this post was submitted on 31 Oct 2024
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This got me curious whether the milk would be any different and, if I'm reading this study correctly, there's practically no difference in content
Said study: https://pubmed.ncbi.nlm.nih.gov/7462406/
Yep. Same software, same hardware, just different config files.
In 2024? Why? Risperdal is such a blunt instrument with respect to its broad affinity for receptors.
Acute care, understood.
i.e. "I need Olanzapine [broad receptor affinity, highly anti-cholinergic, well-tolerated], but, like, faster." I'm surprised that particular aspect of the side effect profile comes into play with acute usage.
Ah, yes, this happens a lot. No, I don't work in the medical field at all. I just know things, for reasons.
i.e. the psychosis has done so much cumulative damage at this point that you need to fall back to the typicals. That explains why the third-gens are useless.
On a different note, have you heard about Cobenfy yet?
https://www.npr.org/sections/shots-health-news/2024/09/27/g-s1-25089/karxt-cobenfy-schizophrenia-psychosis-fda
It obviously isn't suited to the needs of your practice. But I'm really glad we're making progress on alternative treatment approaches, especially novel ones like anti-muscarinics.
Hopefully the new glutamatergics can reach your setting soon.