| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 5858592 | Reproductive Toxicology | 2013 | 8 Pages |
â¢Similar expression of immature Sertoli cells markers are found in adult cryptorchidism and estrogen/antiandrogen exposure.â¢There is similar absence of maturation marker androgen receptor in Sertoli cells of both types of patients.â¢Our data supports the occurrence of true Sertoli cell dedifferentiation caused by estrogen exposure in adult humans.â¢Our data suggests that Sertoli cell maturation is directly disrupted in testicular dysgenesis syndrome.â¢Our data suggests possible toxic effects of environmental factors on human fertility occurring during adulthood.
Studies over the last years show an increase in testicular cancer, hypospadias and cryptorchidism in industrial countries, leading to the concept of testicular dysgenesis syndrome (TDS). It is hypothesized that TDS is caused by estrogen and antiandrogen exposure during fetal life, accompanied by incomplete maturation of testicular Sertoli cells (SC). However, it is not known if SC disruption is a primary cause or a response to fetal Leydig cell testosterone production changes.To determine if SC differentiation is directly affected by estrogens, we compared SC maturation between adult gender reassignment cases exposed to estrogen and antiandrogen therapy, and those of typical TDS in adult cryptorchidism.We found similar expression of immature SC markers M2A antigen, inhibin bodies and Anti Mullerian Hormone, and the absence of maturation marker androgen receptor in SC of both types of patients. These data supports the occurrence of true SC dedifferentiation caused by estrogen exposure in adult humans. Our data also suggests that SC maturation is directly disrupted in TDS.
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