Your search keyword '"Ambiguous genitalia"' showing total 35 results

1. Novel Missense Variant in the SMARCD1 Gene as the Cause of Coffin–Siris Syndrome 11 in a Fetus With Ambiguous Genitalia and Multiple Dysmorphic Features.

Author

Veazey, Rachel A., Fisher, Allan J., Talati, Asha N., Hardisty, Emily, Gilmore, Kelly L., and Vora, Neeta L.

Published

2024

2. Ambiguous genitalia, giant congenital melanocytic nevus and subpulmonic outlet ventricular septal defect in an African child with Neurofibromatosis 1.

Author

Ekure, Ekanem N., Musa, Kareem O., Ulonnam, Ngozi, Kruszka, Paul, Muenke, Maximilian, and Adeyemo, Adebowale A.

Abstract

Neurofibromatosis type 1 is an autosomal dominant multisystemic disease caused by mutation of the neurofibromin (NF1) gene located on chromosome 17q11. We report a case of Neurofibromatosis 1 with ambiguous genitalia, giant congenital melanocytic nevus, and associated subpulmonic outlet ventricular septal defect, hitherto unreported in sub‐Saharan Africa. In addition, a literature review of congenital heart diseases associated with Neurofibromatosis 1 is presented. [ABSTRACT FROM AUTHOR]

Published

2023

3. Clinically diverse and perinatally lethal syndromes with urorectal septum malformation sequence.

Author

Nayak, Shalini S., Harkness, Robert, Shukla, Anju, Banka, Siddharth, Newman, William G., and Girisha, Katta M.

Abstract

Urorectal septum malformation sequence (URSMS) is characterized by a spectrum of anomalies of the urogenital system, hindgut and perineum. It is presumed to be a constellation of an embryonic defect. Herein, we analyzed the clinically diverse syndromes associated with URSMS in our perinatal evaluation unit. We reviewed fetuses with URSMS in referrals for perinatal autopsy over a period of 3 years. Chromosomal microarray and genome sequencing were performed whenever feasible. Literature was reviewed for syndromes or malformations with URSMS. We ascertained URSMS in 12 of the 215 (5%) fetuses. Nine fetuses (75%) had complete URSMS and remainder had partial/intermediate URSMS. Eleven fetuses had malformations of other systems that included: cerebral ventriculomegaly; right aortic arch with double outlet right ventricle; microcephaly with fetal akinesia deformation sequence; ventricular septal defect and radial ray anomaly; thoraco‐abdominoschisis and limb defects; myelomeningocele; spina bifida and fused iliac bones; omphalocele; occipital encephalocele; lower limb amelia and cleft foot. We report on six fetuses with recurrent and five fetuses with unique malformations/patterns where URSMS is a component. Exome sequencing (one family) and genome sequencing (eight families) were performed and were nondiagnostic. Additionally, we review the literature for genetic basis of this condition. URMS is a clinically heterogeneous condition and is a component of several multiple malformation syndromes. We describe several unique and recurrent malformations associated with URSMS. [ABSTRACT FROM AUTHOR]

Published

2023

4. The Development of Normal Fetal External Genitalia Throughout Gestation.

Author

Pinson, Kelsey, Melber, Dora J, Nguyen, Ngoc‐Hieu, Montaney, Laura, Basu, Reshmi, Mims, Joseph, Pretorius, Dolores, and Lamale‐Smith, Leah

Subjects

FETAL ultrasonic imaging, GENITALIA, FETAL development, FEMALE reproductive organs, MALE reproductive organs, PREGNANCY

Abstract

In this review, we describe normal development of fetal genitalia throughout gestation as well as the identification of normal male and female genitalia on ultrasound. We use abnormal and ambiguous genitalia as illustrative tools to assist with the identification of normal genitalia and recognition of some of the most common abnormalities in external genitalia development. [ABSTRACT FROM AUTHOR]

Published

2023

5. Expanding the novel MAPKAPK5–related developmental disorder's genotype–phenotype correlation: Patient report and 19 months of follow‐up.

Author

Vecchio, Davide, Cocciadiferro, Dario, Macchiaiolo, Marina, Gonfiantini, Michaela Veronika, Agolini, Emanuele, Matraxia, Marta, Carboni, Alessia, Coretti, Antonella, Villani, Andrea, Panfili, Filippo Maria, Dentici, Maria Lisa, Buonuomo, Paola Sabrina, Rana, Ippolita, Colafati, Giovanna Stefania, Digilio, Maria Cristina, Novelli, Antonio, and Bartuli, Andrea

Subjects

*CONGENITAL heart disease, *CONGENITAL disorders, *FINGERS, *TOES, *HUMAN abnormalities, *GENITALIA

Abstract

This study aimed to widen the knowledge of a recently identified, autosomal‐recessive, multiple congenital anomalies syndrome to date observed in only other three children. This is the second report of biallelic mutations in MAPKAPK5 whose impairment during human development has been associated with neurological, cardiac, and facial anomalies combined with fingers and toes malformations. Through the affected patients' genetic and phenotypic features overlap, this report confirms MAPKAPK5 as causative gene and adds unique neurodevelopmental characterization. Moreover, based on the complex congenital genitourinary anomalies reported and MAPKAPK5 literature review, we also propose kidney and external genitalia involvement as a key syndromic feature whose expressivity may be more severe in males. [ABSTRACT FROM AUTHOR]

Published

2022

6. Chromosome 9p terminal deletion in nine Egyptian patients and narrowing of the critical region for trigonocephaly.

Author

Mohamed, Amal M., Kamel, Alaa K., Eid, Maha M., Eid, Ola M., Mekkawy, Mona, Hussein, Shymaa H., Zaki, Maha S., Esmail, Samira, Afifi, Hanan H., El‐Kamah, Ghada Y., Otaify, Ghada A., El‐Awady, Heba Ahmed, Elaidy, Aya, Essa, Mahmoud Y., El‐Ruby, Mona, Ashaat, Engy A., Hammad, Saida A., Mazen, Inas, Abdel‐Salam, Ghada M. H., and Aglan, Mona

Subjects

*PLANT chromosomes, *BACTERIAL artificial chromosomes, *CONGENITAL heart disease, *CHROMOSOMES, *DELETION mutation, *DEVELOPMENTAL delay

Abstract

Background: This study aimed to delineate the clinical phenotype of patients with 9p deletions, pinpoint the chromosomal breakpoints, and identify the critical region for trigonocephaly, which is a frequent finding in 9p terminal deletion. Methods: We investigated a cohort of nine patients with chromosome 9p terminal deletions who all displayed developmental delay, intellectual disability, hypotonia, and dysmorphic features. Of them, eight had trigonocephaly, seven had brain anomalies, seven had autistic manifestations, seven had fair hair, and six had a congenital heart defect (CHD). Results: Karyotyping revealed 9p terminal deletion in all patients, and patients 8 and 9 had additional duplication of other chromosomal segments. We used six bacterial artificial chromosome (BAC) clones that could identify the breakpoints at 17–20 Mb from the 9p terminus. Array CGH identified the precise extent of the deletion in six patients; the deleted regions ranged from 16 to 18.8 Mb in four patients, patient 8 had an 11.58 Mb deletion and patient 9 had a 2.3 Mb deletion. Conclusion: The gene deletion in the 9p24 region was insufficient to cause ambiguous genitalia because six of the nine patients had normal genitalia. We suggest that the critical region for trigonocephaly lies between 11,575 and 11,587 Mb from the chromosome 9p terminus. To the best of our knowledge, this is the minimal critical region reported for trigonocephaly in 9p deletion syndrome, and it warrants further delineation. [ABSTRACT FROM AUTHOR]

Published

2021

7. Survey of disorders of sex development in a large cohort of patients with diverse Mendelian phenotypes.

Author

Abualsaud, Dalia, Hashem, Mais, AlHashem, Amal, and Alkuraya, Fowzan S.

Abstract

Disorders of sex development (DSD) are congenital conditions with atypical development of chromosomal, gonadal, or anatomical sex. The estimated incidence ranges from 1 in 4,500–5,500 for strictly defined "ambiguous genitalia" to 1 in 300 or higher when a broader definition is implemented. In this study, we aim to define DSD phenotypes encountered in a large heterogeneous cohort of molecularly characterized Mendelian disorders in a single center. Data were retrieved for patients with documented abnormal genitalia based on the 2006 consensus criteria. Out of 149 patients (129 families) with compatible human phenotype ontology, 76 patients (68 families) had an identified genetic cause and were included in our analysis. Potentially causal variants were identified in 42 genes, and two patients had a dual molecular diagnosis. Six genes have no associated phenotype in OMIM (PIANP, CELSR2, USP2, FAM179B, TXNDC15, and CCDC96). Thirteen genes have non‐DSD OMIM phenotypes, thus we are expanding their phenotype to include DSD. We also highlight how certain disorders are under‐recognized despite their established DSD phenotype in OMIM, especially CTU2‐related DREAM‐PL syndrome and TSPYL1‐related sudden infant death with dysgenesis of the testes syndrome. In conclusion, this study of a large heterogeneous Mendelian cohort expands the list of genes and disorders beyond those classically DSD‐linked. [ABSTRACT FROM AUTHOR]

Published

2021

8. Growth and relationship of phenotypic characteristics with gonadal pathology and tumour risk in patients with 45, X/46, XY mosaicism.

Author

Poyrazoglu, Sukran, Bas, Firdevs, Karaman, Birsen, Yildiz, Melek, Basaran, Seher, and Darendeliler, Feyza

Subjects

*VULVA, *PHENOTYPES, *MOSAICISM, *MALE reproductive organs, *SHORT stature, GONADAL diseases

Abstract

Objective: To evaluate the growth data, gonadal functions and tumour risk in children with 45, X/46, XY mosaicism. Design: We reviewed retrospectively the records of 45 patients with 45, X/46, XY mosaicism or variants presented to our Unit from 1989 to 2019. Results: The age at diagnosis ranged from 0.03 to 17.5 years. Twenty‐eight patients had genital anomaly, 14 patients had female external genitalia and 3 patients had normal male genitalia. Patients showed normal height under 2 years of age. Mean height standard deviation score (HSDS) of 19 patients diagnosed before 2 years of age was −0.9 ± 0.6 and that of 26 patients diagnosed after 2 years of age was −2.6 ± 1.5. Ten patients diagnosed before 2 years of age showed growth deceleration after 2 years of age (HSDS decreasing from −0.6 ± 0.7 to −1.4 ± 0.9). Twenty‐one patients reached adult height (AH). Growth hormone (GH) treatment was initiated in 10 patients. Although AHSDS of GH‐treated patients was significantly greater than their mean HSDS before GH therapy (p =.013), it was not significantly different from AHSDS of the untreated group. Seventeen (37.8%) patients exhibited phenotypical features of Turner syndrome (TS) other than short stature. Two patients with genital anomaly had gonadoblastoma and germ cell neoplasia in situ, and one patient with female external genitalia had gonadoblastoma. Conclusions: GH therapy seems to improve AH of patients. Both patients with genital anomaly and female external genitalia have increased risk of germ cell tumours. [ABSTRACT FROM AUTHOR]

Published

2021

9. Exome sequencing identified compound heterozygous mutations in the SRD5A2 gene in a case of 46,XY ambiguous genitalia.

Author

Mehta, Poonam and Rajender, Singh

Subjects

*GENITALIA, *ANDROGEN-insensitivity syndrome, *GENETIC mutation, *SEX differentiation disorders, *ANDROGEN receptors

Abstract

The disorders of sexual development (DSD) represent an array of phenotypes with ambiguous genitalia. The present case had microphallus with fused and bifid scrotum and was initially assigned androgen insensitivity syndrome; however, sequencing of the complete coding region of the androgen receptor gene failed to identify a causative mutation. We undertook whole exome sequencing for identification of the pathogenic mutation. The most promising pathogenic variants were genotyped using Sanger sequencing to confirm the genotypes. We found compound heterozygous mutations, c.169G>T and c.586G>A in the SRD5A2 gene in this case, resulting in a nonsense (p.Glu57Ter) and a nonsynonymous substitution (p.Gly196Ser), respectively. While the nonsense mutation would result in a truncated protein, p.Gly196Ser substitution has been previously reported to be pathogenic. The mutations were confirmed by Sanger sequencing. Sequencing of 96 normal male individuals did not show the above mutations, suggesting their pathogenic nature. In conclusion, we identified compound heterozygous pathogenic mutations, c.169G>T (p.Glu57Ter) and c.586G>A (p.Gly196Ser), in the SRD5A2 gene in a case of ambiguous genitalia. p.Glu57Ter is a novel mutation, which in compound heterozygote combination with Gly196Ser causes 5a reductase deficiency. [ABSTRACT FROM AUTHOR]

Published

2021

10. Fetal hydrometrocolpos with pre-axial mirror polydactyly as a new variant of McKusick-Kaufman syndrome.

Author

Traisrisilp, Kuntharee, Nunthapiwat, Sujinun, Luewan, Suchaya, and Tongsong, Theera

Abstract

This report describes a variant of McKusick-Kaufman syndrome presenting with a large fetal abdominal cyst of hydrometrocolpos at 37 weeks of gestation. The diagnosis was based on the ultrasound findings of a large homogeneous hypoechoic cyst (diameter of >10 cm) with incomplete septum, thickened wall, superiorly connecting to the dilated uterus, consistent with hydrometrocolpos. Additionally, pre-axial mirror polydactyly of the left foot was suspected. Postnatal examination/work-up confirmed the prenatal findings. This is the first report of prenatal diagnosis of hydrometrocolpos with complex polydactyly of mirror image pre-axial duplications containing nine toes instead of six-toe postaxial polydactyly. [ABSTRACT FROM AUTHOR]

Published

2021

11. Biallelic variants in CTU2 cause DREAM‐PL syndrome and impair thiolation of tRNA wobble U34.

Author

Shaheen, Ranad, Mark, Paul, Prevost, Christopher T., AlKindi, Adila, Alhag, Ahmad, Estwani, Fatima, Al‐Sheddi, Tarfa, Alobeid, Eman, Alenazi, Mona M., Ewida, Nour, Ibrahim, Niema, Hashem, Mais, Abdulwahab, Firdous, Bryant, Emily M., Spinelli, Egidio, Millichap, John, Barnett, Sarah S., Kearney, Hutton M., Accogli, Andrea, and Scala, Marcello

Abstract

The wobble position in the anticodon loop of transfer ribonucleic acid (tRNA) is subject to numerous posttranscriptional modifications. In particular, thiolation of the wobble uridine has been shown to play an important role in codon‐anticodon interactions. This modification is catalyzed by a highly conserved CTU1/CTU2 complex, disruption of which has been shown to cause abnormal phenotypes in yeast, worms, and plants. We have previously suggested that a single founder splicing variant in human CTU2 causes a novel multiple congenital anomalies syndrome consisting of dysmorphic facies, renal agenesis, ambiguous genitalia, microcephaly, polydactyly, and lissencephaly (DREAM‐PL). In this study, we describe five new patients with DREAM‐PL phenotype and whose molecular analysis expands the allelic heterogeneity of the syndrome to five different alleles; four of which predict protein truncation. Functional characterization using patient‐derived cells for each of these alleles, as well as the original founder allele; revealed a specific impairment of wobble uridine thiolation in all known thiol‐containing tRNAs. Our data establish a recognizable CTU2‐linked autosomal recessive syndrome in humans characterized by defective thiolation of the wobble uridine. The potential deleterious consequences for the translational efficiency and fidelity during development as a mechanism for pathogenicity represent an attractive target of future investigations. [ABSTRACT FROM AUTHOR]

Published

2019

12. Cytogenetic profile of patients with clinical spectrum of ambiguous genitalia, amenorrhea, and Turner phenotype: A 21‐year single‐center experience.

Author

Elkarhat, Zouhair, Belkady, Boutaina, Charoute, Hicham, Zarouf, Latifa, Razoki, Lunda, Aboulfaraj, Jamila, Nassereddine, Sanaa, Elbakay, Chadli, Nasser, Boubker, Barakat, Abdelhamid, and Rouba, Hassan

Abstract

The aim of the present study was to determine the frequency and nature of chromosomal abnormalities involved in patients with the clinical spectrum of ambiguous genitalia (AG), amenorrhea, and Turner phenotype, in order to compare them with those reported elsewhere. The study was conducted in the Cytogenetic Department of Pasteur Institute of Morocco, and it reports on the patients who were recruited between 1996 and 2016. Cytogenetic analysis was performed according to the standard method. Among 1,415 patients, chromosomal abnormalities were identified in 7.13% (48/673) of patients with AG, 17.39% (28/161) of patients with primary amenorrhea (PA), 4% (1/25) of patients with secondary amenorrhea, and 23.20% (129/556) of patients with Turner phenotype. However, Turner syndrome was diagnosed in 0.89% (6/673) of patients with AG, 10.56% (17/161) of patients with PA, and 19.78% (110/556) of patients with Turner phenotype. In addition, Klinefelter syndrome and mixed gonadal dysgenesis were confirmed in 2.97% and 1.93% of patients, respectively, with AG, while, chimerism, trisomy 8, and trisomy 13 were confirmed only in 0.15% each. Trisomy 21 was confirmed in patients with AG and Turner phenotype (0.15% and 0.36%, respectively). Moreover, 5.60% (9/161) of patients with PA have been diagnosed as having sex reversal. Thus, the frequency of chromosomal abnormalities observed in Moroccan patients with PA is comparable to that reported in Tunisia, Turkey, Iran, and Hong Kong. However, the frequency is significantly less than that identified in India, Malaysia, Italy, and Romania. [ABSTRACT FROM AUTHOR]

Published

2019

13. Large divergence in testosterone concentrations between men and women: Frame of reference for elite athletes in sex‐specific competition in sports, a narrative review.

Author

Clark, Richard V., Wald, Jeffrey A., Swerdloff, Ronald S., Wang, Christina, Wu, Frederick C. W., Bowers, Larry D., and Matsumoto, Alvin M.

Subjects

*TESTOSTERONE, *ANDROGENS, *PERFORMANCE-enhancing drugs, *ATHLETES' health, *EMERGENCY medicine, *SPORTS medicine

Abstract

Summary: Objective: The purpose of this narrative review was to summarize available data on testosterone levels in normal, healthy adult males and females, to provide a physiologic reference framework to evaluate testosterone levels reported in males and females with conditions that elevate androgens, such as disorders of sex development (DSD), and to determine the separation or overlap of testosterone levels between normal and affected males and females. Methods: A literature review was conducted for published papers, from peer reviewed journals, reporting testosterone levels in healthy males and females, males with 46XY DSD, and females with hyperandrogenism due to polycystic ovary syndrome (PCOS). Papers were selected that had adequate characterization of participants, and description of the methodology for measurement of serum testosterone and reporting of results. Results: In the healthy, normal males and females, there was a clear bimodal distribution of testosterone levels, with the lower end of the male range being four‐ to fivefold higher than the upper end of the female range(males 8.8‐30.9 nmol/L, females 0.4‐2.0 nmol/L). Individuals with 46XY DSD, specifically those with 5‐alpha reductase deficiency, type 2 and androgen insensitivity syndrome testosterone levels that were within normal male range. Females with PCOS or congenital adrenal hyperplasia were above the normal female range but still below the normal male range. Conclusions: Existing studies strongly support a bimodal distribution of serum testosterone levels in females compared to males. These data should be considered in the discussion of female competition eligibility in individuals with possible DSD or hyperandrogenism. [ABSTRACT FROM AUTHOR]

Published

2019

14. Novel mosaic SRY gene deletions in three newborn males with variable genitourinary malformations.

Author

Roberts, Jennifer, Lyalin, Dmitry, Tosatto, Norwood, Rana, Pratibha, Fadoul, Hiba, Welsh, Holly, Zhang, Lei, Cooley, Linda, and Repnikova, Elena

Abstract

Ambiguous genitalia in the newborn can present a diagnostic challenge in medical practice. In most cases, the causes of genitourinary anomalies are not well understood; both genetic and environmental factors are thought to play a role. In this study, we report mosaic SRY gene deletion identified by fluorescence in situ hybridization (FISH) analysis in three unrelated newborn male patients with genital anomalies. G‐banded chromosomes and microarray analysis were normal for all three patients. One patient had microphallus, hypospadias, bifid scrotum, exstrophic perineal tissue identified as a rectal duplication, lumbar vertebral anomalies, scoliosis, and a dysmorphic sacrum. The other two patients had isolated epispadias with the urethral meatus close to the penopubic junction. All three had bilateral palpable gonads in the scrotum. While this is the first report of mosaic SRY deletions, mosaic SRY sequence variants have been described in patients with variable genitourinary anomalies. This study identifies FISH analysis as a reliable method for mosaic SRY deletion detection. We suggest SRY FISH analysis should be used in the clinical workup of patients with genitourinary ambiguity. [ABSTRACT FROM AUTHOR]

Published

2018

15. A novel mutation in steroidogenic factor ( SF1/ NR5A1) gene in a patient with 46 XY DSD without adrenal insufficiency.

Author

Tuhan, H., Anik, A., Catli, G., Onay, H., Aykut, A., Abaci, A., and Bober, E.

Subjects

*GENETIC mutation, *ADRENAL insufficiency, *DYSGENESIS, *MOSAICISM, *ANDROGENS, *GENETICS

Abstract

Steroidogenic factor-1 ( SF-1), also known as nuclear receptor subfamily 5 group A member 1 ( NR5A1), is a member of orphan receptor subfamily and located on chromosome 9 (9q33). In 46, XY individuals with mutation of SF-1 gene, adrenal failure, testis dysgenesis, androgen synthesis defects, hypospadias and anorchia with microphallus, infertility can occur from severe to mild. We report a case of a 20-day-old male who is admitted to our clinic due to ambiguous genitalia. In this report, we describe a novel heterozygous c.814A > C (p. T272P) NR5A1 mutation in a patient with 46, XY DSD without adrenal insufficiency. We describe a novel missense mutation c.814A > C (p. T272P) in NR5A1 gene which had not previously been reported. Also this report highlights that the potential diagnostic utility of next-generation sequencing is an effective strategy versus Sanger sequencing to identify genetic mosaicism in clinical practice. [ABSTRACT FROM AUTHOR]

Published

2017

16. Maternal Uniparental Disomy for Chromosome 6 in a Patient with IUGR, Ambiguous Genitalia, and Persistent Mullerian Structures.

Author

Lazier, Joanna, Martin, Nicole, Stavropoulos, James Dimitrios, and Chitayat, David

Abstract

Maternal uniparental disomy of chromosome 6 [upd(6)mat] is rare and has only been previously reported 13 times with the main associated phenotype being IUGR. We present a case of a male patient with isodisomy upd(6)mat resulting in severe IUGR and ambiguous genitalia, a phenotype not previously described in association with this chromosome finding. The patient initially presented prenatally with IUGR at 19 weeks gestation with placental dysfunction and ambiguous genitalia noted at 27 weeks. Postnatally, the patient had external genital abnormalities, the gonads were in the inguinal canal and there was a rudimentary appearing vagina and uterus. Karyotype is 46, XY and SNP array revealed maternal isodisomy of 171Mb at 6p25.3q27 with no pathogenic copy number variants. To our best knowledge, this is the first case of an XY patient with upd(6) mat with IUGR and ambiguous genitalia, further supporting previous reports regarding an association between upd(6)mat and IUGR. This patient also presented with a disorder of sex development (46, XY DSD) with the sex chromosome being male and positive for the SRY gene, testicular gonadal sex and abnormal external and internal genitalia. [ABSTRACT FROM AUTHOR]

Published

2016

17. Spectrum of urorectal septum malformation sequence.

Author

Shah, Krupa, Nayak, Shalini S., Shukla, Anju, and Girisha, Katta M.

Abstract

Urorectal septum malformation sequence ( URSMS) is a rare spectrum of malformations involving various organ systems. Here, we present eight cases of URSMS, noted in autopsy, with different degrees of complexity, seven being the complete type and one being the partial type. All cases had gastrointestinal tract malformation in the form of the imperforate anus and indeterminate genitalia. Other gastrointestinal tract anomalies were anal agenesis in two cases, anorectal agenesis in two cases, and malformed lower intestinal tract in four cases. The associated renal abnormality was noted in five cases, which were unilateral renal agenesis, dysplastic kidney, hydronephrosis, horseshoe kidney, and unilateral hypoplastic ectopic kidney. External genital malformation, present in both male and female fetuses, included a knob-like structure at perineum in female fetuses, genital fold hypoplasia and penile aplasia or hypoplasia in male fetuses. Skeletal abnormalities included two cases of sacral agenesis and one case of lumbosacral dysraphism. Other anomalies included a case with alobar holoprosencephaly, truncus arteriosus with hypoplastic lungs in one case, and three cases with abdominal wall defects. It is our attempt to delineate a spectrum of abnormalities associated with URSMS. [ABSTRACT FROM AUTHOR]

Published

2016

18. Country-based reference values and international comparisons of clitoral size in healthy Nigerian newborn infants.

Author

Jarrett, Olumide Olatokunbo, Ayoola, Omolola Ouwakemi, Jonsson, Björn, Albertsson‐Wikland, Kerstin, and Ritzen, Martin

Subjects

*GENITAL abnormalities, *NIGERIANS, *CLITORIS, *COMPARATIVE studies, *DISEASES, *VULVA, *NEWBORN infants, *RESEARCH methodology, *MEDICAL cooperation, *REFERENCE values, *RESEARCH, *EVALUATION research, *ANATOMY, DIAGNOSIS of neonatal diseases

Abstract

Aim: Clitoral size references are useful for diagnosing genital abnormalities. Despite the fact that examining the genitalia is an important aspect of newborn evaluation, few studies have been carried out to determine normal clitoral size in newborn infants. The aim of this study was to establish reference values for clitoral size in Nigerian newborn girls and to compare them with references from other ethnic populations.Methods: A total of 244 healthy newborn girls delivered at 28-43 weeks gestation were enrolled in the study, and clitoral lengths and widths were measured at <72 hours.Results: The mean clitoral length was 7.7 mm with a standard deviation of ±1.37 mm, while the mean clitoral width was 4.40 ± 0.89 mm. The clitoral length was significantly longer than those reported for Caucasian (4.00 ± 1.24 mm), Korean (3.82 ± 1.47), Turkish (4.93 ± 1.61) and Japanese (4.30 ± 1.10) babies.Conclusion: The present results make it possible to evaluate clitoral size in Nigerian newborn baby girls in an objective way, to identify genital abnormalities and endocrine disorders. Based on this study, a clitoral length of more than 10 mm would be considered clitoromegaly in a newborn girl in Nigeria. [ABSTRACT FROM AUTHOR]

Published

2015

19. Bifid scrotum and anocutaneous fistula associated with a perineal lipomatous tumor complicated by temporary bilateral cryptorchidism in utero mimicking ambiguous genitalia: 2-D/3-D fetal ultrasonography.

Author

Inde, Yusuke, Terada, Yusuke, Ikegami, Ei, Sekiguchi, Atsuko, Nakai, Akihito, and Takeshita, Toshiyuki

Subjects

*TUMOR diagnosis, *MALE reproductive organ diseases, *CRYPTORCHISM, *SEX differentiation disorders, *FISTULA, *PRENATAL diagnosis, *SCROTUM, *FETUS, *DIAGNOSIS

Abstract

Ambiguous genitalia ( AG) is a morphological diagnosis defined as genitalia not typical of a male or female. Findings mimicking AG, such as penoscrotal anomalies, anorectal malformations, and perineal lipomatous tumors, may prevent accurate identification of the fetal sex. We report a case of bifid scrotum and anocutaneous fistula associated with a perineal lipomatous tumor complicated by temporary bilateral cryptorchidism in utero, which were findings mimicking AG. Several perineal anomalies are associated developmental occurrences. In the present case, the combination of bifid scrotum and temporary bilateral cryptorchidism in the male fetus mimicked the combination of clitoromegaly and prominent labia, which are commonly observed in female fetuses. However, serial systemic assessments using prenatal 2-D/3-D ultrasonography and magnetic resonance imaging were unable to detect the anocutaneous fistula and differentiate the perineal lipomatous tumor. This case report suggests that the prenatal detection of perineal abnormalities may warn obstetricians of potentially undetected congenital perineal anomalies. [ABSTRACT FROM AUTHOR]

Published

2014

20. A patient with a unique frameshift mutation in GPC3, causing Simpson-Golabi-Behmel syndrome, presenting with craniosynostosis, penoscrotal hypospadias, and a large prostatic utricle.

Author

Villarreal, Diana D., Villarreal, Humberto, Paez, Ana Maria, Peppas, Dennis, Lynch, Jane, Roeder, Elizabeth, and Powers, George C.

Abstract

We present a Hispanic male with the clinical and molecular diagnosis of Simpson-Golabi-Behmel syndrome (SGBS). The patient was born with multiple anomalies not entirely typical of SGBS patients, including penoscrotal hypospadias, a large prostatic utricle, and left coronal craniosynostosis. In addition, he demonstrated endocrine anomalies including a low random cortisol level suspicious for adrenal insufficiency and low testosterone level. To our knowledge, this is the first report of a prostatic utricle in SGBS and the second report of craniosynostosis. The unique disease-causing mutation likely arose de novo in the mother. It is a deletion-insertion that leads to a frameshift at the p.S349 residue of GPC3 and a premature stop codon after five more amino acids. P.S349 is the same residue that is normally cleaved by the Furin convertase, although the significance of this novel mutation with respect to the patient's multiple anomalies is unknown. We present this case as the perinatal course of a patient with unique features of SGBS and a confirmed molecular diagnosis. © 2013 Wiley Periodicals, Inc. [ABSTRACT FROM AUTHOR]

Published

2013

21. The perlman syndrome: Familial renal dysplasia with Wilms tumor, fetal gigantism and multiple congenital anomalies.

Author

Neri, Giovanni, Martini‐Neri, Maria Enrica, Katz, Ben E., and Opitz, John M.

Abstract

Introduction The ensuing paper by Professor Giovanni Neri and colleagues was originally published in 1984, American Journal of Medical Genetics 19:195-207. The original article described a new family with a condition that the authors designated as the Perlman syndrome. This disorder, while uncommon, is an important multiple congenital anomaly and dysplasia syndrome; the causative gene was recently identified. This paper is a seminal work and is graciously republished by Wiley-Blackwell in the Special Festschrift issue honoring Professor' Neri. [ABSTRACT FROM AUTHOR]

Published

2013

22. Prenatal Treatment of Congenital Adrenal Hyperplasia-Not Standard of Care.

Author

Witchel, Selma and Miller, Walter

Abstract

Congenital adrenal hyperplasia (CAH) due to steroid 21-hydroxylase deficiency is a common autosomal recessive disorder due to mutations in the CYP21A2 gene. Since genetic counselors play a crucial role in educating families about inherited disorders, they need to have thorough knowledge regarding the pathophysiology of CAH especially the effects on the fetus, the complex genetics of this disorder, and the controversies surrounding experimental prenatal dexamethasone treatment. Affected female fetuses may have varying degree of virilization of the external genitalia. Starting in the 1980's, supraphysiologic glucocorticoid treatment was used to decrease the virilization of the external genitalia of affected female fetuses. However, recent clinical observations, animal studies and greater awareness of the details of human fetal adrenal physiology raise concerns regarding the safety of this prenatal treatment. We review the pathophysiology of CAH, the safety and ethical considerations of prenatal dexamethasone treatment and the views of multiple medical societies that conclude that this experimental therapy should only be done in prospective trials approved by ethical review boards. [ABSTRACT FROM AUTHOR]

Published

2012

23. Chromosome 9p deletion syndrome and sex reversal: Novel findings and redefinition of the critically deleted regions.

Author

Onesimo, Roberta, Orteschi, Daniela, Scalzone, Maria, Rossodivita, Aurora, Nanni, Lorenzo, Zannoni, Gian Franco, Marrocco, Giacinto, Battaglia, Domenica, Fundarò, Carlo, and Neri, Giovanni

Abstract

Deletions of the short arm of chromosome 9 are associated with two distinct clinical entities. Small telomeric 9p24.3 deletions cause genital anomalies in male subjects, ranging from disorder of gonadal sex to genital differentiation anomalies, while large terminal or interstitial deletions result in 9p-malformation syndrome phenotype. The critical region for non-syndromic 46,XY sex reversal was assigned to a 1 Mb interval of chromosome 9p, extending from the telomere to the DMRT genes cluster. The 9p-syndrome was assigned to bands 9p22.3p24.1, but a phenotypic map has not been established for this condition, probably because of the lack of detailed molecular and/or phenotypic characterization, as well as frequent involvement of additional chromosome rearrangements. Here, we describe a unique patient with a small isolated 9p terminal deletion, characterized by array-CGH and FISH, who shows a complex phenotype with multiple physical anomalies, resembling the 9p-syndrome, disorder of sex development with gonadoblastoma, congenital heart defect and epilepsy. The observed deletion includes the 46,XY sex-reversal critical region, excluding the region so far associated with the 9p-syndrome. Genotype-phenotype correlations are tentatively established comparing our patient to seven other previously reported males with isolated terminal 9p deletions, finely defined at a molecular level. Our observations expand the 9p deletion clinical spectrum, and add significantly to the definition of a 9p-syndrome critical region. © 2012 Wiley Periodicals, Inc. [ABSTRACT FROM AUTHOR]

Published

2012

24. Ambiguous genitalia: What prenatal genetic testing is practical?

Author

Adam, Margaret P., Fechner, Patricia Y., Ramsdell, Linda A., Badaru, Angela, Grady, Richard E., Pagon, Roberta A., McCauley, Elizabeth, Cheng, Edith Y., Parisi, Melissa A., and Shnorhavorian, Margarett

Abstract

Concern for ambiguous genitalia or chromosome-phenotype discordance detected in a prenatal setting has increased over the last two decades. Practitioners faced with this prenatal finding have a variety of genetic tests available to them; however, it is unclear to what extent prenatal testing for disorders of sex development (DSD) is useful or practical. We undertook a retrospective review of the medical records of 140 individuals evaluated through the DSD clinic at Seattle Children's Hospital with birthdates from 01/01/1994 through 08/16/2011 to determine the rate of prenatal detection of ambiguous genitalia in individuals with DSD, what prenatal diagnostic workup was undertaken, and the postnatal outcome, including whether a postnatal genetic diagnosis was confirmed. Of all 140 subjects, 34 (24%) were identified prenatally. The most common postnatal diagnoses were penoscrotal hypospadias with transposition of the scrotum with no known genetic cause (24/140; 17%) and 21-hydroxylase deficiency (20/140; 14%). Apart from these, no single diagnosis comprised more than a few cases. Prenatal diagnostic testing varied widely, from no tests to multiple molecular tests with amniotic fluid hormone concentrations. In the absence of other fetal anomalies or growth retardation on ultrasound, prenatal karyotype with fluorescence in situ hybridization for the SRY gene is the most useful test when ambiguous genitalia is suspected. Further prenatal testing for Smith-Lemli-Opitz syndrome in 46,XY individuals and congenital adrenal hyperplasia in 46,XX individuals may be considered. However, targeted molecular testing for rare DSD conditions in the absence of a family history of DSD has a low yield. © 2012 Wiley Periodicals, Inc. [ABSTRACT FROM AUTHOR]

Published

2012

25. Rare case of XX/XY mosaicism and trisomy 13 in early prenatal diagnosis.

Author

Sifakis, Stavros, Anagnostopoulou, Katherine, Plastira, Konstantina, Vrachnis, Nikolaos, Konstantinidou, Anastasia, and Sklavounou, Evangelia

Abstract

Coexistence of XX/XY sex mosaicism and autosomal trisomy in prenatal diagnosis is particularly rare. Herein, we report the first, to our knowledge, case of a fetus with cyclopia, ambiguous genitalia and a 47,XX,+13,inv9[47]/47,XY,+13[13] karyotype detected at 13 weeks of gestation after chorionic villus sampling. Molecular analysis after prenatal diagnosis suggests that this is a case of sex mosaicism coexisting with trisomy 13, rather than chimera. Birth Defects Research (Part A), 2012. © 2012 Wiley Periodicals, Inc. [ABSTRACT FROM AUTHOR]

Published

2012

26. Undervirilization in XY newborns may hide a 5α-reductase deficiency: report of three new SRD5A2 gene mutations L. Maimoun et al. Pitfall in PAIS diagnosis in XY newborn.

Author

Maimoun, L., Philibert, P., Cammas, B., Audran, F., Pienkowski, C., Kurtz, F., Heinrich, C., Cartigny, M., and Sultan, C.

Subjects

*VIRILISM, *GENETIC mutation, *NEWBORN infants, *INTERSEXUALITY, *PHENOTYPES, *MOLECULAR diagnosis, *TESTOSTERONE

Abstract

The observation of ambiguous genitalia in the newborn signals a medical, surgical and psychological emergency. The most crucial decision will be the choice of sex assignment. Rapid and precise diagnosis is thus essential. In XY newborns with normal/high plasma testosterone (T), partial androgen insensitivity syndrome (PAIS) is usually the first diagnosis evoked, which implies an androgen receptor (AR) defect. The diagnosis of steroid-5-alpha-reductase deficiency is rarely considered by the paediatrician. We report three new SRD5A2 gene mutations in four newborns from France, Morocco and Turkey. The newborns presented with ambiguous genitalia and normal plasma T values and the initial diagnosis\PAIS. In all four cases, normal sequences of the complete AR gene excluded this diagnosis and raised the hypothesis of 5α-reductase deficiency. The entire coding region (5 exons) of the SRD5A2 gene was assessed by PCR and direct sequencing analysis. For patient 1, we identified a new homozygous 2bp deletion in exon 1 (c.122_123delAG). Patient 2 had a known homozygous mutation, p.G115D, in exon 2. New compound heterozygous mutations in exon 4 (p.A215V) and exon 5 (p.X255Q) were found in patient 3. Patient 4 presented a new substitution in exon 1 (p.S14R) associated with a known polymorphism (p.V89L). Our data confirm our previous experience and clearly demonstrate that a 5-α reductase defect should be considered in all XY newborns with ambiguous genitalia and normal plasma T secretion, whatever their geographic area or ethnic group; moreover, this defect was not linked to specific phenotype. Early molecular diagnosis is indispensable for the crucial decision of the newborn's sex of rearing. [ABSTRACT FROM AUTHOR]

Published

2010

27. Service users’ experiences of obtaining and giving information about disorders of sex development.

Author

Liao, L.-M., Green, H., Creighton, S. M., Crouch, N. S., and Conway, G. S.

Subjects

*SEXUAL dysfunction, *HEALTH outcome assessment, *GENITAL surgery, *MEDICAL records, *MEDICAL informatics

Abstract

Objective To quantify participants’ experiences of obtaining and giving information about disorders of sex development (DSD). Design Cross-sectional survey study that asked people about their current and past experiences relating to DSD disclosure. Setting A large tertiary referral centre for DSD management in the UK. Population One hundred of 126 people with a confirmed diagnosis of DSD who were invited to participate in the study formed the usable sample. Methods All people who attended clinic for follow-up during the study period and members of a patient support group whose annual meeting fell within the study period were asked to complete the Middlesex Communication Survey. Main outcome measures The Middlesex Communication Survey. Results Younger participants were more likely to report having been appropriately informed about their diagnosis than older people. Nearly half of the former had been fully informed about their diagnosis by age 15 years, compared with 0% of the older age group. In terms of information sharing, mothers were most likely to be the person with whom the participant had shared (almost/all) DSD information (74%), followed by current partners (71%). Information relating to genital surgery, presence of testes and clitoral anomalies were the least likely aspects to have been unambiguously shared with even the most informed person. Conclusions Our results suggest that difficulties in obtaining DSD information from care providers were common, and that communication has improved for younger participants. The study also confirmed that many people with DSD continue to struggle with confiding, even in those closest to them, about aspects of their diagnosis. Care protocol needs to centralise psychological adaptation, which should also be a primary focus for future research. [ABSTRACT FROM AUTHOR]

Published

2010

28. Using virtual reality for evaluation of fetal ambiguous genitalia.

Author

Verwoerd-Dikkeboom, C. M., Koning, A. H. J., Groenenberg, I. A. L., Smit, B. J., Brezinka, C., Van Der Spek, P. J., and Steegers, E. A. P.

Subjects

*VIRTUAL reality, *COMPUTER simulation, *ULTRASONIC imaging, *GENITALIA, *ORGANS (Anatomy), *FETUS

Abstract

The article examines the utility of a virtual reality system in the visualization of three-dimensional (3D) ultrasound images of fetal ambiguous genitalia. A better impression of genital ambiguity can be established by evaluating the genitals in the BARCO I-Space virtual reality system. The system projects stereoscopic images that allow viewers to see a 3D hologram of the data being visualized. It can be applied in cases where depth perception improves visualization of anatomical structures.

Published

2008

29. A visual pitfall: Persistent Mullerian duct syndrome (PMDS).

Author

Marcus, K.A., Halbertsma, F.J.J., Picard, J.Y., and Otten, B.J.

Subjects

*GENITOURINARY organs, *ENDOCRINE glands, *GENITOURINARY manifestations of general diseases, *UROLOGICAL emergencies, *UROGYNECOLOGY, *GENITOURINARY diseases, *UROLOGICAL surgery, *GENITALIA, *GONADS

Abstract

Persistent Müllerian Duct Syndrome (PMDS) is a rare disorder of the anti-mullerian hormone (AMH) synthesis or receptor, which due to the visual contrast of normal masculine external genitalia and female internal genitalia can raise confusion, sometimes during surgery for cryptorchidism or hernia inguinalis. For an acute and accurate analysis of such a situation a thorough knowledge of gonadal embryology is mandatory. The diagnosis is made on finding Müllerian structures in an individual with complete virilization without signs of hypocortisolism or exposition to maternal androgens during foetal life. Karyotyping and gonadal biopsy provide additional information to confirm the diagnosis. As the risk of malignant transformation is not clear, orchidopexy is advised in patients with cryptorchidism, with lifelong palpatory follow-up. In case of urologic symptoms, surgical removal of the Müllerian remnants can be considered, with careful attention for the vulnerable ductus deferens. Despite optimal treatment the prognosis regarding fertility remain uncertain. [ABSTRACT FROM AUTHOR]

Published

2008

30. Contribution of three-dimensional volume contrast imaging to the sonographic assessment of the fetal uterus.

Author

Jouannic, J.-M., Rosenblatt, J., Demaria, F., Jacobs, R., Aubry, M.-C., and Benifla, J.-L.

Subjects

*FETAL ultrasonic imaging, *ULTRASONICS in obstetrics, *FEMALE reproductive organs, *GESTATIONAL age, *OBSTETRICAL research

Abstract

Objective: To investigate the contribution of volume contrast imaging (VCI) in assessing the fetal uterus in normally developed female fetuses. Methods: The pelvis of 38 normal female fetuses was examined at 20-22 and 32-34 weeks' gestation using both conventional two-dimensional (2D) ultrasound and VCI on the same transverse or oblique longitudinal view of the fetal pelvis. Two experienced sonographers evaluated the ability of both techniques to image the fetal uterus. Results were compared by kappa index to evaluate the interobserver variability. Results: A clear picture of the fetal uterus was obtained in 50% and 82-87% of the cases at 20-22 weeks' gestation and in 80-85% and 95-100% of the cases at 32-34 weeks' gestation using conventional 2D ultrasound and VCI, respectively. There was moderate to good agreement of uterus visualization between the two observers, with kappa values ranging from 0.43 to 0.65. The lower level of agreement was obtained for conventional 2D ultrasound during the second trimester. Conclusions: Our results suggest that VCI may be successfully applied to prenatal ultrasonography of the fetal pelvis anatomy. By enhancing the contrast between the intrapelvic organs, VCI provides a clearer picture of the fetal uterus. [ABSTRACT FROM AUTHOR]

Published

2005

31. Abnormal steroidogenesis in three patients with Antley–Bixler syndrome: Apparent decreased activity of 17α-hydroxylase, 17,20-lyase and 21-hydroxylase.

Author

Adachi, Masanori, Asakura, Yumi, Tachibana, Katsuhiko, and Shackleton, Cedric

Subjects

*SKELETON, *HYDROXYLATION, *CRANIOSYNOSTOSES, *ADRENOCORTICAL hormones, *LEANNESS, *ANDROGENS, *LYASES

Abstract

Background: Antley–Bixler syndrome (ABS) is characterized mainly by abnormal skeletal morphonogenesis such as craniosynostosis and radiohumeral synostosis, and by ambiguous genitalia in some cases. The mechanisms resulting in these deformities have not been determined.Methods: The adrenal and gonadal function of three Japanese ABS patients were evaluated. Patient 1 (17-year-old-male) had bilateral cryptoorchidism, delayed puberty and symptoms of glucocorticoid deficiency. Patient 2 (14-year-old male) and patient 3 (4-year-old female) presented with emaciation. Additionally, patient 3 had partial labial fusion and common urogenital sinus. In each patient, blood sampling for steroid analysis before and after rapid adrenocorticotropic hormone (ACTH) stimulation was carried out. Additionally, urinary steroids were quantified. Molecular analysis of CYP17 and CYP21A2 were also performed.Results: All patients showed elevated basal 17α-deoxysteroid levels. Although the 17α-deoxysteroid levels further increased after rapid ACTH stimulation, 17α-hydroxysteroids including cortisol did not respond, suggesting impaired 17α-hydroxylation. Patient 1 and patient 2 showed low adrenal androgen blood levels both before and after rapid ACTH stimulation. Patient 3 showed lower than normal excretions of urinary androgens. Additionally, a prolonged ACTH stimulation in patient 3 failed to elicit significant increase of adrenal androgens. These findings suggested impaired 17,20-lyase activity. In contrast to attenuated 17α-hydroxycorticosteroids, notably cortisol, elevated 17α-hydroxyprogesterone (17OHP) levels were observed, not only in pubertal patients (1 and 2) but also in prepubertal patient 3, indicating impaired 21-hydroxylation. This assumption was supported by increased urinary 21-deoxycortisol metabolite excretion in patients 2 and 3. With the exception of a heterozygous mutation of CYP17 in one of the patients, other mutations of this gene or CYP21A2 were identified in any of the patients.Conclusion: Combined decreased 17α-hydroxylation, 17,20-lyase activity and 21-hydroxylation was detected in three ABS patients. Considering that the enzymes responsible are all cytochrome P450 enzymes and that another cytochrome P450 enzyme, lanosterol 14α-demethylase, has recently been shown to be impaired in an ABS patient, we speculate that dysfunction of a system which commonly regulates cytochrome P 450 activity may be responsible for the ABS phenotype. [ABSTRACT FROM AUTHOR]

Published

2004

32. Genital abnormalities mimicking congenital adrenal hyperplasia in premature infants.

Author

Greaves, R., Kanumakala, S., Read, A., and Zacharin, M.

Subjects

*GENITAL diseases, *ADRENOGENITAL syndrome, *PREMATURE infants, *MEDICAL screening, *BLOOD testing, *BIOCHEMICAL genetics, *GENITAL abnormalities, *GENITOURINARY disease diagnosis, *ADRENAL diseases, *DIFFERENTIAL diagnosis

Abstract

Unusual genital appearances in premature infants can be easily mistaken for true ambiguous genitalia, with alarming consequences. The results of blood and urine tests carried out for premature infants can be misleading due to persistence of the foetal zone of the adrenal cortex. More importantly, misdiagnosis is devastating for the parents and adds significantly to their distress. Here, we describe two patients with transient genital abnormalities and abnormal biochemical tests. [ABSTRACT FROM AUTHOR]

Published

2004

33. Occasional Article Rules for clinical diagnosis in babies with ambiguous genitalia.

Author

Low, Y. and Hutson, J.M.

Subjects

*GENITAL abnormalities, *CHILDREN, *HUMAN embryology, *SEX differentiation (Embryology)

Abstract

Intersex disorders are rare and complex; yet, in each case of genital ambiguity, accurate and expeditious management is required of the clinician. This article reviews the embryology of sexual differentiation, from which some ‘rules’ of diagnosis are derived. A simplified approach to the interpretation of clinical signs in ambiguous genitalia is presented and discussed. [ABSTRACT FROM AUTHOR]

Published

2003

34. Hb H hydrops foetalis syndrome: a case report and review of literature.

Author

Lorey, Fred, Charoenkwan, Pimlak, Witkowska, H. Ewa, Lafferty, John, Patterson, Margaret, Eng, Barry, Waye, John S., Finklestein, Jerry Z., and Chui, David H. K.

Subjects

*HEMOGLOBIN polymorphisms, *EDEMA

Abstract

Haemoglobin H (Hb H) disease is caused by deletion or inactivation of three α-globin genes, leaving only one intact and active α-globin gene. People with Hb H disease usually have moderate anaemia, but are generally thought to be asymptomatic. Some Hb H disease patients require transfusions, and there are reports of fetuses with Hb H disease who have severe anaemia in utero resulting in fatal hydrops foetalis syndrome. We now report a case of Hb H hydrops foetalis syndrome, caused by the inheritance of a hitherto novel α-globin gene point mutation (codon 35 TCC→CCC or Serine→Proline) and an α-thalassaemia deletion of the Filipino type removing all ζ-α-globin genes on the other chromosome 16. The infant was delivered prematurely because of pericardial effusion and fetal distress, and was found to have severe anaemia and congenital anomalies. A review of the relevant literature on this syndrome is presented, and serves to underscore the phenotypic variations of Hb H disease and the need for surveillance for this condition among newborns and genetic counselling in communities with a high proportion of at-risk populations. [ABSTRACT FROM AUTHOR]

Published

2001

35. Neurofibromatosis of the labium majus and clitoris: an unusual image reminiscent of ambiguous genitalia.

Author

Kantarci, Mecit, Alper, Fatih, Aliagaoglu, Cihangir, Yildirim, Umiran, Onbas, Omer, and Sivri, Fazilet

Subjects

*NEUROFIBROMATOSIS, *PHAKOMATOSES, *NEUROFIBROMA, *CLITORIS, *OBSTETRICS, *FEMALE reproductive organs, *GYNECOLOGY, *MEDICINE

Abstract

Examines the occurrence of neurofibromatosis in the labium majus and clitoris. Characterization of neurofibromatosis by neural tumors, café-au-lait spots and Lisch nodules; Enlargement of a pseudo-phallus and a labio-scrotal gonad; Factors contributing in the etiology of acquired clitoral hypertrophy.

Published

2005