Ketamine produces rapid antidepressant effects within 24 hours, thought to involve mTORC1 activation. In a double-blind crossover trial, 20 depressed patients received either rapamycin (an mTORC1 inhibitor) or placebo before ketamine. Rapamycin did not block ketamine's 24-hour antidepressant effects. Over two weeks, rapamycin prolonged ketamine's benefits: response rates were 41% with rapamycin versus 13% with placebo, and remission rates were 29% versus 7%. These findings question whether systemic or local mTORC1 blockade matters and suggest rapamycin may extend ketamine's effects, potentially informing mechanisms of depression relapse.
Ketamine, a drug that blocks NMDA glutamate receptors, produces symptoms resembling schizophrenia. Analyzing the Positive and Negative Syndrome Scale (PANSS) in four groups—135 healthy people given ketamine or saline, 187 chronic ketamine abusers, 154 early-course schizophrenia patients, and 522 chronic schizophrenia patients—revealed five similar symptom dimensions (positive, negative, cognitive, depressed, excitement/dissociation) across all groups. The chronic ketamine group's symptom structure more closely matched the schizophrenia groups than the acute ketamine group did. Symptoms were milder in ketamine users than in schizophrenia patients (Cohen's d = 0.7). The findings suggest ketamine-induced psychosis shares symptom dimensions with schizophrenia, though confounding factors warrant caution.