Discussion
46, XY pure gonadal dysgenesis, previously known as Swyer syndrome, can be caused by mutation in the sex-determining region on Y (SRY) gene located on the distal short arm of the Y chromosome (Yp11.3) [
1]. Mutations in other genes such as SOX9, DAX1, WT-1 and SF1 that are involved in the regulation of SRY expression or act as a transcription activator downstream of SRY in the testis-determining pathway may also result in XY pure gonadal dysgenesis [
2]. The mutations involved in testicular development result in the development of undifferentiated streak gonads, which do not produce antimüllerian hormone or androgens [
1]. Consequently, the vagina, cervix, uterus, and fallopian tubes develop, and external genitalia are those of females because of the absence of androgen action (
Fig. 2).
Unlike the dysgenetic gonads in XY pure gonadal dysgenesis, individuals with CAIS have normal testes, and Leydig cells in the testicle normally produce testosterone. However, androgen action is deficient because of mutations in the androgen receptor gene [
1]. Consequently, the Wolffian duct spontaneously regresses in the absence of androgens and cannot differentiate into the epididymis and vas deferens. And the Sertoli cells in the testes release antimüllerian hormone in the normal manner and induce the regression of müllerian structures [
1]. Therefore, patients with CAIS have a short, blind pouch vagina without a uterus, ovaries, or fallopian tubes (
Fig. 2).
In patients with CAIS, the testes may be located anywhere along the path of embryonic testicular descent; however, they are more commonly located in the inguinal canals or labia majora [
3]. Deeb and Hughes [
4] reported that more than half of patients with CAIS presented with inguinal hernia; half of these were bilateral and one-third contained gonads.
Careful history taking and physical examination are of the utmost importance in the diagnostic process of patients with 46, XY DSD. In both our cases, patients presented with female external genitalia. However, the patient with CAIS was distinguished by adequate breast development, probably due to the action of estrogens unopposed by the action of androgens. Also, MRI can be an effective diagnostic tool for patients with 46, XY DSD, particularly in identifying a hypoplastic uterus in XY pure gonadal dysgenesis and locating cryptorchid testes in CAIS cases. In addition, high serum levels of testosterone also help to distinguish CAIS from XY pure gonadal dysgenesis.
The clinical management of an XY female patient generally includes prophylactic gonadectomy to prevent malignant transformation, appropriate hormone replacement therapy (HRT), and psychological counseling.
Individuals whose karyotypes contain a Y cell are predisposed to gonadal ridge tumors, including gonadoblastomas, dysgerminomas, yolk sac tumors, and choriocarcinomas [
5]. Prophylactic gonadectomy is recommended for these patients to eliminate the risk of potential malignant changes of the gonads [
5]. When considering the timing of gonadectomy in patients with XY pure gonadal dysgenesis, early gonadectomy is advised because of the high risk of malignant potential, which is estimated to be 46% to 75% [
1]. In our case of XY pure gonadal dysgenesis, the patient underwent laparoscopic bilateral gonadectomy and salpingectomy soon after diagnosis. Patients with XY pure gonadal dysgenesis can become pregnant through
in vitro fertilization using donor oocytes [
6]. Compared with XY pure gonadal dysgenesis, gonadectomy is advised after pubertal development is completed in CAIS cases because of the low risk of malignancy before puberty and the fact that unopposed testicular estrogen induces breast development [
7]. In our case of CAIS, the patient underwent prophylactic gonadectomy after the pubertal development, and there was no evidence of malignancy in gonads.
After gonadectomy has been performed, exogenous HRT should be provided for XY female patients to initiate, mature, and maintain secondary sexual characteristics [
8]. Prevention of coronary heart disease and osteoporosis is an additional benefit of estrogen therapy [
8]. For individuals with XY pure gonadal dysgenesis, cyclic estrogen and progestogen therapy initiated after the completion of estrogen-induced breast development will prevent endometrial hyperplasia that may result from unopposed estrogen stimulation [
8]. In both our cases, patients received HRT, which will be continued until they reach 50 years of age.
Psychological counseling for the patient and their parents is an important element of management for patients with 46, XY DSD. In general, most individuals with 46, XY DSD have a completely female phenotype; therefore, female gender identity may be reinforced. When patients experience difficulty with penetration due to vaginal hypoplasia, a functional vagina may be considered for normal sexual satisfaction by progressive vaginal dilation, traditional vaginoplasty or laparoscopic Vecchietti method [
9].
To our knowledge, there have been few report describing the clinical imaging findings in patients with 46, XY DSD. Imaging findings including female external genitalia, streak gonads, and uterus in our case would be help for clinicians to assess patients with 46, XY DSD.