Gastrointestinal dysfunction in autism displayed by altered motility and achalasia in
            <i>Foxp1</i>
            <sup>+/−</sup>
            mice

Fröhlich, Henning; Kollmeyer, Marie Luise; Linz, Valerie Catherine; Stuhlinger, Manuel; Groneberg, Dieter; Reigl, Amelie; Zizer, Eugen; Friebe, Andreas; Niesler, Beate; Rappold, Gudrun

doi:10.1073/pnas.1911429116

Cited by 37 publications

(31 citation statements)

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“…For PG + M, two of the significantly associated SNPs, 19:18793695 and rs13097265, have been previously linked to Barrett’s esophagus and esophageal adenocarcinoma 82 (Supplementary Table 4 ). rs13097265 is located ~60 kb from the FOXP1 gene, and recently a mouse study 83 has shown that Foxp1 protein is expressed in all layers of the murine GI tract (including the myenteric plexus, which is part of the enteric nervous system and regulates gut peristalsis and transit). Altered motility and achalasia has been observed in Foxp1 +/− mice.…”

Section: Discussionmentioning

confidence: 99%

GWAS of peptic ulcer disease implicates Helicobacter pylori infection, other gastrointestinal disorders and depression

et al. 2021

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Genetic factors are recognized to contribute to peptic ulcer disease (PUD) and other gastrointestinal diseases, such as gastro-oesophageal reflux disease (GORD), irritable bowel syndrome (IBS) and inflammatory bowel disease (IBD). Here, genome-wide association study (GWAS) analyses based on 456,327 UK Biobank (UKB) individuals identify 8 independent and significant loci for PUD at, or near, genes MUC1, MUC6, FUT2, PSCA, ABO, CDX2, GAST and CCKBR. There are previously established roles in susceptibility to Helicobacter pylori infection, response to counteract infection-related damage, gastric acid secretion or gastrointestinal motility for these genes. Only two associations have been previously reported for duodenal ulcer, here replicated trans-ancestrally. The results highlight the role of host genetic susceptibility to infection. Post-GWAS analyses for PUD, GORD, IBS and IBD add insights into relationships between these gastrointestinal diseases and their relationships with depression, a commonly comorbid disorder.

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Section: Discussionmentioning

confidence: 99%

GWAS of peptic ulcer disease implicates Helicobacter pylori infection, other gastrointestinal disorders and depression

et al. 2021

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“…Amongst the results we found enrichment for neuromuscular and cardiac function in STRING analysis (S9-20). Some animal models such as FOXP1 , SHANK3 , NOS1 and CHD8 [ 74 , 92 , 94 , 96 , 97 ] have been developed for functional analysis of ASD candidate genes in the gastrointestinal system, which indicates that ASD genes may play an important role in this organ [ 95 ], and yet most research have been mainly focused on the brain in both human and animal models. A greater utilisation of the animal models to explore other systems such as the cardiac and gastrointestinal systems would be welcome.…”

Section: Discussionmentioning

confidence: 99%

Coupling of autism genes to tissue-wide expression and dysfunction of synapse, calcium signalling and transcriptional regulation

et al. 2020

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Autism Spectrum Disorder (ASD) is a heterogeneous disorder that is often accompanied with many co-morbidities. Recent genetic studies have identified various pathways from hundreds of candidate risk genes with varying levels of association to ASD. However, it is unknown which pathways are specific to the core symptoms or which are shared by the co-morbidities. We hypothesised that critical ASD candidates should appear widely across different scoring systems, and that comorbidity pathways should be constituted by genes expressed in the relevant tissues. We analysed the Simons Foundation for Autism Research Initiative (SFARI) database and four independently published scoring systems and identified 292 overlapping genes. We examined their mRNA expression using the Genotype-Tissue Expression (GTEx) database and validated protein expression levels using the human protein atlas (HPA) dataset. This led to clustering of the overlapping ASD genes into 2 groups; one with 91 genes primarily expressed in the central nervous system (CNS geneset) and another with 201 genes expressed in both CNS and peripheral tissues (CNS+PT geneset). Bioinformatic analyses showed a high enrichment of CNS development and synaptic transmission in the CNS geneset, and an enrichment of synapse, chromatin remodelling, gene regulation and endocrine signalling in the CNS+PT geneset. Calcium signalling and the glutamatergic synapse were found to be highly interconnected among pathways in the combined geneset. Our analyses demonstrate that 2/3 of ASD genes are expressed beyond the brain, which may impact peripheral function and involve in ASD co-morbidities, and relevant pathways may be explored for the treatment of ASD co-morbidities.

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“…Our Scn2a gtKO/gtKO mice had a similar ~15% reduced body weight compared to WT throughout life, but close to 80% of Scn2a gtKO/gtKO mice survive to adulthood. Another mouse model of neurodevelopmental disorder, Foxp1 -/-, also has failure to thrive at weaning unless a soft, highcalorie diet is provided [36] which we similarly provided a gel-based high-calorie food source. The combined phenomenon of failure to thrive in adolescence and overeating in adulthood in humans is also evident in Prader-Willi syndrome [37].…”

Section: Discussionmentioning

confidence: 99%

Characterization of a gene-trap knockout mouse model ofScn2aencoding voltage-gated sodium channel Nav1.2

Eaton

Zhang

et al. 2020

Preprint

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Recent large-scale genomic studies have revealed SCN2A as one of the most frequently mutated gene in patients with neurodevelopmental disorders including autism spectrum disorder and intellectual disability. SCN2A encodes for voltage-gated sodium channel isoform 1.2 (Nav1.2), which is mainly expressed in the central nervous system and responsible for the propagation of neuronal action potentials. Homozygous knockout (null) of Scn2a is perinatal lethal, whereas heterozygous knockout of Scn2a results in mild behavior abnormalities. To achieve a more substantial, but not complete, reduction of Scn2a expression, we characterized a Scn2a deficient mouse model using a targeted gene trap knockout (gtKO) strategy to recapitulate loss-of-function SCN2A disorders. This model produces viable homozygous mice (Scn2a gtKO/gtKO ) that can survive to adulthood, with markedly low but detectable Nav1.2 expression. Although Scn2a gtKO/gtKO adult mice possess normal olfactory, taste, hearing, and mechanical sensitivity, they have decreased thermal and cold tolerance. Innate behaviors are profoundly impaired including impaired nesting, marble burying, and mating. These mice also have increased food and water intake with subsequent increases in fecal excretion of more but smaller fecal boli. This novel Scn2a gene trap knockout mouse thus provides a unique model to study pathophysiology associated with Scn2a deficiency.

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Gastrointestinal dysfunction in autism displayed by altered motility and achalasia in Foxp1 ^+/− mice

Cited by 37 publications

References 50 publications

GWAS of peptic ulcer disease implicates Helicobacter pylori infection, other gastrointestinal disorders and depression

GWAS of peptic ulcer disease implicates Helicobacter pylori infection, other gastrointestinal disorders and depression

Coupling of autism genes to tissue-wide expression and dysfunction of synapse, calcium signalling and transcriptional regulation

Characterization of a gene-trap knockout mouse model ofScn2aencoding voltage-gated sodium channel Nav1.2

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Gastrointestinal dysfunction in autism displayed by altered motility and achalasia in Foxp1 +/− mice

Cited by 37 publications

References 50 publications

GWAS of peptic ulcer disease implicates Helicobacter pylori infection, other gastrointestinal disorders and depression

GWAS of peptic ulcer disease implicates Helicobacter pylori infection, other gastrointestinal disorders and depression

Coupling of autism genes to tissue-wide expression and dysfunction of synapse, calcium signalling and transcriptional regulation

Characterization of a gene-trap knockout mouse model ofScn2aencoding voltage-gated sodium channel Nav1.2

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Gastrointestinal dysfunction in autism displayed by altered motility and achalasia in Foxp1 ^+/− mice