One
effective intervention in autism, particularly to reduce stereotypy, is N-acetylcysteine (NAC). Here NAC is being used as an anti-oxidant in
its own right and as a precursor to the body’s own main anti-oxidant, called
GSH. Classic autism is associated with
oxidative stress and so NAC should be beneficial.
In much of
Europe, NAC is seen primarily as a pharmaceutical, in North America, and much of
the rest of the world, NAC is primarily just another supplement.
As a drug,
it is mainly used as a so-called mucolytic
agent, and as such is used as a cough medicine, because it
breaks down mucus and liquefies it, making it easier to cough up. It is frequently prescribed by doctors for
children, but only in some parts of the world.
The problem with NAC, and all supplements, is quality
control. There is pressure to drive down
prices and so quality will vary. NAC is
not particularly stable (it is labile) and so it tends to break down and
release some foul smelling compounds.
For those who remember chemistry from school, the chemical formula is C5H9NO3S
and the following chemical structure:
The smell of rotten eggs is associated with H2S,
hydrogen sulphide/sulfide. The ‘S’ in
NAC is sulphur/sulfur and so when it breaks down or oxidizes you get a nasty
smell.
The question is how much of a smell is normal and how
much means your cheap NAC capsule has spoiled to the point of being worthless?
There is plenty of online discussion on this subject
among regular users of NAC. As usual,
much is nonsense; some people are even saying that NAC has to stink and that it is a
sign that it is good.
When it is freshly produced, there should be very little
smell. When you open the pharmaceutical
NAC from its blister pack there is no smell whatsoever.
Cheap NAC
Since you need large amounts of NAC for treating autism,
I found a brand of the cheap NAC capsules, but I always open the individual
capsules and mix them in juice. I never
had any stinky bad egg smell until recently.
Now as soon as I open the jar, let alone the capsule, there is a potent
smell. Try a jar from a different batch,
same smell. More to the point, I have
noticed small signs of stereotypy when Monty, aged 10 with ASD, goes for a
swim. He is swimming in the water and
then starts wiggling his fingers and looking at them.
So I have decided to switch to the pharmaceutical NAC,
which where we live is called Fluimucil and is made in Switzerland. You buy it in the pharmacy over the counter, but
without a prescription. The cheap NAC
does not say where it is made, or even have a use by date. I suspect that different batches are made by totally
different producers, whichever offers the lowest price.
The well-known expensive brand of NAC sold in the US is actually
produced in Europe, if it turns out to be Swiss, we can probably guess who is
making it for them.
It is clear that when the cheap NAC is very fresh, it works
fine, but I want a product that functions as it should, 100% of the time.
I will see if the small re-emerging signs of stereotypy
disappear with the Swiss NAC.
Anyone
with a serious interest in autism should also be aware of PANDAS (Pediatric Autoimmune Neuropsychiatric Disorders Associated with Streptococcal
Infections) and PANS (Pediatric
Acute-onset Neuropsychiatric Syndrome). These are two syndromes which have acute
onset of symptoms very similar to some of those found in autism. It is claimed to affect 1 in every 200
children in the US.
The
good news is that a very thorough and dedicated doctor called Susan Swedo has worked
logically through from starting to identify the syndrome, all the way through
to treating it. Good job Susan.
Though
she insists that PANDAS and PANS are distinct from autism, one can only wonder
how many other distinct, but yet to be identified, syndromes exist that also
present with autism-like symptoms.
Thanks
to the efforts of Dr Swedo and the US NIMH (National Institute of Mental Health), these two conditions have been remarkably well investigated, in a very
short period of time. It shows what
medical science can achieve when the right people are in charge. It is odd that such effective clinical attention
has not been focused on autism itself.
Here
is a very recent presentation given by Dr Swedo, which really covers all the
important aspects of both PANS and PANDAS.For those with a serious interest, have a look though this post and then
watch the presentation, to get the most from it.
One
of the reasons I was so impressed by how PANDAS has been addressed, as opposed
to the much more common autism, is the before and after data.For example, many people talk about
regressive autism, but nobody quantifies from what, to what.Some children went from a spoken vocabulary
of 10 words to 2 words, while others went from 500 words to zero; there is a
profound (and relevant) difference.
In
the case of PANS and PANDAS we have the before and after artwork from the
affected kids. As usual, a picture is
worth a thousand words.
I
have no great panda pictures, but Monty aged 10 with ASD, brought back his
artwork from school last week and pride of place goes to his picture of two
penguins. We were all more than a little
taken aback to see it. Did he really
draw this? Unassisted? It looks much
more like the work of his big brother.
Even his assistant was surprised and confirmed that this was the result
of his work in the art room for a double lesson. I never expected to be displaying Monty’s
artwork to the world.
Later
in this post you will see the before and after PANDAS artwork.
PANDAS and PANS
When
I first came across a condition known as PANDAS or PANS, I did not take that
much notice; with such a name I assumed it was nonsense. Researchers should give a serious syndrome a
serious name/acronym.
I
imagine that with the ever widening of the diagnosis of autism, some people
with PANDAS (Pediatric
Autoimmune Neuropsychiatric Disorders Associated with Streptococcal
Infections) /PANS (Pediatric
Acute-onset Neuropsychiatric Syndrome) have been misdiagnosed as
autistic and vice versa.
When
you look at the symptoms and apparent cause of PANDAS/PANS you may wonder how
many other similar conditions exist within the myriad of conditions leading to
autism.
The
shocking regression in cognitive function (illustrated by children’s drawings
further down the page) produced by this condition and the fact that it can be
reversed, should really be carefully evaluated in comparison to regressive
autism.
It
would be appear that all of this is caused by an immune system gone
“haywire”. I wonder how many other
immune dysfunctions leading to regression and odd behaviours will be identified
in future decades.
The
treatment for all these current, and future, conditions are likely to revolve
around immunomodulatory therapy, ranging from very cheap steroids (prednisone)
to the very expensive, like IVIG (Intravenous immunoglobulin)
If
you have a case of regressive autism and the expert says it does not fit the
definition of PANDAS/PANS, he might think the case is closed.Perhaps it should not be.
I
suggest that immune over-activation is involved in both groups of autism:-
Early onset
autism
In these cases the immune activation is secondary;
when it occurs the existing autism just gets much worse. In some cases these flare-ups are evidently caused
by food allergies/intolerance or pollen allergies.
Regressive
Autism
I think that in mild cases, some autism may be solely
an over-activation of the immune system, without any of the channelopathies and
other dysfunctions common in classic autism.
I would put PANS/PANDAS is this category. I suggest that many other cases of regressive
autism could be traced back to allergies and food intolerance, which triggered
an immune over-response.
It does seem that many regressions followed a viral
infection, and of course, many people believe their regression was triggered by
vaccines. I expect in most cases the
vaccine is just a scapegoat, but I very much doubt it is in every case.
I do not expect there will be any research in this
area, because the results would inevitably be misinterpreted by the
public. What a pity.
If
we better understood what events could radically disrupt brain function, we
might be able to better understand how to treat the resulting neuropsychiatric phenomena, known as regressive autism, PANDAS, PANS and other, yet to be
invented, acronyms.
A serious condition with some serious
followers
Many
people’s knowledge of autism seems to come from sound bites from scientific
luminaries like Oprah, Jenny McCarthy and
even Donald Trump. Somewhat remarkably,
the PANS doctors are actually a very serious bunch, under the umbrella of the
International OCD Foundation (and the NIMH). This
foundation is a serious organisation with a scientific advisory board loaded
with people from top US Medical Schools.
Not only have they concisely
explained the symptoms, but they have also found therapies; albeit, they do not
really know why they work.
There is also a very serious parent
run organisation called PANDAS Network.
About
PANDAS and PANS
In the early 1990s, 50 years after
Kanner noticed autism, researchers in the US noticed what they thought was an
odd acute-onset type of Obsessive Compulsive Disorder (OCD). At first it was thought
that only streptococcal infections and Scarlet fever
triggered this abrupt regression in the child’s behaviour and cognitive
performance. The first name they came up
with was PANDAS, (Pediatric Autoimmune Neuropsychiatric Disorders Associated with Streptococcal
Infections); when reports came in that many other infections caused acute
regression the name got changed to PANS (Pediatric Acute-onset Neuropsychiatric Syndrome).
It
is pretty clear to me that some people diagnosed with regressive autism
actually have PANS. I have from two
sources a list of symptoms:-
International
OCD Foundation
Acute sudden
onset of OCD
Challenges
with eating, and at the extreme end, anorexia
Sensory
issues such as sensitivity to clothes, sound, and light
Handwriting
noticeably deteriorates
Urinary
frequency or bedwetting
Small
motor skills deteriorate - a craft project from yesterday is now
impossible to complete (see images below)
Tics
Inattentive,
distractible, unable to focus and has difficulties with memory
Overnight
onset of anxiety or panic attacks over things that were no big deal a few
days ago, such as thunderstorms or bugs
Suddenly
unable to separate from their caregiver, or to sleep alone
Screaming
for hours on end
Fear of
germs and other more traditional-looking OCD symptoms
US National Institute of Mental
Health
Severe
separation anxiety (e.g., child can't leave parent's side or needs to
sleep on floor next to parent's bed, etc.)
Generalized
anxiety. which may progress to episodes of panic and a
"terror-stricken look"
Motoric
hyperactivity, abnormal movements, and a sense of restlessness
Sensory
abnormalities, including hyper-sensitivity to light or sounds, distortions
of visual perceptions, and occasionally, visual or auditory hallucinations
Concentration
difficulties, and loss of academic abilities, particularly in math and
visual-spatial areas
Increased
urinary frequency and a new onset of bed-wetting
Irritability
(sometimes with aggression) and emotional liability. Abrupt onset of
depression can also occur, with thoughts about suicide.
Developmental
regression, including temper tantrums, "baby talk" and
handwriting deterioration (also related to motor symptoms)
In
case you want to see what they mean by regression, look at these pictures drawn
by a child with PANDAS before and after treatment. Panel A is before and Panel B is after. Source International
OCD Foundation
Treatment
Compared to Autism, a very refreshing
approach is taken to treating PANS.
The treatments include:-
·Treatment with antibiotics
to eradicate the infection, if it is still present.
In spite of what your doctor might tell you,
if your child has regressive autism, you would be well advised to check and
re-check that he/she does not have PANS or a (yet to be identified) variant thereof.
The immune-based therapies that ultimately
are proved to be successful in PANS are highly likely to be helpful in treating
the kind of autism in which the immune system remains in a state of
over-activation. Also the
immune-therapies being trialled for autism, if successful, might very likely be
helpful alternative therapies for PANS; the therapy I have in mind is TSO.
Classic early-onset autism, as researched in
post-mortem studies at the Courchesne lab and elsewhere, is associated with
physical brain abnormalities, that should be irreversible. It would seem that PANS is something entirely
different and should be treatable and potentially fully recoverable.
For those of you unaware of Courchesne, here
is a short video; he is quoted by many of the leading autism researchers, so I
hope he has got things right.
Where does regressive autism fit in? I really doubt that all those people with
regressive autism have the physical brain abnormalities of classic autism. Research has shown that regressive autism has
even higher bio-markers of neuroinflammation than classic autism. Perhaps regressive autism is
neuroinflammation, without physical brain abnormalities?
Just as PANS is a mini-spectrum of
conditions, pathologically distinct from early onset autism, I suspect that
regressive autism is equally pathologically distinct from early onset autism.
Why does it matter? Well if you want to treat something, it helps
to know what you are dealing with.
PANS looks like it has some clever people
working on it. Regressive autism, which may
indeed be the most prevalent type, is in need of some similarly clever people.
Conclusion
If
regressive autism is your area of interest, I would suggest you look very
carefully at PANS/PANDAS and the therapies that have been shown to be
effective.
If
you have PANS/PANDAS, taking a look at the experimental immunomodulatory therapy
used in autism might be very worthwhile, for example the TSO therapy from Coronado Bioscience.
We
know that PANS/PANDAS is caused by an ongoing inappropriate immune response,
but we do not know how this is mediated into the odd behaviours. One possible mechanism would be via a
weakening of the blood brain barrier (BBB).
It has been shown that the similar mechanism controls the BBB and the
gut immune barrier.
Clever
research into Celiac Disease has resulted in the discovery ofZonulin, which is now known to be the only physiological
modulator of both these barriers. Using
a type of laboratory test called ELISA, it is now possible to measure Zonulin
levels. If people diagnosed with
PANS/PANDAS were shown to have low Zonulin levels, we could assume that the BBB
was compromised; this would certainly advance understanding of the condition. It
would of course point the way to new therapies.
The
school year is coming to an end and now we get the results of assessment week,
the end of year tests.
Personally
I never liked exams, or rather revising for them, but for teachers, assessment
is a big part of what they do. I used to
be asked at the start of the school year for a list of benchmarks to measure my
son Monty’s progress during the year, since the usual benchmarks were seen not as
applicable. Then we would spend lots of
time discussing the list.
Typical
kids just follow the standard curriculum and get their standardized progress
tests. If you follow an ABA program, you
are constantly measuring performance and you only progress when you master a
skill, so it is like continuous assessment.
Monty,
aged 10 with ASD, goes to a very small international school. So there is no special needs teacher, no IEP
(individual educational plan), just a nice friendly environment. This works very well because it means you can
build your own educational system, not restricted by any rigid rules.
From
the age of about four years old till seven or eight, in effect, Monty’s
curriculum was the ABBLS (Assessment of
Basic Language and Learning Skills), which is a rather intimidating list of 544 skills
from 25 skill areas including language, social interaction, self-help, academic
and motor skills that most typically developing children acquire prior to
entering kindergarten. These are very
basic skills, that we never had to teach to Ted, Monty’s big brother, but
without these skills you really cannot do much. They are the basic skills on
which everything else is built. It
includes things like toilet training, stacking coloured blocks in order and, at
the intellectual end, involves ultra-basic speech, being about to count and
being able to read.
When your child has just a
handful of these 544 skills, it appears that you have a mountain to climb;
indeed you do.
Fortunately for us, Monty’s
then Assistant and best pal, Irena, took on much of this daunting task.He did become verbal, he did learn to read,
he learned how to write and yes, finally, got to grips with numeracy.(All without any help from drugs)
This all occurred in parallel with going to "school".The learning all occurred at home, school was
just for practice.
Back then, the end of year
report did not really have much importance.
At some point you do hope that
school will actually be a place for learning.
It does appear that in many
cases of “inclusion”, school is little more than daycare. Some special schools are brilliant, but even
if you live near one, they tend to be hugely expensive and access is highly
restricted.
My observation of the limited
number of people with autism I am familiar with, is that they tend not to get
on with each other; they actually like to be around nice friendly neurotypical
kids. Until you get to secondary school,
many kids are nice to special needs kids.
After that, most really are not nice at all, and any idea of going to
school for “socialization” becomes nonsense, because the “normal” kids openly seem
to ignore, provoke and even hate the kids with HFA/Asperger’s. Sad, but true.
What is Normal for Kids with Classic Autism?
Most kids with classic autism
end up in a special school, or a special needs unit attached to a mainstream
school.
One of our former 1:1
assistants was a trainee at the local special school and later became a teacher
at another one. We discussed what went
on there and I did visit a few the school a few times. It was much better than I expected, but was
more about keeping the kids calm and under control, than academic advancement. There were 6 kids per member of staff and the
kids had very mixed ability, they were just grouped by age.
I took a look at Treehouse,
the leading autism school in London, to see what is in their curriculum.
In the US there are many such
schools.In Europe, Treehouse is quite
well known, because it seems to be unique.One of our former ABA consultants from the US used to work at Treehouse
and another former one is on the Board of Governors.Our current ABA consultant was doing her PhD
in Behavioral Science in the US, when the founders of Treehouse visited the
leading US autism schools for inspiration many years ago.A small world indeed.
In fact the Treehouse curriculum
bears little resemblance to what goes on in mainstream schools.
I really do not understand
what kids with classic autism can achieve in big mainstream schools, even with
an assistant. I just discussed this with
Monty’s teacher, how can you “include” a child who has no understanding of what
you are teaching the other kids?
Two year ago I agreed with our
school to hold Monty back by two years, to be at his academic level, so he is
two years older than most of his classmates.
There is no rush to get to secondary/high school.
The question I have had for a
long time is whether Monty will be able to learn at school. To date he has had thousands of hours of 1:1
learning at home, following his home program, which now combines ABA-based
learning of things like social skills, conversation etc., with academic work
like numeracy and verbal comprehension.
School for Learning?
My plan, when I realized that
drug interventions do really cognitively improve autism, was to retain my model
of school in the morning and 1:1 learning at home in the afternoon and aim for a
time when school could genuinely be for learning.
The good news is that we
really do seem to have reached that point.
I had the end of year meeting
with Monty’s class teacher and it was almost as if we were discussing a regular
kid. For a start, we were discussing results
from standard tests for science, maths and English provided by Cambridge
University for international schools following their primary curriculum, so
much less scope for the usual “sympathy grading”.
Lots
of kids do get extra time in tests, for example if they have dyslexia. Why not for autism? The Asperger’s boy in Monty’s brother’s
class gets an easier English test and extra time.
In
Monty’s case, I did not want extra time; anyway he does not need it. If he does not understand what to do, extra
time is no help. The question was
whether his assistant should give him any “hints” as to what the questions mean,
when she knows he really does know the answer. (e.g. when asked verbally by the teacher, so not in writing, "what is the next factor of 5, after 30")
We
had this debate and we agreed; no help of any kind. That way at least the test tells us something
useful. If the test is based on
prompting/help, how big was the prompt?
Better to see the real result and then we can do the “oh, but he really
can do that”.
So
this year was the first time we have the same tests as the other kids and
definitely no help. This is the result:-
Speaking
and Listening C+
Reading B+
Writing B+
Mathematics C+
Science A-
ICT A+
Music A
Art A
Well the results show Monty
ended Year 3 ahead of anyone’s expectations, including the teacher.
I think the art teacher was
probably being over generous, which is what tends to happen (sympathy grading). ICT (Information and Communication Technology) is pretty basic
at this level, but Monty can do it all.
When it comes to music, Monty is in his element; he can read music,
plays his piano and has started to sing.
So the grades seem to be genuine,
and he was not at the bottom of the class in any subject. That might not be a
common educational benchmark, but I think it is a pretty good one to see if
“inclusion” is really working.
As I said to his present
teacher, only two years ago he was hitting his then class teacher, assistant and
even, on rare occasions, his classmates.
Back then there was very little learning going on at school and not much
social interaction either.
Cognitive Enhancement
Along with greatly improved
social skills, simple conversation with peers, and even some sporting ability,
has come cognitive enhancement. He still is not “normal”, but it is a remarkable transition nonetheless.
How far he can get following
the mainstream curriculum is an open question, but it is far further than anyone
could have dreamed of, until he started his drug therapy.
I continue to be amazed, but
the gains are almost entirely reversed if he stops taking his drugs.
Following up
on recent posts about PAK1, whose presence is required for 70% of cancers to
grow and MIT have implicated in several types of autism, I have collected all
the data I can find to make trials of PAK1 inhibition in autism.
I contacted
the leading Japanese researcher who has developed PAK1 therapies for various
kinds of tumor, mainly found in neurofibromatosis, but also brain tumors and
even epilepsy. He suggested the dosage
of the CAPE-rich propolis from New Zealand and also suggested another drug
called Fingolimod/Gilenya.
This drug is an
immunomodulating drug, approved for treating multiple sclerosis, but it is also
a PAK1 inhibitor. It appears to cross
the blood brain barrier. The downside it
that Gilenya is hugely
expensive, costing around $50,000 a year.
While
Tonegawa's group at MIT continue to develop their new PAK1 inhibitors, I am
concerned that they will end up with a drug costing as much as Gilenya, which
will put it out of reach of most people, even if it was effective.
So that
brings me back to the trials I propose.
Trial 1 - BIO
30 Propolis
This is a
natural product and as such will appeal to many of this blogs readers. It needs no prescription from your
doctor. You can buy it over the internet
from numerous pharmacies in New Zealand.
The dosage
proposed for autism by the Japanese Researcher is 1-2 ml per 10 kg of body
weight.
It appears that
about 1% of people have an allergy to bee products. If you are in the 99%, it is reported that
even very much larger doses of BIO 30 have no side effects.
Trial 2 - Ivermectin/Stromectol
This is the
cheap drug that is used to treat parasites, but turns out to be a PAK1
inhibitor. It was also recently shown to
kill leukemia cells.
Here I will
draw on the autism worm-dosage used by Dr Wu, who prescribes Ivermectin in the
belief that the autistic kids’ behaviours are driven by worms.
Dr Yu is
combining Ivermectin with other anti-parasite drugs. I am assuming he “got it right for the wrong
reason”, in other words the worms are not the issue, PAK1 is the issue.
Below is the
dosage Dr Yu suggests in his autism presentation and one case report where
there was a before and after evaluation.
Here the ATEC was used, which is a scale designed by Bernard Rimland and Stephen M.Edelson of the Autism Research Institute (the DAN people).
From what I
could find, a single dose of Ivermectin (Stromectol) should kill the
parasites. Pets are given the same drug
on a regular basis, some preventatively.
In low doses
it appears to be very safe, but not in high doses.
Strongyloidiasis is a human parasitic disease
caused by the nematode (roundworm). On
the site RXLIST.com the dosage for Strongyloidiasis is:-
The above is
for a single dose therapy. Dr Wu’s worms
are either much more resilient, or his much higher and multiple dose therapy is
actually working for entirely different reasons.
Trial 3 -
Fingolimod/Gilenya
Given the
huge cost of Gilenya, I cannot imagine anybody trying it for autism. Perhaps Novartis would like to donate some?
We did cover
immunomodulatory therapy in earlier posts and it was Dr Chez who likes to write
about this subject, in relation to autism.
He has published several trials and a good book.
Perhaps he
should do the Gilenya trial?
The Blood Brain Barrier
I did ask
the Japanese researcher if CAPE, the anti-PAK1 ingredient of the New Zealand
propolis can cross the blood brain barrier, since it is claimed that Ivermectin
does not. He says that BIO30 and
Fingolimod/Gilenya cross the BBB.
In this
research the aim was to confirm the mechanism behind why inflammation causes
the blood brain barrier (BBB) to leak.
It has been suggested that the leaky BBB is a key part of autism. The less leaky it is the better for
autism. Since pro-inflammatory agents
like histamine and IL-6 really do make autism worse, it is highly relevant that
the research shows that pro-inflammatory agents cause the BBB to let through more of the substances that it is supposed to keep out.
Perhaps the
ever-present pro-inflammatory cytokines found in autism, mean that the BBB is
always partially compromised. A drug
like Ivermectin might therefore pass more freely across the BBB, than would be
expected in other people.
So
Ivermectin might remain a cheap alternative to Gilenya.Dr
Yu’s case studies perhaps warrant some more serious attention.
Will it work?
There are
good reasons why PAK1 inhibition should have a positive effect. It is definitely not quack science, it is the serious MIT kind.
In treating Neurofibromatosis
NF-1 tumors, it does seem to be more effective at stopping new tumors, rather
than shrinking existing ones. This perhaps should not be surprising, since
PAK1 is needed for a tumor to grow and may not be needed for it to live. At much higher doses, it is reported that existing tumors shrink. So with autism, maybe PAK1 is needed early on,
before birth; blocking PAK1 in a 10 year old may be pointless.
The only
way to find out for sure if it works in your type of autism is to try it.
If it does
not work for Monty, aged 10 with ASD, we cannot say it will not work in
somebody’s two year old with a different type of autism.
Also, in
Monty, the PAK1 effect might already be being mitigated by his existing drugs.
It would be
helpful if there was a clinical trial, but there is not.
Conclusion
Trial 1 is
easy to do at home, and if you do it for a month, you would need two bottles of
propolis, costing $50 including shipping from New Zealand.
Since the
Nobel Laureate from MIT tells us that autism requires PAK1 and that, in mouse
models of autism, PAK1 inhibitors are effective treatments, it seems odd nobody
has tried it. In PAK1-driven
Neurofibromatosis, there are now many people claiming BIO30 to be effective. In this condition you can measure/count the
tumors, so I guess they should know if it works.
The MIT-inspired
drugs, likeTonegawa’s FRAX486 will
not be available for many years, and who knows how much they will cost.
In the case
of Ivermectin, somebody really should look at the toxicology data and see how
safe regular usage would be in humans.
The Leukemia researchers proposed this drug be actively developed, but
nothing seems to have happened. Just for
a few days, Trial 2 would not seem to be too risky.
We agree to
leave trial 3 to Dr Chez, in Sacramento.
