Visual impairment in FOXG1-mutated individuals and mice

Boggio, Elena; Pancrazi, Laura; Gennaro, Mariangela; Rizzo, Caterina Lo; Mari, Francesca; Meloni, Ilaria; Ariani, Francesca; Panighini, Anna; Novelli, Elena; Biagioni, Martina; Strettoi, Enrica; Hayek, Joussef; Rufa, Alessandra; Pizzorusso, Tommaso; Renieri, Alessandra; Costa, Mario

doi:10.1016/j.neuroscience.2016.03.027

Cited by 40 publications

(41 citation statements)

References 54 publications

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“…In recent years, the visual cortex has become an important model to assess cortical processing in mouse model of neurodevelopmental disorders ( 12 , 27 , 28 ). For instance, the use of visually evoked responses has been suggested as a relatively common quantitative method to directly compare cortical function in RTT patients and mouse models carrying mecp2 mutations ( 11 , 12 ).…”

Section: Discussionmentioning

confidence: 99%

Searching for biomarkers of CDKL5 disorder: early-onset visual impairment in CDKL5 mutant mice

Mazziotti

Lupori

Sagona

et al. 2017

Human Molecular Genetics

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CDKL5 disorder is a neurodevelopmental disorder still without a cure. Murine models of CDKL5 disorder have been recently generated raising the possibility of preclinical testing of treatments. However, unbiased, quantitative biomarkers of high translational value to monitor brain function are still missing. Moreover, the analysis of treatment is hindered by the challenge of repeatedly and non-invasively testing neuronal function. We analyzed the development of visual responses in a mouse model of CDKL5 disorder to introduce visually evoked responses as a quantitative method to assess cortical circuit function. Cortical visual responses were assessed in CDKL5 null male mice, heterozygous females, and their respective control wild-type littermates by repeated transcranial optical imaging from P27 until P32. No difference between wild-type and mutant mice was present at P25-P26 whereas defective responses appeared from P27-P28 both in heterozygous and homozygous CDKL5 mutant mice. These results were confirmed by visually evoked potentials (VEPs) recorded from the visual cortex of a different cohort. The previously imaged mice were also analyzed at P60–80 using VEPs, revealing a persistent reduction of response amplitude, reduced visual acuity and defective contrast function. The level of adult impairment was significantly correlated with the reduction in visual responses observed during development. Support vector machine showed that multi-dimensional visual assessment can be used to automatically classify mutant and wt mice with high reliability. Thus, monitoring visual responses represents a promising biomarker for preclinical and clinical studies on CDKL5 disorder.

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Section: Discussionmentioning

confidence: 99%

Searching for biomarkers of CDKL5 disorder: early-onset visual impairment in CDKL5 mutant mice

Mazziotti

Lupori

Sagona

et al. 2017

Human Molecular Genetics

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“…37 Less than 10 adults with FOXG1 mutations have been described so far, mainly within large series of patients. [37][38][39] Their phenotype is characterised by severe postnatal microcephaly, severe ID, absent language, autistic traits, epilepsy 38 and a typical hyperkineticdyskinetic movement disorder. 40 Poor sleep patterns, irritability in infancy, unexplained episodes of crying, recurrent aspiration and GERD have also been reported.…”

Section: Patients With Foxg1 Pathogenic Variantsmentioning

confidence: 99%

Phenotypes in adult patients with Rett syndrome: results of a 13-year experience and insights into healthcare transition

et al. 2020

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BackgroundRett syndrome is a complex genetic disorder with age-specific manifestations and over half of the patients surviving into middle age. However, little information about the phenotype of adult individuals with Rett syndrome is available, and mainly relies on questionnaires completed by caregivers. Here, we assess the clinical manifestations and management of adult patients with Rett syndrome and present our experience in transitioning from the paediatric to the adult clinic.MethodsWe analysed the medical records and molecular data of women aged ≥18 years with a diagnosis of classic Rett syndrome and/or pathogenic variants in MECP2, CDKL5 and FOXG1, who were in charge of our clinic.ResultsOf the 50 women with classic Rett syndrome, 94% had epilepsy (26% drug-resistant), 20% showed extrapyramidal signs, 40% sleep problems and 36% behavioural disorders. Eighty-six % patients exhibited gastrointestinal problems; 70% had scoliosis and 90% low bone density. Breathing irregularities were diagnosed in 60%. None of the patients had cardiac issues. CDKL5 patients experienced fewer breathing abnormalities than women with classic Rett syndrome.ConclusionThe delineation of an adult phenotype in Rett syndrome demonstrates the importance of a transitional programme and the need of a dedicated multidisciplinary team to optimise the clinical management of these patients.

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“…EEG is relatively inexpensive compared to other imaging methodologies. Similar to MRI, EEG holds high translational potential from the laboratory to the clinic and also holds high translational potential from animal models to humans, as similar neurophysiological signals and even event related paradigms can be applied across species [32–34]. …”

Section: Developmental Neuroscience Methods To Study Early Brain Devementioning

confidence: 99%

The emergence of autism spectrum disorder

Varcin

Jeste

2017

Current Opinion in Psychiatry

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Purpose of review We review studies of infants at risk for autism spectrum disorder (ASD), proposing that the earliest manifestations of disrupted brain development can shed light on pre-behavioural markers of risk and mechanisms underlying the heterogeneity of ASD. Recent findings Prospective, longitudinal studies of infants at-risk for ASD have revealed that behavioural signs of ASD are generally not observed until the second year of life. The developmental signs within the first year are often subtle and rooted in processes outside the core diagnostic domains of ASD, such as motor and visual-perceptual function. However, studies examining early brain development and function have identified a myriad of atypicalities within the first year that are associated with risk for ASD. Summary Longitudinal studies of high risk infants provide a unique opportunity to identify and quantify the sources of the atypical development and developmental heterogeneity of ASD. Integration of assays of behaviour and brain in the first year of life, expansion of the definition of high-risk, and coordinated efforts in multi-site investigations to adequately power integrative studies will lead to new insights into mechanisms of atypical development and, ultimately, the ideal timing and target for interventions that aim to attenuate delays or impairments.

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Visual impairment in FOXG1-mutated individuals and mice

Cited by 40 publications

References 54 publications

Searching for biomarkers of CDKL5 disorder: early-onset visual impairment in CDKL5 mutant mice

Searching for biomarkers of CDKL5 disorder: early-onset visual impairment in CDKL5 mutant mice

Phenotypes in adult patients with Rett syndrome: results of a 13-year experience and insights into healthcare transition

The emergence of autism spectrum disorder

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