Your search keyword '"Bladder Exstrophy genetics"' showing total 9 results

1. WNT3 involvement in human bladder exstrophy and cloaca development in zebrafish.

Author

Baranowska Körberg I, Hofmeister W, Markljung E, Cao J, Nilsson D, Ludwig M, Draaken M, Holmdahl G, Barker G, Reutter H, Vukojević V, Clementson Kockum C, Lundin J, Lindstrand A, and Nordenskjöld A

Subjects

Animals, Gene Expression, Gene Knockdown Techniques, Genetic Association Studies, High-Throughput Nucleotide Sequencing, Humans, Mice, Models, Molecular, Mutation, NIH 3T3 Cells, Open Reading Frames, Penetrance, Phenotype, Polymorphism, Single Nucleotide, Protein Conformation, Protein Transport, RNA, Messenger genetics, Wnt3 Protein chemistry, Wnt3 Protein metabolism, Bladder Exstrophy genetics, Cloaca embryology, Cloaca metabolism, Wnt3 Protein genetics, Zebrafish embryology, Zebrafish genetics

Abstract

Bladder exstrophy, a severe congenital urological malformation when a child is born with an open urinary bladder, is the most common form of bladder exstrophy-epispadias complex (BEEC) with an incidence of 1:30,000 children of Caucasian descent. Recent studies suggest that WNT genes may contribute to the etiology of bladder exstrophy. Here, we evaluated WNT-pathway genes in 20 bladder exstrophy patients using massively parallel sequencing. In total 13 variants were identified in WNT3, WNT6, WNT7A, WNT8B, WNT10A, WNT11, WNT16, FZD5, LRP1 and LRP10 genes and predicted as potentially disease causing, of which seven variants were novel. One variant, identified in a patient with a de novo nonsynonymous substitution in WNT3 (p.Cys91Arg), was further evaluated in zebrafish. Knock down of wnt3 in zebrafish showed cloaca malformations, including disorganization of the cloaca epithelium and expansion of the cloaca lumen. Our study suggests that the function of the WNT3 p.Cys91Arg variant was altered, since RNA overexpression of mutant Wnt3 RNA does not result in embryonic lethality as seen with wild-type WNT3 mRNA. Finally, we also mutation screened the WNT3 gene further in 410 DNA samples from BEEC cases and identified one additional mutation c.638G>A (p.Gly213Asp), which was paternally inherited. In aggregate our data support the involvement of WNT-pathway genes in BEEC and suggest that WNT3 in itself is a rare cause of BEEC., (© The Author 2015. Published by Oxford University Press. All rights reserved. For Permissions, please email: journals.permissions@oup.com.)

Published

2015

2. Y chromosome aberration in a patient with cloacal-bladder exstrophy-epispadias complex: an unusual finding.

Author

Nishi MY, Martins TC, Costa EM, Mendonca BB, Giron AM, and Domenice S

Subjects

Adolescent, Female, Humans, Bladder Exstrophy genetics, Chromosomes, Human, Y genetics, Cloaca, Epispadias genetics, Sex Chromosome Aberrations

Abstract

Chromosome aberrations or genetic syndromes associated with cloacal-bladder exstrophy complex have rarely been reported. The aim of this report is to describe a 14 year-old female Brazilian patient with a complex urogenital malformation, short stature, lack of secondary se-xual characteristics and Y chromosome aberration. A girl with cloacal bladder exstrophy complex was referred for evaluation of short stature and absence of secondary sexual characteristics. Pre-pubertal levels of gonadotropins and sex steroids were observed at the beginning of monitoring, but follow-up showed a progressive increase in testosterone levels. The patient underwent gonadectomy and testicular tissue was identified without dysgenetic characteristics. She had a 46,X,inv(Y)(p11.1q11.2) karyotype, normal SRY sequence, and no Y deletions. The pericentric inversion of Y chromosome apparently did not contribute to the development of the complex urogenital malformation in this patient. Currently, no teratogenic agent, environmental factor, or defective genes have been recognized as etiologic factors for this type of urogenital malformation.

Published

2013

3. Gender assignment for newborns with 46XY cloacal exstrophy: a 6-year followup survey of pediatric urologists.

Author

Diamond DA, Burns JP, Huang L, Rosoklija I, and Retik AB

Subjects

Adolescent, Adult, Bladder Exstrophy diagnosis, Bladder Exstrophy genetics, Child, Child, Preschool, Decision Making, Disorders of Sex Development diagnosis, Disorders of Sex Development genetics, Disorders of Sex Development surgery, Female, Follow-Up Studies, Humans, Infant, Infant, Newborn, Male, Middle Aged, Pilot Projects, Practice Patterns, Physicians', Reproducibility of Results, Retrospective Studies, Sex Distribution, Time Factors, Young Adult, Bladder Exstrophy surgery, Cloaca abnormalities, Patient Selection, Sex Chromosome Aberrations, Sex Determination Analysis methods, Surveys and Questionnaires, Urologic Surgical Procedures

Abstract

Purpose: Gender assignment for newborns with ambiguous genitalia remains a challenge. An initial survey of colleagues on this subject was performed in 2004. Our objective was to understand the basis for the attitudes and practices of pediatric urologists in regard to gender assignment for 46XY cloacal exstrophy in a 6-year followup survey., Materials and Methods: A survey on a case of 46XY cloacal exstrophy was completed by 191 of the 263 fellows (73%) in the Urology Section, American Academy of Pediatrics. Questions referred to gender assignment, surgery timing, clinical outcomes and respondent demographics., Results: Of the fellows 79% favored male gender assignment. The most important factor in male assignment remained androgen brain imprinting (97%) while in female assignment it was surgical success in creating functional genitalia (96%). Respondent characteristics associated with assigning female gender were longer practice duration (greater than 15 years) (p <0.03), having trained in programs where female gender was always or usually assigned (p <0.02) and not being a fellowship program director (0 of 27 respondents, p <0.03). There was an evolution among respondents from female gender assignment earlier in the career to male assignment currently (p <0.0001)., Conclusions: Most pediatric urologists favor male gender assignment for 46XY cloacal exstrophy, which is a significant increase in 6 years. This change represents an evolution from female to male gender assignment and virtual unanimity among fellowship directors to gender assign male. Longer practicing clinicians perceived better outcomes for female gender assignment. If this reflects true clinical outcomes, the trend toward the eventual disappearance of female gender assignment for 46XY cloacal exstrophy is concerning., (Copyright © 2011 American Urological Association Education and Research, Inc. Published by Elsevier Inc. All rights reserved.)

Published

2011

4. OEIS complex associated with chromosome 1p36 deletion: a case report and review.

Author

El-Hattab AW, Skorupski JC, Hsieh MH, Breman AM, Patel A, Cheung SW, and Craigen WJ

Subjects

Anus, Imperforate complications, Bladder Exstrophy genetics, Chromosome Disorders genetics, Female, Hernia, Umbilical complications, Humans, In Situ Hybridization, Fluorescence, Infant, Karyotyping, Prognosis, Abnormalities, Multiple genetics, Anus, Imperforate genetics, Chromosome Deletion, Chromosomes, Human, Pair 1, Cloaca abnormalities, Hernia, Umbilical genetics, Spine abnormalities

Abstract

OEIS complex (Omphalocele, Exstrophy of the cloaca, Imperforate anus, and Spine abnormalities) is a rare defect with estimated incidence of 1 in 200,000 live births. Most cases are sporadic, with no obvious cause. However, it has been rarely reported in patients with family members having similar malformations or with chromosomal anomalies. In addition, OEIS complex has been observed in association with environmental exposures, twinning, and in vitro fertilization. Monosomy 1p36 is the most common terminal deletion syndrome, with a prevalence of 1 in 5,000 newborns. It is characterized by specific facial features, developmental delay, and heart, skeletal, genitourinary, and neurological defects. We describe an infant with OEIS complex and 1p36 deletion who had features of both disorders, including omphalocele, cloacal exstrophy, imperforate anus, sacral multiple segmentation, renal malposition and malrotation, genital anomalies, diastasis of the symphysis pubis, microbrachycephaly, large anterior fontanel, cardiac septal defects, rib fusion, a limb deformity, developmental delay, and typical facial features. Chromosomal microarray analysis detected a 2.4 Mb terminal deletion of chromosome 1p. This is the first reported case with OEIS complex in association with a chromosome 1p36 deletion., (Copyright 2010 Wiley-Liss, Inc.)

Published

2010

5. The exstrophy-epispadias complex.

Author

Ebert AK, Reutter H, Ludwig M, and Rösch WH

Subjects

Abnormalities, Multiple pathology, Bladder Exstrophy embryology, Bladder Exstrophy genetics, Bladder Exstrophy surgery, Counseling, Diagnosis, Differential, Epispadias embryology, Epispadias genetics, Epispadias surgery, Female, Humans, Male, Osteotomy, Prenatal Diagnosis, Prognosis, Bladder Exstrophy pathology, Cloaca abnormalities, Epispadias pathology

Abstract

Exstrophy-epispadias complex (EEC) represents a spectrum of genitourinary malformations ranging in severity from epispadias (E) to classical bladder exstrophy (CEB) and exstrophy of the cloaca (EC). Depending on severity, EEC may involve the urinary system, musculoskeletal system, pelvis, pelvic floor, abdominal wall, genitalia, and sometimes the spine and anus. Prevalence at birth for the whole spectrum is reported at 1/10,000, ranging from 1/30,000 for CEB to 1/200,000 for EC, with an overall greater proportion of affected males. EEC is characterized by a visible defect of the lower abdominal wall, either with an evaginated bladder plate (CEB), or with an open urethral plate in males or a cleft in females (E). In CE, two exstrophied hemibladders, as well as omphalocele, an imperforate anus and spinal defects, can be seen after birth. EEC results from mechanical disruption or enlargement of the cloacal membrane; the timing of the rupture determines the severity of the malformation. The underlying cause remains unknown: both genetic and environmental factors are likely to play a role in the etiology of EEC. Diagnosis at birth is made on the basis of the clinical presentation but EEC may be detected prenatally by ultrasound from repeated non-visualization of a normally filled fetal bladder. Counseling should be provided to parents but, due to a favorable outcome, termination of the pregnancy is no longer recommended. Management is primarily surgical, with the main aims of obtaining secure abdominal wall closure, achieving urinary continence with preservation of renal function, and, finally, adequate cosmetic and functional genital reconstruction. Several methods for bladder reconstruction with creation of an outlet resistance during the newborn period are favored worldwide. Removal of the bladder template with complete urinary diversion to a rectal reservoir can be an alternative. After reconstructive surgery of the bladder, continence rates of about 80% are expected during childhood. Additional surgery might be needed to optimize bladder storage and emptying function. In cases of final reconstruction failure, urinary diversion should be undertaken. In puberty, genital and reproductive function are important issues. Psychosocial and psychosexual outcome depend on long-term multidisciplinary care to facilitate an adequate quality of life.

Published

2009

6. Psychopathology, psychosocial, gender and cognitive outcomes in patients with cloacal exstrophy.

Author

Mukherjee B, McCauley E, Hanford RB, Aalsma M, and Anderson AM

Subjects

Adolescent, Adult, Anxiety diagnosis, Bladder Exstrophy genetics, Bladder Exstrophy surgery, Child, Cloaca surgery, Depression diagnosis, Epispadias genetics, Epispadias surgery, Female, Humans, Interview, Psychological, Karyotyping, Male, Personality Inventory, Reoperation, Self Concept, Sexuality, Wechsler Scales, Anxiety psychology, Bladder Exstrophy psychology, Cloaca abnormalities, Depression psychology, Epispadias psychology, Gender Identity, Neuropsychological Tests, Social Adjustment

Abstract

Purpose: Psychological functioning, as reflected in psychopathology, psychosocial functioning, gender identity, gender role and cognitive abilities, was examined in a sample of patients with cloacal exstrophy., Materials and Methods: Nine participants 11 to 37 years old completed the evaluation. Standardized measures were used and participant responses were compared to the norms of the various instruments. Gender reassigned participants with cloacal exstrophy were compared with nonassigned participants with cloacal exstrophy. Mean differences between the 2 groups were calculated using the t test., Results: Overall the participants with cloacal exstrophy reported good psychological functioning. Significant differences between reassigned and nonassigned participants were found in the area of depression. All participants had a stable gender identity. XY females showed more male-typical gender roles. There were no significant group differences on cognitive assessments. Reassigned and nonassigned participants did not differ in IQ., Conclusions: Although being born with cloacal exstrophy puts patients at risk for psychopathology and psychosocial problems, it does not necessarily mean that these problems will develop. With the appropriate support these patients can have remarkably well adjusted lives.

Published

2007

7. Gender identity outcome in female-raised 46,XY persons with penile agenesis, cloacal exstrophy of the bladder, or penile ablation.

Author

Meyer-Bahlburg HF

Subjects

Adolescent, Bladder Exstrophy genetics, Child, Disorders of Sex Development psychology, Female, Gonadal Dysgenesis, 46,XY psychology, Humans, Male, Sex Characteristics, Sexual Behavior, Sexual Dysfunctions, Psychological therapy, Time Factors, Bladder Exstrophy therapy, Cloaca abnormalities, Disorders of Sex Development therapy, Gender Identity, Gonadal Dysgenesis, 46,XY therapy, Penis abnormalities, Penis injuries, Psychosexual Development

Abstract

This review addresses the long-term gender outcome of gender assignment of persons with intersexuality and related conditions. The gender assignment to female of 46,XY newborns with severe genital abnormalities despite a presumably normal-male prenatal sex-hormone milieu is highly controversial because of variations in assumptions about the role of biological factors in gender identity formation. This article presents a literature review of gender outcome in three pertinent conditions (penile agenesis, cloacal exstrophy of the bladder, and penile ablation) in infancy or early childhood. The findings clearly indicate an increased risk of later patient-initiated gender re-assignment to male after female assignment in infancy or early childhood, but are nevertheless incompatible with the notion of a full determination of core gender identity by prenatal androgens.

Published

2005

8. Cloacal exstrophy in an infant with 9q34.1-qter deletion resulting from a de novo unbalanced translocation between chromosome 9q and Yq.

Author

Thauvin-Robinet C, Faivre L, Cusin V, Khau Van Kien P, Callier P, Parker KL, Fellous M, Borgnon J, Gounot E, Huet F, Sapin E, and Mugneret F

Subjects

Abnormalities, Multiple, Adult, Anus, Imperforate pathology, Cloaca pathology, Female, Humans, Infant, Karyotyping, Male, Pregnancy, Bladder Exstrophy genetics, Chromosome Deletion, Chromosomes, Human, Pair 9 genetics, Chromosomes, Human, Y genetics, Cloaca abnormalities, Translocation, Genetic

Abstract

Cloacal exstrophy is a rare malformation, belonging to a spectrum of birth defects, which, in order of severity, includes phallic separation with epispadias, pubic diastasis, bladder exstrophy, and cloacal exstrophy. This malformation overlaps the OEIS complex (O = omphalocele, E = bladder exstrophy, I = imperforate anus, S = spinal defects). The etiology of cloacal exstrophy is unknown to date. It may result from either a single defect of early blastogenesis or a defect of mesodermal migration during the primitive streak period. We report an infant with cloacal exstrophy, exomphalos, right kidney agenesis, ambiguous external genitalia, and axial hypotonia. The karyotype showed a de novo unbalanced translocation between the long arm of chromosome 9 and the long arm of chromosome Y resulting in a 9q34.1-qter deletion. Reviewing the literature, we did not find any observation of cloacal exstrophy associated with a structural chromosomal abnormality. The steroidogenic factor 1 (SF1) gene, included in the deleted region, was a good candidate gene but no pathogenic mutation was found by direct sequencing. We hypothesize that another gene, expressed early in embryogenesis and responsible for cloacal exstrophy, is present in the 9q34.1-qter region., (Copyright 2003 Wiley-Liss, Inc.)

Published

2004

9. Management of cloacal exstrophy.

Author

Mitchell ME and Plaire C

Subjects

Bladder Exstrophy genetics, Bladder Exstrophy psychology, Bladder Exstrophy surgery, Disorders of Sex Development genetics, Disorders of Sex Development pathology, Disorders of Sex Development psychology, Epispadias genetics, Epispadias psychology, Epispadias surgery, Female, Gender Identity, Genotype, Humans, Infant, Newborn, Male, Psychosexual Development, Urogenital Surgical Procedures methods, Cloaca abnormalities, Cloaca surgery, Disorders of Sex Development surgery

Published

2002