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News / Spectrum

Untangling biological threads from autism's phenotypic patchwork
reveals four core subtypes

People belonging to the same subtype share genetic variants,
behaviors and often co-occurring diagnoses, according to a new
preprint.

By Holly Barker
3 October 2024 | 5 min read
 
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https://doi.org/10.53053/ZDMW5762
Cite this article
https://doi.org/10.53053/ZDMW5762 https://doi.org/10.53053/ZDMW5762 -
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Illustration of hands sewing red and white threads in a DNA-like
pattern into a blue-gray fabric.
New threads: The genetic variants associated with each autism
subgroup influence gene expression at different stages of
development, a new analysis reveals.
Illustration by Rebecca Horne
Headshot of Holly Barker.
Holly Barker
Contributing writer
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Tags:
Spectrum, Autism, Gene expression, Modeling, Rare variants, Simons
Simplex Collection, SPARK

Despite the huge variation in how autistic people experience the
condition, they can be divided into just four subgroups, according to
a preprint. The people in these groups--who share similar traits and
life outcomes--carry gene variants that implicate distinct biological
pathways, the researchers found.

Each group is associated with specific genetic variants that
influence gene expression at different stages of development, the
investigation revealed. The work includes genetic and phenotypic data
from more than 5,000 autistic children.

Identifying autism subtypes has been on the minds of autism
researchers for many years, says Thomas Frazier, professor of
psychology at John Carroll University, who was not involved in the
work. "But what's really cool is that they link that to the
underlying biology. To my knowledge, this is the first study to do
this in a comprehensive, replicable way."

Autism traits vary dramatically from person to person, and that
diversity is reflected in the hundreds of genetic variants linked to
the condition. But in most cases, genetic differences haven't been
reliably mapped to autism traits, and two people with the same
variant can show different phenotypes.

That lack of progress could stem from focusing on a single trait at
the expense of the interactions among multiple genetic variants, says
lead investigator Olga Troyanskaya, professor of computer science and
integrative genomics at Princeton University and deputy director for
genomics at the Flatiron Institute. "It's not as simple as a single
variant associated with a single phenotype. It's a highly complex
process," she says. (The Flatiron Institute, and the datasets
Troyanskaya's team used in the study, are funded by the Simons
Foundation, The Transmitter's parent organization.)

"

With more data and potentially even better phenotyping, there may be
more than these four categories.

--
-- Anoushka Joglekar

Instead, Troyanskaya and her colleagues investigated the variants
associated with a person's collection of characteristics. They
applied a statistical model to data on the traits and behaviors of
5,392 autistic people from the SPARK research cohort. By adjusting
the number of groups, the team found the most significant
similarities among participants when the model sorted the cohort into
four autism subtypes.

The largest group--consisting of 1,976 people--shows mild challenges in
core autism traits, whereas the smallest--554 people--has severe
difficulties across those same traits. The other two subtypes are
somewhere in between: One group specifically experiences social
challenges and disruptive behavior, and the other shows developmental
delay and difficulties in select traits.

T

he algorithm organized data from an independent cohort, the Simons
Simplex Collection (SSC), in a similar way, the team found.
Considering the differences in the data--clinicians gather information
for the SSC, whereas SPARK consists of parent-filled
questionnaires--the consistency "is a very good sign that we're
finding true, clinically relevant biology here," Troyanskaya says.

People belonging to the same subtype often share the same
co-occurring diagnoses, further analysis found. Those with social
difficulties and disruptive behavior, for instance, are more likely
than the other groups to have a diagnosis of attention-deficit/
hyperactivity disorder or anxiety, and those in the strongly affected
group are more likely to show cognitive impairment.

People of the same subtype often harbor the same autism-linked common
variants, according to a comparison of polygenic scores for 2,293 of
the autistic children and 3,179 unaffected siblings from the SSC. And
a search for rare mutations uncovered more spontaneous--or de
novo--variants among the strongly affected group, whereas those with
developmental delay harbor more inherited variants.

Variants associated with each subtype influence different biological
pathways, hinting that distinct mechanisms underlie autism's
phenotypic differences. For example, the variants detected among the
mildly autistic group alter histone methylation, whereas those
identified in the developmental delay subtype affect neuronal action
potentials.

T

he variants contribute to changes in gene expression at different
points in development, the study also found. The subtype
characterized by developmental delay--which consisted of children
diagnosed with autism at an early age--possesses variants that affect
gene expression during fetal and neonatal development. And those with
social problems and disruptive behavior--who are often diagnosed later
in childhood--harbor variants that influence gene expression after
birth.

The findings were posted on medRxiv in August.

The results suggest that a subtype's genetic profile could--at least
in part--determine clinical milestones, says study investigator Aviya
Litman, a Ph.D. candidate in Troyanskaya's lab. Given more data, the
team's approach could inform parents and guardians of potential
milestone delays, Litman and her colleagues say.

In fact, the researchers plan to train their model with more data as
they become available, including noncoding and whole-genome
sequences, says Natalie Sauerwald, associate research scientist of
computational genomics at the Flatiron Institute and an investigator
on the study. More detailed genetic data could provide more insight
into the mechanistic differences between autism subtypes, Sauerwald
says.

And larger datasets may reveal more nuance between autism subtypes.
"With more data and potentially even better phenotyping, there may be
more than these four categories," says Anoushka Joglekar, a
computational biologist at the biotech company Immunai, who was not
involved in the work. By analyzing whole genomes, the team may
uncover important epigenetic mechanisms, she adds.

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latest advancements in autism research.

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tags:
Spectrum, Autism, Gene expression, Modeling, Rare variants, Simons
Simplex Collection, SPARK

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