The Genetics of Autism

Muhle, Rebecca; Trentacoste, Stephanie; Rapin, Isabelle

doi:10.1542/peds.113.5.e472

Cited by 1,083 publications

(808 citation statements)

References 224 publications

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“…(Chugani et al, 1999;Chandana et al, 2005). A serotonergic (5-HT) deficit during cortical development, moreover, is compatible with reports of treatment successes using serotonin uptake blockers as well as with genetic linkage studies suggesting impairments in genes linked to proper serotonin neurotransmission (Cabelli et al, 1995;Klauck et al, 1997;Anderson et al, 2002;Veenstra-VanderWeele et al, 2002;Conroy et al, 2004;Coutinho et al, 2004;McCauley et al, 2004;Muhle et al, 2004;Murphy et al, 2004;Nabi et al, 2004;Coon et al, 2005;Mulder et al, 2005;Scott and Deneris, 2005;Whitaker-Azmitia, 2005). It is interesting in this context to note that a defective serotonergic innervation is also compatible with alterations of brainstem segmentation genes such as engrailed or Hox 2, which have been implicated in autism (Polleux and Lauder, 2004;Bartlett et al, 2005;Benayed et al, 2005).…”

Section: Neonatal Serotonin Depletions As An Animal Model For Autismsupporting

confidence: 69%

“…Thus, other cognitive-emotional behavioral features might be under the control of sex hormones as well. Substantial sex dimorphism does exist in several disorders that involve 5-HT imbalances, including autism, depression and anxiety disorders (Earls, 1987;Halbreich and Kahn, 2001;Muhle et al, 2004). Serotonin may not have the same saliency in male and female cortical development and later plasticity, rendering each sex differentially susceptible to 5-HT imbalances in various brain regions.…”

Section: Sex Differencesmentioning

confidence: 99%

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Neonatal serotonin depletion alters behavioral responses to spatial change and novelty

et al. 2007

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Multiple brain disorders that show serotonergic imbalances have a developmental onset. Experimental models indicate a role for serotonin as a morphogen in brain development. To selectively study the effects of serotonin depletions on cortical structural development and subsequent behavior, we developed a mouse model in which a serotonin neurotoxin, 5,7-dihydroxytryptamine (5,7-DHT), is injected into the medial forebrain bundle (mfb) on the day of birth. Littermates with saline injections into the mfb and age matched mice served as controls. This study characterized the extent and duration of serotonergic denervation after the selective neonatal lesion and investigated effects on exploratory behavior, spatial learning and anxiety in mice of both sexes. We report significant decreases in the serotonergic (5-HT) innervation to cortex and hippocampus, but not to subcortical forebrain structures in 5,7-DHT-lesioned mice. The depletion of 5-HT fibers in cortical areas was long lasting in lesioned mice but autoradiographic binding to high affinity 5-HT transporters was only transiently reduced. Male but not female lesioned mice reduced their exploration significantly in response to spatial rearrangement and object novelty, suggesting increased anxiety in response to change but normal spatial cognition. Our data show that developmental disruptions in the serotonergic innervation of cortex and hippocampus are sufficient to induce permanent, sex specific, behavioral alterations. These results may have significant implications for understanding brain disorders presenting with cortical morphogenetic abnormalities and altered serotonin neurotransmission, such as autism, schizophrenia and affective disorders.

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Section: Neonatal Serotonin Depletions As An Animal Model For Autismsupporting

confidence: 69%

Section: Sex Differencesmentioning

confidence: 99%

Neonatal serotonin depletion alters behavioral responses to spatial change and novelty

et al. 2007

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“…With the exception of the socially transmitted food preference task, where food consumption was impaired in both sexes, male neonatally 5,7-DHT-lesioned male mice were affected uniquely or more markedly than female lesioned mice. This may be highly relevant in regards to autism where, by most accounts, four times as many males as females are diagnosed [87,107,118,126]. Our own developmental observations in male and female mice [31] together with the data from Chugani's group [27,28] suggest that magnitude of an early postnatal peak or elevation in cortical serotonergic innervation is sex specific.…”

Section: Discussionmentioning

confidence: 67%

Modeling early cortical serotonergic deficits in autism

Boylan

Blue

Höhmann

2007

Behavioural Brain Research

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Autism is a developmental brain disorder characterized by deficits in social interaction, language and behavior. Brain imaging studies demonstrate increased cerebral cortical volumes and micro-and macroscopic neuroanatomic changes in children with this disorder. Alterations in forebrain serotonergic function may underlie the neuroanatomic and behavioral features of autism. Serotonin is involved in neuronal growth and plasticity and these actions are likely mediated via serotonergic and glutamatergic receptors. Few animal models of autism have been described that replicate both etiology and pathophysiology. We report here on a selective serotonin (5-HT) depletion model of this disorder in neonatal mice that mimics neurochemical and structural changes in cortex and, in addition, displays a behavioral phenotype consistent with autism. Newborn male and female mice were depleted of forebrain 5-HT with injections of the serotonergic neurotoxin, 5,7-dihydroxytryptamine (5,7-DHT), into the bilateral medial forebrain bundle (mfb). Behavioral testing of these animals as adults revealed alterations in social, sensory and stereotypic behaviors. Lesioned mice showed significantly increased cortical width. Serotonin immunocytochemistry showed a dramatic long-lasting depletion of 5-HT containing fibers in cerebral cortex until postnatal day (PND) 60. Autoradiographic binding to high affinity 5-HT transporters was significantly but transiently reduced in cerebral cortex of 5,7-DHT-depleted mice. AMPA glutamate receptor binding was decreased at PND 15. We hypothesize that increased cerebral cortical volume and sensorimotor, cognitive and social deficits observed in both 5-HT-depleted animals and in individuals with autism, may be the result of deficiencies in timely axonal pruning to key cerebral cortical areas.

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“…4,7,8 It has been estimated that 10-15 genes may be implicated in the regulation of the complex genetic risk of autism-spectrum disorders. [9][10][11][12] However, the risk is not conferred in a Mendelian fashion and identification of these genes has been hampered further by the probably small population effect sizes of each of them, and the lack of clear pathophysiology hints to suggest particularly strong candidate genes. Therefore, the typical approach to-date has been the performance of genome scans.…”

Section: Introductionmentioning

confidence: 99%

A heterogeneity-based genome search meta-analysis for autism-spectrum disorders

et al. 2005

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Autism and autism-spectrum disorders exhibit high heritability, although specific susceptibility genes still remain largely elusive. We performed a heterogeneity-based genome search meta-analysis (HEGESMA) of nine genome scans on autism or autism-spectrum disorders. Each genome scan was separated in 30 cM bins and the maximum linkage statistic from each bin was ranked. Significance for each bin's average rank and for between-scan heterogeneity (dis-similarity in the average ranks) was obtained through Monte Carlo tests. For autism, data from 771 affected sibpairs were synthesized across six separate genome scans. Region 7q22-q32 reached genome-wide significance both in weighted and unweighted analyses, with evidence for significantly low between-scan heterogeneity. The flanking chromosomal region 7q32-qter reached the less stringent threshold of suggestive significance, with no evidence for low between-scan heterogeneity. For autism-spectrum disorders (634 affected sibpairs from five separate scans), no chromosomal region reached genome-wide significance. However, suggestive significance was reached for the chromosomal regions 17p11.2-q12 and 10p12-q11.1 in weighted analyses. There was evidence for significantly high between-scan heterogeneity for the former region. The meta-analysis suggests that the 7q22-q32 region should be further scrutinized for autism susceptibility genes, while autism-spectrum disorders seem to have quite diverse linkage signals across scans, possibly suggesting genetic heterogeneity across subsyndromes and subpopulations.

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The Genetics of Autism

Cited by 1,083 publications

References 224 publications

Neonatal serotonin depletion alters behavioral responses to spatial change and novelty

Neonatal serotonin depletion alters behavioral responses to spatial change and novelty

Modeling early cortical serotonergic deficits in autism

A heterogeneity-based genome search meta-analysis for autism-spectrum disorders

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