Table 3.
Effects of sex hormones and raloxifene for the treatment of insomnia in postmenopausal schizophrenic patients.
| Hormone | Hypothesis | Findings |
|---|---|---|
| Estradiol | Estradiol is capable of preventing dopamine D1/D2-receptor-mediated disruptions of sensorimotor gating in animal models. | Is estradiol a potential target for the treatment of insomnia? No results for postmenopausal populations. |
| Progesterone | Brexanolone, a synthetic allopregnanolone, prevents depression-like behaviors in animal models. | The psychotropic properties of progesterone have not been evaluated in postmenopausal schizophrenic patients. |
| Testosterone | High testosterone–estradiol ratio at menopause. Testosterone implicated in physiopathology of schizophrenia. | The use of testosterone to treat insomnia has not been evaluated. |
| Dehydroepiandrosterone (DHEA) | Precursors of androgens in women may be effective for the treatment of insomnia at menopause. | Potentially effective for the treatment of psychotic or cognitive symptoms; no results for insomnia. |
| Raloxifene (SERMs) | Positive effect on sleep in healthy women. | Potential effectiveness in postmenopausal schizophrenia. Future studies should consider insomnia as a primary outcome. |