Is it possible to improve neurodevelopmental abnormalities in Down syndrome?

Bartesaghi, Renata; Guidi, Sandra; Ciani, Elisabetta

doi:10.1515/rns.2011.037

Cited by 70 publications

(74 citation statements)

References 324 publications

(500 reference statements)

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“…As mentioned above, evidence for the role of DYRK1A in various DS phenotypes is partially derived from studies performed in several segmental trisomic mouse models of DS that overexpress different sets of orthologous genes of human chromosome 21 (Hsa21), including Dyrk1A (Rueda et al, 2012;Bartesaghi et al, 2011) and in transgenic mice overexpressing DYRK1A in artificial bacterial or yeast chromosomes or carrying extra copies of the corresponding murine cDNA (De la Torre et al, 2014;Ahn et al, 2006;Altafaj et al, 2001;Smith et al, 1997).…”

Section: Accepted Manuscriptmentioning

confidence: 99%

“…TS mice replicate many DS-like abnormalities, including alterations in behavior, learning and memory, brain morphology and hypocellularity, neurogenesis, neuronal connectivity and electrophysiological and neurochemical processes (Rueda et al, 2012;Bartesaghi et al, 2011). Similar to DS individuals, the TS mouse also shows age-dependent cognitive decline and degeneration starting at the age of 6 months, including cholinergic and noradrenergic neuron degeneration, increases in the levels of APP protein and Aβ peptides and tau hyperphosphorylation (Millan Sanchez et al, 2012;Rueda et al, 2010;Netzer et al, 2010;Liu et al, 2008;Seo et al, 2005).…”

Section: Accepted Manuscriptmentioning

confidence: 99%

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Normalizing the gene dosage of Dyrk1A in a mouse model of Down syndrome rescues several Alzheimer's disease phenotypes

García-Cerro

Rueda

Vidal

et al. 2017

Neurobiology of Disease

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The intellectual disability that characterizes Down syndrome (DS) is primarily caused by prenatal changes in central nervous system growth and differentiation. However, in later life stages, the cognitive abilities of DS individuals progressively decline due to accelerated aging and the development of Alzheimer's disease (AD) neuropathology. The AD neuropathology in DS has been related to the overexpression of several genes encoded by Hsa21 including DYRK1A (dualspecificity tyrosine-(Y)-phosphorylation regulated kinase 1A), which encodes a protein kinase that performs crucial functions in the regulation of multiple signaling pathways that contribute to normal brain development and adult brain physiology. Studies performed in vitro and in vivo in animal models overexpressing this gene have demonstrated that the DYRK1A gene also plays a crucial role in several neurodegenerative processes found in DS. The Ts65Dn (TS) mouse bears a partial triplication of several Hsa21 orthologous genes, including Dyrk1A, and replicates many DS-like abnormalities, including age-dependent cognitive decline, cholinergic neuron degeneration, increased levels of APP and Aβ, and tau hyperphosphorylation. To use a more direct approach to evaluate the role of the gene dosage of Dyrk1A on the neurodegenerative profile of this model, TS mice were crossed with Dyrk1A KO mice to obtain mice with a triplication of a segment of Mmu16 that includes this gene, mice that are trisomic for the same genes but only carry two copies of Dyrk1A, euploid mice with a normal Dyrk1A dosage, and CO animals with a single copy of Dyrk1A. Normalizing the gene dosage of Dyrk1A in the TS mouse rescued the density of senescent cells in the cingulate cortex, hippocampus and septum, prevented cholinergic neuron degeneration, and reduced App expression in the hippocampus, Aβ load in the cortex and hippocampus, the expression of phosphorylated tau at the Ser202 residue in the hippocampus and cerebellum and the levels of total tau in the cortex, hippocampus and cerebellum. Thus, the present study provides further support for the role of the Dyrk1A gene in several AD-like phenotypes found in TS mice and indicates that this gene could be a therapeutic target to treat AD in DS.

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Section: Accepted Manuscriptmentioning

confidence: 99%

Section: Accepted Manuscriptmentioning

confidence: 99%

Normalizing the gene dosage of Dyrk1A in a mouse model of Down syndrome rescues several Alzheimer's disease phenotypes

García-Cerro

Rueda

Vidal

et al. 2017

Neurobiology of Disease

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“…This defect translates into a diffused reduction in the number of neurons across the whole DS brain. 3,6 The increase in the repertoire of functions along the time course of mammalian evolution is due to an increase in the relative number of neurons populating the brain, culminating in the unique brain functions possessed by nonhuman and human primates. Therefore, the reduced neuron number in DS is very likely a key determinant underlying the poor performance of individuals with DS in many cognitive functions and behaviors.…”

Section: The Gene Burden Impairs Brain Development In Down Syndromementioning

confidence: 99%

“…Brain abnormalities in DS were thought to be irreversible, but during the last decade several preclinical studies have shown that in mouse models of DS it is possible to improve or even rescue the major neurodevelopmental alterations of the trisomic brain. [3][4][5] These discoveries obviously give new hope for therapeutic interventions in individuals with DS.…”

Section: Introductionmentioning

confidence: 99%

Epigallocatechin gallate: A useful therapy for cognitive disability in Down syndrome?

et al. 2017

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“…Estas alteraciones del neurodesarrollo limitan en grado variable el desempeño cognitivo y las funciones neuropsicológicas (Bartesaghi, Guidi & Ciani, 2011). En este sentido, la afectación hipocampal compromete la memoria explícita.…”

Section: Síndrome De Downunclassified

Síndrome de Down, cerebro y desarrollo

Molero‐Chamizo¹,

Urbina²

2013

Summa Psicológica

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ResumenEn esta revisión describiremos brevemente los aspectos fundamentales que caracterizan a la Psicología del Desarrollo y a la Neurociencia, como disciplinas científicas necesarias en el estudio y la comprensión del desarrollo ontogenético y sus trastornos. Esto nos permitirá concretar la naturaleza de las distintas etapas del desarrollo, y evaluar los sustratos cerebrales de la conducta asociados a estos cambios evolutivos. Finalmente, expondremos las características neurobiológicas y evolutivas de un trastorno del neurodesarrollo determinado genéticamente, el síndrome de Down.Palabras clave: cerebro, desarrollo, síndrome de Down, trastorno y trisomía. AbstractIn this review we briefly describe the main aspects that characterize the Developmental Psychology and Neuroscience as scientific disciplines necessary in the study and understanding of ontogenetic development and it disorders. This allows us to specify the nature of the different stages of development and to evaluate the neural substrates of behavior associated with these evolutionary changes. Finally, we discuss the neurobiological and evolutionary characteristics of a genetically determined neurodevelopmental disorder, the Down syndrome.

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Is it possible to improve neurodevelopmental abnormalities in Down syndrome?

Cited by 70 publications

References 324 publications

Normalizing the gene dosage of Dyrk1A in a mouse model of Down syndrome rescues several Alzheimer's disease phenotypes

Normalizing the gene dosage of Dyrk1A in a mouse model of Down syndrome rescues several Alzheimer's disease phenotypes

Epigallocatechin gallate: A useful therapy for cognitive disability in Down syndrome?

Síndrome de Down, cerebro y desarrollo

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