Meta‐analysis of association between obsessive‐compulsive disorder and the 3′ region of neuronal glutamate transporter gene <i>SLC1A1</i>

Stewart, S. Evelyn; Mayerfeld, C.; Arnold, Paul; Crane, Jacquelyn; Ó'Dúshláine, Colm; Fagerness, Jesen; Yu, Dongmei; Scharf, Jeremiah M.; Chan, Elisa K.; Kassam, Faazil; Moya, Pablo R.; Wendland, Jens R.; Delorme, Richard; Richter, Margaret A.; Kennedy, James L.; Veenstra‐VanderWeele, Jeremy; Samuels, Jack; Greenberg, Benjamin D.; McCracken, James T.; Knowles, James A.; Fyer, Abby J.; Rauch, Scott L.; Riddle, Mark A.; Grados, Marco A.; Bienvenu, O. Joseph; Cullen, Bernadette; Wang, Youfa; Shugart, Yin Yao; Piacentini, John; Rasmussen, Steven A.; Nestadt, Gerald; Murphy, Dennis L.; Jenike, Michael A.; Cook, Edwin H.; Pauls, David L.; Hanna, Gregory L.; Mathews, Carol A.

doi:10.1002/ajmg.b.32137

Cited by 88 publications

(60 citation statements)

References 88 publications

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…Although the genetic studies show one of the highest effect sizes for association of the glutamatergic system and OCD, only few groups have reported findings related to imaging genetics in OCD and genetic variants of glutamatergic genes (Arnold et al, 2009a(Arnold et al, , 2009bWu et al, 2012). The results of these investigations coincide with findings from meta-analyses and GWAS; taken together, these observations support the involvement of the glutamatergic system in OCD (Stewart et al, 2013a(Stewart et al, , 2013bTaylor, 2013). The existing literature on imaging-genetic studies with respect to OCD provides evidence of increasing specificity of brain structure and/or activity findings exerted by variants in genes involved in the serotonergic (5-HTTLPR, HTR2A) and glutamatergic (SLC1A1, SAPAP) systems.…”

Section: Discussionsupporting

confidence: 63%

“…This stipulation led to the retrieval of a small collection of manuscripts describing association analyses of genetic variants with neuroimaging techniques in OCD (n = 8). The present study focused on the most significant and nominally significant genes associated with OCD as inclusion criteria by cross-referencing these publications with GWAS and meta-analyzed genetic association (Azzam and Mathews, 2003;Lin, 2007;Pooley et al, 2007;Stewart et al, 2013aStewart et al, , 2013bTaylor, 2013;Walitza et al, 2014b). A publication by Hoexter et al (2009) was not included in the review because it did not include genetic association results in addition to their findings of single-photon emission computed tomography or magnetic resonance imaging in OCD.…”

Section: Resultsmentioning

confidence: 99%

See 1 more Smart Citation

Imaging genetics in obsessive-compulsive disorder: Linking genetic variations to alterations in neuroimaging

Grünblatt

Hauser

Walitza

2014

Progress in Neurobiology

View full text Add to dashboard Cite

Obsessive-compulsive disorder (OCD) occurs in ∼1-3% of the general population, and its often rather early onset causes major disabilities in the everyday lives of patients. Although the heritability of OCD is between 35 and 65%, many linkage, association, and genome-wide association studies have failed to identify single genes that exhibit high effect sizes. Several neuroimaging studies have revealed structural and functional alterations mainly in cortico-striato-thalamic loops. However, there is also marked heterogeneity across studies. These inconsistencies in genetic and neuroimaging studies may be due to the heterogeneous and complex phenotypes of OCD. Under the consideration that genetic variants may also influence neuroimaging in OCD, researchers have started to combine both domains in the field of imaging genetics. Here, we conducted a systematic search of PubMed and Google Scholar literature for articles that address genetic imaging in OCD and related disorders (published through March 2014). We selected 8 publications that describe the combination of imaging genetics with OCD, and extended it with 43 publications of comorbid psychiatric disorders. The most promising findings of this systematic review point to the involvement of variants in genes involved in the serotonergic (5-HTTLPR, HTR2A), dopaminergic (COMT, DAT), and glutamatergic (SLC1A1, SAPAP) systems. However, the field of imaging genetics must be further explored, best through investigations that combine multimodal imaging techniques with genetic profiling, particularly profiling techniques that employ polygenetic approaches, with much larger sample sizes than have been used up to now.

show abstract

Section: Discussionsupporting

confidence: 63%

Section: Resultsmentioning

confidence: 99%

Imaging genetics in obsessive-compulsive disorder: Linking genetic variations to alterations in neuroimaging

Grünblatt

Hauser

Walitza

2014

Progress in Neurobiology

View full text Add to dashboard Cite

show abstract

“…Interestingly, they also found sexually dimorphic effect of MAO-A on genetic susceptibility to OCD. As mentioned above, an association between a glutamate transporter gene that encodes EAAT3 ( SLC1A1 ) and OCD was reported by several independent groups ( 56 -59 ), although a meta-analysis of these data did not identify signifi cant association ( 59 ). Glutamate system genes warrant further investigation as functional candidates for OCD, based on multiple lines of evidence, including: 1) elevated glutamate levels in brain regions within OCD patients in magnetic resonance spectroscopy studies ( 76 -78 ); 2) corticostriatal glutamatergic mediation of stereotypic behavior in mice ( 79 ) and results of glutamate modulating agent augmentation studies in OCD ( 80 , 81 ).…”

Section: Neuropsychiatric Disorders Frequently Comorbid With Ocdmentioning

confidence: 98%

“…and several groups reported an association between this gene and OCD ( 56 -59 ). Most recently, a meta-analysis of SLC1A1 found only weak associations between OCD and a single nucleotide polymorphism (SNP) rs301443 in the overall sample and between OCD and SNP rs12682807 in males-only, neither of which maintained signifi cance following correction for multiple testing ( 59 ). The second genome-wide scan was performed in 219 families at an approximate density of 9 cM, and found suggestive signals from chromosomes 3q27-28, 7p, 1q, 15q, and 6q ( 54 ).…”

Section: Neuropsychiatric Disorders Frequently Comorbid With Ocdmentioning

confidence: 99%

Obsessive Compulsive Disorder

Murphy¹,

Stewart²,

Obregon³

2016

The Medical Basis of Psychiatry

View full text Add to dashboard Cite

OCD is the fourth most common neuropsychiatric disorder with lifetime prevalence estimates of 0.4-3.5%. Family and twin studies suggest a strong genetic component, and molecular genetic studies are being carried out to identify genes contributing risk to OCD. It is postulated as a frontal-striatal disorder and functional neuroimaging studies provide a strong support for the dysfunction of cortico-striatal-thalamic-cortical neurocircuit. OCD can be secondary to a variety of medical conditions that range from deteriorative neurological illness, to head injury, and to autoimmune disorders. Few reports and no controlled studies exist in the treatment of acquired/secondary OCD. Both CBT and pharmacotherapy are effective fi rst-line treatment modalities for OCD. Brain stimulation and/or psychosurgery have been tried with varying success in treatment of refractory OCD. Environmental, genetic, and clinical factors interact in a complex fashion in the individual patient. This chapter will examine OCD from the medical perspective.Keywords Obsessive compulsive disorder · Cortical-striatal-thalamo-cortical circuit · Genetics · Neuroimaging · Autoimmune · Treatment IntroductionAs defi ned in DSM-5, obsessive compulsive disorder (OCD) is characterized by obsessions (recurrent, unwanted, and distressing thoughts, images, or impulses) and/or compulsions (complex, repetitive, rule-governed behaviors that the patient feels driven to perform). Patients usually try to actively dismiss obsessions or neutralize them by seeking reassurance, avoiding situational triggers, or engaging in compulsions. Obsessions and compulsions are maladaptive, and lead to impaired functioning. They typically center on four themes: contamination, sexual/aggressive/checking, and ordering and symmetry. Common compulsions include excessive cleaning, checking behaviors, ordering and arranging rituals, counting, and repeating routine activities. Compulsions usually involve observable behaviors (e.g., hand-washing) but may also consist of covert mental rituals (e.g., counting, or ritualized performance of mental math). Symptom themes can vary over the course of the illness but those without a personal or family history of tics are more likely to have more frequent contamination themes. In the DSM-5, hoarding has been categorized as a distinct disorder, and is no longer considered a specifi c form of OCD. The addition of a separate diagnosis is supported by extensive research suggesting that, although the two disorders can co-occur, patients with symptoms of hoarding have a number of signifi cant phenomenological differences than those with OCD, including distinct cognitive processes, reinforcement patterns, and response to treatments commonly used to address symptoms of OCD ( 1 ).The proposed lifetime prevalence of OCD in the pediatric and adult population ranges from 0.4 to 3.5% in national and international epidemiological samples ( 2 -7 ). Approximately half of all OCD patients fi rst present in childhood, before age 15 ( 8 ) with biphasic symptom p...

show abstract

“…One of the more consistently replicated genetic findings in OCD is an association with the neuronal glutamate transporter SLC1A1 (protein: EAAT3 or EAAC1) [18][19][20][21][22][23][24] , although a recent meta-analysis showed only a modest association of 2/9 SNPs with OCD 25 , and SLC1A1 has not emerged as a probable locus from recent GWAS studies 15,16 . Findings cluster in the 3′ region, with most evidence for association with the rs301430C allele.…”

Section: Slc1a1mentioning

confidence: 99%

Dissecting OCD Circuits: From Animal Models to Targeted Treatments

Ahmari¹,

Dougherty²

2015

Anxiety Disorders

View full text Add to dashboard Cite

Obsessive Compulsive Disorder (OCD) is a chronic, severe mental illness with up to 2-3% prevalence worldwide, which has been classified as one of the world's 10 leading causes of illness-related disability according to the World Health Organization, largely because of the chronic nature of disabling symptoms 1 . Despite the severity and high prevalence of this chronic and disabling disorder, there is still relatively limited understanding of its pathophysiology. However, this is now rapidly changing due to development of powerful technologies that can be used to dissect the neural circuits underlying pathologic behaviors. In this article, we describe recent technical advances that have allowed neuroscientists to start identifying the circuits underlying complex repetitive behaviors using animal model systems. In addition, we review current surgical and stimulation-based treatments for OCD that target circuit dysfunction. Finally, we discuss how findings from animal models may be applied in the clinical arena to help inform and refine targeted brain stimulation-based treatment approaches.

show abstract

Meta‐analysis of association between obsessive‐compulsive disorder and the 3′ region of neuronal glutamate transporter gene SLC1A1

Cited by 88 publications

References 88 publications

Imaging genetics in obsessive-compulsive disorder: Linking genetic variations to alterations in neuroimaging

Imaging genetics in obsessive-compulsive disorder: Linking genetic variations to alterations in neuroimaging

Obsessive Compulsive Disorder

Dissecting OCD Circuits: From Animal Models to Targeted Treatments

Contact Info

Product

Resources

About