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ASPARTAME —THE
SHOCKING STORY
OF THE
WORLD'S
BESTSELLING
SWEETENER
Pat Thomas,
Health Editor
THE ECOLOGIST
MAGAZINE
September 2005
Aspartame is the
most
controversial
food additive in
history. The
most recent
evidence,
linking it to
leukemia and
lymphoma, has
added
substantial fuel
to the ongoing
protests of
doctors,
scientists and
consumer groups
who allege that
this artificial
sweetener should
never have been
released onto
the market and
that allowing it
to remain in the
food chain is
killing us by
degrees.
Once upon a
time, aspartame
was listed by
the Pentagon as
a biochemical
warfare agent.
Today it's an
integral part of
the modern diet.
Sold
commercially
under names like
NutraSweet and
Canderel,
aspartame can be
found in more
than 5,000
foods, including
fizzy drinks,
chewing gum,
table-top
sweeteners, diet
and diabetic
foods, breakfast
cereals, jams,
sweets,
vitamins,
prescription and
over-the-counter
drugs. This
means that there
is a good chance
that you and
your family are
among the two
thirds of the
adult population
and 40 per cent
of children who
regularly ingest
this artificial
sweetener.
Because it
contains no
calories,
aspartame is
considered a
boon to
health-conscious
individuals
everywhere; and
most of us, if
we think about
it at all, think
it is safe. But
independent
scientists say
aspartame can
produce a range
of disturbing
adverse effects
in humans,
including
headaches,
memory loss,
mood swings,
seizures,
multiple
sclerosis and
Parkinson's-like
symptoms, tumors
and even death.
Concerns over
aspartame's
toxicity meant
that for eight
years, the US
Food and Drug
Administration
(FDA) denied it
approval,
effectively
keeping it off
the world
market. This
caution was
based on
compelling
evidence,
brought to light
by numerous
eminent
scientists,
litigators and
consumer groups,
that aspartame
contributed to
serious central
nervous system
damage and had
been shown to
cause cancer in
animals.
Eventually,
however,
political
muscle, won out
over scientific
rigor, and
aspartame was
approved for use
in 1981 (see
timeline for
details).
The FDA's
about-turn
opened the
floodgates for
aspartame's
swift approval
by more than 70
regulatory
authorities
around the
world. But, as
the remarkable
history of the
sweetener shows,
the clean bill
of health given
to it by
government
regulators -
whose raison
d'ętre should be
to protect the
public from harm
— is simply not
worth the paper
it is printed
on.
DECEMBER 1965
While working on
an ulcer drug, a
chemist at
pharmaceutical
manufacturer GD
Searle
accidentally
discovers
aspartame, a
substance that
is 180 times
sweeter than
sugar, yet has
no calories.
SPRING 1967
Searle begins
safety tests,
necessary for
FDA approval.
AUTUMN 1967
GD Searle
approaches
eminent
biochemist Dr
Harry Waisman,
director of the
University of
Wisconsin's
Joseph P Kennedy
Jr Memorial
Laboratory of
Mental
Retardation
Research and a
respected expert
in the toxicity
of phenylalanine
(which comprises
50 per cent of
the aspartame
formula), to
conduct a study
of the effects
of aspartame on
primates. Of
seven monkeys
fed aspartame
mixed with milk,
one dies and
five others have
grand mal
epileptic
seizures.
SPRING 1971
Dr John Olney,
professor of
neuropathology
and psychiatry
at Washington
University in St
Louis School of
Medicine, whose
research into
the neurotoxic
food additive
monosodium
glutamate (MSG,
a chemical
cousin of
aspartame) was
responsible for
having it
removed from
baby foods,
informs Searle
that his studies
show that
aspartic acid,
one of the main
constituents of
aspartame,
causes holes in
the brains of
infant mice. One
of Searle's
researchers, Ann
Reynolds,
confirms Olney's
findings in a
similar study.
FEBRUARY 1973
Searle applies
for FDA approval
and submits over
100 studies it
claims support
aspartame's
safety. Neither
the dead monkeys
nor the mice
with holes in
their brains are
included in the
submission.
12 SEPTEMBER
1973
In a memorandum,
Dr Martha M
Freeman of the
FDA Division of
Metabolic and
Endocrine Drug
Products
criticises the
inadequacy of
the information
submitted by
Searle with
particular
regard to one of
the compound's
toxic breakdown
products,
diketopiperazine
(DKP). She
recommends that
marketing of
aspartame be
contingent upon
the sweetener's
proven clinical
safety.
26 JULY 1974
FDA commissioner
Dr Alexander
Schmidt grants
aspartame its
first approval
as a 'food
additive' for
restricted use
in dry foods.
This approval
comes despite
the fact that
his own
scientists found
serious
deficiencies in
the data
submitted by
Searle.
AUGUST 1974
Before aspartame
can reach the
marketplace, Dr
John Olney,
James Turner
(attorney,
consumer
advocate and
former 'Nader's
Raider' who was
instrumental in
removing the
artificial
sweetener
cyclamate from
the US market),
and the group
Label Inc (Legal
Action for
Buyers'
Education and
Labeling) file a
formal objection
to aspartame's
approval with
the FDA, citing
evidence that it
could cause
brain damage,
particularly in
children.
JULY 1975
Concerns about
the accuracy of
test data
submitted to the
FDA by Searle
for a wide range
of products
prompt Schmidt
to appoint a
special task
force to examine
irregularities
in 25 key
studies for
aspartame and
Searle drugs
Flagyl,
Aldactone and
Norpace.
5 DECEMBER1975
Searle agrees to
an inquiry into
aspartame safety
concerns. Searle
withdraws
aspartame from
the market
pending its
results. The
sweetener
remains off the
market for
nearly 10 years
while
investigations
into its safety
and into
Searle's alleged
fraudulent
testing
procedures are
ongoing.
However, the
inquiry board
does not convene
for another four
years.
24 MARCH 1976
The FDA task
force completes
its 500 page
report on
Searle's testing
procedures. The
final report
notes faulty and
fraudulent
product testing,
knowingly
misrepresented
product testing,
knowingly
misrepresented
and
'manipulated'
test data, and
instances of
irrelevant
animal research
in all the
products
reviewed.
Schmidt says:
'[Searle's
studies were]
incredibly
sloppy science.
What we
discovered was
reprehensible.'
JULY 1976
The FDA forms a
new task force,
headed by
veteran
inspector Jerome
Bressler, to
further
investigate
irregularities
in Searle's
aspartame
studies
uncovered by the
original task
force. The
findings of the
new body will
eventually be
incorporated
into a document
known as the
Bressler Report.
10 JANUARY 1977
FDA chief
counsel Richard
Merrill formally
requests the US
Attorney's
office to begin
grand jury
proceedings to
investigate
whether
indictments
should be filed
against Searle
for knowingly
misrepresenting
findings and
'concealing
material facts
and making false
statements' in
aspartame safety
tests. This is
the first time
in the FDA's
history that it
requests a
criminal
investigation of
a manufacturer.
26 JANUARY 1977
While the grand
jury
investigation is
underway, Sidley
& Austin, the
law firm
representing
Searle, begins
recruitment
negotiations
with Samuel
Skinner, the US
attorney in
charge of the
investigation.
Skinner removes
himself form the
investigation
and the case is
passed to
William Conlon.
8 MARCH 1977
Searle hires
prominent
Washington
insider Donald
Rumsfeld as its
new CEO to try
to turn the
beleaguered
company around.
A former member
of Congress and
defence
secretary in the
Ford
administration,
Rumsfeld brings
several of his
Washington
colleagues in as
top management.
1 JULY 1977
Samuel Skinner
leaves the US
Attorney's
office and takes
a job with
Searle's law
firm. Conlon
takes over
Skinner's old
job.
1 AUGUST 1977
The Bressler
Report is
released. It
focuses on three
key aspartame
studies
conducted by
Searle. The
report finds
that in one
study 98 of the
196 animals died
but weren't
autopsied until
later dates,
making it
impossible to
ascertain the
actual cause of
death. Tumors
were removed
from live
animals and the
animals placed
back in the
study. Many
other errors and
inconsistencies
are noted. For
example, a rat
was reported
alive, then
dead, then
alive, then dead
again. Bressler
comments: 'The
question you
have got to ask
yourself is: why
wasn't greater
care taken? Why
didn't Searle,
with their
scientists,
closely evaluate
this, knowing
full well that
the whole
society, from
the youngest to
the elderly,
from the sick to
the unsick . . .
will have access
to this
product.'
The FDA creates
yet another task
force to review
the Bressler
Report. The
review is
carried out by a
team at the
FDA's Center for
Food Safety and
Applied
Nutrition and
headed by senior
scientist
Jacqueline
Verrett.
28 SEPTEMBER
1977
The FDA
publishes a
report
exonerating
Searle of any
wrongdoing in
its testing
procedures.
Jacqueline
Verrett will
later testify to
the US Senate
that her team
was pressured
into validating
data from
experiments that
were clearly a
'disaster'.
8 DECEMBER 1977
Despite
complaints from
the Justice
Department,
Conlon stalls
the grand jury
prosecution for
so long that the
statute of
limitations on
the aspartame
charges runs out
and the
investigation is
dropped. Just
over a year
later Conlon
joins Searle's
law firm, Sidley
& Austin.
1978
The journal
Medical World
News reports
that the
methanol content
of aspartame is
1,000 times
greater than
most foods under
FDA control. In
high
concentrations
methanol, or
wood alcohol, is
a lethal poison.
1979
In spite of the
uncertainties
over aspartame's
safety in the
US, aspartame
becomes
available,
primarily in
pharmaceutical
products, in
France. It is
sold under the
brand name
Canderel and
manufactured by
the food
corporation
Merisant.
1 JUNE 1979
The FDA finally
establishes a
public board of
inquiry (PBOI),
comprising three
scientists whose
job it is to
review the
objections of
Olney and Turner
to the approval
of aspartame and
rule on safety
issues
surrounding the
sweetener.
30 SEPTEMBER
1980
The FDA's PBOI
votes
unanimously
against
aspartame's
approval,
pending further
investigations
of brain tumors
in animals. The
board says it
'has not been
presented with
proof of
reasonable
certainty that
aspartame is
safe for use as
a food
additive'.
1980
Canderel is now
marketed
throughout much
of Europe (but
not in the UK)
as a low-calorie
sweetener.
JANUARY 1981
Rumsfeld states
in a Searle
sales meeting
that he is going
to make a big
push to get
aspartame
approved within
the year.
Rumsfeld vows to
'call in his
markers' and use
political rather
than scientific
means to get the
FDA on side.
20 JANUARY 1981
Ronald Reagan is
sworn in as
president of the
US. Reagan's
transition team,
which includes
Rumsfeld,
nominates Dr
Arthur Hull
Hayes Jr to be
the new FDA
commissioner.
21 JANUARY 1981
One day after
Reagan's
inauguration,
Searle
re-applies to
the FDA for
approval to use
aspartame as a
food sweetener.
MARCH 1981
An FDA
commissioner's
panel is
established to
review issues
raised by the
PBOI.
19 MAY 1981
Arthur Hull
Hayes Jr,
appoints a
five-person
commission to
review the
PBOI's decision.
Three of the
five FDA
scientists on it
advise against
approval of
aspartame,
stating on the
record that
Searle's tests
are unreliable
and not adequate
to determine the
safety of
aspartame. Hayes
installs a sixth
member on the
commission, and
the vote becomes
deadlocked.
15 JULY 1981
Hayes ignores
the
recommendations
of his own
internal FDA
team, overrules
the PBOI
findings and
gives initial
approval for
aspartame to be
used in dry
products on the
basis that it
has been shown
to be safe for
its proposed
uses.
22 OCTOBER 1981
The FDA approves
aspartame as a
tabletop
sweetener and
for use in
tablets,
breakfast
cereals, chewing
gum, dry bases
for beverages,
instant coffee
and tea,
gelatines,
puddings,
fillings,
dairy-product
toppings and as
a flavor
enhancer for
chewing gum.
1982
The
aspartame-based
sweetener Equal,
manufactured by
Merisant, is
launched in the
US.
15 OCTOBER 1982
The FDA
announces that
Searle has filed
a petition for
aspartame to be
approved as a
sweetener in
carbonated
beverages,
children's
vitamins and
other liquids.
1983
Searle attorney
Robert Shapiro
gives aspartame
its commercial
name,
NutraSweet. The
name is
trademarked the
following year.
Shapiro later
becomes
president of
Searle. He
eventually
becomes
president and
then chairman
and CEO of
Monsanto, which
will buy Searle
in 1985.
8 JULY 1983
Aspartame is
approved for use
in carbonated
beverages and
syrup bases in
the US and,
three months
later, Britain.
Before the end
of the year
Canderel tablets
are launched in
the UK. Granular
Canderel follows
in 1985.
8 AUGUST 1983
James Turner, on
behalf of
himself and the
Community
Nutrition
Institute, and
Dr Woodrow
Monte, Arizona
State
University's
director of food
science and
nutritional
laboratories,
file petitions
with the FDA
objecting to
aspartame
approval based
on possible
serious adverse
effects from the
chronic intake
of the
sweetener. Monet
also cites
concern about
the chronic
intake of
methanol
associated with
aspartame
ingestion.
SEPTEMBER 1983
Hayes resigns as
FDA commissioner
under a cloud of
controversy
about his taking
unauthorized
rides aboard a
General Foods
jet (General
Foods was and is
a major
purchaser of
aspartame). He
serves briefly
as provost at
New York Medical
College, and
then takes a
position as
senior
scientific
consultant with
Burston-Marsteller,
the chief public
relations firm
for both Searle
and Monsanto.
AUTUMN 1983
The first
carbonated
beverages
containing
aspartame go on
sale in the US.
17 FEBRUARY 1984
The FDA denies
Turner and
Monte's requests
for a hearing,
noting that
aspartame's
critics had not
presented any
unresolved
safety
questions.
Regarding
aspartame's
breakdown
components, the
FDA says that it
has reviewed
animal, clinical
and consumption
studies
submitted by the
sweetener's
manufacturer, as
well as the
existing body of
scientific data,
and concludes
that 'the
studies
demonstrated the
safety of these
components'.
MARCH 1984
Public
complaints about
the adverse
effects of
aspartame begin
to come in. The
FDA requests
that the US
agency the
Centers for
Disease Control
and Prevention
(CDC) begins
investigations
of a select
number of cases
of adverse
reactions to
aspartame.
30 MAY 1984
The FDA approves
aspartame for
use in
multivitamins.
JULY 1984
A study by the
state of Arizona
Department of
Health into
aspartame is
published in the
Journal of
Applied
Nutrition. It
determines that
soft drinks
stored at
elevated
temperatures
promote more
rapid
deterioration of
aspartame into
poisonous
methanol.
2 NOVEMBER 1984
The CDC review
of public
complaints
relating to
aspartame
culminates in a
report,
Evaluation of
Consumer
Complaints
Related to
Aspartame Use,
which reviews
213 of 592 cases
and notes that
re-challenge
tests show that
sensitive
individuals
consistently
produce the same
adverse symptoms
each time they
ingested
aspartame. The
reported
symptoms
include:
aggressive
behavior,
disorientation,
hyperactivity,
extreme
numbness,
excitability,
memory loss,
loss of depth
perception,
liver
impairment,
cardiac arrest,
seizures,
suicidal
tendencies and
severe mood
swings. The CDC
nevertheless
concludes that
aspartame is
safe to ingest.
On the same day
that the CDC
exonerates
aspartame, Pepsi
announces that
it is dropping
saccharin and
adopting
aspartame as the
sweetener in all
its diet drinks.
Others quickly
follow suit.
1 OCTOBER 1985
Monsanto, the
producer of
recombinant
bovine growth
hormone,
genetically
engineered soya
beans, the
pesticide
Roundup and many
other industrial
and agricultural
chemicals,
purchases Searle
for $2.7
billion.
21 APRIL 1986
The US Supreme
Court, headed by
Justice Clarence
Thomas, a former
Monsanto
attorney,
refuses to
consider
arguments from
the Community
Nutrition
Institute and
other consumer
groups that the
FDA has not
followed proper
procedures in
approving
aspartame, and
that the liquid
form of the
artificial
sweetener may
cause brain
damage in heavy
users of
low-calorie soft
drinks.
16 OCTOBER 1986
Turner files
another
citizen's
petition, this
time concerning
the risk of
seizures and eye
damage from
aspartame. The
petition argues
that medical
records of 140
aspartame users
show them to
have suffered
from epileptic
seizures and eye
damage after
consuming
products
containing the
sweetener and
that the FDA
should ban
aspartame as an
'imminent hazard
to the public
health'.
21 NOVEMBER 1986
The FDA denies
Turner's new
petition,
saying: 'The
data and
information
supporting the
safety of
aspartame are
extensive. It is
likely that no
food product has
ever been so
closely examined
for safety.
Moreover, the
decisions of the
agency to
approve
aspartame for
its uses have
been given the
fullest airing
that the legal
process
requires.'
28 NOVEMBER 1986
The FDA approves
aspartame for
non-carbonated
frozen or
refrigerated
concentrates and
single-strength
fruit juice,
fruit drinks,
fruit-flavored
drinks,
imitation
fruit-flavored
drinks, frozen
stock-type
confections and
novelties,
breath mints and
tea beverages.
DECEMBER 1986
The FDA declares
aspartame safe
for use as an
inactive
ingredient,
provided
labeling meets
certain
specifications.
1987
NutraSweet's
aspartame patent
runs out in
Europe, Canada
and Japan. More
companies are
now free to
produce
aspartame
sweeteners in
these countries.
2 JANUARY 1987
An FDA report on
adverse
reactions
associated with
aspartame states
the majority of
the complaints
about aspartame
— now numbering
3,133 — refer to
neurological
effects.
12 OCTOBER 1987
United Press
International, a
leading global
news-syndication
organization,
reports that
more than 10
federal
officials
involved in the
decision to
approve
aspartame have
now taken jobs
in the private
sector that are
linked to the
aspartame
industry.
3 NOVEMBER 1987
A US Senate
hearing is held
to address the
issue of
aspartame safety
and labeling.
The hearing
reviews the
faulty testing
procedures and
the
'psychological
strategy' used
by Searle to
help ensure
aspartame's
approval. Other
information that
comes to light
includes the
fact that
aspartame was
once on a
Pentagon list of
prospective
biochemical-warfare
weapons.
Numerous medical
and scientific
experts testify
as to the
toxicity of
aspartame. Among
them is Dr.
Verrett, who
reveals that,
while compiling
its 1977 report,
her team was
instructed not
to comment on or
be concerned
with the overall
validity of the
studies. She
states that
questions about
birth defects
have not been
answered. She
also states that
increasing the
temperature of
the product
leads to an
increase in
production of
DKP, a substance
shown to
increase uterine
polyps and
change blood
cholesterol
levels. Verrett
comments: 'It
was pretty
obvious that
somewhere along
the line, the
bureau officials
were working up
to a whitewash.'
1989
The FDA has
received more
than 4,000
complaints from
consumers about
adverse
reactions to the
sweetener.
14 OCTOBER 1989
Dr HJ Roberts,
director of the
Palm Beach
Institute for
Medical
Research, claims
that several
recent aircraft
accidents
involving
confusion and
aberrant pilot
behavior were
caused by
ingestion of
products
containing
aspartame.
20 JULY 1990
The Guardian
publishes a
major
investigation of
aspartame and
delivers to
government
officials 'a
dossier of
evidence' that
draws heavily on
the transcripts
of the Bressler
Report and
demands that the
government
review the
safety of
aspartame. No
review is
undertaken. The
Guardian is
taken to court
by Monsanto and
forced to
apologize for
printing its
story.
1991
The US National
Institutes of
Health publishes
Adverse Effects
of Aspartame:
January '86
through December
'90, a
bibliography of
167 studies
documenting
adverse effects
associated with
aspartame.
1992
NutraSweet signs
agreements with
Coca-Cola and
Pepsi
stipulating that
it is their
preferred
supplier of
aspartame.
30 JANUARY 1992
The FDA approves
aspartame for
use in malt
beverages,
breakfast
cereals, and
refrigerated
puddings and
fillings and in
bulk form (in
large packages
like sugar) for
tabletop use.
NutraSweet
markets these
bulk products
under the name
'NutraSweet
Spoonful'.
14 DECEMBER 1992
NutraSweet's US
patent for
aspartame
expires, opening
up the market
for other
companies to
produce the
substance.
19 APRIL 1993
The FDA approves
aspartame for
use in hard and
soft candies,
non-alcoholic
flavored
beverages, tea
beverages, fruit
juices and
concentrates,
baked goods and
baking mixes,
and frostings,
toppings and
fillings for
baked goods.
28 FEBRUARY 1994
Aspartame now
accounts for the
majority (75 per
cent) of all the
complaints in
the US
adverse-reaction
monitoring
system. The US
Department of
Health and Human
Services
compiles a
report that
brings together
all current
information on
adverse
reactions
attributed to
aspartame. It
lists 6,888
complaints,
including 649
reported by the
CDC and 1,305
reported by the
FDA.
APRIL 1995
Consumer
activist, and
founder of
anti-aspartame
group Mission
Possible, Betty
Martini uses the
US's Freedom of
Information Act
to force the FDA
to release an
official list of
adverse effects
associated with
aspartame
ingestion.
Culled from
10,000 consumer
complaints, the
list includes
four deaths and
more than 90
unique symptoms,
a majority of
which are
connected to
impaired
neurological
function. They
include:
headache;
dizziness or
problems with
balance; mood
change; vomiting
and nausea;
seizures and
convulsions;
memory loss;
tremors; muscle
weakness;
abdominal pains
and cramps;
change in
vision;
diarrhea;
fatigue and
weakness; skin
rashes;
deteriorating
vision; joint
and
musculoskeletal
pain.
By the FDA's own
admission, fewer
then 1 per cent
of those who
have problems
with something
they consume
ever report it
to the FDA. This
means that
around 1 million
people could
have been
experiencing
adverse effects
from ingesting
aspartame.
12 JUNE 1995
The FDA
announces it has
no further plans
to continue to
collect adverse
reaction reports
or monitor
research on
aspartame.
27 JUNE 1996
The FDA removes
all restrictions
from aspartame
use, and
approves it as a
general-purpose
sweetener',
meaning that
aspartame can
now be used in
any food or
beverage.
NOVEMBER 1996
Drawing on data
compiled by the
US National
Cancer
Institute's
Surveillance,
Epidemiology and
End Results
program, which
collects and
distributes data
on all types of
cancer, Olney
publishes
peer-reviewed
research in the
Journal of
Neuropathology
and Experimental
Neurology. It
shows that
brain-tumor
rates have risen
in line with
aspartame
consumption and
that there has
been a
significant
increase in the
conversion of
less deadly
tumors into much
more deadly
ones.
DECEMBER 1996
The results of a
remarkable study
conducted by Dr
Ralph G. Walton,
professor of
clinical
psychology at
Northeastern
Ohio
Universities,
are revealed.
Commissioned by
the hard-hitting
US national news
program 60
Minutes, it
sheds some light
on the absurdity
of
aspartame-safety
studies. Walton
reviewed 165
separate studies
published in the
preceding 20
years in
peer-reviewed
medical
journals.
Seventy-four of
the studies were
industry-funded,
all of which
attested to
aspartame's
safety. Of the
other 91
non-industry
funded studies,
84 identified
adverse health
effects. Six of
the seven
non-industry
funded studies
that were
favorable to
aspartame were
from the FDA,
which has a
public record of
strong
pro-industry
bias. To this
day, the
industry-funded
studies are the
ones that are
always quoted to
the press and in
official
rebuttals to
aspartame
critics. They
are also the
studies given
the greatest
weight during
the approval
process and in
official safety
reviews.
10 FEBRUARY 1998
Monsanto
petitions the
FDA for approval
of a new
tabletop
sweetener called
Neotame. It is
around 60 times
sweeter than
aspartame and up
to 13,000 times
sweeter than
sugar. Neotame
is less prone to
breaking down in
heat and in
liquids than
aspartame
because of the
addition of
3,3-dimethylbutyl,
a poorly studied
chemical with
suspected
neurotoxic
effects.
Strengthening
the bond between
aspartame's main
constituents
eliminates the
need for a
health warning
directed at
people suffering
from PKU.
13 MAY 1998
Independent
scientists from
the University
of Barcelona
publish a
landmark study
clearly showing
that aspartame
is transformed
into
formaldehyde in
the bodies of
living specimens
(in this case
rats), and that
this
formaldehyde
spreads
throughout the
specimens' vital
organs,
including the
liver, kidneys,
eyes and brain.
The results fly
in the face of
manufacturers'
claims that
aspartame does
not break down
into
formaldehyde in
the body, and
bolster the
claims of
aspartame
critics that
many of the
symptoms
associated with
aspartame
toxicity are
caused by the
poisonous and
cumulative
effects of
formaldehyde.
OCTOBER 1998
The UK's Food
Commission
publishes two
surveys on
sweeteners. The
first shows that
several leading
companies,
including St
Ivel, Müller and
Sainsbury's,
have ignored the
legal
requirement to
state 'with
sweeteners' next
to the name of
the product. The
second reveals
that aspartame
not only appears
in 'no-sugar
added' and
'light'
beverages but
also in ordinary
non-dietetic
drinks because
it's three times
cheaper than
ordinary sugar.
8 FEBRUARY 1999
Monsanto files a
petition with
the FDA for
approval of the
general use of
Neotame.
20 JUNE 1999
An investigation
by The
Independent on
Sunday reveals
that aspartame
is made using a
genetic
engineering
process.
Aspartame
component
phenylalanine is
naturally
produced by
bacteria. The
newspaper
reveals that
Monsanto has
genetically
engineered the
bacteria to make
them produce
more
phenylalanine.
Monsanto claims
that the process
had not been
revealed
previously
because no
modified DNA
remains in the
finished
product, and
insists that the
product is
completely safe;
though
scientists
counter that
toxic effects
cannot be ruled
out in the
absence of
long-term
studies.
A Monsanto
spokeswoman says
that while
aspartame for
the US market is
often made using
genetic
engineering,
aspartame
supplied to
British food
producers is
not. The extent
to which US
brands of
low-calorie
products
containing
genetically
engineered
aspartame have
been imported
into Britain is
unclear.
MAY 2000
Monsanto, under
pressure — not
least from the
worldwide
resistance to
genetically
manipulated food
and ongoing
lawsuits — sells
NutraSweet to JW
Childs
Associates, a
private-equity
firm comprised
of several
former Monsanto
managers, for
$440m. Monsanto
also sells its
equity interest
in two European
sweetener joint
ventures,
NutraSweet AG
and
Euro-Aspartame
SA.
10 DECEMBER 2001
The UK's Food
Standards Agency
requests that
the European
Commission
Scientific
Committee on
Food conducts an
updated review
of aspartame.
The committee is
asked to look
carefully at
more than 500
scientific
papers published
between 1988 and
2000 and any
other new
scientific
research not
examined
previously.
9 JULY 2002
The FDA approves
the tabletop and
general use of
Neotame. The
'fast-track'
approval raises
eyebrows
because,
historically,
the FDA takes at
least 10 years
to approve food
additives.
Neotame is also
approved for use
in Australia and
New Zealand, but
has yet to be
approved in the
UK.
10 DECEMBER 2002
The European
Commission
Scientific
Committee on
Food publishes
its final report
on aspartame.
The 24-page
report largely
ignores
independent
research and
consumer
complaints,
relying instead
on frequently
cited articles
in books and
reviews put
together by
employees or
consultants of
aspartame
manufacturers.
When independent
research is
cited, it is
generally
refuted with
industry-sponsored
data. An animal
study showing
aspartame's
disruption of
brain chemistry,
a human study
linking
aspartame to
neurophysiological
changes that
could increase
seizure risk,
another linking
aspartame use
with depression
in individuals
susceptible to
mood disorder,
and two others
linking
aspartame
ingestion with
headaches are
all dismissed.
The report's
conclusion
amounts to a
single sentence:
'The committee
concluded that
there is no
evidence to
suggest that
there is a need
to revise the
outcome of the
earlier risk
assessment or
the [acceptance
daily intake]
previously
established for
aspartame.'
As with the FDA,
there are
concerns about
the neutrality
of some of the
committee's
members and
their links with
the
International
Life Sciences
Institute (ILSI),
an industry
group that
funds, among
other things,
research into
aspartame. ILSI
members include
Monsanto,
Coca-Cola and
Pepsi.
19 FEBRUARY 2003
Members of the
European
Parliament's
Environment,
Public Health
and Consumer
Policy Committee
approve the use
of sucralose
(see page 50)
and an
aspartame-acesulfame
salt compound
(manufactured in
Europe by the
aspartame-producing
Holland
Sweetener
Company and sold
under the name
Twinsweet),
agreeing to
review of the
use of both in
three years'
time. At the
same time, a
request by
European greens
that the
committee
re-evaluate the
safety of
aspartame and
improve the
labeling of
aspartame-containing
products is
rejected.
MAY 2004
The
feature-length
documentary
Sweet Misery is
released on DVD
(see http://www.soundandfuryproductions.com).
Part-documentary,
part-detective
story, it
includes
interviews with
people who have
been harmed by
aspartame, as
well as credible
testimony from
advocates,
doctors, lawyers
and long-time
campaigners,
including James
Turner, HJ
Roberts and
renowned
neurosurgeon Dr.
Russell
Blaylock. (UK
orders: Namaste
Publishing,
info@namastepublishing.co.uk)
SEPTEMBER 2004
US consumer
group the
National Justice
League files a
$350m class
action lawsuit
against the
NutraSweet
Corporation (the
current owner of
aspartame
products), the
American
Diabetes
Association and
Monsanto. Some
50 other
defendants have
yet to be named,
but mentioned
throughout the
lawsuit is the
central role of
Donald Rumsfeld
in helping to
get aspartame
approved through
the FDA. The
plaintiffs
maintain that
this litigation
will prove how
deadly aspartame
is when it is
consumed by
humans. Little
progress has
been made so far
in bringing the
action to court.
MARCH 2005
The NutraSweet
Company reopens
its plant in
Atlanta,
Georgia,
(dormant since
2003) in order
to meet
increased demand
for its
sweetener.
Aspartame, sold
commercially as
NutraSweet,
Equal,
Equal-Measure,
Spoonful,
Canderel and
Benevia, is
currently
available in
more than 100
countries and
used in more
than 5,000
products by at
least 250
million people
every day.
Worldwide, the
aspartame
industry's sales
amount to more
than $1 billion
yearly. The US
is the primary
consumer.
JULY 2005
The Ramizzini
Institute in
Bologna, a
non-profit,
private
institution set
up to research
the causes of
cancer, releases
the results of a
very large,
long-term animal
study into
aspartame
ingestion. Its
study shows that
aspartame causes
lymphomas and
leukemia in
female animals
fed aspartame at
doses around 20
milligrams per
kilogram of body
weight, or
around half the
accepted daily
intake for
humans.
ASPARTAME
REACTIONS:
A HIDDEN
EPIDEMIC
Aspartame has
been linked to a
host of
devastating
central nervous
system disorders
When aspartame
was approved for
use, Dr HJ
Roberts,
director of the
Palm Beach
Institute for
Medical
Research, had no
reason to doubt
the FDA's
decision. 'But
my attitude
changed,' he
says, 'after
repeatedly
encountering
serious
reactions in my
patients that
seemed
justifiably
linked to
aspartame.'
Twenty years on,
Roberts has
coined the
phrase
'aspartame
disease' to
describe the
wide range of
adverse effects
he has seen
among
aspartame-guzzling
patients.
He estimates:
'Hundreds of
thousands of
consumers, more
likely millions,
currently suffer
major reactions
to products
containing
aspartame.
Today, every
physician
probably
encounters
aspartame
disease in
everyday
practice,
especially among
patients with
illnesses that
are undiagnosed
or difficult to
treat.'
As a guide for
other doctors,
Roberts, a
recognised
expert in
difficult
diagnoses, has
published a
lengthy series
of case studies,
Aspartame
Disease: an
ignored epidemic
(Sunshine
Sentinel Press),
in which he
meticulously
details his
treatment of
1,200
aspartame-sensitive
individuals, or
'reactors',
encountered in
his own
practice.
Following
accepted medical
procedure for
detecting
sensitivities to
foods, Roberts
had his patients
remove aspartame
from their
diets. With
nearly two
thirds of
reactors,
symptoms began
to improve
within days of
removing
aspartame, and
improvements
were maintained
as long as
aspartame was
kept out of
their diet.
Roberts' case
studies parallel
much of what was
revealed in the
FDA's report on
adverse
reactions to
aspartame - that
toxicity often
reveals itself
through central
nervous system
disorders and
compromised
immunity. His
casework shows
that aspartame
toxicity can
mimic the
symptoms of
and/or worsen
several diseases
that fall into
these broad
categories.
Case studies,
especially a
large series
like this,
address some of
the issues
surrounding
real-world use
in a way that
laboratory
studies never
can; and the
conclusions that
can be drawn
from such
observations
aren't just
startling, they
are also
potentially
highly
significant. In
fact, Roberts
believes that
one of the major
problems with
aspartame
research has
been the
continued
over-emphasis on
laboratory
studies. This
has meant that
the input of
concerned
independent
physicians and
other interested
persons,
especially
consumers, is
'reflexively
discounted as
"anecdotal"'.
Many of the
diseases listed
by Roberts fall
into the
category of
medicine's
'mystery
diseases' —
conditions with
no clear
etiology and few
effective cures.
And while no one
is suggesting
that aspartame
is the single
cause of such
diseases,
Roberts'
research
suggests that
some people
diagnosed with,
for example,
multiple
sclerosis,
Parkinson's or
chronic fatigue
syndrome may end
up on a regimen
of potentially
harmful drugs
that could have
been avoided if
they simply
stopped
ingesting
aspartame-laced
products.
Conditions
Mimicked By
Aspartame
Toxicity
• Multiple
sclerosis
• Parkinson's
disease
• Alzheimer's
disease
• Fibromyalgia
• Arthritis
• Multiple
chemical
sensitivity
• Chronic
fatigue syndrome
• Attention
deficit disorder
• Panic disorder
depression and
other
psychological
disorders
• Lupus
• Diabetes and
diabetic
complications
• Birth defects
• Lymphoma
• Lyme disease
• Hypothyroidism
ASPARTAME'S
TOXIC CONTENTS
Aspartame is
made up of three
chemicals: the
amino acids
aspartic acid
and
phenylalanine,
and methanol.
The chemical
bond that holds
these
constituents
together is
fairly weak. As
a result,
aspartame
readily breaks
down into its
component parts
in a variety of
circumstances:
in liquids;
during prolonged
storage; when
exposed to heat
in excess of 86°
Fahrenheit (30°
Centigrade); and
when ingested.
These
constituents
further break
down into other
toxic
by-products,
namely
formaldehyde,
formic acid and
aspartylphenylalanine
diketopiperazine
(DKP).
Manufacturers
argue that the
instability of
aspartame is
irrelevant since
its constituents
are all found
naturally in
food. This is
only partially
true and ignores
the fact that in
food amino acids
like aspartic
acid and
phenylalanine
are bound to
proteins, which
means that
during digestion
and metabolism
they are
released slowly
into the body.
In aspartame,
these amino
acids are in an
unbound or
'free' form that
releases greater
amounts of these
chemicals into
the system much
more quickly.
Similarly, the
methanol present
in natural foods
like fruits, for
example, is
bound to pectin
and also has a
co-factor,
ethanol, to
mediate some of
its effects. No
such chemical
'back-stops'
exist in
aspartame.
According to
neuroscientist
Russell
Blaylock, the
effect of
aspartame's
breakdown
components on
brain function
is central to
its known
adverse effects.
Like monosodium
glutamate (MSG)
and L-cysteine,
an amino acid
found in
hydrolysed
vegetable
protein,
aspartame is
what is known as
an 'excitotoxin'
- a chemical
transmitter that
allows brain
cells to
communicate.
Blaylock has
written a book
about them,
Excitotoxins:
the taste that
kills, and says:
'Even a minute
over-concentration
of these
chemicals causes
the brain cells
to become so
over-excited
that they very
quickly burn
themselves out
and die.'
While aspartame
manufacturers
say aspartame
cannot penetrate
the blood-brain
barrier — the
tightly-walled
membrane that
keeps toxins
from reaching
the brain,
Blaylock
counters that a
number of
factors make the
blood-brain
barrier more
porous,
including
exposure to
pesticides,
hypoglycemia,
all immune
diseases (such
as lupus and
diabetes),
Alzheimer's and
Parkinson's,
strokes
(including
silent strokes)
and a whole
range of medical
drugs. Under
these
conditions,
ingesting
aspartame-laced
foods may cause
a spike in the
level of
excitotoxins
that directly
reach the brain,
thus increasing
the likelihood
of adverse
effects. Each of
aspartame's main
constituents is
a known
neurotoxin
capable of
producing a
unique array of
adverse effects.
PHENYLALANINE
The essential
amino acid
phenylalanine
comprises 50 per
cent of
aspartame. In
people disorder,
phenylketonuria
(PKU) with the
genetic the
liver cannot
metabolise
phenylalanine,
causing it to
build up in the
blood and
tissues.
Chronically high
levels of
phenylalanine
and its
breakdown
products cause
significant
neurological
problems, which
is why foods and
beverages
containing
aspartame must
carry a warning
for PKU
sufferers.
But according to
Dr. HJ Roberts,
sensitivity to
aspartame is not
limited to PKU
sufferers. PKU
carriers -
people who
inherited the
gene for the
disorder but do
not themselves
have the
condition
(around 2 per
cent of the
general
population) -
are also more
prone to adverse
effects. In
Roberts' data
there is also a
high incidence
of aspartame
reactions among
the close
relatives of
patients who
cannot tolerate
aspartame.
Furthermore,
there is
evidence that
ingesting
aspartame,
especially along
with
carbohydrates,
can lead to
excess levels of
phenylalanine in
the brain even
among those not
affected by PKU.
Although
phenylalanine is
sometimes used
as a treatment
for depression,
excessive
amounts in the
brain can cause
levels of the
mood regulator
serotonin to
decrease, making
depression more
serious or
likely. Build-up
of phenylalanine
in the brain can
also worsen
schizophrenia or
make individuals
more susceptible
to seizures.
Moreover,
decrease in
serotonin levels
can result in
carbohydrate
craving. This
could explain
aspartame's lack
of effectiveness
as a diet aid.
DKP
DKP is a
breakdown
product of
phenylalanine
that forms when
aspartame-containing
liquids are
stored for
prolonged
periods. In
animal
experiments it
has produced
brain tumors,
uterine polyps
and changes in
blood
cholesterol.
Before the FDA
approved
aspartame, the
amount of DKP in
our diets was
essentially
zero. So no
claim of DKP's
safety can be
accepted as
genuine until
good-quality
long-term
studies have
been performed.
No such studies
have been done.
ASPARTIC ACID
Aspartic acid
(also known as
aspartate) is a
non-essential
amino acid that
comprises 40 per
cent of
aspartame. In
the brain, it
functions as a
neurotransmitter
- facilitating
the transfer of
information from
one nerve cell
(neuron) to
another. Both
human and animal
experiments have
demonstrated a
significant
spike in
blood-plasma
levels of
aspartate after
the
administration
of aspartame in
liquids. Too
much aspartate
in the brain
produces free
radicals,
unstable
molecules that
damage and kill
brain cells.
Humans are five
times more
sensitive to the
effects of
aspartic acid
(as well as
glutamic acid,
found in MSG)
than rodents,
and 20 times
more sensitive
than monkeys,
because we
concentrate
these excitatory
amino acids in
our blood at
much higher
levels and for a
longer period of
time. Aspartic
acid has a
cumulative
harmful effect
on the endocrine
and reproductive
systems. Several
animal
experiments have
shown that
excitotoxins can
penetrate the
placental
barrier and
reach the fetus.
In addition, as
levels of
aspartic acid
rise in the body
so do levels of
the key
neurotransmitter
norepinephrine
(also known as
noradrenaline),
a 'stress
hormone' that
affects parts of
the human brain
where attention
and impulsivity
are controlled.
Excessive
norepinephrine
is associated
with symptoms
such as anxiety,
agitation and
mania.
METHANOL
Methanol (wood
alcohol)
comprises 10 per
cent of
aspartame. It is
a deadly poison
that is
liberated from
aspartame at
temperatures in
excess of 86°
Fahrenheit (30°
centigrade) -
for instance,
during storage
or inside the
human body. The
US Environmental
Protection
Agency considers
methanol a
'cumulative
poison due to
the low rate of
excretion once
it is absorbed',
meaning that
even small
amounts in
aspartame-containing
foods can build
up over time in
the body.
The most well
known problems
from methanol
poisoning are
vision
disorders,
including misty
or blurry
vision, retinal
damage and
blindness. Other
symptoms include
headaches,
Tinnitus,
dizziness,
nausea,
gastrointestinal
disturbances,
weakness,
vertigo, chills,
memory lapses,
numbness and
shooting pains
in the
extremities
behavioral
disturbances,
and neuritis.
The EPA tightly
controls
methanol
exposure,
allowing only
very minute
levels to be
present in foods
or in
environmental
exposures. But
Blaylock says:
'The level
allowed in
NutraSweet is
seven times the
amount that the
EPA will allow
anyone else to
use.'
FORMALDEHYDE
The methanol
absorbed from
aspartame is
converted to
formaldehyde in
the liver.
Formaldehyde is
a neurotoxin and
known
carcinogen. It
causes retinal
damage and birth
defects,
interferes with
DNA replication,
and has been
shown to cause
squamous-cell
carcinoma, a
form of skin
cancer, in
animals. Several
human studies
have found that
chronic,
low-level
formaldehyde
exposure has
been linked with
a variety of
symptoms,
including
headaches,
fatigue, chest
tightness,
dizziness,
nausea, poor
concentration
and seizures.
FORMIC ACID
Formic acid is a
cumulative
poison produced
by the breakdown
of formaldehyde.
It concentrates
in the brain,
kidneys, spinal
fluid and other
organs, and is
highly toxic to
cells. Formic
acid can lead to
accumulation of
excessive acid
in the body
fluids - a
condition known
as acidosis. The
small amounts of
formic acid
derived from the
methanol
absorbed from
aspartame may or
may not be
dangerous; there
are no human or
mammalian
studies to
enlighten us.
ASPARTAME: TIME
FOR ACTION
The story of
aspartame is the
story of the
triumph of
corporate might
over scientific
rigor. It shines
a spotlight on
the archaic and
unbalanced
procedure for
approving food
additives.
We ingest food
additives daily,
yet their
approval does
not require the
same scientific
thoroughness as
drug approval;
and, unlike
drugs, there is
no requirement
for surveillance
of adverse
effects that
crop up once the
additive is in
use.
Approval does
not involve
looking at what
people are
already eating
and whether the
proposed
substance will
interact with
other additives.
Nor does it take
into account
whether the
additive
exacerbates
damage caused by
other aspects of
the modern
lifestyle (for
instance, the
neurological
damage caused by
pesticide
ingestion or
exposure). Nor
does it look for
subtle chronic
effects (for
instance, the
gradual build-up
of methanol in
the body with
regular
aspartame
ingestion).
There are other
problems. Most
studies into
aspartame are
animal studies,
which are
notoriously
difficult to
relate to
humans. So why
bother
performing them
in the first
place? The
answer is,
manufacturers
and regulators
use animal
research as a
double-edged
sword. If an
animal study
reveals no
evidence of
harm, the
manufacturer can
use it to
support its
case. If it
reveals harm,
however, the
manufacturer is
free to
flip-flop into
the argument
that the results
of animal
studies are
inconclusive in
relation to
humans. Faced
with
inconclusive
evidence
regulators will
always err on
the side of the
manufacturer,
who has after
all demonstrated
proper
bureaucratic
procedure by
funding and
submitting its
animal tests for
consideration.
The approval
process for any
substance that
humans put in
their mouths on
a daily basis
should be based
on solid human
data and on the
precautionary
principle when
such data is not
available. But,
as it stands,
the regulation
of food
additives in the
US, the UK and
elsewhere leaves
the burden of
proof of harm on
average people,
despite the fact
that most of us
are either too
detached or too
timid to
complain or
simply don't
have the energy
to take on
multinational
corporations.
The history of
aspartame is all
the more
remarkable
because of the
number of
motivated people
who have refused
to accept the
mantra 'if it's
approved by the
government it
must be safe'.
Nearly every
piece of
independent
research shows
the outrage of
these people,
who have had to
withstand
threats of
litigation and
being vilified
in the media as
'hysterics', is
justified.
After 30 years
of aspartame's
commercial
success, it
would be easy to
conclude it is
too late to act.
And yet earlier
this year
hundreds of
products were
swept off
supermarket
shelves on the
chance that they
might have
contained
minuscule
amounts of a
potentially
carcinogenic
dye, Sudan 1. No
studies existed
to show that
Sudan 1 could
cause cancer in
humans. The
likelihood of
any one person's
exposure to
Sudan 1 being
high enough to
produce a tumor
was minute.
Nevertheless, on
the basis of the
precautionary
principle,
action was
taken.
Aspartame is not
a life-saving
drug. It is not
even a very
effective diet
aid, as shown by
widespread
obesity in the
West. Until the
many concerns
about it have
been examined in
'corporate-neutral',
large-scale,
long-term,
randomized,
double-blind,
placebo-controlled
human trials
(the gold
standard of
scientific
proof) it should
be taken out of
our food.
SUCRALOSE: LIFE
AFTER ASPARTAME
Aspartame should
never have
reached the
marketplace. But
even if the
authorities were
to remove it
from sale
tomorrow, how
much faith
should consumers
place in the
other artificial
sweeteners on
the market? PAT
THOMAS REPORTS
There is not a
single
artificial
sweetener on the
market that can
claim, beyond
all reasonable
doubt, to be
safe for humans
to consume.
Saccharin,
cyclamate and
acesulfame-K
have all been
show to cause
cancer in
animals. Even
the family of
relatively
benign
sweeteners known
as polyols, such
as sorbitol and
mannitol, can
cause gastric
upset if eaten
in quantity.
NutraSweet
believes that
its new
aspartame-based
sweetener,
Neotame, is
'revolutionary';
but, seemingly,
it is only amore
stable version
of aspartame.
This leaves the
market wide open
for sucralose.
Sucralose, sold
commercially as
Splenda, was
discovered in
1976 by
researchers
working for
British sugar
refiner Tate &
Lyle. Four years
later, Tate &
Lyle joined
forces with
Johnson &
Johnson to
develop and
commercialize
sucralose under
the auspices of
a new company,
McNeil Specialty
Products (now
called McNeil
Nutritionals).
Sucralose has
been approved by
more than 60
regulatory
bodies
throughout the
world, and is
now in more than
3,000 products
worldwide. In
the US,
Coca-Cola has
developed a new
diet drink
sweetened with
Splenda, and
other major soft
drink
manufacturers
are expected to
follow suit.
Splenda has had
to rethink its
slogan "made
from sugar, so
it tastes like
sugar" in the
wake of a heated
US legal
challenge and a
recent ruling by
the New Zealand
Advertising
Standards
Authority that
said it confused
and misled
consumers. While
it is true that
sugar, or
sucrose, is one
of the starting
materials for
sucralose, its
chemical
structure is
significantly
different from
that of sucrose.
In a complex
chemical
process, the
sucrose is
processed with,
among other
things, phosgene
(a
chemical-warfare
agent used
during WWI, now
a common
intermediary in
the production
of plastics,
pesticides and
dyes), and three
atoms of
chlorine are
selectively
substituted for
three hydroxyl
(hydrogen and
oxygen) groups
naturally
attached to the
sugar molecule.
This process
produces
1,6-dichloro-1,6-dideoxy-beta-D-fructofuranosyl-4-chloro4-deoxy-alpha-D-galactopyranoside
(also known as
trichlorogalactosucrose
or sucralose), a
new chemical
substance which
Tate & Lyle
calls a
'water-soluble
chlorocarbohydrate'.
Accepting Tate &
Lyle's
classification
of sucralose as
a
chlorocarbohydrate
at face value
raises
reasonable
concerns about
its suitability
as a food
additive.
Chlorinated
carbohydrates
belong to a
class of
chemicals known
as chlorocarbons.
This class of
chemicals
includes a
number of
notorious human
and
environmental
poisons,
including
polychlorinated
biphenyls
(PCBs);
aliphatic
chlorinated
carbohydrates;
aromatic
chlorinated
carbohydrates
such as DDT;
organochlorine
pesticides such
as aldrin and
dieldrin; and
aromatic
chlorinated
ethers such as
polychlorinated
dioxins (PCDD)
and
polychlorinated
dibenzofurans (PCDF).
Most of the
synthetic
chlorinated
compounds that
we ingest, such
as the pesticide
residues in our
food and water,
bio-accumulate
slowly in the
body; and many
cause
developmental
problems in the
womb or are
carcinogenic.
How do we know
that sucralose
is any
different?
Tate & Lyle
insists that
sucralose passes
through the body
virtually
intact, and that
the tight
molecular bond
between the
chlorine atoms
and the sugar
molecule results
in a very stable
and versatile
product that is
not metabolised
in the body for
calories. This
doesn't mean,
however, that
sucralose is not
metabolised in
the body at all,
and critics like
HJ Roberts argue
that, during
storage and in
the body,
sucralose breaks
down into among
other things 1,6
dichlorofructose,
a chlorinated
compound that
has not been
adequately
tested in
humans.
Tate & Lyle
maintains that
sucralose and
its breakdown
products have
been extensively
tested and
proven safe for
human
consumption. The
company notes
that in seeking
approval from
the US Food and
Drug
Administration
(FDA), McNeil
Specialty
Products
submitted more
than 110 studies
that attested to
the safety of
sucralose.
BUT CAN
CONSUMERS TRUST
THIS RESEARCH
DATA?
The vast
majority of
studies
submitted to the
FDA were
unpublished
animal and
laboratory
studies
performed by
Tate & Lyle
itself, and
therefore liable
to charges of
potentially
unacceptable
bias. Only five
involved human
subjects, and
these were
short-term,
often
single-dose,
studies that
clearly could
not adequately
reflect the
expected
real-world usage
of sucralose.
After questions
were raised by
the FDA about
the safety of
sucralose for
diabetics, and
prior to
approval, a
further five
human studies
were eventually
submitted. On 1
April 1998 the
FDA approved
sucralose for
limited uses;
one year later
it approved it
as a
general-purpose
sweetener.
Some questions
about
sucralose's
safety, arising
from the data
submitted to the
FDA, remain
unanswered.
These studies
included
unsettling
findings about
animals, which,
when exposed to
high doses of
sucralose,
experienced:
• Shrunken
thymus and
spleen;
• Enlarged liver
and kidneys; and
• Reduced growth
rate in adults
and newborns
In the FDA's
'final-rule'
report, several
of the studies
submitted by
McNeil were
found to have
'inconclusive'
results or were
'insufficient'
to draw firm
conclusions from
them. These
included:
• A test that
examined the
clastogenic
activity
(ability to
break
chromosomes
apart) of
sucralose, and a
test that looked
for chromosomal
aberrations in
human
lymphocytes
exposed to
sucralose';
• A series of
three animal
genotoxicity
studies; and
• Laboratory
studies using
lymphoma tissue
from mice which
showed that
sucralose was
weakly
mutagenic'
(capable of
causing cellular
mutations).
Clastogenic,
genotoxic and
mutagenic
substances are
all potential
risk factors in
the development
of cancer.
In addition to
these, three
studies that
looked at very
specific
'anti-fertility'
effects of
sucralose and
its breakdown
products,
especially with
regard to sperm
production were
also deemed
insufficient;
this is
particularly
worrying, since
other 'chlorosugars',
such as
6-chloroglucose,
are currently
being studied as
anti-spermatogenic
drugs.
Furthermore, the
administration
observed that
McNeil had
failed to
explain
satisfactorily a
reduction in
body weight seen
in animals fed
sucralose and
that 'additional
study data were
needed to
resolve this
issue'.
Ironically for a
product that
'tastes like
sugar', McNeil
argued that
weight loss was
due to the
'reduced
palatability of
sucralose-containing
diets'. FDA
reviewers also
found that at
mid to high
doses there was
a trend towards
'decreasing
white blood cell
and lymphocyte
counts with
increasing dose
levels of
sucralose'. This
was dismissed as
having no
'statistical
significance' by
the FDA; in
healthy animals
and humans this
may be so, but
what happens
when already
immune-compromised
individuals
ingest sucralose?
Tate & Lyle says
that any
lingering
concerns about
sucralose are
unfounded and
that only a
small amount,
15-20 per cent,
of sucralose is
absorbed and
broken down in
the human gut.
The rest passes
through the body
unmetabolised
and is excreted
in urine and
faeces. This in
itself provokes
important
questions.
• What happens
to sucralose
that is flushed
down the toilet?
Does it remain
stable or react
with other
substances (for
instance, the
chlorine used in
water-treatment
plants, or
microbial life)
to form new
compounds?
• Is sucralose
or any resulting
chemical
compound it may
form safe for
the environment?
Is it harmful to
aquatic life or
wild animals?
• Will sucralose
begin to appear
in our water
supply, in the
way that certain
drugs have,
silently
increasing our
exposure to it?
And would that
increased
exposure be
safe?
PUBLISH AND BE
SUED
In the face of
emerging public
criticism,
lawyers for Tate
& Lyle are
already gearing
up for a battle.
According to
attorney James
Turner, a key
player in the
aspartame drama,
'There's going
to be a huge
fight about
Splenda in the
next few
months.[Tate &
Lyle's] lawyers
are already on
the case trying
to shut
everybody up'.
It's a tactic
that worked well
for Monsanto,
which certainly
used legal
pressure against
anyone who
criticised
NutraSweet.
Recently, the
publisher of the
local newspaper
the Brighton
Argus considered
it prudent to
publish an
apology composed
by Tate & Lyle
(or their
lawyers) or face
a legal action
for defamation
and loss of
sales after
printing an
article
suggesting that
sucralose was
harmful to
humans.
Tate & Lyle's
first
high-profile
victim, however,
was
www.mercola.com
— one of the
world's most
visited internet
health sites.
Run by Dr.
Joseph Mercola,
the site has
been a vocal
critic of
sucralose for
years. Instead
of carrying
freely available
information on
sucralose that
might stimulate
spirited public
debate, it now
carries the
following
message:
'Attorneys
acting on behalf
of the
manufacturers of
sucralose, Tate
& Lyle Plc,
based in London,
England, have
requested that
the information
contained on
this page not be
made available
to internet
users in
England.'
At this point,
concerned
consumers should
be asking
themselves
several
questions. Does
the story of
sucralose sound
familiar? If
sucralose is
safe beyond any
reasonable
doubt, why is
there such a
fervent need to
suppress any
criticism of it?
Finally, whom do
such tactics
really serve? Do
they serve the
consumer and the
principles of
choice,
information,
safety and
redress? Or do
they serve the
corporate
machine and its
need to keep
generating
profits without
taking
responsibility
for the human
cost of doing
so?
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