But Marks points out that the FDA typically follows the advice of its independent advisory committees — and the one that evaluated MDMA in June overwhelmingly voted against approving the drug, citing problems with clinical trial design that the advisers felt made it difficult to determine the drug’s safety and efficacy. One concern was about the difficulty of conducting a true placebo-controlled study with a hallucinogen: around 90% of the participants in Lykos’s trials guessed correctly whether they had received the drug or a placebo, and the expectation that MDMA should have an effect might have coloured their perception of whether it treated their symptoms.

Another concern was about Lykos’s strategy of administering the drug alongside psychotherapy. Rick Doblin, founder of the Multidisciplinary Association for Psychedelic Studies (MAPS), the non-profit organization that created Lykos, has said that he thinks the drug’s effects are inseparable from guided therapy. MDMA is thought to help people with PTSD be more receptive and open to revisiting traumatic events with a therapist. But because the FDA doesn’t regulate psychotherapy, the agency and advisory panel struggled to evaluate this claim. “It was an attempt to fit a square peg into a round hole,” Marks says.

  • I'm back on my BS 🤪@lemmy.autism.place
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    3 months ago

    around 90% of the participants in Lykos’s trials guessed correctly whether they had received the drug or a placebo

    I understand the logic with using a placebo comparison, but who cares if people got better solely because they know they took ecstasy?

    • SynonymousStoat@lemmy.world
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      3 months ago

      I’m no scientist, but I don’t really know how you can have a study of a psychoactive drug and the participants not be able to guess if they had the drug or the placebo.

      • WhatAmLemmy@lemmy.world
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        3 months ago

        These people are scientific bureaucrats who just go “computer says no”. This is clearly a case where “the gold standard” fails and another approach is necessary. That’s if they’re not on the payroll of big pharma to hamstring adoption of alternatives they can’t patent.

        • ArcticDagger@feddit.dkOP
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          3 months ago

          I agree that it’s a shame that it’s so difficult to eliminate the placebo effect from psychoactive drugs. There’s probably alternative ways of teasing out the effect, if any, from MDMA therapy, but human studies take a long time and, consequently, costs a lot of money. I’d imagine the researchers would love to do the studies, but doesn’t have the resources for it

          I think the critique about conflicts of interest seems a bit misguided. It’s not the scientists who doesn’t want to move further with this. It’s the FDA

          • lolcatnip@reddthat.com
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            3 months ago

            I didn’t think the idea of a placebo effect is even valid for a treatment for which no placebo exists. At best, it’s a thought experiment, but IMHO it’s more of a distinction without a difference.

            • ArcticDagger@feddit.dkOP
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              3 months ago

              That’s an interesting point. But maybe there are some compounds that can induce a state that fools people who’ve never tried psychoactive compounds? I’ve heard of studies using dehydrated water as a placebo for alcohol as it induces some of the same effects:

              Like ethanol, heavy water temporarily changes the relative density of cupula relative to the endolymph in the vestibular organ, causing positional nystagmus, illusions of bodily rotations, dizziness, and nausea. However, the direction of nystagmus is in the opposite direction of ethanol, since it is denser than water, not lighter.

              https://en.m.wikipedia.org/wiki/Heavy_water

              • WhatAmLemmy@lemmy.world
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                3 months ago

                That example is not a placebo. It’s the opposite of a placebo. A placebo is supposed to be the control. The baseline “truth” in a hypothesis. The entire idea of the placebo effect is that the individual’s own psychology — their expectation of an effect — induces a physiological response, which pollutes the baseline hypothesis and all test data. Thus, the entire purpose of a double blind is to negate that bias from impacting the researcher, or the rat being studied.

                That is fucking stupid when studying pretty much any drug people bother to take recreationally. They take them recreationally because they have an acutely noticeable effect. Unless you’re a virgin amish person or child, you’re gonna know when you’re drunk or high; MDMA, LSD, or Psilocybin are on a whole other level, especially at the doses taken for psychiatric treatment. A placebo would only make sense if you were testing micro-doses that are so low they’re widely considered to be imperceptible.

                So no. The “gold standard” is wholly insufficient to adequately study drugs that induce a significant psychological response. These drugs need to be analyzed by people who hold a greater understanding of their effects, and our perception of reality, than bureaucrats who have zero experience with what they’re studying. The only thing worse than a pseudo double blind would be rejecting significant drugs because they don’t fit into our existing ape-like understanding of reality (or capitalism), resigning to “computer says no”, and preventing millions of people from receiving an improvement in their quality of life; ignorance, stupidity, and maliciousness can cause the same level of damage.

    • ArcticDagger@feddit.dkOP
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      3 months ago

      But if they know they’re getting ecstasy, the improvement might originate from placebo which means that they’re not actually getting better from ecstasy. They’re just getting better because they think they should be getting better

      • Hamartiogonic@sopuli.xyz
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        3 months ago

        Yeah, that’s the thing with placebo. It’s surprisingly effective, and separating the psychological effect from actual chemistry can be very tricky. If most participants can correctly identify if they’re bing fed the real drug or a placebo, it makes it impossible to figure out how much each effect contributes to the end result. Ideally, you would only use effective medicine that does not need the placebo effect to actually work.

        Imagine, if all medicine had lots of placebo effect in them. How would you treat patients who are in a coma or otherwise unconscious?

        • rand_alpha19@moist.catsweat.com
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          3 months ago

          So, let’s just use an example of a pill that treats headaches so I can understand, because I’m kinda stupid.

          It works super well, and most patients taking it in double blind trials find it relieves headache pain considerably. Why is it a bad thing, to the point of rejecting it as a treatment, that the patient feels that the pill is working very well and has concluded on their own that this is probably not a placebo?

          I can understand a patient being misled by coincidence, but surely a measurable, verifiable, and repeatable benefit to the patient compared to pills without medicinal ingredients would warrant a different conclusion, wouldn’t it?

          In your coma scenario, I’m sure there is a statistical analysis that can be performed to show with a degree of certainty that a specific medication has a higher likelihood of being effective than a placebo in a controlled experiment.

          I commented on this same story a while ago when it first broke that it was likely to be rejected and I don’t think anyone explained it in the thread.

          • Hamartiogonic@sopuli.xyz
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            3 months ago

            Statistical tests are very picky. They have been designed by mathematicians in a mathematical ideal vacuum void of all reality. The method works in those ideal conditions, but when you take that method and apply it in messy reality where everything is flawed, you may run into some trouble. In simple cases, it’s easy to abide by the assumptions of the statistical test, but as your experiment gets more and more complicated, there are more and more potholes for you to dodge. Best case scenario is, your messy data is just barely clean enough that you can be reasonably sure the statistical test still works well enough and you can sort of trust the result up to a certain point.

            However, when you know for a fact that some of the underlying assumptions of the statistical test are clearly being violated, all bets are off. Sure, you get a result, but who in their right mind would ever trust that result?

            If the test says that the medicine is works, there’s clearly financial incentive to believe it and start selling those pills. If it says that the medicine is no better than placebo, there’s similar incentive to reject the test result and demand more experiments. Most of that debate goes out the window if you can be reasonably sure that the data is good enough and the result of your statistical test is reliable enough.

      • I'm back on my BS 🤪@lemmy.autism.place
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        3 months ago

        Yeah, that’s my point. What does it matter that they got better because they think they should get better? To me, what matters is that they got better, regardless of the reason. Bonus: they got high on ecstasy while under medical supervision.

        Option A: Take a pill that doesn’t feel like ecstasy and no one gets better.

        Option B: Don’t tell patients that ecstasy makes them feel better. Give them ecstacy. 20% of patients get better.

        Option C: Tell patients that ecstasy can make them feel better. Give them ecstacy. 40% of patients get better.

        Personally, option C seems like the most effective and thus preferred option. I don’t see any downside whatsoever.