Time Magazine
Monday, April 29,
2002
The Secrets of Autism
The number of children diagnosed with autism and Asperger's in the U.S. is
exploding. Why?
By J. Madeleine Nash
Tommy Barrett is a dreamy-eyed fifth-grader who lives with his parents, twin
brothers, two cats and a turtle in San Jose, Calif., the heart of Silicon
Valley. He's an honor-roll student who likes math and science and video games.
He's also a world-class expert on Animorph and Transformer toys. "They're
like cars and trains and animals that transform into robots or humans — I love
them!" he shouts exuberantly.
And that is sometimes a problem. For a time, in fact, Tommy's fascination
with his toys was so strong that when they weren't around he would pretend to be
the toys, transforming from a truck into a robot or morphing into a kitten. He
would do this in the mall, in the school playground and even in the classroom.
His teachers found this repetitive pantomime delightful but disturbing, as did
his mother Pam. By that point, there were other worrisome signs. Pam Barrett
recalls that as a 3-year-old, Tommy was a fluent, even voluble talker, yet he
could not seem to grasp that conversation had reciprocal rules, and, curiously,
he avoided looking into other people's eyes. And although Tommy was obviously
smart — he had learned to read by the time he was 4 — he was so fidgety and
unfocused that he was unable to participate in his kindergarten reading group.
When Tommy turned 8, his parents finally learned what was wrong. Their bright
little boy, a psychiatrist informed them, had a mild form of autism known as
Asperger syndrome. Despite the fact that children with Asperger's often respond
well to therapy, the Barretts, at that moment, found the news almost unbearable.
That's because just two years earlier Pam and her husband Chris, operations
manager of a software-design company, had learned that Tommy's twin brothers
Jason and Danny were profoundly autistic. Seemingly normal at birth, the twins
learned to say a few words before they spiraled into their secret world, quickly
losing the abilities they had just started to gain. Instead of playing with
toys, they broke them; instead of speaking, they emitted an eerie, high-pitched
keening.
First Jason and Danny, now Tommy. Pam and Chris started to wonder about their
children's possible exposure to toxic substances. They started scanning a
lengthening roster of relatives, wondering how long autism had shadowed their
family.
The anguish endured by Pam and Chris Barrett is all too familiar to tens of
thousands of families across North America and other parts of the world. With a
seeming suddenness, cases of autism and closely related disorders like
Asperger's are exploding in number, and no one has a good explanation for it.
While many experts believe the increase is a by-product of a recent broadening
of diagnostic criteria, others are convinced that the surge is at least in part
real and thereby cause for grave concern.
In the Barretts' home state of California, for instance, the number of
autistic children seeking social services has more than quadrupled in the past
15 years, from fewer than 4,000 in 1987 to nearly 18,000 today. So common are
cases of Asperger's in Silicon Valley, in fact, that Wired magazine coined a
cyber-age term for the disorder, referring to its striking combination of
intellectual ability and social cluelessness as the "geek syndrome."
Wired went on to make a provocative if anecdotal case that autism and Asperger's
were rising in Silicon Valley at a particularly alarming rate — and asked
whether "math-and-tech genes" might be to blame.
Yet the rise in autism and Asperger's is hardly confined to high-tech
enclaves or to the children of computer programmers and software engineers. It
occurs in every job category and socioeconomic class and in every state.
"We're getting calls from school systems in rural Georgia," observes
Sheila Wagner, director of the Autism Resource Center at Atlanta's Emory
University. "People are saying, 'We never had any kids with autism before,
and now we have 10! What's going on?'"
It's a good question. Not long ago, autism was assumed to be comparatively
rare, affecting as few as 1 in 10,000 people. The latest studies, however,
suggest that as many as 1 in 150 kids age 10 and younger may be affected by
autism or a related disorder — a total of nearly 300,000 children in the U.S.
alone. If you include adults, according to the Autism Society of America, more
than a million people in the U.S. suffer from one of the autistic disorders
(also known as pervasive developmental disorders or pdds). The problem is five
times as common as Down syndrome and three times as common as juvenile diabetes.
No wonder parents are besieging the offices of psychologists and
psychiatrists in their search for remedies. No wonder school systems are adding
special aides to help teachers cope. And no wonder public and private research
institutions have launched collaborative initiatives aimed at deciphering the
complex biology that produces such a dazzling range of disability.
In their urgent quest for answers, parents like the Barretts are provoking
what promises to be a scientific revolution. In response to the concerns they
are raising, money is finally flowing into autism research, a field that five
years ago appeared to be stuck in the stagnant backwaters of neuroscience. Today
dozens of scientists are racing to identify the genes linked to autism. Just
last month, in a series of articles published by Molecular Psychiatry,
scientists from the U.S., Britain, Italy and France reported that they are
beginning to make significant progress.
Meanwhile, research teams are scrambling to create animal models for autism
in the form of mutant mice. They are beginning to examine environmental factors
that might contribute to the development of autism and using advanced
brain-imaging technology to probe the deep interior of autistic minds. In the
process, scientists are gaining rich new insights into this baffling spectrum of
disorders and are beginning to float intriguing new hypotheses about why people
affected by it develop minds that are strangely different from our own and yet,
in some important respects, hauntingly similar.
AUTISM'S GENETIC ROOTS
Autism was first described in 1943 by Johns Hopkins psychiatrist Leo Kanner,
and again in 1944 by Austrian pediatrician Hans Asperger. Kanner applied the
term to children who were socially withdrawn and preoccupied with routine, who
struggled to acquire spoken language yet often possessed intellectual gifts that
ruled out a diagnosis of mental retardation. Asperger applied the term to
children who were socially maladroit, developed bizarre obsessions and yet were
highly verbal and seemingly quite bright. There was a striking tendency,
Asperger noted, for the disorder to run in families, sometimes passing directly
from father to son. Clues that genes might be central to autism appeared in
Kanner's work as well.
But then autism research took a badly wrong turn. Asperger's keen insights
languished in Europe's postwar turmoil, and Kanner's were overrun by the
Freudian juggernaut. Children were not born autistic, experts insisted, but
became that way because their parents, especially mothers, were cold and
unnurturing.
In 1981, however, British psychiatrist Dr. Lorna Wing published an
influential paper that revived interest in Asperger's work. The disorder
Asperger identified, Wing observed, appeared in many ways to be a variant of
Kanner's autism, so that the commonalities seemed as important as the
differences. As a result, researchers now believe that Asperger and Kanner were
describing two faces of a highly complicated and variable disorder, one that has
its source in the kaleidoscope of traits encoded in the human genome.
Researchers also recognize that severe autism is not always accompanied by
compensatory intellectual gifts and is, in fact, far likelier to be
characterized by heartbreaking deficits and mental retardation.
Perhaps the most provocative finding scientists have made to date is that the
components of autism, far more than autism itself, tend to run in families. Thus
even though profoundly autistic people rarely have children, researchers often
find that a close relative is affected by some aspect of the disorder. A sister
may engage in odd repetitive behavior or be excessively shy; a brother may have
difficulties with language or be socially inept to a noticeable degree. In
similar fashion, if one identical twin has autism, there is a 60% chance that
the other will too and a better than 75% chance that the twin without autism
will exhibit one or more autistic traits.
How many genes contribute to susceptibility to autism? Present estimates run
from as few as three to more than 20. Coming under intensifying scrutiny, as the
papers published by Molecular Psychiatry indicate, are genes that regulate the
action of three powerful neurotransmitters: glutamate, which is intimately
involved in learning and memory, and serotonin and gamma-aminobutiric acid (gaba),
which have been implicated in obsessive-compulsive behavior, anxiety and
depression.
Those genes hardly exhaust the list of possibilities. Among the suspects are
virtually all the genes that control brain development and perhaps cholesterol
and immune-system function as well. Christopher Stodgell, a developmental
toxicologist at New York's University of Rochester, observes that the process
that sets up the brain resembles an amazingly intricate musical score, and there
are tens of thousands of genes in the orchestra. If these genes do what they're
supposed to do, says Stodgell, "then you have a Mozart's Concerto for
Clarinet. If not, you have cacophony."
A DIFFERENCE OF MIND
Autistic people often suffer from a bewildering array of problems — sensory
disturbances, food allergies, gastrointestinal problems, depression, obsessive
compulsiveness, subclinical epilepsy, attention-deficit hyperactivity disorder.
But there is, researchers believe, a central defect, and that is the difficulty
people across the autistic spectrum have in developing a theory of mind. That's
psychologese for the realization, which most children come to by the age of 4,
that other people have thoughts, wishes and desires that are not mirror images
of their own. As University of Washington child psychologist Andrew Meltzoff
sees it, the developmental stage known as the terrible twos occurs because
children — normal children, anyway — make the hypothesis that their parents
have independent minds and then, like proper scientists, set out to test it.
Children on the autistic spectrum, however, are "mind blind"; they
appear to think that what is in their mind is identical to what is in everyone
else's mind and that how they feel is how everyone else feels. The notion that
other people — parents, playmates, teachers — may take a different view of
things, that they may harbor concealed motives or duplicitous thoughts, does not
readily occur. "It took the longest time for Tommy to tell a lie,"
recalls Pam Barrett, and when he finally did, she inwardly cheered.
Meltzoff believes that this lack can be traced to the problem that autistic
children have in imitating the adults in their lives. If an adult sits down with
a normal 18-month-old and engages in some interesting behavior — pounding a
pair of blocks on the floor, perhaps, or making faces — the child usually
responds by doing the same. Young children with autism, however, do not, as
Meltzoff and his colleague Geraldine Dawson have shown in a series of playroom
experiments.
The consequences of this failure can be serious. In the early years of life,
imitation is one of a child's most powerful tools for learning. It is through
imitation that children learn to mouth their first words and master the rich
nonverbal language of body posture and facial expression. In this way, Meltzoff
says, children learn that drooping shoulders equal sadness or physical
exhaustion and that twinkling eyes mean happiness or perhaps mischievousness.
For autistic people — even high-functioning autistic people — the ability
to read the internal state of another person comes only after long struggle, and
even then most of them fail to detect the subtle signals that normal individuals
unconsciously broadcast. "I had no idea that other people communicated
through subtle eye movements," says autistic engineer Temple Grandin,
"until I read it in a magazine five years ago."
At the same time, it is incorrect to say autistic people are cold and
indifferent to those around them or, as conventional wisdom once had it, lack
the high-level trait known as empathy. Last December, when Pam Barrett felt
overwhelmed and dissolved into tears, it was Danny, the most deeply autistic of
her children, who rushed to her side and rocked her back and forth in his arms.
Another misperception about people with autism, says Karen Pierce, a
neuroscientist at the University of California at San Diego, is the notion that
they do not register faces of loved ones as special — that, in the words of a
prominent brain expert, they view their own mother's face as the equivalent of a
paper cup. Quite the contrary, says Pierce, who has results from a neuroimaging
study to back up her contention. Moreover, the center of activity in the
autistic mind, she reported at a conference held in San Diego last November,
turns out to be the fusiform gyrus, an area of the brain that in normal people
specializes in the recognition of human faces.
In a neuroimaging study, Pierce observed, the fusiform gyrus in autistic
people did not react when they were presented with photographs of strangers, but
when photographs of parents were substituted, the area lit up like an explosion
of Roman candles. Furthermore, this burst of activity was not confined to the
fusiform gyrus but, as in normal subjects, extended into areas of the brain that
respond to emotionally loaded events. To Pierce, this suggests that as babies,
autistic people are able to form strong emotional attachments, so their social
aloofness later on appears to be the consequence of a brain disorganization that
worsens as development continues.
In so many ways, study after study has found, autistic people do not parse
information as others do. University of Illinois psychologist John Sweeney, for
example, has found that activity in the prefrontal and parietal cortex is far
below normal in autistic adults asked to perform a simple task involving spatial
memory. These areas of the brain, he notes, are essential to planning and
problem solving, and among their jobs is keeping a dynamically changing spatial
map in a cache of working memory. As Sweeney sees it, the poor performance of
his autistic subjects of the task he set for them — keeping tabs on the
location of a blinking light — suggests that they may have trouble updating
that cache or accessing it in real time.
To Sweeney's collaborator, University of Pittsburgh neurologist Dr. Nancy
Minshew, the images Sweeney has produced of autistic minds in action are
endlessly evocative. They suggest that essential connections between key areas
of the brain either were never made or do not function at an optimal level.
"When you look at these images, you can see what's not there," she
says, conjuring up an experience eerily akin to looking at side-by-side
photographs of Manhattan with and without the Twin Towers.
A MATTER OF MISCONNECTIONS
Does autism start as a glitch in one area of the brain — the brainstem,
perhaps — and then radiate out to affect others? Or is it a widespread problem
that becomes more pronounced as the brain is called upon to set up and utilize
increasingly complex circuitry? Either scenario is plausible, and experts
disagree as to which is more probable. But one thing is clear: very early on,
children with autism have brains that are anatomically different on both
microscopic and macroscopic scales.
For example, Dr. Margaret Bauman, a pediatric neurologist at Harvard Medical
School, has examined postmortem tissue from the brains of nearly 30 autistic
individuals who died between the ages of 5 and 74. Among other things, she has
found striking abnormalities in the limbic system, an area that includes the
amygdala (the brain's primitive emotional center) and the hippocampus (a
seahorse-shaped structure critical to memory). The cells in the limbic system of
autistic individuals, Bauman's work shows, are atypically small and tightly
packed together, compared with the cells in the limbic system of their normal
counterparts. They look unusually immature, comments University of Chicago
psychiatrist Dr. Edwin Cook, "as if waiting for a signal to grow up."
An intriguing abnormality has also been found in the cerebellum of both
autistic children and adults. An important class of cells known as Purkinje
cells (after the Czech physiologist who discovered them) is far smaller in
number. And this, believes neuroscientist Eric Courchesne, of the University of
California at San Diego, offers a critical clue to what goes so badly awry in
autism. The cerebellum, he notes, is one of the brain's busiest computational
centers, and the Purkinje cells are critical elements in its data-integration
system. Without these cells, the cerebellum is unable to do its job, which is to
receive torrents of information about the outside world, compute their meaning
and prepare other areas of the brain to respond appropriately.
Several months ago, Courchesne unveiled results from a brain-imaging study
that led him to propose a provocative new hypothesis. At birth, he notes, the
brain of an autistic child is normal in size. But by the time these children
reach 2 to 3 years of age, their brains are much larger than normal. This
abnormal growth is not uniformly distributed. Using mri-imaging technology,
Courchesne and his colleagues were able to identify two types of tissue where
this mushrooming in size is most pronounced.
These are the neuron-packed gray matter of the cerebral cortex and white
matter, which contains the fibrous connections projecting to and from the
cerebral cortex and other areas of the brain, including the cerebellum. Perhaps,
Courchesne speculates, it is the signal overload caused by this proliferation of
connections that injures the Purkinje cells and ultimately kills them. "So
now," says Courchesne, "a very interesting question is, What's driving
this abnormal brain growth? If we could understand that, then we might be able
to slow or stop it."
A proliferation of connections between billions of neurons occurs in all
children, of course. A child's brain, unlike a computer, does not come into the
world with its circuitry hard-wired. It must set up its circuits in response to
a sequence of experiences and then solder them together through repeated
neurological activity. So if Courchesne is right, what leads to autism may be an
otherwise normal process that switches on too early or too strongly and shuts
off too late — and that process would be controlled by genes.
Currently Courchesne and his colleagues are looking very closely at specific
genes that might be involved. Of particular interest are the genes encoding four
brain-growth regulators that have been found in newborns who go on to develop
mental retardation or autism. Among these compounds, as National Institutes of
Health researcher Dr. Karin Nelson and her colleagues reported last year, is a
potent molecule known as vasoactive intestinal peptide. vip plays a role not
only in brain development but in the immune system and gastrointestinal tract as
well, a hint that other disorders that so frequently accompany autism may not be
coincidental.
The idea that there might be early biomarkers for autism has intrigued many
researchers, and the reason is simple. If one could identify infants at high
risk, then it might become possible to monitor the neurological changes that
presage the onset of behavioral symptoms, and someday perhaps even intervene in
the process. "Right now," notes Michael Merzenich, a neuroscientist at
the University of California, San Francisco, "we study autism after the
catastrophe occurs, and then we see this bewildering array of things that these
kids can't do. What we need to know is how it all happened."
The genes that set the stage for autistic disorders could derail developing
brains in a number of ways. They could encode harmful mutations like those
responsible for single-gene disorders — cystic fibrosis, for instance, or
Huntington's disease. They could equally well be garden-variety variants of
normal genes that cause problems only when they combine with certain other
genes. Or they could be genes that set up vulnerabilities to any number of
stresses encountered by a child.
A popular but still unsubstantiated theory blames autism on the MMR (measles,
mumps and rubella) vaccine, which is typically given to children at around 15
months. But there are many other conceivable culprits. Researchers at the
University of California at Davis have just launched a major epidemiological
study that will test the tissues of both autistic and nonautistic children for
residues of not only mercury but also pcbs, benzene and other heavy metals. The
premise is that some children may be genetically more susceptible than others to
damage by these agents, and so the study will also measure a number of other
genetic variables, like how well these children metabolize cholesterol and other
lipids.
Drugs taken by some pregnant women are also coming under scrutiny. At the
University of Rochester, embryologist Patricia Rodier and her colleagues are
exploring how certain teratogens (substances that cause birth defects) could
lead to autism. They are focusing on the teratogens' impact on a gene called
hoxa1, which is supposed to flick on very briefly in the first trimester of
pregnancy and remain silent ever after. Embryonic mice in which the rodent
equivalent of this gene has been knocked out go on to develop brainstems that
are missing an entire layer of cells.
In the end, it is not merely possible but likely that scientists will
discover multiple routes — some rare, some common; some purely genetic, some
not — that lead to similar end points. And when they do, new ideas for how to
prevent or correct autism may quickly materialize. A decade from now, there will
almost certainly be more effective forms of therapeutic intervention, perhaps
even antiautism drugs. "Genes," as the University of Chicago's Cook
observes, "give you targets, and we're pretty good at designing drugs if we
know the targets."
Paradoxically, the very thing that is so terrible about autistic disorders
— that they affect the very young — also suggests reason for hope. Since the
neural connections of a child's brain are established through experience,
well-targeted mental exercises have the potential to make a difference. One of
the big unanswered questions, in fact, is why 25% of children with seemingly
full-blown autism benefit enormously from intensive speech- and social-skills
therapy — and why the other 75% do not. Is it because the brains of the latter
are irreversibly damaged, wonders Geraldine Dawson, director of the University
of Washington's autism center, or is it because the fundamental problem is not
being adequately addressed?
The more scientists ponder such questions, the more it seems they are holding
pieces of a puzzle that resemble the interlocking segments of Tommy Barrett's
Transformer toys. Put the pieces together one way, and you end up with a normal
child. Put them together another way, and you end up with a child with autism.
And as one watches Tommy's fingers rhythmically turning a train into a robot, a
robot into a train, an unbidden thought occurs. Could it be that some dexterous
sleight of hand could coax even profoundly autistic brains back on track? Could
it be that some kid who's mesmerized by the process of transformation will
mature into a scientist who figures out the trick?
