.7% compared with 23.2% in healthy male infants of the same age (P = 0.0037); there was no difference in %FM between the treated XXY boys and controls. Reported side effects were minimal and self-limited; no serious adverse events occurred. Conclusions Adiposity of untreated infants was 15% greater than that of male controls by 5 months of age. Testosterone treatment for infants with XXY resulted in positive changes in body composition.

Published

2019

85. Screening, prenatal diagnosis, and prenatal decision for sex chromosome aneuploidy

Author

Yong Xu, Yang Liu, Zhiyong Xu, Liyanyan Deng, Jiansheng Xie, Ying Hao, and Liyuan Chen

Subjects

0301 basic medicine, medicine.medical_specialty, Decision Making, Chromosome Disorders, Prenatal diagnosis, Sensitivity and Specificity, Pathology and Forensic Medicine, 03 medical and health sciences, Sex chromosome aneuploidy, 0302 clinical medicine, Pregnancy, Prenatal Diagnosis, Genetics, Humans, Medicine, Child, Pregnancy outcomes, Molecular Biology, Sex Chromosome Aberrations, X chromosome, Monosomy X, business.industry, Obstetrics, Infant, Chromosome, Aneuploidy, Predictive value, 030104 developmental biology, Child, Preschool, 030220 oncology & carcinogenesis, Molecular Medicine, Female, business

Abstract

Objective: To assess the performance of non-invasive prenatal testing (NIPT) in screening sex chromosome aneuploidy (SCA), and explore prenatal decision-making in NIPT positive cases.Methods: The study retrospectively analyses singleton pregnancies who underwent NIPT screening. Clinical data, diagnostic results, and pregnancy outcomes were also collected.Results: There were 140 positive screens for SCA, including 62 cases of 45,X, 29 cases with 47,XXX, 28 cases of 47,XXY, 20 cases of 47,XYY, and one case of lower X chromosome. Karyotypic information was available in 103 cases. The positive predictive value was 26.09% for 45,X, 85.00% for 47,XXX, 85.00% for 47,XXY, and 68.75% for 47,XYY. The termination rates of 45,X, 47,XXX, 47,XXY, 47,XYY were 83.33%, 26.67%, 82.35%, and 54.54%, respectively (not including mosaic cases).Conclusion: Our findings demonstrated that the NIPT performed better in predicting sex chromosome trisomies than monosomy X even though false-positive cases do exist in NIPT. For ...

Published

2019

86. Cortical gray matter structure in boys with Klinefelter syndrome

Author

Lara C. Foland-Ross, David S. Hong, Sharon Bade Shrestha, Allan L. Reiss, Lindsay C. Chromik, and Maureen Gil

Subjects

Male, medicine.medical_specialty, Neuroscience (miscellaneous), Audiology, Gray (unit), Article, 03 medical and health sciences, Sex chromosome aneuploidy, 0302 clinical medicine, Klinefelter Syndrome, medicine, Humans, Radiology, Nuclear Medicine and imaging, Testosterone replacement, Gray Matter, Testosterone, business.industry, Brain, Cognition, Dorsomedial prefrontal cortex, medicine.disease, 030227 psychiatry, Psychiatry and Mental health, Phenotype, Klinefelter syndrome, business, Insula, 030217 neurology & neurosurgery

Abstract

Klinefelter syndrome (KS, 47,XXY) is a common sex chromosome aneuploidy in males that is associated with a wide range of cognitive, social and emotional characteristics. The neural bases of these symptoms, however, are unclear. Brain structure in 19 pre- or early-pubertal boys with KS (11.5 ± 1.8 years) and 22 typically developing (control) boys (8.1 ± 2.3 years) was examined using surface-based analyses of cortical gray matter volume, thickness and surface area. Boys in the KS group were treatment-naive with respect to testosterone replacement therapy. Reduced volume in the insula and dorsomedial prefrontal cortex was observed in the KS relative to the TD group, as well as increased volume in the parietal, occipital and motor regions. Further inspection of surface-based metrics indicated that whereas KS-associated increases in volume were driven by differences in thickness, KS-associated reductions in volume were associated with decreases in surface area. Exploratory analyses additionally indicated several correlations between brain structure and behavior, providing initial support for a neural basis of cognitive and emotional symptoms of this condition. Taken together, these data add support for a neuroanatomical phenotype of KS and extend previous studies through clarifying the precise neuroanatomical structural characteristics of that give rise to volumetric alterations.

Published

2021

87. Maternal X chromosome copy number variations are associated with discordant fetal sex chromosome aneuploidies detected by noninvasive prenatal testing.

Author

Wang, Shaowei, Huang, Shuai, Ma, Linlin, Liang, Lin, Zhang, Junrong, Zhang, Jianguang, and Cram, David S.

Subjects

*X chromosome, *DNA copy number variations, *ANEUPLOIDY, *PRENATAL diagnosis, *PREGNANT women, *LEUCOCYTES, *NUCLEOTIDE sequencing

Abstract

Background The sensitivity and specificity of noninvasive prenatal testing (NIPT) for detection of sex chromosome aneuploidies (SCAs) compared to common autosomal trisomies are significantly lower. We speculated that in addition to altered maternal X chromosome karyotype, maternal X chromosome copy number variations (CNVs) may also contribute to discordant NIPT SCA results. Methods Clinical NIPT was performed for pregnant women at a single hospital. Copy number variation sequencing (CNV-Seq) was used to identify and quantitate the copy number of maternal X chromosome CNVs for each positive SCA pregnancy. Results Two out of 25 SCA positive NIPT samples had slightly abnormal ChrX/ChrY z-scores and were referred for invasive test confirmation. However, fetal karyotypes were found to be normal. CNV-Seq analysis of the maternal white blood cell DNA archived from the original two NIPT blood samples identified small CNVs spanning the STS gene, which is associated with X-linked ichthyosis. Correcting for the altered plasma levels of X chromosome DNA caused by the two CNVs and, taking into consideration the phenotypic consequences for X-linked disease, both fetuses were diagnosed as normal. Conclusions Maternal DNA sequencing is recommended for all positive NIPT SCA results to avoid unnecessary referral for invasive testing and also to evaluate the risk to the fetus of X-linked disease. [ABSTRACT FROM AUTHOR]

Published

2015

88. 'How Should I Tell my Child?' Disclosing the Diagnosis of Sex Chromosome Aneuploidies.

Author

Dennis, Anna, Howell, Susan, Cordeiro, Lisa, and Tartaglia, Nicole

Abstract

To date, the disclosure of a sex chromosome aneuploidy (SCA) diagnosis to an affected individual has not been explored. This study aimed to assess the timing and content revealed to an affected child by his or her parent(s), resources accessed in preparation, parental feelings of preparedness, common parental concerns, and recommendations for disclosure approaches. Two online surveys were created: 1) for parents of a child with a diagnosis and 2) for individuals with a diagnosis. One-hundred thirty-nine parent surveys (XXY n = 68, XXX n = 21, XYY n = 9, other SCAs n = 41) and 67 individual surveys (XXY n = 58, XXX n = 9) were analyzed. Parents most frequently discussed the topics of learning disabilities (47 %) and genetics (45 %) with their child during the initial disclosure. A significantly greater proportion of parent respondents reported feeling prepared vs. unprepared for disclosure, regardless of their child's diagnosis (z-test of proportions, all p's < 0.001). Both prepared and unprepared parents most frequently accessed resources such as websites, support groups, and discussion with the child's physician prior to disclosure, with unprepared parents accessing fewer resources ( M = 2.0 ± 1.41) than prepared parents [ M = 2. ± 1.56; t(101) =−2.02, p < 0.05]. Common parental concerns included making the conversation age-appropriate, discussing infertility, and possible impact on the child's self-esteem. Both parent and individual respondents endorsed being honest with the child, disclosing the diagnosis early and before puberty, and discussing the diagnosis gradually over time. These results provide recommendations for parents, and suggest benefits from additional resources and supports to alleviate concerns when approaching diagnosis disclosure. [ABSTRACT FROM AUTHOR]

Published

2015

89. Factors associated with adaptation to Klinefelter syndrome: The experience of adolescents and adults.

Author

Turriff, Amy, Levy, Howard P., and Biesecker, Barbara

Subjects

*KLINEFELTER'S syndrome, *DISEASES in teenagers, *SEX chromosomes, *ANEUPLOIDY, *PSYCHOLOGICAL adaptation

Abstract

Objective The purpose of this study was to understand the impact of living with Klinefelter syndrome (XXY) as an adolescent or an adult and to examine the factors that contribute to adaptation. Methods Individuals ( n = 310) aged 14–75 years with self-reported XXY were recruited from online support networks to complete a self-administered survey. Perceived consequences, perceived severity, perceived stigma, and coping were measured and evaluated as correlates of adaptation. Results The use of problem-focused coping strategies was positively correlated with adaptation ( p < 0.01) and age was negatively correlated with adaptation ( p < 0.05). Conclusion The majority of participants reported significant negative consequences of XXY, including infertility, psychological co-morbidities and differences in appearance. How participants coped with their negative appraisals was the greatest predictor of adaptation. Practice implications Interventions designed to help individuals reframe negative appraisals, to increase perceived manageability of the challenges of living with XXY, and to facilitate effective coping may improve adaptation among individuals with XXY. [ABSTRACT FROM AUTHOR]

Published

2015

90. A case-control study of brain structure and behavioral characteristics in 47, XXX syndrome.

Author

Lenroot, R. K., Blumenthal, J. D., Wallace, G. L., Clasen, L. S., Lee, N. R., and Giedd, J. N.

Subjects

*TRIPLE X syndrome, *X chromosome, *CHROMOSOME abnormalities, *NEUROANATOMY, *MAGNETIC resonance imaging of the brain, *CASE-control method

Abstract

Trisomy X, the presence of an extra X chromosome in females (47, XXX), is a relatively common but under-recognized chromosomal disorder associated with characteristic cognitive and behavioral features of varying severity. The objective of this study was to determine whether there were neuroanatomical differences in girls with Trisomy X that could relate to cognitive and behavioral differences characteristic of the disorder during childhood and adolescence. MRI scans were obtained on 35 girls with Trisomy X (mean age 11.4, SD 5.5) and 70 age- and sex-matched healthy controls. Cognitive and behavioral testing was also performed. Trisomy X girls underwent a semi-structured psychiatric interview. Regional brain volumes and cortical thickness were compared between the two groups. Total brain volume was significantly decreased in subjects with Trisomy X, as were all regional volumes with the exception of parietal gray matter. Differences in cortical thickness had a mixed pattern. The subjects with Trisomy X had thicker cortex in bilateral medial prefrontal cortex and right medial temporal lobe, but decreased cortical thickness in both lateral temporal lobes. The most common psychiatric disorders present in this sample of Trisomy X girls included anxiety disorders (40%), attention-deficit disorder (17%) and depressive disorders (11%). The most strongly affected brain regions are consistent with phenotypic characteristics such as language delay, poor executive function and heightened anxiety previously described in population-based studies of Trisomy X and also found in our sample. [ABSTRACT FROM AUTHOR]

Published

2014

91. Detection of fetal sex chromosome aneuploidy by massively parallel sequencing of maternal plasma DNA: initial experience in a Chinese hospital.

Author

Yao, H., Jiang, F., Hu, H., Gao, Y., Zhu, Z., Zhang, H., Wang, Y., Guo, Y., Liu, L., Yuan, Y., Zhou, L., Wang, J., Du, B., Qu, N., Zhang, R., Dong, Y., Xu, H., Chen, F., Jiang, H., and Liu, Y.

Subjects

*SEX chromosomes, *ANEUPLOIDY, *REPRODUCTION, *GENETICS, *PREGNANT women

Abstract

ABSTRACT Objectives To evaluate the performance of a massively parallel sequencing ( MPS)-based test in detecting fetal sex chromosome aneuploidy ( SCA) and to present a comprehensive clinical counseling protocol for SCA-positive patients. Methods This was a retrospective study in a large patient cohort of 5950 singleton pregnancies which underwent MPS-based testing as a prenatal screening test for trisomies 21, 18 and 13, with X and Y chromosomes as secondary findings, in Southwest Hospital in China. MPS-based SCA-positive women were offered the choice of knowing whether their SCA results were positive and those who did commenced a two-stage post-test clinical counseling protocol. In Stage 1, general information about SCA was given, and women were given the option of invasive testing for confirmation of findings; in Stage 2, those who had chosen to undergo invasive testing were informed about the specific SCA affecting their fetus and their management options. Results Thirty-three cases were classified as SCA-positive by MPS-based testing. After Stage 1 of the two-stage post-test clinical counseling session, 33 (100%) of these pregnant women chose to know the screening test results, and 25 (75.76%) underwent an invasive diagnostic procedure and karyotype analysis, in one of whom karyotyping failed. In thirteen cases, karyotyping confirmed the MPS-based test results (two X0 cases, seven XXX cases, three XXY cases and one XYY case), giving a positive predictive value of 54.17% (13/24 cases confirmed by karyotyping). After post-test clinical counseling session Stage 2, seven women chose to terminate the pregnancy: one X0 case, two XXX cases, the three XXY cases and the single XYY case. Six women decided to continue with pregnancy: one X0 case and five XXX cases. Conclusion Our study showed the feasibility of clinical application of the MPS-based test in the non-invasive detection of fetal SCA. Together with a two-stage post-test clinical counseling protocol, it leads to a well-informed decision-making procedure. Copyright © 2014 ISUOG. Published by John Wiley & Sons Ltd. [ABSTRACT FROM AUTHOR]

Published

2014

92. Assessment of Fetal Sex Chromosome Aneuploidy Using Directed Cell-Free DNA Analysis.

Author

Nicolaides, Kypros H., Musci, Thomas J., Struble, Craig A., Syngelaki, Argyro, and Gil, M.M.

Subjects

*SEX chromosomes, *ANEUPLOIDY, *DNA analysis, *TRISOMY, *CHROMOSOME abnormalities, *DIAGNOSIS of fetus abnormalities, *FIRST trimester of pregnancy

Abstract

Objective: To examine the performance of chromosome-selective sequencing of cell-free (cf) DNA in maternal blood for assessment of fetal sex chromosome aneuploidies. Methods: This was a case-control study of 177 stored maternal plasma samples, obtained before fetal karyotyping at 11-13 weeks of gestation, from 59 singleton pregnancies with fetal sex chromosome aneuploidies (45,X, n = 49; 47,XXX, n = 6; 47,XXY, n = 1; 47,XYY, n = 3) and 118 with euploid fetuses (46,XY, n = 59; 46,XX, n = 59). Digital analysis of selected regions (DANSR™) on chromosomes 21, 18, 13, X and Y was performed and the fetal-fraction optimized risk of trisomy evaluation (FORTE™) algorithm was used to estimate the risk for non-disomic genotypes. Performance was calculated at a risk cut-off of 1:100. Results: Analysis of cfDNA provided risk scores for 172 (97.2%) samples; 4 samples (45,X, n = 2; 46,XY, n = 1; 46,XX, n = 1) had an insufficient fetal cfDNA fraction for reliable testing and 1 case (47,XXX) failed laboratory quality control metrics. The classification was correct in 43 (91.5%) of 47 cases of 45,X, all 5 of 47,XXX, 1 of 47,XXY and 3 of 47,XYY. There were no false-positive results for monosomy X. Discussion: Analysis of cfDNA by chromosome-selective sequencing can correctly classify fetal sex chromosome aneuploidy with reasonably high sensitivity. © 2013 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published

2014

93. Identification of novel candidate gene loci and increased sex chromosome aneuploidy among infants with conotruncal heart defects.

Author

Osoegawa, Kazutoyo, Iovannisci, David M., Lin, Bin, Parodi, Christina, Schultz, Kathleen, Shaw, Gary M., and Lammer, Edward J.

Abstract

Congenital heart defects (CHDs) are common malformations, affecting four to eight per 1,000 total births. Conotruncal defects are an important pathogenetic subset of CHDs, comprising nearly 20% of the total. Although both environmental and genetic factors are known to contribute to the occurrence of conotruncal defects, the causes remain unknown for most. To identify novel candidate genes/loci, we used array comparative genomic hybridization to detect chromosomal microdeletions/duplications. From a population base of 974,579 total births born during 1999-2004, we screened 389 California infants born with tetralogy of Fallot or d-transposition of the great arteries. We found that 1.7% (5/288) of males with a conotruncal defect had sex chromosome aneuploidy, a sevenfold increased frequency (relative risk = 7.0; 95% confidence interval 2.9-16.9). We identified eight chromosomal microdeletions/duplications for conotruncal defects. From these duplications and deletions, we found five high priority candidate genes ( GATA4, CRKL, BMPR1A, SNAI2, and ZFHX4). This is the initial report that sex chromosome aneuploidy is associated with conotruncal defects among boys. These chromosomal microduplications/deletions provide evidence that GATA4, SNAI2, and CRKL are highly dosage sensitive genes involved in outflow tract development. Genome wide screening for copy number variation can be productive for identifying novel genes/loci contributing to non-syndromic common malformations. © 2013 Wiley Periodicals, Inc. [ABSTRACT FROM AUTHOR]

Published

2014

94. Cell-free DNA screening for aneuploidies in 7113 pregnancies: single Italian centre study

Author

Anthony Cesta, Claudio Giorlandino, Salvatore Longo, Antonella Cima, Maria Antonietta Barone, Antonella Viola, Alvaro Mesoraca, Katia Margiotti, Davide Sparacino, and Claudio Dello Russo

Subjects

Adult, medicine.medical_specialty, Trisomy 13 Syndrome, Dna testing, 03 medical and health sciences, Sex chromosome aneuploidy, Young Adult, 0302 clinical medicine, Pregnancy, Prenatal Diagnosis, Genetics, Retrospective analysis, medicine, chromosome aneuploidies, Humans, Mass Screening, Short Paper, 030212 general & internal medicine, Genetic Testing, Retrospective Studies, 030219 obstetrics & reproductive medicine, business.industry, Obstetrics, Clinical performance, Chromosome, High-Throughput Nucleotide Sequencing, Karyotype, General Medicine, Middle Aged, medicine.disease, Aneuploidy, cffDNA, Cell-free fetal DNA, Italy, Female, next-generation sequencing, Down Syndrome, Trisomy, business, Cell-Free Nucleic Acids, Trisomy 18 Syndrome, cell-free foetal DNA, NIPT

Abstract

IntroductionNon-invasive prenatal testing (NIPT) using cell-free foetal DNA has been widely accepted in recent years for detecting common foetal chromosome aneuploidies, such as trisomies 13, 18 and 21, and sex chromosome aneuploidies. In this study, the practical clinical performance of our foetal DNA testing was evaluated for analysing all chromosome aberrations among 7113 pregnancies in Italy.MethodsThis study was a retrospective analysis of collected NIPT data from the Ion S5 next-generation sequencing platform obtained from Altamedica Medical Centre in Rome, Italy.ResultsIn this study, NIPT showed 100% sensitivity and 99.9% specificity for trisomies 13, 18 and 21. Out of the 7113 samples analysed, 74 cases (1%) were positive by NIPT testing; foetal karyotyping and follow-up results validated 2 trisomy 13 cases, 5 trisomy 18 cases, 58 trisomy 21 cases and 10 sex chromosome aneuploidy cases. There were no false-negative results.ConclusionIn our hands, NIPT had high sensitivity and specificity for common chromosomal aneuploidies such as trisomies 13, 18 and 21.

Published

2020

95. Application of Trophoblast in Noninvasive Prenatal Testing

Author

Lihua Wu, Shaopeng Huang, Ruiyu Li, and Qing Ye

Subjects

0301 basic medicine, 030219 obstetrics & reproductive medicine, medicine.diagnostic_test, business.industry, Trophoblast, General Medicine, medicine.disease, Andrology, 03 medical and health sciences, Sex chromosome aneuploidy, 030104 developmental biology, 0302 clinical medicine, Bronchoalveolar lavage, medicine.anatomical_structure, embryonic structures, medicine, Blastocyst, Klinefelter syndrome, business, reproductive and urinary physiology

Abstract

After multiple divisions, the oosperm forms a morula composed of about 32 cells, then the cells begin to differentiate and form blastocyst...

Published

2020

96. Update on noninvasive prenatal testing: A review based on current worldwide research

Author

Osamu Samura

Subjects

medicine.medical_specialty, Genetic counseling, Trisomy, 03 medical and health sciences, Sex chromosome aneuploidy, 0302 clinical medicine, Pregnancy, Prenatal Diagnosis, medicine, False positive paradox, Humans, Genetic Testing, Intensive care medicine, Sex Chromosome Aberrations, 030219 obstetrics & reproductive medicine, Clinical screening, business.industry, Obstetrics and Gynecology, Diagnostic test, Aneuploidy, Pregnancy Trimester, First, 030220 oncology & carcinogenesis, Female, Down Syndrome, business, Trisomy 18 Syndrome

Abstract

Eight years have passed since noninvasive prenatal testing (NIPT) was clinically evaluated and data on NIPT for trisomy 21, 18 and 13 were collected. The data revealed that NIPT is more accurate than conventional first-trimester screening. However, there is still insufficient data regarding the clinical use of NIPT results in detecting sex chromosome aneuploidies or whole-genome regions. NIPT is already being used as a clinical screening method globally. However, it is an unconfirmed diagnostic test and the results must be interpreted with caution as they may yield false negatives, false positives or inconclusive results. Therefore, the aim of this review is to highlight the current status of information, including the different methodologies, shortcomings and implications, regarding NIPT after its adoption worldwide. It is important to include genetic counseling when implementing NIPT. Going forward, the knowledge obtained to date, including the associated shortcomings, must be considered in evaluating the effectiveness of NIPT in detecting genetic abnormalities.

Published

2020

97. Family Experiences and Attitudes About Receiving the Diagnosis of Sex Chromosome Aneuploidy in a Child

Author

Sharron Close, Kirsten A. Riggan, and Megan Allyse

Subjects

Male, Parents, Pediatrics, medicine.medical_specialty, media_common.quotation_subject, Specialty, Prenatal diagnosis, Chromosome Disorders, Article, Sex chromosome aneuploidy, Optimism, Pregnancy, Prenatal Diagnosis, XYY Karyotype, Genetics, medicine, Humans, Genetic Testing, Clinical care, Child, Genetics (clinical), Depression (differential diagnoses), Sex Chromosome Aberrations, Genetic testing, media_common, Sex Chromosomes, medicine.diagnostic_test, business.industry, Aneuploidy, Attitude, Child, Preschool, Anxiety, Female, medicine.symptom, business

Abstract

The most common sex chromosome aneuploidies (SCA) (47, XXY; 47, XYY; 47, XXX) frequently result in a milder phenotype than autosomal aneuploidies. Nevertheless, these conditions are highly variable and more symptomatic phenotypes may require significant clinical involvement, including specialty care. While historically most individuals with mild phenotypes remained undiagnosed during their lifetime, the increasing use of genetic testing in clinical care has increased the prenatal and postnatal diagnosis of SCAs. These genetic tests are frequently ordered by non-genetic providers who are also responsible for delivering the diagnosis. We surveyed parents of children (n=308) to evaluate their experience of receiving a diagnosis and their support needs. The majority (73.3%) received the diagnosis from a non-genetic medical provider. Following a prenatal diagnosis parents reported experiencing depression, anxiety, and less optimism than those receiving a postnatal diagnosis. Few parents reported receiving materials explaining their child’s condition that they found to be up-to-date, accurate, and unbiased. The frequently negative reported experiences of parents at time of diagnosis suggests more educational opportunities should be provided for non-genetic providers in order to become more informed about these conditions and communicate the diagnosis in a way parents experience as supportive.

Published

2020

98. Genes that escape from X-chromosome inactivation: Potential contributors to Klinefelter syndrome

Author

Bradley P. Balaton, Maria Jose Navarro‐Cobos, and Carolyn J. Brown

Subjects

0301 basic medicine, Male, Pseudoautosomal region, 030105 genetics & heredity, Biology, Y chromosome, X-inactivation, 03 medical and health sciences, Klinefelter Syndrome, X‐chromosome inactivation, Genes, X-Linked, X Chromosome Inactivation, Genetics, medicine, Gene silencing, Animals, Humans, Gene, Genetics (clinical), X chromosome, Chromosomes, Human, X, Dosage compensation, Chromosomes, Human, Y, Research Reviews, Research Review, sex chromosome aneuploidy, medicine.disease, 030104 developmental biology, Gene Expression Regulation, escape from XCI, dosage compensation, Female, Klinefelter syndrome

Abstract

One of the two X chromosomes in females is epigenetically inactivated, thereby compensating for the dosage difference in X‐linked genes between XX females and XY males. Not all X‐linked genes are completely inactivated, however, with 12% of genes escaping X chromosome inactivation and another 15% of genes varying in their X chromosome inactivation status across individuals, tissues or cells. Expression of these genes from the second and otherwise inactive X chromosome may underlie sex differences between males and females, and feature in many of the symptoms of XXY Klinefelter males, who have both an inactive X and a Y chromosome. We review the approaches used to identify genes that escape from X‐chromosome inactivation and discuss the nature of their sex‐biased expression. These genes are enriched on the short arm of the X chromosome, and, in addition to genes in the pseudoautosomal regions, include genes with and without Y‐chromosomal counterparts. We highlight candidate escape genes for some of the features of Klinefelter syndrome and discuss our current understanding of the mechanisms underlying silencing and escape on the X chromosome as well as additional differences between the X in males and females that may contribute to Klinefelter syndrome.

Published

2020

99. Delivering the Diagnosis of Sex Chromosome Aneuploidy: Experiences and Preferences of Parents and Individuals

Author

Christina A. Nyquist, Megan Allyse, Jason S. Egginton, Carolina Jaramillo, Kirsten A. Riggan, and Sean M. Phelan

Subjects

Adult, Male, Parents, medicine.medical_specialty, Adolescent, Sex Chromosome Disorders of Sex Development, Prenatal diagnosis, Interviews as Topic, Young Adult, 03 medical and health sciences, Sex chromosome aneuploidy, 0302 clinical medicine, 030225 pediatrics, medicine, Humans, Child, Obstetrics, business.industry, Infant, Chromosome, Aneuploidy, medicine.disease, Child, Preschool, Pediatrics, Perinatology and Child Health, Female, Klinefelter syndrome, business, Attitude to Health

Abstract

Increased prenatal diagnoses of sex chromosome aneuploidies (SCAs) amid limited knowledge of their prognoses heighten the need to understand how families contend with the implications of an SCA. To explore the experiences of parents and individuals who received a genetic diagnosis of an SCA (excluding Turner syndrome), we conducted semistructured qualitative telephone interviews with 43 participants affected by these conditions. Parents (n = 35) and individuals (n = 8) expressed almost unanimous interest in more optimistic portrayals of their condition from their providers, even when the prognosis is uncertain. While some participants reported success in receiving accurate information from their provider and identifying supportive resources, numerous families received outdated or misleading information about their condition and lacked direction in accessing follow-up care and support. Parents desire greater coordination of their child’s medical care and access to care that approaches an SCA holistically. Opportunities remain to improve the diagnosis and care of individuals with SCAs.

Published

2018

100. Cataract in a patient with 47,XYY sex chromosome aneuploidy

Author

V. Cortés-González, C. Villanueva-Mendoza, S. Arenas, and A. Medina-Andrade

Subjects

Pregnancy, Pediatrics, medicine.medical_specialty, Abstract case, business.industry, High myopia, Tall Stature, General Medicine, medicine.disease, Peripheral blood, 03 medical and health sciences, Facial dysmorphism, Sex chromosome aneuploidy, 0302 clinical medicine, 030225 pediatrics, 030221 ophthalmology & optometry, medicine, Etiology, business

Abstract

Case report The case concerns a 16-year-old boy with a history of high myopia and unilateral congenital cataract, tall stature for age, facial dysmorphism, hypermobile metacarpal-phalangeal joints, as well as behavioral problems. The mother had a history of recurrent pregnancy loss. Chromosomal analysis of the peripheral blood lymphocytes reported 47,XYY. Discussion Patients with sex chromosome aneuploidy 47,XYY have higher risk of congenital malformations, although ophthalmological anomalies are unusual. Evaluation of patients with tall stature and behavioral problems should include a chromosomal analysis in order to determine the etiology.

Published

2018