scholarly journals Crossed Testicular Ectopia-A Rare Anamoly

2015 ◽  
Vol 01 (01) ◽  
pp. 015-018
Author(s):  
Noopur Priya ◽  
Luv Luthra ◽  
Sweta Agrawal
Keyword(s):  
Congenital Anomaly ◽  
Inguinal Hernia ◽  
Undescended Testis ◽  
Male Child ◽  
Mullerian Duct ◽  
Transverse Testicular Ectopia ◽  
True Hermaphroditism ◽  
Persistent Mullerian Duct Syndrome ◽  
Testicular Ectopia ◽  
Duct Syndrome

AbstractCrossed Testicular Ectopia (CTE)/Transverse Testicular Ectopia (TTE) is a rare but well-known congenital anomaly, in which both gonads migrate toward the same hemiscrotum. It is usually associated with other abnormalities such as persistent Mullerian duct syndrome, True Hermaphroditism, Inguinal Hernia, Hypospadias, Pseudohermaphroditism, and scrotal anomalies. We report a case of 6 years old male child with right undescended testis and empty left scrotum. Diagnosis was confirmed preoperatively by ultrasound followed by open inguinal exploration for orchidopexy.

scholarly journals TRANSVERSE TESTICULAR ECTOPIA

2016 ◽  
Vol 23 (05) ◽  
pp. 627-629
Author(s):  
Fayyaz Ahmad Orfi ◽  
Saira Shakeel ◽  
Farrukh Shahzad
Keyword(s):  
Inguinal Hernia ◽  
Hernia Repair ◽  
Congenital Anomalies ◽  
Fibrous Tissue ◽  
Mullerian Duct ◽  
Left Testis ◽  
Transverse Testicular Ectopia ◽  
Persistent Mullerian Duct Syndrome ◽  
Testicular Ectopia ◽  
Duct Syndrome

Crossed testicular ectopia (CTE) is a rare congenital anomaly14. It is also knownas transverse testicular ectopia (TTE). In this condition both testis descend/migrate towardsthe same hemi-scrotum. About 100 cases have been reported so far. It may be associatedwith other congenital anomalies which include persistent Mullerian Duct Syndrome, truehermaphroditism, pseudo-hermaphroditism, inguinal hernia, hypospadias and scrotalanomalies. We are reporting one such case in 6 years old boy who presented to CMH Malir inMarch 2014 with left inguinal hernia and per-operatively found to have right testis in left inguinalcanal. Left testis had descended into left upper scrotum. Vasa were tethered together in upperportion by fibrous tissue. Right testis and vas was separated, mobilized extra-peritonially anddone in right scrotum (ipsilateral). Left orchiopexy was done in left scrotum. Hernia repair wasthen preformed. Post-op u/s scan was done to detect any other associated pathology whichwas negative. In most of the published reports diagnosis was made per-operatively as was thecase in this patient.

scholarly journals Genetic and histopathological analysis of transverse testicular ectopia without persistent Müllerian duct syndrome: two case reports

2020 ◽  
Vol 14 (1) ◽  
Author(s):  
Takashi Nagai ◽  
Kentaro Mizuno ◽  
Masayuki Usami ◽  
Hidenori Nishio ◽  
Taiki Kato ◽  
...  
Keyword(s):  
Placental Alkaline Phosphatase ◽  
Mullerian Duct ◽  
Müllerian Duct ◽  
Transverse Testicular Ectopia ◽  
Persistent Müllerian Duct Syndrome ◽  
Persistent Mullerian Duct Syndrome ◽  
Relaxin Family ◽  
Variant Analysis ◽  
Testicular Ectopia ◽  
Duct Syndrome

Abstract Background Transverse testicular ectopia (TTE) is a rare anomaly in which both testes descend through a single inguinal canal into the same hemiscrotum. Although almost 20–50% of patients with TTE exhibit persistent Müllerian duct syndrome (PMDS) and many genetic analyses have been performed, no reports have described the genes contributing to TTE without PMDS. Here, we report two cases of TTE without PMDS using immunohistochemical staining and genetic analysis. Case presentation Two Asian patients with TTE without PMDS were subjected to orchiopexy. We performed testicular biopsies during operation and obtained blood samples before the operation. Testicular tissues were stained for c-kit, placental alkaline phosphatase (PLAP), and undifferentiated embryonic cell transcription factor 1 (UTF1) to evaluate the presence of intratubular malignant germ cells. Additionally, we performed polymerase chain reaction-based direct sequencing to identify single nucleotide polymorphisms in genes associated with regression of the Müllerian duct and testicular descent (that is, anti-Müllerian hormone [AMH], AMH receptor 2 [AMHR2], insulin-like 3 [INSL3], and relaxin family peptide receptor 2 [RXFP2]). The three-dimensional structures of proteins were predicted using SWISS-MODEL. In immunohistochemical analysis, c-kit and UTF1 were positive, whereas PLAP was negative in three testicular tissue samples from the two patients. These features were also detected on the unaffected side. In variant analysis, common missense variants in the AMH gene (g.365G>T; c.165G>T; p.Ser49Ile [rs10407022]) were observed. All variants in INSL3 and RXFP2 genes were intronic or silent. Conclusions Because UTF1, a specific marker of spermatogonial stem cell activity, was expressed in both the affected and unaffected sides in the testicular tissues of two patients, the risk of malignancy may be high in these patients. Although the etiology of TTE without PMDS remains unclear, our variant analysis results were consistent with previous reports, and variants in the AMH gene (rs10407022) may contribute to the specific phenotype of TTE without PMDS.

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