Neuroimmunology of Autism Spectrum Disorder: David Marc, B.SC., & Kelly Olson PH.D
Neuroimmunology of Autism Spectrum Disorder: David Marc, B.SC., & Kelly Olson PH.D
Neuroimmunology of Autism Spectrum Disorder: David Marc, B.SC., & Kelly Olson PH.D
ABSTRACT
Autism is a developmental disorder characterized by immunological and neurological abnormalities. The role of cytokines in the pathophysiology
of autism has been researched suggesting a relationship with altered blood-brain barrier permeability and subsequent neuroinflammation.
Cytokine recruitment to the CNS may result in altered neurotransmitter signaling and the behavioral manifestation of autism symptoms. Other
immune mediated events such as changes in the number and activity of natural killer cells, macrophages, immunoglobulins, and glutathione may
contribute to altered neuronal signaling and neurotransmitter imbalances. The purpose of this overview is to examine the relationship between
immune system and nervous system dysfunction to determine biomarkers for autism spectrum disorder. We will explore the utility of serum
cytokines and urinary neurotransmitter analyses as biomarkers for autism.
Autism is a pervasive developmental disorder communication between peripheral immune cells and CNS
characterized by impaired development of social interaction and neurons (Dunn, 2006). The purpose of this overview is to identify
communication, and a markedly restricted repertoire of activities neurological and immunological abnormalities that exist in
and interests (American Psychiatric Association, 1994). The exact individuals with autism. Further, it will become critically apparent
etiology of autism remains largely unknown, however, literature that neuroimmune biomarker testing for autism can identify these
has emerged to suggest genetic, neurological, immunological, and abnormalities and ensure therapeutic effectiveness.
(Pavlov et al., 2003). In addition, enhanced vagal efferent activity (IgG4) production in children with autism. Elevated IgG
can trigger the release of acetylcholine from peripheral antibodies have been identified against brain-specific proteins in
parasympathetic nerve endings, decreasing the release of pro- the hypothalamus and thalamus of autistic children, again
inflammatory cytokines (Pavlov et al., 2003). It is therefore suggesting autoimmunity (Cabanlit et al., 2007).
evident that the immune system and nervous system communicate Although limited studies on autism and autoimmunity
to maintain homeostasis, yet under excessive immune challenges exist, it has been hypothesized that the excess transport and
alterations in neuronal signaling can develop. synthesis of proinflammatory chemokines, cytokines, and
Studies have shown that peripheral activation of immunoglobulins from the periphery to the CNS contribute to the
cytokines can lead to CNS release of various neurotransmitters. development of autoimmune responses (Cohly & Panja, 2005).
Specifically, IL-1 administration may promote CNS release of Autoimmunity may lead to dysregulated neuronal signaling
norepineprhine, serotonin, dopamine, glutamate, and gamma- causing behavioral manifestation of autism symptoms. Therefore,
amino-butyric-acid (GABA) (Dunn, 1992; Zalcman et al., 1994; assessment of immune and nervous system function may provide
Casamenti et al., 1999; Luk et al., 1999; Huang and O’Banion, biochemical targets to treat patients with these behavioral
1998). With enhanced turnover of these neurotransmitters, abnormalities.
significant neurological and behavioral alterations transpire.
NERVOUS SYSTEM BIOMARKERS AND AUTISM
Research has shown how immune challenges can alter
Biomarkers are substances used as indicators of a
neurotransmission leading to behavioral changes and psychiatric
biologic state. Research has revealed the clinical utility of urinary
disorders (Kronfol & Remick, 2000). For example, elevated
neurotransmitters as practical biomarkers to associate with
levels of interleukin-6 (IL-6) have been associated with depressive
neurotransmission (Kusaga et al., 2002; Hughes et al., 2004).
symptoms (Bob et al., 2009).
Urinary neurotransmitter analysis is an innovative, minimally
In Autism, alteration in immune system function may
invasive method to assess peripheral neurotransmitter levels, and
contribute to impaired neurological signaling. A possible
has a breadth of data to support its usefulness in clinical practice.
mechanism contributing to neuronal dysfunction in the autistic
In the 1950’s, research uncovered correlations between urinary
brain is the transport of noxious substances across the blood-brain
catecholamine levels and psychiatric symptoms, such as depression
barrier into the CNS leading to autoimmunity. Studies have shown
and anxiety (Bergsman, 1959; Carlsson et al., 1959). Recent
how cytokines, chemokines, immunoglobulins, and natural killer
research has examined the utility of urinary neurotransmitter
cells promote the recruitment of noxious chemicals in the brains of
analysis to categorize subsets of depression and anxiety, and to
autistic individuals, as well as contribute to autoimmunity
determine pharmaceutical intervention(s) (Hughes et al., 2004;
(Ashwood et al., 2006). Proinflammatory chemokines, such as
Otte et al., 2005). Notwithstanding, urinary neurotransmitter
monocyte chemotactic protein-1 (MCP-1) and thymus activation-
analysis can further be used to assess Attention-Deficit-
regulated chemokine (TARC), along with cytokines, such as TNF-
Hyperactivity Disorder (ADHD). Subjects with ADHD tend to
α, were consistently elevated in the brains of individuals with
have decreased urinary monoamine neurotransmitter levels
autism (Cohly & Panja, 2005). The transport or synthesis of
(specifically, beta-phenylethylamine (PEA)) that can impair mood
cytokines in the brain may contribute to neuroinflammation and
and attention (Kusaga et al., 2002). What’s more, decreased beta-
possible neurotransmitter imbalances (Cohly & Panja, 2005).
PEA levels may contribute to symptoms of inattentiveness (Berry,
Furthermore, Ashwood and colleagues (2008) found that reduced
2004).
levels of the modulatory cytokine, transforming growth factor-β1
Overall, urinary neurotransmitter assessment can be a
(TGF-β1), in autistic children contributed to the dysregulation of
useful tool in any clinical practice, especially those managing
adaptive behaviors and predisposal for autoimmune responses.
psychiatric disorders. Urinary neurotransmitter analysis can
Autoimmunity can be detrimental to normal neuronal signaling and
identify neurotransmitter abnormalities that may contribute to
result in significant behavioral abnormalities (Ashwood et al.,
behavioral changes, and thereby allow more appropriate treatment
2006). Vojdani and colleagues (2008) reported decreased natural
selection (Kahane, 2009).
killer cell activity in autistic children with low intracellular levels
In autism, urinary neurotransmitter analysis has been
of glutathione, IL-2, and IL-15. Decreased natural killer cell
utilized to examine biochemical abnormalities. As such, urinary
activity has been associated with autoimmunity through alteration
serotonin has been the primary urinary neurotransmitter evaluated
of cytokine production (Johansson et al, 2005). Lastly, Entrom
in autistic individuals. Abnormalities in urinary serotonin have
and colleagues (2009) demonstrated elevated immunoglobulin G4
been linked to immunological disturbances. A recent study found is due to decreased numbers of Purkinje cells located in the
consistent elevations in the number of mast cells, along with cerebellum. Altered Purkinje cell population can eventually lead
elevated levels of urinary serotonin, in autistic patients (Castellani to disrupted and weakened motor coordination (Palmen, Engeland,
et al., 2009). Food, stress, or viruses can stimulate mast cells in the Hof, & Schmitz, 2004). Taken together, abnormal brain growth
intestines and brains of young children. Localized and systemic could be another factor that can contribute to peripheral
immune activation can lead to enhanced cytokine and serotonin neurotransmitter imbalances and behavioral manifestation of
release from mast cells and disruption in the lining of the intestines symptoms.
and the blood-brain-barrier causing altered neuronal signaling What’s more, abnormal neural development and
(Castellani et al., 2009). As mentioned previously, a compromised function may result from cytokine recruitment to the CNS and
blood-brain barrier permits noxious substances entry into the brain therefore amino acid and neurotransmitter alterations (Cohly &
and contribute to neuroinflammation. CNS neurotransmitter Panja, 2005). Changes in amino acid levels may lead to elevated
abnormalities may result from neuroinflammation leading to or insufficient neurotransmitter activity and thus can interfere with
behavioral changes. normal cognitive development (Aldred, et al., 2003). During
As identified in autistic individuals, raised peripheral infancy and adolescence, maintenance of optimal neuronal
glutamate levels may also result from a compromised blood-brain signaling is essential to ensure normal development of attentional
barrier (Moreno-Fuenmayor, et al, 1996, Yip, 2007). Elevated processes, memory, and overall cognitive function, lending
plasma glutamate has been attributed to decreased levels of its rate credence to the importance of early intervention through laboratory
limiting enzyme glutamic acid decarboxylase (GAD) in autistic analysis of neurotransmitters and cytokines.
individuals (Shinohe, 2006, Yip, 2007). Specifically, Fatemi and
CONCLUSION
colleagues (2002a) and Yip and others (2007) reported a reduced
Immune system and nervous system activity must be
number of GAD 65 and 67 proteins in Purkinje cells in autistic
viewed and examined as one system functioning in parallel. It is
cerebella. The decreased GAD may be due to autoantibodies
well established that neurological and immunological
specific for GAD, which has been detected in various neurological
abnormalities exist in autistic individuals, however, the
disorders (Manto et al., 2007). These autoantibodies attack the
relationship between neural and immune function has just recently
body's own cells, tissues, and/or organs, causing inflammation and
been emphasized. Food, stress, and viruses can activate immune
tissue damage. Because GAD converts glutamate to gamma-
cells in the periphery and result in CNS disruptions. This may lead
immunobutyric acid (GABA), a decrease in this enzyme will cause
to inflammation in the brain and eventually to behavior changes
subsequent increases in glutamate levels (Yip, 2007). Clinically,
(Castellani et al., 2009). Healthcare practitioners should
high glutamate levels can be excitotoxic and may lead to
understand and evaluate the status of the nervous system together
neurodegeneration and cognitive dysfunction (Ha et al., 2009).
with the immune system to best optimize therapeutic
Studies have demonstrated that particular biochemical
intervention(s). Through the development of innovative laboratory
measurements, such as in plasma amino acid levels, are elevated in
tests to analyze neurotransmitters and cytokines, comprehensive
children with autism when compared to controls. Autistic children
information can be obtained to determine neurological and
demonstrated elevated levels of plasma glutamate and aspartic acid
immunological abnormalities. These biochemical measures can
along with taurine, phenylalanine, asparagine, tyrosine, alanine,
serve as biomarkers for clinical symptoms, as well as provide
and lysine (Moreno-Fuenmayor, Borjas, arrieta, Valera, and
significant guidance for therapeutic selection to reestablish
Socorro-Candanoza, 1996; Aldred, Moore, Fitzgerald, and Waring,
physiological homeostasis and to benefit overall health and
2003). These amino acid alterations may be caused by immune
wellbeing.
mediated events, vitamin insufficiency, alterations in
neurotransmitter transport, or metabolic derangement. REFERENCES
Imaging studies have further revealed abnormalities in Acosta, M.T., & Pearl, P.L. (2004). Imaging data in autism: From structure to malfunction.
Seminars in Pediatric Neurology, 11, 205-213.
autistic individuals, which suggest that abnormal brain growth in
Aldred, S., Moore, K.M., Fitzgerald, M., & Waring, R.H. (2003). Plasma amino acid levels in
many major brain structures such as cerebellum, cerebral cortex, children with autism and their families. Journal of Autism and Developmental
Disorders, 33, 93-97.
amygdala, hippocampus, corpus collosum, basal ganglia, and brain
American Psychiatric Association. Diagnostic and statistical manual of metal disorders. DSM-IV.
stem may contribute to behavioral abnormalities in autism 4th ed. Washington, DC: American Psychiatric Association, 1994.
(Courchesne et al., 2001; Acosta and Pearl, 2004). Moreover, Ashwood, P., Enstrom, A., Krakowiak, P., Hertz-Picciotto, I., Hansen, R.L., Croen, L.A., et al.
(2008). Decreased transforming growth factor beta1 in autism: A potential link
research shows that reduced cerebellar volume in the autistic brain
between immune dysregulation and impairment in clinical behavioral outcomes. Ha, J.S., Leem C.S., Maeng, J.S., Kwon, K.S., & Park, S.S. (2009). Chronic glutamate toxicity in
Journal of Neuroimmunology, 204(1-2), 149-153. mouse cortical neuron culture. Brain Research, [Epub ahead of print].
Ashwood, P., Willis, S., & Van de Water, J. (2006). The immune response in autism: a new Hansen, M.K., Taishi, P., Chen, Z. et al. (1998). Vagotomy blocks the induction of interleukin-1β
frontier for autism research. Journal of Leukocyte Biology, 80, 1-15. (IL-1β) mRNA in the brain of rats in response to systemic IL-1β. Journal of
Neuroscience, 18, 2247-2253.
Bergsman, A. (1959) The urinary excretion of adrenaline and noradrenaline in some mental
diseases; a clinical and experimental study. Acta psychiatrica Scandinavica. Huang, T.L., & O”Banion, M.K. (1998). Interleukin-1β and tumor necrosis factor-alpha suppress
Supplementum, 133, 1-107. dexamethasone induction of glutamine synthetase in primary mouse astrocytes.
Journal of Neuroscience, 71, 1436-1442.
Berry, M.D. (2004a) Mammalian central nervous system trace amines. Pharmacologic
amphetamines, physiologic neuromodulators. Journal of Neurochemistry, 90(2), Hughes, J.W., Watkins, L., Blumenthal, J.A., Kuhn, C., & Sherwood, A. (2004) Depression and
257-271. anxiety symptoms are related to increased 24-hour urinary norepinephrine
excretion among healthy middle-aged women. Journal of Psychosomatic
Bob, P., Raboch, J., Maes, M., Susta, M., Pavlat, J., Jasova, D. et al. (2009). Depression, Research, 57(4), 353-358.
traumatic stress and interleukin-6. Journal of Affective Disorders, [Epub ahead of
print]. Iversson, S.A., Bjerre, L., Vegfors, P., & Ahlfors, K. (1990). Autism as one of several
abnormalities in two children with congenital cytomegalovirus infection.
Borish, L.C., & Steinke, J.W. (2003). 2. Cytokines and chemokines. Journal of Allergy and Neuropediatrics, 21, 102-103.
Clinical Immunology, 111(2), S460-S475.
Johansson, S., Berg, L., Hall, H., & Hoglund, P. (2005). NK cells: Elusive players in
Burger, R.A., & Warren, R.P. (1998). Possible immunogenetic basis for autism. Mental autoimmunity. Trends in Immunology, 26, 613-618.
Retardation and Developmental Disabilities Research Reviews, 4, 137-141.
Kahane, A. (2009). Urinary Neurotransmitter Analysis as a Biomarker for Psychiatric Disorders.
Cabanlit, M., Wills, S., Goines, P., Ashwood, P., & Van de Water, J. (2007). Brain-specific Townsend Letter, 1, 70-72.
autoantibodies in the plasma of subjects with autistic spectrum disorder. The New
York Academy of Sciences, 1107, 92-103. Kibersti, P., & Roberts, L. (2002). It's Not Just the Genes. Science, 296, 685.
Carlsson, A., Rasmussen, E.B., & Kristjansen, P. (1959) The urinary excretion of adrenaline and Kronfol, Z., & Remick, D. (2000). Cytokines and the brain: implications for clinical psychiatry.
noradrenaline by depressive patients during iproniazid treatment. Journal of American Journal of Psychiatry, 158(7), 1163-1164.
Neurochemistry, 4, 321-324.
Kusaga, A., Yamashita, Y., Koeda, T., Hiratani, M., Kaneko, M., Yamada, S., & Matsuishi, T.
Casamenti, F., Prosperi, C., Scali, C., et al. (1999). Interleukin-1β activates forebrain glial cells (2002) Increased urine phenylethylamine after methylphenidate treatment in
and increases nitric oxide production and cortical glutamate and GABA release children with ADHD. Annals of Neurology, 52(3), 372-374.
in vivo: Implications for Alzheimer’s disease. Neuroscience, 91, 831-842.
Layé, S., Bluthé, R.M., Kent, S. et al. (1995). Subdiphragmatic vagotomy blocks induction of Il-1
Castellani, M.L., Conti, C.M., Kempuraj, D.J., Salini, V., Vecchiet, J., & Tete, S. (2009). Autism mRNA in mice brain in response to peripheral LPS. American Journal of
and immunity: revisited study. International Journal of Immunopathology and Physiology, 268, R1327-R1331.
Pharmacology, 22(1), 15-19.
Luk, W.P, Zhang, Y., White, T.D. et al. (1999). Adenosine. A mediator of interleukin-1β –
Cohen, D., Pichard, N., Tordjman, S., Baumann, C., Burglen, L., Excoffier, E., Lazar, G., Mazet, induced hippocampol synaptic inhibition. Journal of Neuroscience, 19, 4238-
P., Pinquier, C., Verloes, A., & Heron, D. (2005). Specific genetic disorders and 4244.
autism: Clinical contribution towards their identification. Journal of Autism and
Developmental Disorders, 35, 103-116. Manto, M.U., Laute, M.A., Aguera, M., Rogemond, V., Pandolfo, M., & Honnorat, J. (2007).
Effects of anti-glutamic acid decarboxylase antibodies associated with
Cohly, H.H., & Panja, A. (2005) Immunological findings in autism. International Review of neurological diseases. Annals of Neurology, 61(6), 544-551.
Neurobiology, 71, 317-341.
Maier, S.F., Goehler, L.E., Fleshner, M. et al. (1998). The role of the vagus nerve in cytokine-to-
Courchesne, E., Karns, C.M., Davis, H.R., Ziccardi, R., Carper, R.A., Tigue, Z.D., Chisum, H.J., brain communication. Annals of the New York Academy of Sciences, 840, 289-
Moses, P., Pierce, K., Lord, C., et al. (2001). Unusual brain growth patterns in 300.
early life in patients with autistic disorder: An MRI study. Neurology, 57, 245-
254. Moreno-Fuenmayor, H., Borjas, L., Arrieta, A., Valera, V., & Socorro-Candanoza, L. (1996).
Plasma excitatory amino acids in autism. The Journal of Clinical Investigation,
Crawley, J.N. (2007). Testing hypotheses about autism. Science, 318, 56-57. 37(2), 113-128.
Dunn, A.J. (1992). Endotoxin-induced activation of cerebral catecholamine and serotonin Otte, C., Neylan, T.C., Pipkin, S.S., Browner, W.S., & Whooley, M.A. (2005) Depressive
metabolism: Comparison with interleukin-1. Journal of Pharmacology and symptoms and 24-hour urinary norepinephrine excretion levels in patients with
Experimental Therapeutics, 261, 964-969. coronary disease: findings from the Heart and Soul Study. American Journal of
Psychiatry, 162(11), 2139-2145.
Dunn, A.J. (2006). Effects of cytokines and infections on brain neurochemistry. Clinical
Neuroscience Research, 6(1-2), 52-68. Palmen, S., Engelan, H., Hof, P.R., & Schmitz, C. (2004). Neuropathological findings in autism.
Brain, 127, 2572-2583.
Edelson, S.B., & Cantor, D.S. (2000). The neurotoxic etiology of the autistic spectrum disorder:
A replicative study. Toxicology and Industrial Health, 16, 239-247. Pavlov, V.A., Wang, H., Czura, C.J., Friedman, S.G., & Tracey, K.J. (2003). The cholinergic
anti-inflammatory pathway: a missing link in neuroimmunomodulation.
Ek, M., Kurosawa, M., Lundeberg, T., et al. (1998). Activation of vagal afferents after Molecular Medicine, 9(5-8), 125-134.
intravenous injection of interleukin-1β: Role of endogenous prostaglandins.
Journal of Neuroscience, 18, 9471-9479. Polleux, F., & Lauder, J.M. (2004). Toward a developmental neurobiology of autism. Mental
Retardation and Developmental Disabilities Research Reviews, 10, 303-317.
Enstrom, A., Krakowiak, P., Onore, C., Pessah, I.N., Hertz-Picciotto, I., Hansen, R.L. et al.
(2009). Increased IgG4 levels in children with autism disorder. Brain, Behavior, Shi, L., Fatemi, S.H., Sidwell, R.W. & Patterson, P.H. (2003). Maternal influenza infection
and Immunity, 23(3), 389-395. causes marked behavioral and pharmacological changes in the offspring. Journal
of Neuroscience, 23, 297-302.
Fatemi, S.H., Earle, J., Kanodia, R., Kist, D., Emamian, E.S., Patterson, P.H., Shi, L., & Sidwell,
R. (2002). Prenatal viral infection leads to pyramidal cell atrophy and Shinohe, et al. (2006). Increased serum levels of glutamate in adult patients with autism. Progress
macrocephaly in adulthood: Implications for genesis of autism and in Neuro-Psychopharmacology and Biological Psychiastry, 30, 1472-1477.
schizophrenia. Cellular and Molecular Neurobiology, 22, 25-33.
Yip, J., Soghomonia, J.J., & Blatt, G.J. (2007). Decreased GAD67 mRNA levels in cerebellar
Fatemi, et al. (2002a). Glutamic acid decarbosylase 65 and 67 kDa proteins are reduced in autistic Purkinje cells in autism: Pathophysiological implications. Acta Neuropathology,
parietal and cerebellar cortices. Biological Psychiatry, 52, 805-810. 113, 559-568.
Ganong, W.F. (2000). Circumventricular organs: Definition and role in the regulation of Vojdani, A., Campbell, A.W., Anyanwu, E., Kashanian, A., Bock, K. & Vojdani, E. (2002).
endocrine and autonomic function. Clinical and Experimental Pharmacology and Antibodies to neuron-specific antigens in children with autism: Possible cross-
Physiology, 27(5-6), 422-427. reaction with encephalitogenic proteins from milk, Chlamydia pneumoniae and
Stretoccoccus group A. Journal of Neuroimmunology, 129, 168-177.
Glessner, J.T., Wang, K., Cai, G., Korvatska, O., Kim, C.E., Wood, S., et al. (2009). Autism
genome-wide copy number variation reveals ubiquitin and neuronal genes. Vojdani, A., Mumper, E., Granpeesheh, D., Mielke, L., Traver, D., Bock, K., et al. (2008). Low
Nature, [Epub ahead of print]. natural killer cell cytotoxic activity in autism: The role of glutathione, IL-2 and
IL-15. Journal of Neuroimmunology, 205(1-2), 148-154.
Goehler, L.E., Gaykema, R.P., Nguyen, K.T. et al. (1999). Interleukin-1β in immune cells of the
abdominal vagus nerve: A link between the immune and nervous systems? Wakefield, A.J., Murch, S.H., Anthony, A., Linnell, J., Casson, D.M., Malik, M., Berelowitz, M.,
Journal of Neuroscience, 19, 2799-2806. Dhillon, A.P., Thomson, M.A., Valentine, A., Davies, S.E., & Walker-Smith,
J.A. (1998). Ileal-lymphoid-nodular hyperplasia, non-specific colitis, and
Gutierrez, E.G., Banks, W.A., & Kastin, A.J. (1993). Murine tumor necrosis factor alpha is pervasive developmental disorder in children. Lancet, 351, 637-641.
transported from blood to brain in the mouse. Journal of Neuroimmunology, 47,
169-176. Wang, K., Zhang, H., Ma, D., Bucan, M., Glessner, J.T., Abrahams, B.S., et al. (2009). Common
genetic variants on 5p14.1 associate with autism spectrum disorder. Nature,
Gutierrez, E.G., Banks, W.A., & Kastin, A.J. (1994). Blood-borne interleukin-1 receptor [Epub ahead of print]
antagonist crosses the blood brain barrier. Journal of Neuroimmunology, 55, 153-
160. Zalcman, S., Gree-Johnson, J.M., Murray, L. et al. (1994). Cytokine-specific central monoamine
alterations induced by interleukin-1-2, and -6. Brain Research, 15, 287-290.