Finally, the Chemical Imbalance Myth Has Been Put to Bed

There is no evidence that depression is caused by lower levels or reduced activity of serotonin in the brain, according to a recent analysis of 17 previous studies. 

The analysis, carried out by Joanna Moncrieff, MD, a professor of psychiatry at University College London, and her colleagues, tells us pretty much what we've known all along. The chemical imbalance marketing myth has been used as an indicator that people need antidepressants.

The response to this analysis, by many psychiatrists at least, has been eye-opening.

The Science Media Centre (SMC), whom I've wrote about before on this blog, were rolling out their 'experts'.

Dr Michael Bloomfield, Consultant Psychiatrist and UKRI Principal Clinical Research Fellow, Translational Psychiatry Research Group Head, UCL, said:

"The findings from this umbrella review are really unsurprising. Depression has lots of different symptoms and I don’t think I’ve met any serious scientists or psychiatrists who think that all causes of depression are caused by a simple chemical imbalance in serotonin."

Bloomfield really needs to brush up on his research skills. Just two years ago, Adrienne Nagy, Board President of the National Alliance on Mental Illness (NAMI), America's largest grassroots mental health organization, had this to say:

"We're continually trying to educate the public to know that mental illness is an illness like any other illness—it's a biochemical imbalance in the brain. It's no different than diabetes or heart failure."

Other examples of psychiatrists promoting the chemical imbalance theory can be viewed here.

Another SMC 'expert', Prof David Nutt, Edmond J Safra Chair and Head of the Centre for Neuropsychopharmacology, Imperial College London, seemed to be digging his heels in when reacting to the Moncrieff analysis with:

"It is only recently that we have developed the technology to measure serotonin release in the living human brain and in the first study of this type (currently under review) we did find decreased serotonin release capacity in people with depression. So, to dismiss the serotonin hypothesis of depression at this point is premature."

Nutt has, in the past, received grants and personal fees from Lundbeck and GSK and personal fees from Lilly, BMS, Otsuka, Servier, and Pfizer, the majority of whom market and manufacture SSRI's, the very same types of drugs promoted to correct a chemical imbalance. I think it's no coincidence that Nutt still wants to hold on to the serotonin hypothesis of depression.

The general consensus (from psychiatry) of this new analysis seems to be, 'So what, we've known all along that it was just a theory'. I think they're either missing the point or being deliberately obtuse.

Samei Huda, author and consultant psychiatrist, Pennine Care NHS Foundation Trust, went one further. 

Here's a screenshot of his tweet which implies Moncrieff and her colleagues have "right-wing associations."

Huda is well-known to members of the #PrescribedHarm community on Twitter, he is also well known for baiting Twitter psychologists and others with accusations of racism or right-wing associations, myself included.

I find his above tweet was specifically constructed to be inflammatory. Huda can be followed here. I blocked him a couple of years ago.

The point many psychiatrists, on Twitter at least, seem to be missing is patients have been sold a lie. Not one single psychiatrist has been able to answer the following, Is the patient, taking SSRIs, at risk or is increasing serotonin in the brain deemed safe?

These days, Twitter psychiatrists tend to block patient accounts who raise concerns, or even questions such as mine above.

The reaction has been eye-opening particularly when you contrast it with 'expert' reactions to the Cipriani 2018 study that claimed antidepressants work and are effective. Not only were 'experts' gushing over Cipriani's study, some were even calling for more antidepressants to be prescribed.

Professor Carmine Pariante, spokesperson for the Royal College of Psychiatrists, said of the Cipriani analysis "This finally puts to bed the controversy on antidepressants, clearly showing that these drugs do work in lifting mood and helping most people with depression."

A year later, Pariante was interviewed by BBC's Angela Rippon. According to Pariante, his team "chemically induce brain cells in test tubes to mirror the state of depression. Antidepressant medication  is then added". Furthermore, according to Pariante, "There is no evidence that we are over prescribing antidepressants, yes more antidepressants are prescribed today than 10 years ago but, in fact, most people who need antidepressants are not receiving an antidepressant."

Yes, he really did say this.

You can watch the full show, Truth or Scare, here.

The SMC's 'expert' reaction can be viewed here.

Bob Fiddaman

Pariante's Dish of the Day

Image courtesy of @AuntyPsychiatry

Knock! Knock!

Who's there?

Dishes.

Dishes who?

Dishes psychobabble at its finest.

Psychiatrist Carmine Pariante is a key opinion leader who often speaks on behalf of the Royal College of Psychiatrists (RCP), the coven that continually promotes bizarre brain disorders and the brain pellets whilst downplaying the adverse effects these toxins cause, to include horrific withdrawal problems and iatrogenic deaths.

Yesterday Pariante caused a Twitter storm when promoting his appearance on BBC's "Truth or Scare," hosted by former newsreader and British icon, Angela Rippon.

The bizarre rantings of Pariante had me perplexed. I'm going to try to dissect his comments for you but, frankly, I may need help from readers given I can't understand how anyone can make such outlandish and unproven claims. Watching the show I couldn't help but think of the Brothers Grimm fairy tales.

I interviewed Pariante myself months ago, an interview that came to an abrupt end because it seemed we couldn't adequately address the first and most important issue. (See here)

The BBC show, Truth Or Scare, sets out to prove whether stories in the media are true versions of facts or if merely scary stories.

Pariante was batting for the side of the pill-pushers. It seems he was batting alone as there was no invite, to my knowledge, of any batter from the other side of the issue, one who could rebut Pariante's televised claims. It seems the BBC may want only one opinion regarding brain pellets and depression.

BBC host, Rippon, took everything Pariante said at face value and never once asked for evidence. (More on this later.) She kicked off the show by asking Pariante to explain depression in laypersons terms. Here's where the fun starts so hold on to your sides, folks, as they just might split!

"Brain cells are close but they are not physically connected so to communicate they need a chemical to go from one cell to another", claimed Pariante, adding, "People with depression need a stronger connection."

Pariante then showed Rippon an explanation of this by, um, well, by knocking on doors in a corridor. (See video below** where he appears around the 3 minutes, 12-second mark.)

Rippon then tells viewers, "For a more scientific explanation of how antidepressants work, Professor Pariante has recreated the effects of antidepressants in a culture lab." She adds, "His team chemically induce brain cells in test tubes to mirror the state of depression. Antidepressant medication is then added."

Pariante, speaking with Rippon, says, "If you induce depression in a dish, as you can see, new brain cells stop growing and you have much fewer cells compared to healthy conditions."

Pariante then claims that once an antidepressant is added the number of new brain cells "rises again".

I was just digesting the "depression in a dish" claim when Rippon claimed, "The Science certainly seems clear."

At this point, I had to dry my eyes and change my underpants. Biting the table leg didn't help with my state of uncontrollable laughter either.

Pariante later backs up his "Depression in a dish" claims by quoting the Cipriani study (back story here) - Pariante claims that Cipriani's study "clearly shows antidepressants improve the symptoms of depression."

When asked about the 'dark side' of antidepressants, Pariante said, "Antidepressants are no more or no less than any other medication, they are effective in most people, they are tolerated in most people, and in some people there are side effects, in a very small number of people there are severe side effects, but that's like all medication."

When asked about the dependency on antidepressants Pariante says, "There is no evidence that we are over prescribing antidepressants, yes more antidepressants are prescribed today than 10 years ago but, in fact, most people who need antidepressants are not receiving an antidepressant."

Yes, he really did say this, and he also neglected to share that a recent study found nearly 56% of people taking brain pellets suffer withdrawal effects and 1.8 million people are currently at risk of severe symptoms when they decide to come off these drugs. (1) If Pariante gets his wish, these figures will, no doubt, rise.

The show (skit) also features two former patients who have opinions about brain pellets. It's well worth watching if only to see the performance of Pariante and some of his bizarre claims and also how Angela Rippon seems almost smitten with him.

"The science certainly seems clear" wins a gold star for the BBC's most unscientific quote of the year. Rippon's quote was based on walking around a lab with a guy in a white coat knocking on doors and examining slides of depression produced in Petri dishes.

Approximately two hours after the show was aired on BBC, Pariante, rather bizarrely tweeted the following:

He really does himself no favours.

Here's the video.

** The video was downloaded directly from the Stress, Psychiatry and Immunology Lab - SPI Lab Facebook page. Any copyright issues should be taken up with the owner of this page, ironically, Carmine Pariante.

If you can't get the video to work, try here.


Bob Fiddaman


(1) Millions are warned over ‘severe’ side-effects while coming off anti-depressants with 56% of patients suffering withdrawal effects

Life-Saving Evidence

Last month the Q & A between myself and Carmine Pariante broke down. For those who don't know, Pariante is a professor of biological psychiatry at the Institute of Psychiatry at King's College, London, and consultant perinatal psychiatrist at the South London and Maudsley NHS Trust. He apparently has no sway in whatever the Royal College of Psychiatrists (RCP) say or do yet always seems to speak on their behalf.

Pariante was interviewed on BBC Radio 4 today after the subject of brain pellet withdrawal once again made the news in the New York Times. He was introduced as someone "from the Royal College" and proceeded to carefully and selectively bang the drum regarding the safety of brain pellets, so much so that even RCP were tweeting his quotes from the show (Fig1). Quite why Pariante is the College spokesperson is anyone's guess.

Check out the use of the word 'most'.

What irks me more than anything with the above tweet is that features a certain unproven claim in that brain pellets save lives. There will be many who claim that they do, I for one, find this ludicrous given that nobody can prove this. Sure, we get those people who claim, I would have killed myself if it wasn't for Prozac, Paxil etc but they cannot be 100% certain that they would have gone on to complete suicide, even if previously they had experienced suicidal thoughts.

This "life-saving" claim really has no substance and shouldn't be allowed, or at the very least should be preceded by, "they can induce suicide in people." One thing I've noticed about high profile shrinks such as Pariante is that they never ever talk about brain pellets inducing suicide, at least not on radio or TV shows, and certainly not in the mainstream media.

During my Q&A with Pariante last month he had this to say to me about brain pellet-induced deaths:

"I accept that it is possible that some patients might have died as a consequence of taking antidepressants, and my heart goes to them and to their families. But these, as tragic and sad as they are, are very rare events."

No mention of this in today's BBC show though.

Pariante was invited to speak today after the show had previously aired Daily Mail columnist, Sarah Vine, who spoke about her own troubles trying to withdraw from brain pellets. Adding their voices were Prof John Read and Patient safety advocate James Moore. Everything they said was pretty much undone with Pariante's 'life-saving claim'.

I'm getting sick to the back teeth of this outlandish claim and it beggars belief why nobody ever presses these key opinion leaders for evidence.

If, as both Pariante and Vine suggested, brain pellets save lives don't you think this would be a huge marketing advantage for the drug companies? I've read through every single leaflet in brain pellet boxes (SSRIs) not once do the drug companies claim that their product can save your life, so why does Pariante et al claim otherwise? If drug companies had evidence that their product was, in fact, a miracle pill, don't you think they would have used this as a major selling point?

What does Pariante know that we don't?

The radio show was, for me at least, disappointing. Why is nobody asking these shrinks how they can prescribe brain pellets when they have never seen the full safety data of the said brain pellets? Has journalism become so poor that the newer breed of writers have not grasped how to ask for supporting evidence when someone makes outlandish claims, or have they not grasped how to get to the root of a problem with decent questions?

If prescribers, such as Pariante do not have the full safety data then they know very little about withdrawal. They have no withdrawal data from drug companies either unless they care to trawl through countless pages of files released in drug company litigation. The evidence is there, they're just too lazy or pig-shit ignorant to read it.

Brain pellets do not save lives, to suggest that they do is a real kick in the teeth for those who have lost loved ones to brain pellet-induced suicide. It's a carefully crafted piece of PR spin, it's a trump card that they hold because (they claim) they have seen many patients saved by SSRIs.

Quite strange then, that these same shrinks have, for nearly 40 years not witnessed 'anyone in their clinical practice' suffering from severe brain pellet withdrawal. They see what they want to see, or what they are paid to see.

That not so nice acronym, N.I.C.E, was mentioned in the BBC show. They claim they are working on developing new guidelines for prescribers - they, just like every man and his dog, have never seen the full safety data that the drug companies hold, they, just like every man and his dog, are assuming that the evidence supports brain pellet use because they have published papers to prove this. What they don't tell you is the published papers are ghostwritten by the drug companies who pay key opinion leaders to add their names to these shoddy publications.

Here's a thought to ponder on. Why do you think drug companies don't say "THESE DRUGS WILL SAVE YOUR LIFE" on the insert in the box that accompanies brain pellets? Would it be something to do with making fraudulent claims?

Have you ever heard of anyone suing drug companies because the brain pellets didn't save their loved one's life? Of course not, because drug companies don't make this absurd claim.

Meantime, these brain pellets are responsible for endless misery, be it through the mourning of a loss of a loved one or watching a loved one's personality change as he/she tries to cope with the horrendous withdrawal effects these toxic chemicals cause.

I'm reminded of a quote from the late, great, Christopher Hitchens:

"What can be asserted without evidence can also be dismissed without evidence."

Pariante has, in the past, received funding from brain pellet manufacturers, Johnson & Johnson, GlaxoSmithKline, Lundbeck and Pfizer (source)

Bob Fiddaman

Q&A with Carmine Pariante

Carmine Pariante FRCPsych is a professor of biological psychiatry at the Institute of Psychiatry at King's College, London, and consultant perinatal psychiatrist at the South London and Maudsley NHS Trust. He received his PhD from the University of London and his MD from Gemelli University, Rome (Source Wikipedia)

Toward the end of last year, I became increasingly concerned about the behaviour of some of the psychiatrists on Twitter, many of whom were (and still are) belittling patients harmed by brain pellets.

I was hoping to discuss this in person with Carmine Pariante but due to logistics and time restraints, this never happened. Instead, we both agreed on a Q&A.

Sadly, for me at least, communication between us (via email) came to an abrupt end.

My reasons for ceasing communication can be seen in the thread of emails below. I will leave it to readers of this blog to decide whether or not I made the correct decision in ending the conversation.

Carmine wanted the last word but because he opened the questioning and was given ample opportunity to express himself, I have denied this request. I did inform him, however, that he can leave a comment on here if he wishes or publish this Q&A with his additional comment on his own website.

As a side note, when I eventually retire from this often dark and depressing arena, I hope some of the newer advocates, of which there are plenty, take up the issue of clinical trial data that is withheld and ghostwritten literature. It's the single most important issue regarding brain pellets, any other debate is irrelevant until this issue has been tackled and resolved. We need to speak about this because it has been sidestepped for far too long.

Bob Fiddaman

--

Q&A with Carmine Pariante

** Some grammatical errors have been rectified

Pariante
All medications have profound side effects: antibiotics, painkillers, or drugs for cardiovascular disorders. People suffer severe and life-threatening, unpredictable adverse effects taking many common medications. Do you think that antidepressants are simply like any other drugs: helpful and safe for a lot of people; ineffective, unsafe and intolerable in an important minority of patients; and tragically able to cause severe, unpredictable, life-threatening adverse effects in a small minority of patients? If not, how are they different from other medications?

Fiddaman
First off, I'm happy you raised this issue as it seems to be the defence of many psychiatrists when the efficacy and dangerous issues of antidepressants are raised.

Yes, all medicines carry risks of adverse events but, in the main, those other medicines target specific areas or diseases. I wouldn't really class suicidality as an "adverse event", to do so plays it down and it becomes lumped together with headaches, nausea, dizziness etc, as do the issues of withdrawal, birth defects, sexual dysfunction.

Antidepressants can induce suicidal thinking and, in some cases, completion of suicide, I hope we can agree on that?

To take a gun and pull a trigger, to tie a noose and wrap it around your neck, to take a knife and stab yourself through the heart, to jump from a bridge to your death, all carry horrifying images but this is the stark reality of it for some people. These should never be classed merely as 'adverse events' - these are people, both young and old, who, because of antidepressants, killed themselves because of an inner restlessness (akathisia) caused by these drugs. Nobody in authority, except for a small handful, seems to want to address this issue, opting instead to deflect by wishing to talk about the adverse events of 'other drugs.' I have never seen any discussion by yourself or RCP that tackles this issue. It's almost as if its a taboo subject for you or something you, and your peers, are ignorant of?

Do I think antidepressants are safe and effective for a lot of people and not safe for a minority? - No. I think both prescriber and patient believe they are safe and effective when in actual fact this may just be the placebo effect at work. If, as you suggest, they do help people then I'd like to know how? Aspirin, for example, helps by targeting the pain and swelling - What do antidepressants target, why do people seem to do well on them (group A) when others don't (Group B)? What is it that group A has that group B doesn't? Also, one should not use the term 'safe and effective' when one knows that they cannot clearly state this because of the suicide link. Isn't it more important to say, these drugs could induce suicide but are safe and effective for others? What's more important to you given that you, or anyone else for that matter, have never seen the raw data that drug companies seem reluctant to release?

I think depression is over-diagnosed and, as a result, antidepressants are over-prescribed. If you see today's figures as a modern-day clinical trial then the results will, of course, favour their safety and efficacy - the more taking them actually masks the problems people face whilst on them, be it suicidal thoughts or withdrawal problems. If, for example, two in ten people suffer at the hands of antidepressants then prescribing more would eventually bring this figure down. In any event, the apparent safety and efficacy of these group of drugs are based on 8 to 12-week clinical trials. In the real world, people are taking them for much longer. In the real world, people aren't 'severely' depressed, as they are in clinical trials, they may just be going through a bad stage of their life because they may need help due to circumstances in their environment. A pill cannot magically pay bills, fix broken marriages, or help a child pass exams but, for some prescribers, this seems to be the reason why they prescribe them.

I feel the question you asked here is irrelevant when the focus should not be 'other meds cause problems' - the focus should be, 'we acknowledge that these drugs can make people self-harm, have suicidal thoughts or, at worst, kill themselves and/or others.' This is what needs to be addressed, along with a whole other multitude of dangerous adverse events associated with these drugs. Talking about it and referencing 'other drugs have adverse events' is shying away and playing down the risks.

If an airline company had a fleet of ten 737's and one of those planes was unsafe to fly in, I doubt very much if the airline CEO would say 'one of our planes, we don't know which one, is unsafe to fly in but the other 9 are safe'.

In the case of antidepressants, prescribers are, in essence, playing Russian Roulette when they prescribe them. It's an unfair advantage prescribers have as they never take turns in pulling the trigger.

Pariante
I should probably start by stating one thing on which I am sure you and I both agree. I am, like you (and many others) very concerned that antidepressants (especially the selective serotonin reuptake inhibitors) may have more frequent negative effects than originally thought, in terms of reactions to both taking the antidepressants and to stopping them. The reasons behind this slow building of awareness within the medical and psychiatry communities are multiple.

Certainly, there has been a lack of transparency on such data from clinical trials conducted by pharmaceutical companies in the 90’s and early 2000’s , before current guideline and practice changed.

But there is also an objective difficulty, at times, to distinguish between these described negative effects of antidepressants (for example, the increased anxiety, physical agitation and suicidal ideation, which has been typically described in young patients) and the increased anxiety, physical agitation and suicidal ideation that are common symptoms during a depressive illness.

Withdrawal symptoms at the time of stopping these drugs (especially if stopped abruptly) have been well described and are recognizable, but distinguishing symptoms that develop weeks or months after stopping antidepressants from the relapse of the depressive illness  (which, in most patients, has a continuous, peak-and-trough natural course), is very difficult.

Of course, we do need to develop better clinical and research understanding of these negative effects.

There is one thing on which we obviously disagree: you believe that antidepressants are not helpful at all, to any patients, and thus, for you, any negative effect is an unjustified burden. I do not agree with you on this.

Most of the medical and psychiatric communities, and hundreds of studies conducted so far, clearly show that antidepressants do work in improving the core symptoms of depression – especially, the pervasive sadness and lack of hope and motivation that so many patients describe as unbearable, in their account of this serious condition.

We shall not forget that most people who commit suicide suffer from depression and that antidepressants, when you study a large population of patients taking antidepressants, do reduce suicides rates in adults and older people (although in young people, as I have said before, it might be different).

You say that antidepressants do not work, that they have only a “placebo effect” and thus that they are like “dummy” pills. But this is simply not correct: hundreds of studies have been conducted comparing antidepressants to a placebo (“dummy pills”), showing that antidepressants are better than placebo in improving the aforementioned core symptoms of depression – the pervasive sadness and lack of hope and motivation.

Moreover, there have been many studies who have examined other drugs that affect the brain (for example, opioids and benzodiazepines), which in theory should have a very strong placebo effect, yet they lack this specific antidepressant effect of improving the pervasive sadness and lack of hope and motivation.

Of course, you are right that antidepressants are not safe and effective for everybody, for 100% of patients who take them. In fact, only 50% of patients respond very well to an antidepressant, and probably only around 75% are somehow helped. And yes, some people suffer from severe negative effects, sometimes life-threatening.

I accept that it is possible that some patients might have died as a consequence of taking antidepressants, and my heart goes to them and to their families. But these, as tragic and sad as they are, are very rare events.

Many more patients do not die, do not take their own life, because they are on antidepressants.  Not only the scientific and clinical studies demonstrate this, but also the testimony of many such patients who have gone public with their positive, life-saving experience with antidepressants.

In response to one of your comments, I would like to stress that this is the same exact situation that afflicts all branches of medicine. People suffer from negative effects of medications, or even die, because they take drugs for pain, hypertension, infection, cardiac problems: all drugs have the potential to induce negative (and sometimes life-threatening) effects. Your example of the airline company applies to all of medicine.

Yet we take medications because we know that in general, we are more likely to benefit than to suffer from them; that many more people benefit from them than suffer from their negative consequences.

It is the same for antidepressants – although I acknowledge that, if you think that there is no benefit from taking antidepressants, you may only see the burden. But clinical and research evidence (and patients’ accounts) tell us that these drugs do help patients.

Of course, you are right that there is a risk that antidepressants may be prescribed too much, to people who do not need them – and, for these people, the negative effects would outweigh the benefits.

However, all the clinical guidelines are strongly preventing this from happening. Clinicians and psychiatrists are reminded over and over again that antidepressants should only be prescribed to people with ‘clinically-significant depression’, and not to people with a ‘bad stage in their life’, to use your words.

‘Clinically-significant depression’ means being so sad and hopeless and tired that we cannot go to work, or socialize with friends, for weeks and months; that our work and family life suffer; that we feel that life is no longer worth living; that we think about taking our own life, or that we plan to do so. These are the people that should be prescribed antidepressants.

Yes, more antidepressants are prescribed today than 10 years ago, but this may also mean that more people are seeking help because the stigma against depression has reduced. It does not need to be a bad thing if these drugs are taken only by the people who really need them.

Where do we go from here?

Personally, I am grateful to the ‘harmed’ patients community who, through social media and advocacy, has raised awareness of the fact that antidepressants may have more serious negative effects than we originally thought.

The question now is: how do we help these patients, and help the patients who may be suffering from such negative effects in the future, while also at the same time protecting the patients who are benefiting from taking antidepressants, and will continue to do so in the future?

How do we bring my community and your community together, since we both want the same things: help people who suffer from depression?

Fiddaman
You and I will have to agree to disagree on the points you raise, Carmine, otherwise, we will get bogged down in missing the glaringly obvious. Before I answer your question, regarding the prescribing community and the prescribed harm community moving forward, I'd like for you to answer the following...

Do you think withholding clinical trial data is appropriate?

Do you think ghostwriting is acceptable?

Pariante
**Note**
Carmine added a personal note to this email suggesting that I was being discourteous. I have not added the personal note but it can be provided should the need arise

Let me first clarify that I can only express an opinion as a scientist. I have never been involved in conducting or participating to, a commercial clinical trial, or a trial for regulatory purposes, nor I have ever worked work for a regulatory agency; so I am not familiar in details with the process required by the FDA or equivalent regulatory bodies.

Having said that, as a scientist, let me say again that I believe that, in general, it is not appropriate to withhold any type of clinical data, and, in fact, any type of data.

As I have mentioned before, pre-registration of clinical trials and of analyses has changed the culture both for scientists and for pharmaceutical companies. Analyses of both efficacy (whether a drug work or not) and safety (what are the side effects)  should now be routinely pre-registered as part of the process, and the data presented when the study has been completed.

Again, as I have said before, for releasing individual-patients data there are additional issues such as confidentiality of patients, but there are procedures in place to do this, when ethically possible, and there are different types of processes based on whether the data are released to a public database or to an independent group of scientists for re-analyses.

I repeat again that clinical trial data – and in fact, any data – should never be withdrawn just because the researchers do not like the results!

Regarding ghostwriting, again as a scientist, to me being an author of a scientific paper requires full knowledge of the data. For a clinical trial, these include efficacy, safety, and other clinical, biological or psychological measures that are relevant to the paper.  In addition to the knowledge of the data, an author would need to be fully aware of the analyses and their implications. If you define as ‘ghostwriting’ the practice of appearing as an author on a scientific paper without such full knowledge, then let me say again that I am always against it.

Fiddaman
Having re-read your note to me, I'm surprised at your hurt tone. I and lots of others have been damaged by treatment. This is not something to handle lightly by saying something along the lines of, "Now, don't be angry." I am angry with the system. I'm also now concerned. I had no idea whether you do clinical research or not. The issue is your practice as a clinician and that of your colleagues. I fail to see how any of you can safely treat me or those I love if you have no access to the data and if the entire literature on meds is ghostwritten.

The extreme example of this at present is the ever-increasing use of antidepressants for teens where up to 100,000 children are on them. Yet there is not one positive trial of these drugs for children who are depressed, not one. Even the Prozac trials, that got Prozac licensed, are negative. Ditto for the paroxetine trials for children when the FDA issued an approvable letter for it.

Some doctors won't be too concerned by the sufferings of their patients (out of sight, out of mind). But even for you, the worry must be that patients in general, or the managements who employ doctors, are eventually going to wonder if you're worth having. Unless someone like you gets to grips with these issues, which you're better placed to do than I, you are at risk if/when things go horribly wrong. If there is no place in the system for recognising that treatment can kill or maim, you, the prescriber, are likely to end up in the firing line. Despite what you may think about my stance on antidepressants, I don't want this to happen to you or your colleagues.

How can any prescriber at the moment relay informed consent to any of their patients? From my point of view, I'd love some sense that you were bothered by this issue, Carmine, because then I'd think we might make some progress.

As I stated, I'm surprised at your hurt tone. Yet I do find it refreshing to see a doctor who feels and shares emotion. I say this given that many doctors cannot recognize, or refuse to acknowledge, the "hurt" they cause others when blindly prescribing. Blind prescribing is common given that doctors give people antidepressants without knowing the risks because doctors, yourself included, haven't seen the data.

Pariante
Why do you say I am not bothered by the data not being available - I keep saying that I am! I am also saying that the situation is improving with new rules and regulation

I have not said “don’t be angry” at the situation or the system - I said don’t be angry at me, Carmine, who is talking to you

Doctors in all specialities prescribe based on guideline; guidelines are written based on independent review of the evidence by experts, and the evidence includes safety and efficacy data. It is simply not true that all the l literature on meds is ghostwritten - and in any case, I condemn ghostwriting and I am confident that data transparency is much more advanced now.

So I am really not sure I understand where you and I disagree.

Fiddaman
This is a very important subject we are talking about please try and stop taking things personally. I am just asking questions that I feel many may like to see your answers.

Close to all the literature on on-patent drugs is ghostwritten. Nice Guidelines, where they refer to drugs, are based on ghostwritten literature and they have no access to the data. Being independent is meaningless if the conclusions are predetermined by the ghostwriting.

Where is the evidence to show anything is better?

Pariante
I disagree that the situation is, today, as grim as you depict it, although I agree that this has been an important problem in the past.

First of all, all the drugs that you and the community of harmed patients are concerned about (such as SSRIs) have been off patent for many years, often decades. The data have been released in the last few years and in fact, this is the reason why we do know so much more now about their adverse effects, as the many scientific papers on antidepressant-induced suicidal ideation or severe withdrawal symptoms testify.

Second, for the (very few) newer drugs still on patent or in development, there are clear rules and regulations for all trials to be registered before the results are known, and for all data (efficacy, safety, factors influencing response) to be published when the study has been completed.

Ghostwriting is unequivocally criticized or banned, and rightly so, by scientific journals and medical organisations.

The NICE or other experts panels have access to published scientific data which today is presented with excellent ethical and professional standard – because of the new rules and regulations, and also because of a change in culture about data transparency across scientists, pharmaceutical companies and regulatory bodies.

Has this been a problem in past? Yes, of course. But I think that the present is better and the future will be even better.

Fiddaman
You casually claim, “the present is better and the future will be even better.” yet provide no evidence to support your claim. You don't know whether the drugs you prescribe are safe because you've never seen the clinical trial data. NICE doesn't know either as they have never seen the drug company data. It is deeply disturbing that none of these facts appears to bother you and fellow prescribers.

Patient safety cannot be a chief concern and the Hippocratic Oath cannot be honoured when ghostwriting and cherry-picked data is an accepted, routine practice. Despite your claims, things have actually gotten worse, not better. Consider:

• The recent approval of esketamine, a new mind-altering drug marketed to treat depression, is based on some of the shoddiest trials ever conducted.
• Current antidepressant trials in children are now being conducted in Colombia, the Russian Federation, Ukraine, American foster homes and correctional facilities (Lundbeck's vortioxetine trials). Everyone knows the reasons why and none are for the benefit of product consumers.

You should be more concerned about the data you don't see, rather than what you do see. I asked a critical question about clinical trial data and ghostwriting because this is the foundation upon which fraudulent and harmful psychiatric prescribing is built. Whether it be delusion or deceit, most psychiatrists cannot or will not acknowledge that they are unsure about drug safety. To do so would expose psychiatry's cracked foundation and bring the walls tumbling down.

I have been a drug safety advocate for more than a decade. My readers are intelligent and I respect their time. Your limp-wristed response is offensive. I must conclude that continuing our Q&A is unfortunately of little or no benefit to readers.

Thank you for your time. I will post our brief Q&A on my blog as previously promised. You are free to do the same.

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Is This The World We Created?

You know that every day a helpless child is born

Who needs some loving care inside a happy home

Somewhere a wealthy man is sitting on his throne

Waiting for life to go by.

Is this the world we created?

We made it on our own.

Is this the world we devastated

Right to the bone?

If there's a God in the sky looking down,

What can he think of what we've done

To the world that He created?

'Is This The World We Created?'

Mercury, May

I'm dumbfounded and disappointed at recent events in the business of psychiatry. Why is the blindingly obvious ignored or downplayed by people in positions of power-positions that could be used to save human suffering and lives?

This isn't intended to target psychiatrist and Royal College of Psychiatrists spokesperson, Carmine Pariante. I've been pleasantly surprised that in recent weeks Pariante has been open for civil discussion shown on Twitter.He appears to understand the need for informed consent and has even suggested that drug safety advocates work alongside psychiatry. I have to give him a hearty round of applause for not taking the stance many psychiatrists take on Twitter. That is, they cry "pill-shaming" when a victim of "antidepressant" ADRs speaks out. Others simply block patient advocates who share research and experiences via Twitter.  (See ~ Who's Hiding the Clinical Trial Benefits of Antidepressants?)

However, what I do take umbrage with is Pariante's recent stance on an article I sent to him via his Twitter feed. The article, from journalist, Kirstie Brewer, was featured on the BBC website and entitled, 'I was suicidal - the NHS didn't know what to do with me'.

It's important to click on the link (here) to review this article as it is the same link I sent to Pariante asking if he thought it was possibly drug related? (1)

(1)

Notice my use of the word 'possibly' in the tweet. I wasn't categorically stating that the young woman featured in the article had attempted suicide because of the meds she was prescribed since age 13. (After re-reading the article, I learned that she was 13 and not 11.) I was just opening a dialogue about ADRs and causation. However, in this instance, it seemed Pariante didn't want to play ball with me. (2) (3) (4)

(2)

(3)

(4)

I was dumbfounded that Pariante wouldn't even entertain the possibility that the young woman featured in the article could have been suffering from psychosis as a result of the drugs she had been prescribed from a young age. Instead, he shifted the conversation suggesting that neither he or I knew any clinical details regarding this young woman. That may be so but here's some selective text taken from the article that begs the question, "What is Pariante failing to see here?" The relevant points are in bold font.

It was the ninth time in the space of 10 days that Sherry Denness had tried to kill herself. "It felt like checkmate - there were no open doors or other ways for my life to turn, I just wanted to die," she says.

Only just 18, Sherry has been diagnosed with a number of mental health conditions, including borderline personality disorder (BPD) and attention deficit hyperactivity disorder (ADHD).

On seven of her nine suicide attempts, which took place in November last year, the teenager had landed in A&E, been patched up and deemed well enough to be sent home with no further help. Another time she'd taken all of her prescribed medication in one go and ended up in critical care for two days. 

"I was psychotic and I was hearing Kieran in my head telling me I need to leave the house." Kieran is one of the voices Sherry hears - the worst one, she says.

She was 11 when she was first assessed by the Child and Adolescent Mental Health Services (Camhs.) Eventually, at 13, she was given treatment for ADHD.

"I have been to A&E a lot of times for self-harm and suicide attempts", Sherry Says.

With all these references in plain sight, I find it remarkable and quite telling that Pariante refuses to accept the 'possibility' that her deterioration might be drug-related.

Let's take a look at a research study (SSRI - Induced Extrapyramidal Side-Effects And Akathisia Implications for Treatment) from almost 20 years ago. It was authored by Roger Lane and featured in J Psychopharmacol.1998;12(2):192-214.review. 

A note of interest here: Between 1992 - 2001 Roger Lane was the Senior Medical Director at Pfizer. Today he is the Vice President, Clinical Development Neurology for Ionis Pharmaceuticals.

Lane wrote:

“It has been suggested that SSRI-induced akathisia may be associated with the emergence of ego-dystonic suicidality (Lipinski et al., 1989: Rothschild and Locke, 1991: Hamilton and Opler, 1992). The most consistent factor implicated in these anecdotal accounts of rare adverse reactions involving suicidal ideation and behavior during fluoxetine treatment was the development of akathisia with agitation, restlessness and dysphoria (Power and Cowen, 1992).”

“It may be less of a question of patients experiencing fluoxetine-induced suicidal ideation, than patients feeling that ‘death is a welcome result’ when the acutely discomforting symptoms of akathisia are experienced on top of already distressing disorders."

During the 20 years in which this word, 'Akathisia' was mentioned, there have been many deaths by suicide whilst patients have been on prescription drugs. On one side of the fence, we have psychiatrists who claim that the SSRI/akathisia link is not proven despite the research and causation admission noted above. On the other side, we have loved ones whose family members, including children and young adults, have had psychotic reactions to SSRIs that precipitated unimaginably violent deaths.

When faced with possibilities of causation, Pariante should be stepping up to the plate and looking into SSRI-induced psychosis. He should, at the very least, acknowledge the possibility that these drugs can and do precipitate psychosis and death for unsuspecting ADR victims.

Last year the subject of drug-induced akathisia was highlighted in Chicago in the case of Dolin Vs GSK. The transcripts and trial exhibits have now been made public for more than a year (See the right-hand side of this blog). During the trial, it was learned that the victim, Stewart Dolin, leaped to his death because he was suffering from drug-induced akathisia. After a 6-week long trial, the jury found for the plaintiff, Stewart's wife, Wendy. They carefully reached this verdict after hearing 6 weeks of evidence presented by both Dolin and GSK.

Another active Twitter psychiatrist is Duncan Double. Double disputes that SSRIs can induce akathisia and after sending him a link to the Dolin transcripts and trial exhibits he had this to say:

"Legal judgment is not necessarily the same as scientific fact."

Upon informing him, the jury sat through six weeks of evidence Double remarkably replied:

"One doesn’t know which bit of evidence the jury based its decision on."

I told him good jury's don't base a decision on one bit of evidence, they base it on all.

Hours later, Double tweeted:

Nice, and kind of big of the man to state that he was wrong. This, however, didn't last for long as later in the day he bizarrely stated, "I’d still like to debate whether I might  be right."

So, just two instances of psychiatry at work here.

I'm not definitively claiming that the young woman featured in the BBC news article tried to take her life because the "drugs made her do it." There may be other mitigating circumstances. You see, I'm open to other possibilities whereas, it appears, Pariante and Double are not, despite Pfizer's own scientist stating, "death is a welcome result’ when the acutely discomforting symptoms of akathisia are experienced."

I wrote a book back in 2011 called, "The Evidence, However, is Clear." It would appear I was wrong because, for some, the evidence is invisible. Yet sometimes we find ADR evidence that was unwittingly documented by people who are no longer visible but speak from the dead. I'm talking about a diary kept by a young woman who, just like the young woman featured in the BBC article, was harmed by a medical field whose diagnoses are largely based on guesswork.

Natalie Gehrki was just a year older than the woman featured in the BBC article noted above. There are striking similarities between both, and we can learn much from the experiences of each young woman. Natalie was prescribed the SSRI, Zoloft, NOT for "depression." She never received any specific diagnosis at the time of her death. Doctors who are unfamiliar with akathisia and serotonin toxicity often don't take the correct steps to stop it. Natalie died less than two days after her doctor increased Zoloft-over the phone to the maximum legal dose allowable, 200mgs.

There are many more Natalie's out there, some dead and some still alive. We owe it to them to warn of akathisia. If two publically renowned psychiatrists won't discuss SSRI-induced akathisia and the necessary steps to prevent akathisia & SSRI deaths, we must rely on teenagers with first-person insight and no conflicts of interest.

Dr. Oz's Fantasy World

On a related note, last week Dr. Oz ran a show that was supposed to be a serious examination of the connection between drugs and violence. It was shockingly bias and omitted critical information. Natalie's mom, Kristina, was one of many viewers who wrote to the Dr. Oz producer. Her letter is beneath the video.

Here's Natalie.

And here's Natalie's mother, Kristina, writing to the producer of the Dr. Oz show.

Dear Ms. Varney,

I'm writing to express my shock and dismay regarding Dr. Oz's recent show about drugs & violence. As a trained journalist, I expected a variety of experts would discuss reliable data, relevant pharma documents, legal cases and consumers' reported ADR experiences. Instead, I quickly learned your panel of three  "experts" all had ethical &/or financial conflicts of interest. While Dr. Oz casually and promptly glossed over these conflicts, declaring conflicts of interest does not remove these conflicts of interest.

I waited in vain to hear from experts with opposing viewpoints to the pharma-connected panel. But few of these experts were featured and those that were received minimal air time. This includes Wendy Dolin, founder of MISSD. When you flashed on the screen the 3 million settlement a jury awarded for her husband's prescribed Paxil death, it was misleading and offensive. Not only has Ms. Dolin not received a penny from GSK after the jury's wrongful death award, it was beyond the pale to flash a cash amount on the screen. Such sensationalized antics are akin to a sordid game-show gimmick.

Given your producers felt this financial info was necessary for viewers to know, I pose the question: Why didn't you similarly treat your panel in the same manner? When Dr. Oz was glossing over conflicts of interest; you could have visually informed your viewers of the amount of money each panel member has already taken from pharma. Your slanted, one-sided journalism has been the topic of much negative discussion on many social media feeds. But even if the public didn't notice the appalling bias, as a producer you should have recognized such before airing.

Lastly, aside from a professional and academic background in journalism and crisis communication, I am the mother of a 19-year-old daughter whose death was precipitated by another SSRI (Zoloft). Medical experts determined Natalie was suffering from prescribed akathisia and serotonin toxicity prior to her death. After death blood tests showed she could not efficiently metabolize SSRI toxins. Her prescribed tragedy is found at https://rxisk.org/kidnapped-natalies-story/ and https://www.youtube.com/watch?v=1haYwZGcSRY 

Your irresponsible journalism was a disservice to public health and safety. Undoubtedly, it will cause avoidable suffering and more ADR-related deaths. Nothing can change the damage caused by the show you produced. Nevertheless, you have an ethical obligation to apologize and air a follow-on show that transparently shares unbiased accurate data in a fair and balanced manner.

Regards,
Kristina Gehrki

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Bob Fiddaman