Table of Contents<\/b><\/p>\n [\/vc_column_text][\/vc_column][\/vc_row][vc_row el_id=”introduction”][vc_column][vc_single_image image=”4868″ img_size=”full”][vc_column_text single_style=””]<\/p>\n Current knowledge dictates that neurotransmitter system dysfunction could be the cause of autism spectrum disorder (ASD), by affecting neuronal migration, differentiation, synaptogenesis, and eventually developmental process of the brain. Major projection pathways of the biogenic amine neurotransmitter systems in the human brain. Shown are the projections of the serotonin, dopamine, norepinephrine,<\/i><\/b> and epinephrine systems<\/i><\/b> using the neurotransmitters. The views are midsagittal sections through the human brain, depicting the medial surface of the right hemisphere; the front pole is at left. In each image, the primary source of the biogenic amine is bold type and colored accordingly.<\/p>\n [\/vc_column_text][\/vc_column][\/vc_row][vc_row][vc_column][vc_custom_heading text=”Introduction”][vc_column_text single_style=””]<\/p>\n Neurotransmitters, also called chemical transmitters or chemical messenger, any of a group of chemical agents released by neurons to stimulate or inhibit neighboring neurons or muscle or gland cells, thus impulse to be propagated from one cell to the next throughout the nervous system [1]. Neurotransmitters are chemical messengers by which neurons communicate with each other, and play crucial roles in normal development of brain, memory, motor activity, and behavior regulation. Current knowledge dictates that neurotransmitter system dysfunction could be the cause of autism spectrum disorder (ASD), by affecting neuronal migration, differentiation, synaptogenesis, and eventually developmental process of the brain. In this context, several neurotransmitter systems have been investigated and dysfunction of these systems has been demonstrated to be responsible for the pathophysiology of ASD. In the literature, neurotransmitters that are most commonly associated with the pathogenesis of ASD are serotonergic, glutamatergic, GABAergic, and dopaminergic systems (Figure 1)<\/b>.<\/p>\n [\/vc_column_text][\/vc_column][\/vc_row][vc_row][vc_column][vc_column_text single_style=””]<\/p>\n I. What is known <\/strong><\/p>\n Even though there is no general consensus concerning the exact nature of neurochemical brain abnormalities in individuals with ASD. However, there is ample evidence that several of the major neurochemicals that are classified as neurotransmitters, neuromodulators,<\/i><\/b> and neurotrophins,<\/i><\/b> are affected one way or another. Here we have summarized evidence pertaining to each of these neurochemical substances in ASD, in an order that reveals the established significance from best to least well established in a sequential manner [2]. (cf. previous blog entitled as \u2018The Neurotypical Brain versus the Autistic Brain: Neurotypical Brain Chemistry<\/a><\/i>)<\/p>\n [\/vc_column_text][\/vc_column][\/vc_row][vc_row][vc_column][vc_column_text single_style=””]<\/p>\n (i) Serotonin:<\/b> Serotonin (aka: 5-hydroxytrptamine or 5-HT) is a monoamine chemical messenger derived from the amino acid tryptophan that plays significant roles in many organ systems, including the cardiovascular, gastrointestinal, and central nervous systems. Even though most of the body\u2019s serotonin is located within platelets and enterochromaffin cells, its function as a neurotransmitter in the central nervous system (CNS) is particularly prominent. Serotonin in the brain is most produced by neurons located in the raphe nucleus in the brainstem, and it regulates several brain functions, including mood, sleep, and satiety, via widespread projections of these neurons towards multiple brain areas, including the cerebral cortex, limbic system, midbrain, and hind brain (Figure 2<\/b>).<\/p>\n [\/vc_column_text][vc_column_text single_style=””]<\/p>\n Serotonin is transmitted from one neuron to another neuron by a serotonin transporter (SERT or 5-HTT)<\/b> substance. 5-HTT is also known as the sodium-dependent serotonin transporter<\/i><\/b> and solute carrier family 6 member 4,<\/i><\/b> is a protein that in human is encoded by the SLC6A4<\/i><\/b> gene.<\/p>\n [\/vc_column_text][vc_column_text single_style=””]<\/p>\n Neurons communicate by using chemical messengers like serotonin between cells. The transporter protein, by recycling serotonin, regulates its concentration in a gap or synapse, and thus its effects on a receiving neuron\u2019s receptors. SERT\/5-HTT is a type of monoamine transporter protein that transports the neurotransmitter serotonin from the synaptic cleft back to the presynaptic neuron, in a process known as serotonin reuptake; thus plays an important role in the pathophysiology of several psychiatric and\/or neuro-psychiatric disorders, including ASD.<\/p>\n [\/vc_column_text][vc_single_image image=”4867″ img_size=”full”][vc_column_text single_style=””]<\/p>\n (a)<\/b> Serotonin is derived from the amino acid tryptophan by a two-step process that requires the enzymes tryptophan-5-hydroxylase and a decarboxylase (right panel<\/i><\/b>). (b)<\/b> Major projection pathway of the monoamine neurotransmitter system in the human brain. Shown are the projections of the serotonin system<\/i><\/b> using the neurotransmitter (left panel<\/i>)<\/b>. The views are midsagittal sections through the human brain, depicting the medial surface of the right hemisphere; the front pole is at left. In each image, the primary source of the biogenic amine is bold type and colored accordingly.<\/p>\n [\/vc_column_text][vc_column_text single_style=””]<\/p>\n Abnormalities of serotoninergic system or its expression in the human brain could therefore arise in any one of the following three ways:<\/p>\n [\/vc_column_text][vc_column_text single_style=””]<\/p>\n [\/vc_column_text][vc_column_text single_style=””]<\/p>\n The potential effects of serotonin-related abnormalities in ASD are wide-ranging, given the fact that serotonin acts not only as a neurotransmitter, but also as a neuromodulator, and prenatally, as a neurotrophins<\/b><\/i>. Several scientific reports have evidently shown that all three abnormalities occur more often in subjects with ASD than in neurotypical (NT) individuals. However, none of these three types of abnormalities co-occurs in every autistic subject, or even for that matter in a majority of subjects with ASD [3].<\/p>\n [\/vc_column_text][vc_column_text single_style=””]<\/p>\n (ii) Glutamate and GABA:<\/b> As a rule, glutamate is the most abundant excitatory neurotransmitter, and GABA (gamma-aminobutyric acid) the most abundant inhibitory neurotransmitter, operating throughout the brain. The normal expression of both these chemical substances, i.e., production, transportation, and reception, is essential to maintain a balance between hyper- (too much) and hypo- (too little) neural activity. Thus, any abnormalities associated with either of these neurotransmitters may potentially perturb this balance in one or the other direction (Figure 3; Figure 4<\/b>).<\/p>\n [\/vc_column_text][vc_column_text single_style=””]<\/p>\n At the level of brain, the theory that ASD might result from an imbalance<\/i><\/b> between the major excitatory and inhibitory neurotransmitters, glutamate and GABA was initially pronounced. The subsequently named \u2018EI theory (Emotional Intelligence)\u2019<\/i><\/b> elicited considerable interest among autism researcher. Thereafter, in numerous studies, reduced levels of GABA have now been demonstrated in the brains of individuals with ASD [4]. Moreover, there is also some evidence to suggest that a surplus of glutamate is detected in the brains of individuals with ASD. Most significantly, even if the levels of glutamate expression are within normal limits in ASD, decreased inhibitory control associated with reduced GABA expression by itself lead to higher-than-normal levels of excitation, and \u2018noise\u2019<\/i><\/b> in the neural transmission system.<\/p>\n [\/vc_column_text][vc_single_image image=”4866″ img_size=”full”][vc_column_text single_style=””]<\/p>\n Glutamate synthesis and cycling between neurons and glia, the so-called \u2018glutamate \u2013 glutamine cycle.\u2019<\/i><\/b> Glutamate is the major excitatory neurotransmitter<\/i><\/b> in the brain. Glutamate is a nonessential amino acid<\/i><\/b> that does not cross the blood-brain barrier (BBB)<\/i><\/b> and must be synthesized from local precursors. Glutamine<\/i><\/b> is the most prevalent precursor in synaptic terminals for glutamate synthesis. Glutamine is released by glial cells and, once within the presynaptic terminal of the neuron, it is metabolized to glutamate by the mitochondrial enzyme glutaminase. Glutamate can also be synthesized by the process of transamination of 2-oxoglutarate, an intermediate of the tricarboxylic acid (TCA) cycle. Thus, some of the glucose<\/i><\/b> metabolized by neurons can also be utilized for glutamate synthesis. [VGLUT \u2013 vesicular glutamate transporter; EAAT \u2013 excitatory amino acid transporter; SN1 \u2013 system N1 transporter (glutamine transporter); SAT2 \u2013 system A transporter]<\/p>\n [\/vc_column_text][vc_single_image image=”4865″ img_size=”full”][vc_column_text single_style=””]<\/p>\n GABA is the major inhibitory neurotransmitter<\/i><\/b> in the brain. Glucose<\/i><\/b> is the predominant precursor for GABA synthesis. Initially, glucose is metabolized to glutamate by the tricarboxylic acid (TCA) cycle enzymes, although glutamine<\/i><\/b> and pyruvate<\/i><\/b> can also act as precursor substances. GABAergic neurons express glutamic acid decarboxylase (GAD), which is found almost uniquely in these neurons. GAD catalyzes the conversion of glutamate to GABA. GAD requires pyridoxal phosphate as a cofactor<\/i><\/b> for optimal activity. Since pyridoxal phosphate is derived from vitamin B6, a B6 deficiency can lead to reduced GABA synthesis<\/i><\/b>. \u2018The significance of this become obvious after a disastrous series of infant deaths, linked to the omission of vitamin B6 from infant formula.\u2019<\/i> The absence of B6 resulted in a substantial reduction in GABA content of the brain, and the ensuing loss of synaptic inhibition caused seizures in newborns that in some cases were fatal. More recently, seizures due to B6 deficiency have been reported in adults. [GABA \u2013 gamma amino butyric acid; GABA receptors \u2013 gamma amino butyric receptors; GAT \u2013 GABA transporter type 1, 2, or 3]<\/p>\n [\/vc_column_text][vc_column_text single_style=””]<\/p>\n (iii) Dopamine:<\/b> As in the case of serotonin, there are clearly demonstrated abnormalities, conceivably of various kinds, in the dopaminergic system in individuals with ASD [5]. Besides, it has long been suggested that dysfunctioning of the dopaminergic system contributes to motor abnormalities<\/i><\/b> in ASD (Figure 5<\/b>).<\/p>\n [\/vc_column_text][vc_single_image image=”4863″ img_size=”full”][vc_column_text single_style=””]<\/p>\n (a)<\/b> Dopamine is synthesized from the amino acids, phenylalanine<\/i><\/b> or tyrosine<\/i><\/b> via sequential reactions catalyzed primarily by phenylalanine hydroxylase, tyrosine hydroxylase, and DOPA decarboxylase (right panel<\/i><\/b>). (b)<\/b> Major projection pathway of the biogenic amine neurotransmitter system in the human brain. Shown are the projections of the dopamine system<\/i><\/b> using the neurotransmitter (left panel<\/i><\/b>). The views are midsagittal sections through the human brain, depicting the medial surface of the right hemisphere; the front pole is at left. In each image, the primary source of the biogenic amine is bold type and colored accordingly.<\/p>\n [\/vc_column_text][vc_column_text single_style=””]<\/p>\n In recent years, abnormalities of dopamine production, transmission, and reception have been associated with the following:<\/p>\n [\/vc_column_text][vc_column_text single_style=””]<\/p>\n [\/vc_column_text][vc_column_text single_style=””]<\/p>\n (iv) Acetylcholine:<\/b> Unlike the serotonergic and dopaminergic systems, the cholinergic system was not vigorously studied in individual with ASD until the beginning of the current century. A post-mortem study, nevertheless, showed reduction in the numbers of acetylcholine receptors (the so-called ionotropic nicotinic receptors, nAChRs<\/i><\/b>), in the parietal lobes of individuals with ASD [6]. Since then, it has been determined that the reduced numbers of nicotinic receptor cells are found to be widespread in the brains of autistic individuals; with possible implications for understanding disabilities of attention, memory and learning, as well as possibly the imbalance between excitatory and inhibitory brain activity in ASD. In this context, the case for developing treatments essentially targeting nicotinic receptor cells has been widely discussed.<\/p>\n [\/vc_column_text][vc_column_text single_style=””]<\/p>\n (v) Oxytocin:<\/b> The role of oxytocin in sexual behaviors and childbirth was known nearly a century ago. Oxytocin is a naturally occurring nine-peptide amino acid<\/i><\/b>, synthesized in the hypothalamus and stored and released by the posterior pituitary. Oxytocin is important in a broad range of behaviors, including bonding, nurturing, and social recognition. Through these behaviors, along with others, oxytocin is thought to facilitate the development of attachment and social skills. For example, in humans, parental oxytocin levels have been associated with parental touch and engagement, thus creating a \u2018parent-infant dyad<\/b><\/i>\u2019 through which bonding and learning occur. Considering its role in social behavior, the potential of oxytocin as a therapeutic agent for social difficulties in ASD is a focus of current research (Figure 6<\/b>).<\/p>\n [\/vc_column_text][vc_single_image image=”4869″ img_size=”full”][vc_column_text single_style=””]<\/p>\n Oxytocin<\/i><\/b> is a naturally occurring nine-peptide amino acid that is synthesized in the hypothalamus and stored and released by the posterior pituitary. Oxytocin is important in a broad range of behaviors, including bonding, nurturing, and social recognition. Vasopressin is structurally similar to oxytocin. Vasopressin<\/i><\/b> is a nine-amino acid peptide hormone synthesized by hippocampal magnocellular and parvocellular neurons. It is synthesized as pre-pro-vasopressin in the neuron cell bodies and is cleaved into vasopressin prior to reaching the posterior pituitary, where it is then released. Vasopressin is involved in multiple systemic functions, including maintenance of cardiovascular homeostasis, increased water retention, and regulation of the body\u2019s response to stress. [ACTH \u2013 adreno corticotropic hormone; \u03b1-MSH \u2013 alpha-melanocyte-stimulating hormone]<\/p>\n [\/vc_column_text][vc_column_text single_style=””]<\/p>\n [\/vc_column_text][vc_column_text single_style=””]<\/p>\n Findings from a spate of research studies are, however, quite mixed [7]. So, the jury is still out as to the role or reduced oxytocin production\/transportation\/reception as a contributory case of ASD; also, as to the usefulness of oxytocin-based treatments.<\/p>\n [\/vc_column_text][vc_column_text single_style=””]<\/p>\n (vi) Vasopressin: Vasopressin is a nine-amino acid peptide hormone<\/i><\/b><\/b> synthesized by hippocampal magnocellular and parvocellular neurons. It is synthesized as pre-pro-vasopressin in the neuron cell bodies and is cleaved into vasopressin prior to reaching the posterior pituitary, where it is then released. It is involved in multiple systemic functions, including maintenance of cardiovascular homeostasis, increased water retention, and regulation of the body\u2019s response to stress (Figure 6<\/b>).<\/p>\n [\/vc_column_text][vc_column_text single_style=””]<\/p>\n Besides, vasopressin, through neuronal projections in the brain, is considered to be involved in various social and cognitive functions, including anxiety, fear, and aggression. Vasopressin is structurally similar to oxytocin;<\/i><\/b> preclinical and clinical evidence suggests that these hormones work together to influence social behaviors, including love, sexual behavior, and parental behavior. Using animal studies, it has been shown that the hormone vasopressin has some role in the regulation of social behavior. On these grounds, it has been postulated to play a role in causing ASD, and studies of oxytocin and vasopressin are frequently undertaken together [8].<\/p>\n [\/vc_column_text][vc_column_text single_style=””]<\/p>\n [\/vc_column_text][vc_column_text single_style=””]<\/p>\n (vii) Brain-derived neurotrophic factor (BDNF) and Reelin:<\/b> BDNF and Reelin, in humans, are encoded by the BDNF<\/i><\/b> and RELN<\/i><\/b> genes, respectively [9 -10].<\/p>\n [\/vc_column_text][vc_column_text single_style=””]<\/p>\n BDNF<\/b> is one of the neurotropic factors that supports differentiation, maturation, and survival of neurons in the nervous system. BDNF exhibits neuroprotective effects under adverse conditions, for example, glutamatergic stimulation, cerebral ischemia, hypoglycemia, and neurotoxicity. Moreover, BDNF promotes and controls growth of neo-neurons from neural stem cells (neurogenesis).<\/p>\n [\/vc_column_text][vc_column_text single_style=””]<\/p>\n Reelin<\/b> is a large secreted extracellular matrix glycoprotein that helps regulate the process of neuronal migration and positioning in the developing brain by controlling cell-cell interactions. Besides this important role in early development, reelin continues to work in the adult brain. Thus, during embryonic development and adulthood, reelin exerts several critical functions in the brain such as, the regulation of neuronal migration, dendritic growth and branching, dendritic spine formation, as well as synaptogenesis and synaptic plasticity.<\/p>\n [\/vc_column_text][vc_column_text single_style=””]<\/p>\n Because BDNF and reelin act in concert to regulate many processes during neural development and maintenance, including cell migration and neural plasticity,<\/i><\/b> the question that needs to be addressed is, whether the abnormalities of brain anatomy that had been established might result from neurotropic abnormalities – i.e., abnormalities in those neurochemicals that are significantly involved in constructing and positioning nerve cells in the developing embryo and fetus, and thereafter renewing and maintaining them.<\/p>\n [\/vc_column_text][vc_column_text single_style=””]<\/p>\n As mentioned earlier, serotonin, which is actively involved in brain-building pre- and postnatally, is also known to express in abnormal levels or quantities in the autistic brain; and GABA, which is a neurotrophins as well as major neuromodulator, has been shown to be depleted or expressed at reduced levels in the brains of individuals with autism. Unlike serotonin and GABA, investigation of the expression levels of BDNF and reelin has not generated consistent findings. As a result, uncertainty remains, regarding the potential role of both BDNF and reelin in the genetic and neurobiological bases of autism.<\/p>\n [\/vc_column_text][vc_column_text single_style=””]<\/p>\n (xiii) Norepinephrine (aka noradrenalin):<\/b> Norepinephrine appears to have little or any explanatory value for ASD when considered alone (Figure 7)<\/b>.<\/p>\n [\/vc_column_text][vc_single_image image=”4864″ img_size=”full”][vc_column_text single_style=””]<\/p>\n (a)<\/b> The amino acid tyrosine<\/i><\/b> is the precursor for all three catecholamines, viz., dopamine, norepinephrine, and epinephrine. Dopamine is derived from the amino acid tyrosine. Norepinephrine is produced from dopamine and is a precursor molecule for the hormone epinephrine (right panel<\/i><\/b>). (b)<\/b> Major projection pathways of the catecholamine neurotransmitter systems in the human brain. Shown are the projections of the norepinephrine<\/i><\/b> and epinephrine systems<\/i><\/b> using the neurotransmitters (left panel<\/i><\/b>). The views are midsagittal sections through the human brain, depicting the medial surface of the right hemisphere; the front pole is at left. In each image, the primary source of the biogenic amine is bold type and colored accordingly.<\/p>\n [\/vc_column_text][vc_column_text single_style=””]<\/p>\n Nonetheless, the adrenal glands form part of the hypothalamic-pituitary-adrenal axis (HPA)<\/i><\/b>. HPA is a major component of neuroendocrine system that governs reactions pertaining to stress, thus regulates many body processes, as next below, cortisol.<\/p>\n [\/vc_column_text][vc_column_text single_style=””]<\/p>\n (ix) Cortisol:<\/b> cortisol is a steroid hormone that is secreted by the adrenal glands<\/i><\/b> (which sit on top of each kidney) in response to stress. Variations in cortisol levels are associated with the \u2018sleep-wake cycle.<\/i><\/b>\u2019 Observations of vulnerability to anxiety disorders, as well sleep disturbances in children with ASD, have led to some earlier studies of cortisol level. Since then, studies have continued somewhat intermittently, and with mixed findings.<\/p>\n [\/vc_column_text][vc_column_text single_style=””]<\/p>\n (x) Testosterone:<\/b> The higher incidence of autism in male individuals might provide valuable clues to the etiology of the condition, which has been described as an \u2018extreme of the male brain\u2019 [11]. According to the \u2018extreme male brain (EMB)<\/i><\/b>\u2019 theory that postulates exposure to abnormally high levels of testosterone in utero<\/i><\/b> could result in excessively masculinized brain development in individuals, who subsequently diagnosed with ASD. This theory needs further validation from other independent research groups to strengthen the case as hypothesized. However, an \u2018extreme male brain\u2019 might throw light on something to sex-specific genetic effects,<\/p>\n [\/vc_column_text][vc_column_text single_style=””]<\/p>\n [\/vc_column_text][vc_column_text single_style=””]<\/p>\n In fact, there is some evidence indicating that brain development in females diagnosed with ASD, as well as in males with ASD, resembles brain development in typically developing (TD) males, rather than TD females.<\/p>\n [\/vc_column_text][vc_column_text single_style=””]<\/p>\n\n
\n<\/a><\/li>\nFigure 1. Distribution of Biogenic Amine Neurotransmitters in the Human Brain.<\/h3>\n
Figure 2. Biosynthetic Pathway and Distribution of Serotonin Neurotransmitter in the Human Brain.<\/h3>\n
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Figure 3. Glutamate Synthesis and Cycling.<\/h3>\n
Figure 4. GABA Synthesis, Release, and Uptake.<\/h3>\n
Figure 5. Biosynthetic Pathway and Distribution of Dopamine Neurotransmitter in the Human Brain.<\/h3>\n
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Figure 6. Neuropeptide Amino Acid Sequences \u2013 Pituitary Peptides.<\/h3>\n
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Figure 7. Biosynthetic Pathway and Distribution of Norepinephrine and Epinephrine Neurotransmitters in the Human Brain.<\/h3>\n
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Table 1. Partial list of neurotransmitters organized by chemical properties.<\/h3>\n
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