Linkage and association analysis at the serotonin transporter (<i>SLC6A4</i>) locus in a rigid‐compulsive subset of autism

McCauley, Jacob L.; Olson, Lana M.; Dowd, Michael; Amin, Taneem; Steele, A.; Blakely, Randy D.; Folstein, Susan E.; Haines, Jonathan L.; Sutcliffe, James S.

doi:10.1002/ajmg.b.20151

Cited by 131 publications

(123 citation statements)

References 39 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%

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%

Neonatal serotonin depletion alters behavioral responses to spatial change and novelty

et al. 2007

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“…Elucidation of the genetic variants and their biological impact offers the possibility of prenatal counselling, earlier identification of at-risk children, development of animal models and pursuit of biology-informed therapeutics. With these goals, we and others have pursued genome-wide linkage analyses of autism, identifying a strong linkage signal at 17q11.2-17q21 (Cook et al 1997;McCauley et al 2004;Stone et al 2004;Cantor et al 2005;Sutcliffe et al 2005). Although the linkage signal we obtained was already highly significant, particularly for a complex neurobehavioral disorder (HLODw5), linkage increased substantially when male-only subject families were included in the analysis (HLODw8).…”

Section: Introductionmentioning

confidence: 88%

Enhanced activity of human serotonin transporter variants associated with autism

Prasad

Steiner

Sutcliffe

et al. 2008

Phil. Trans. R. Soc. B

119

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Rare, functional, non-synonymous variants in the human serotonin (5-hydroxytryptamine, 5-HT) transporter (hSERT) gene (SLC6A4) have been identified in both autism and obsessive-compulsive disorder (OCD). Within autism, rare hSERT coding variants associate with rigid-compulsive traits, suggesting both phenotypic overlap with OCD and a shared relationship with disrupted 5-HT signalling. Here, we document functional perturbations of three of these variants: Ile425Leu; Phe465Leu; and Leu550Val. In transiently transfected HeLa cells, the three variants confer a gain of 5-HT transport phenotype. Specifically, enhanced SERT activity was also observed in lymphoblastoid lines derived from mutation carriers. In contrast to previously characterized Gly56Ala, where increased transport activity derives from catalytic activation, the three novel variants exhibit elevated surface density as revealed through both surface antagonist-binding and biotinylation studies. Unlike Gly56Ala, mutants Ile425Leu, Phe465Leu and Leu550Val retain a capacity for acute PKG and p38 MAPK regulation. However, both Gly56Ala and Ile425Leu demonstrate markedly reduced sensitivity to PP2A antagonists, suggesting that deficits in trafficking and catalytic modulation may derive from a common basis in perturbed phosphatase regulation. When expressed stably from the same genomic locus in CHO cells, both Gly56Ala and Ile425Leu display catalytic activation, accompanied by a striking loss of SERT protein.

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“…They had a median age of 5.6 years (range, 4.8-11); all had a particular phenotype, with unusual motor agitation and a high number of various stereotypies. Moreover, four patients with a median age of 7 years (range 2-7) had high HVA/5-HIAA (patients 1,5,12,14).…”

Section: Rd and Csf Neurotransmittersmentioning

confidence: 99%

Evaluation of CSF neurotransmitters and folate in 25 patients with Rett disorder and effects of treatment

Temudo

Ríos

Prior

et al. 2009

Brain and Development

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Background: Rett disorder (RD) is a progressive neurodevelopmental entity caused by mutations in the MECP2 gene. It has been postulated that there are alterations in the levels of certain neurotransmitters and folate in the pathogenesis of this disease. Here we re-evaluated this hypothesis. Patients and methods: We evaluated CSF folate, biogenic amines and pterines in 25 RD patients. Treatment with oral folinic acid was started in those cases with low folate. Patients were clinically evaluated and videotaped up to 6 months after therapy. Results: CSF folate was below the reference values in 32% of the patients. Six months after treatment no clinical improvement was observed. Three of the four patients with the R294X mutation had increased levels of a dopamine metabolite associated to a particular phenotype. Three patients had low levels of a serotonin metabolite. Two of them were treated with fluoxetine and one showed clinical improvement. No association was observed between CSF folate and these metabolites, after adjusting for the patients age and neopterin levels. Conclusion: Our results support that folinic acid supplementation has no significant effects on the course of the disease. We report discrete and novel neurotransmitter abnormalities that may contribute to the pathogenesis of RD highlighting the need for further studies on CSF neurotransmitters in clinically and genetically well characterized patients.

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Linkage and association analysis at the serotonin transporter (SLC6A4) locus in a rigid‐compulsive subset of autism

Cited by 131 publications

References 39 publications

Neonatal serotonin depletion alters behavioral responses to spatial change and novelty

Neonatal serotonin depletion alters behavioral responses to spatial change and novelty

Enhanced activity of human serotonin transporter variants associated with autism

Evaluation of CSF neurotransmitters and folate in 25 patients with Rett disorder and effects of treatment

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