Panel rejects psychedelic drug MDMA as a PTSD treatment in possible setback for advocates

WCVBILLIONEWSCENTER FIVE CHRISTOPHER. THANK YOU. FIVE ON YOUR MENTAL HEALTH TONIGHT, FINDING MAGIC IN MUSHROOMS. THERE’S NEW RESEARCH THAT SUGGESTS PSYCHEDELIC DRUGS MAY HELP SOME PATIENTS WITH DEPRESSION AND ANXIETY. HERE TO TALK ABOUT THAT IS DOCTOR MICHELLE DIBLASI, A PSYCHIATRIST AT TUFTS MEDICAL CENTER. HAPPY NEW YEAR, DOCTOR. HEY, DOCTOR, IT’S GREAT TO SEE YOU. SO, SO I’VE BEEN LOOKING AT THIS LIST OF DRUGS, AND THERE ARE SHROOMS, THERE’S LSD, THERE’S ECSTASY. YOU SAY THOSE THREE THINGS SO PEOPLE GO, WHAT? SO WHY DO MENTAL HEALTH EXPERTS THINK THAT THEY OFFER SIGNIFICANT HEALTH BENEFITS? YEAH, I HAVE TO SAY IT IS KIND OF STARTLING SEEING THINGS LIKE LSD, MAGIC MUSHROOMS, ECSTASY. BEING TOLD THAT THESE COULD HAVE POSITIVE BENEFITS FOR OUR MENTAL HEALTH. BUT THERE IS NEW RESEARCH THAT’S STARTING TO SHOW THAT THE MAIN INGREDIENTS IN SOME OF THESE PSYCHEDELIC DRUGS, LIKE MDMA AND ECSTASY, COULD HELP WITH SOME PEOPLE WITH POST-TRAUMATIC STRESS DISORDER OR PSILOCYBIN, WHICH IS FOUND IN MAGIC MUSHROOMS OR OR LSD, COULD HELP WITH DEPRESSION OR ANXIETY. BUT AGAIN, THESE ARE ONLY IN CERTAIN POPULATIONS. AND OF COURSE, UNDER VERY STRICT MEDICAL MONITORING. AND DOSING. SO SO THE RESEARCH, WHICH SOUNDS INTERESTING TO TOTALLY ILLEGAL. ARE THERE OTHER RISKS. YEAH. I MEAN HONESTLY I THINK THE BIGGEST RISK IS THAT THIS IS NOW GOING TO START TO BE REALLY BIG IN THE HEADLINES. I MEAN, WE’RE ALREADY TALKING ABOUT IT RIGHT. AND SO PEOPLE ARE GOING TO START SEEING THIS, YOU KNOW, THAT MAGIC MUSHROOMS AND LSD AND ECSTASY COULD BE HELPFUL. AND SO I REALLY THINK THE BIGGEST RISK IS PEOPLE STARTING TO SELF EXPERIMENT WITH THESE THINGS. AND SO I JUST WANT TO REMIND PEOPLE THAT YES, THEY COULD BE PROMISING FOR HELPING PEOPLE IN THE FUTURE. BUT AGAIN, THESE STUDIES ARE GOING TO BE DONE UNDER REALLY CAREFUL MEDICAL MONITORING. AND ONLY IN THE RIGHT PATIENT POPULATION. RIGHT. SOME OF THESE ACTUAL PSYCHEDELIC DRUGS COULD HARM PEOPLE, RIGHT? IF YOU HAVE LIKE BIPOLAR DISORDER OR ARE PRONE TO PSYCHOSIS OR HAVE SCHIZOPHRENIA. SO WE NEED TO BE REALLY CAREFUL AND WAIT UNTIL ALL THE EVIDENCE SORT OF UNFOLDS AND IS REVIEWED. AND THAT WAS WONDERFULLY PUT. SO. BUT BUT GIVEN ALL OF THAT, DOCTOR, LET’S JUST KIND OF LOOK AT THE FUTURE. IN YOUR OPINION, DOES DOES ONE APPEAR TO HAVE MORE POTENTIAL THAN THE OTHERS AND MAYBE GET A SHOT AT FDA APPROVAL? YOU KNOW, I FEEL LIKE ACTUALLY, AT LEAST ONE OF THESE MAY GET FDA APPROVAL, MAYBE BY THE END OF EVEN 2024. SO WITHIN THE NEXT YEAR, I MEAN, MDMA HAS BEEN SHOWING SOME REALLY, YOU KNOW, ROBUST STUDIES FOR PEOPLE WHO ARE STRUGGLING WITH POST TRAUMATIC STRESS DISORDER. UM, SO THAT’S A POSSIBILITY. YOU KNOW, LIKE I MENTIONED, PSILOCYBIN FOR DEPRESSION. AND SO I THINK IN THE NEXT YEAR TO TWO YEARS, SOME OF THESE MAY ACTUALLY GET FDA APPROVAL. AND SO I THINK THERE’S A LOT MORE RESEARCH TO COME. BUT I KNOW I’M PRETTY EXCITED TO SEE IF MAYBE WE CAN HAVE MORE TOOLS IN OUR TOOLBOX TO WORK WITH PEOPLE WHO ARE REALLY STRUGGLING WITH SEVERE MENTAL ILLNESS. DOCTOR MICHELL

Federal health advisers voted Tuesday against a first-of-a-kind proposal to begin using the mind-altering drug MDMA as a treatment for PTSD, handing a potentially major setback to psychedelic advocates who hope to win a landmark federal approval and bring the banned drugs into the medical mainstream. The panel of advisers to the Food and Drug Administration sided 10-1 against the overall benefits of MDMA when used to treat post-traumatic stress disorder. They cited flawed study data, questionable research conduct and significant drug risks, including the potential for heart problems, injury and abuse."It seems like there are so many problems with the data — each one alone might be OK, but when you pile them on top of each other … there's just a lot of questions I would have about how effective the treatment is," said Dr. Melissa Decker Barone, a psychologist with the Department of Veterans Affairs.The FDA is not required to follow the group's advice and is expected to make its final decision by August, but the negative opinion could strengthen FDA's rationale for rejecting the treatment. The vote followed hours of pointed questions and criticisms about the research submitted on MDMA — sometimes called ecstasy or molly. Panelists pointed to flawed studies that could have skewed the results, missing follow-up data on patient outcomes and a lack of diversity among participants. The vast majority of patients studied were white, with only five Black patients receiving MDMA, raising questions about the generalizability of the results."The fact that this study has so many white participants is problematic because I don't want something to roll out that only helps this one group," said Elizabeth Joniak-Grant, the group's patient representative.The FDA advisers also drew attention to allegations of misconduct in the trials that have recently surfaced in news stories and a report by the nonprofit Institute for Clinical and Economic Review, which evaluates experimental drug treatments. The incidents include a 2018 report of apparent sexual misconduct by a therapist interacting with a patient.Lykos Therapeutics, the company behind the study, said it previously reported the incident to the FDA and regulators in Canada, where the therapist is based. Lykos is essentially a corporate spinoff of the nation's leading psychedelic advocacy group, the Multidisciplinary Association for Psychedelic Studies, or MAPS, which funded the studies. The group was founded in 1986 to promote the benefits of MDMA and other mind-altering substances.MDMA is the first in a series of psychedelics — including LSD and psilocybin — that are expected to come before the FDA in the next few years. The panel's negative ruling could further derail financial investments in the fledgling industry, which has mainly been funded by a small number of wealthy backers.MDMA's main effect is triggering feelings of intimacy, connection and euphoria. When used to enhance talk therapy, the drug appears to help patients process their trauma and let go of disturbing thoughts and memories.But the panel struggled with the reliability of those results, given the difficulties of objectively testing psychedelic drugs.Because MDMA causes intense, psychological experiences, almost all patients in two key studies of the drug were able to guess whether they had received the MDMA or a dummy pill. That's the opposite of the approach generally required for high-quality drug research, in which bias is minimized by "blinding" patients and researchers to whether they received the drug under investigation."I'm not convinced at all that this drug is effective based on the data I saw," said Dr. Rajesh Narendran, a University of Pittsburgh psychiatrist who chaired the panel.Panelists also noted the difficulty of knowing how much of patients' improvement came from MDMA versus simply undergoing the extensive therapy, which totaled more than 80 hours for many patients. Results were further marred by other complicating factors, including a large number of patients who had previously used MDMA or other psychedelics drugs recreationally.Nearly three dozen public speakers also addressed the panel, including veterans who said they benefitted from MDMA therapy, medical professionals who advised against its use and journalists and independent researchers who reiterated the allegations of misconduct in the trials.

WASHINGTON —

The panel of advisers to the Food and Drug Administration sided 10-1 against the overall benefits of MDMA when used to treat post-traumatic stress disorder. They cited flawed study data, questionable research conduct and significant drug risks, including the potential for heart problems, injury and abuse.

"It seems like there are so many problems with the data — each one alone might be OK, but when you pile them on top of each other … there's just a lot of questions I would have about how effective the treatment is," said Dr. Melissa Decker Barone, a psychologist with the Department of Veterans Affairs.

The FDA is not required to follow the group's advice and is expected to make its final decision by August, but the negative opinion could strengthen FDA's rationale for rejecting the treatment.

The vote followed hours of pointed questions and criticisms about the research submitted on MDMA — sometimes called ecstasy or molly. Panelists pointed to flawed studies that could have skewed the results, missing follow-up data on patient outcomes and a lack of diversity among participants. The vast majority of patients studied were white, with only five Black patients receiving MDMA, raising questions about the generalizability of the results.

"The fact that this study has so many white participants is problematic because I don't want something to roll out that only helps this one group," said Elizabeth Joniak-Grant, the group's patient representative.

The FDA advisers also drew attention to allegations of misconduct in the trials that have recently surfaced in news stories and a report by the nonprofit Institute for Clinical and Economic Review, which evaluates experimental drug treatments. The incidents include a 2018 report of apparent sexual misconduct by a therapist interacting with a patient.

Lykos Therapeutics, the company behind the study, said it previously reported the incident to the FDA and regulators in Canada, where the therapist is based. Lykos is essentially a corporate spinoff of the nation's leading psychedelic advocacy group, the Multidisciplinary Association for Psychedelic Studies, or MAPS, which funded the studies. The group was founded in 1986 to promote the benefits of MDMA and other mind-altering substances.

MDMA is the first in a series of psychedelics — including LSD and psilocybin — that are expected to come before the FDA in the next few years. The panel's negative ruling could further derail financial investments in the fledgling industry, which has mainly been funded by a small number of wealthy backers.

MDMA's main effect is triggering feelings of intimacy, connection and euphoria. When used to enhance talk therapy, the drug appears to help patients process their trauma and let go of disturbing thoughts and memories.

But the panel struggled with the reliability of those results, given the difficulties of objectively testing psychedelic drugs.

Because MDMA causes intense, psychological experiences, almost all patients in two key studies of the drug were able to guess whether they had received the MDMA or a dummy pill. That's the opposite of the approach generally required for high-quality drug research, in which bias is minimized by "blinding" patients and researchers to whether they received the drug under investigation.

"I'm not convinced at all that this drug is effective based on the data I saw," said Dr. Rajesh Narendran, a University of Pittsburgh psychiatrist who chaired the panel.

Panelists also noted the difficulty of knowing how much of patients' improvement came from MDMA versus simply undergoing the extensive therapy, which totaled more than 80 hours for many patients. Results were further marred by other complicating factors, including a large number of patients who had previously used MDMA or other psychedelics drugs recreationally.

Nearly three dozen public speakers also addressed the panel, including veterans who said they benefitted from MDMA therapy, medical professionals who advised against its use and journalists and independent researchers who reiterated the allegations of misconduct in the trials.

Panel rejects psychedelic drug MDMA as a PTSD treatment in possible setback for advocates

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