Modulation of Neuritogenesis by a Protein Implicated in X-Linked Mental Retardation

Jiao, Xuan; Chen, Hongxin; Chen, Jianmin; Herrup, Karl; Firestein, Bonnie L.; Kiledjian, Megerditch

doi:10.1523/jneurosci.5954-08.2009

Cited by 28 publications

(25 citation statements)

References 39 publications

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“…All of these hypotheses need to be further confirmed. Additionally, the duplication might not act directly, but rather predispose the patients to the action of other factors that cause the clinical features [Seminara et al, 2000;Davies et al, 2009;Jiao et al, 2009]. However, the observation of talipes anomalies reported in 3 patients in association with the patient with talipes collected by Faletra et al [2011] together with common neurological impairment have led Esplin et al [2014] to recognize a classical, common phenotype for patients affected by the Xp22.31 duplication, including DD/ID, feeding difficulties, ASD, hypotonia, seizures, and talipes.…”

Section: Discussionmentioning

confidence: 99%

Microcephaly/Trigonocephaly, Intellectual Disability, Autism Spectrum Disorder, and Atypical Dysmorphic Features in a Boy with Xp22.31 Duplication

et al. 2018

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The Xp22.31 segment of the short arm of the human X chromosome is a region of high instability with frequent rearrangement. The duplication of this region has been found in healthy people as well as in individuals with varying degrees of neurological impairment. The incidence has been reported in a range of 0.4-0.44% of the patients with neurological impairment. Moreover, there is evidence that Xp22.31 duplication may cause a common phenotype including developmental delay, intellectual disability, feeding difficulty, autistic spectrum disorders, hypotonia, seizures, and talipes. We report on a patient with microcephaly and trigonocephaly, moderate intellectual disability, speech and language delay, and poor social interaction in addition to minor but atypical dysmorphic features. This report provides further insight into the pathogenicity of the Xp22.31 duplication by extending knowledge of its clinical features. This case, in association with those reported in the literature, indicates that the Xp22.31 duplication may contribute to cause pathological phenotypes with minor facial dysmorphisms, microcephaly, and intellectual disability as main features.

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Section: Discussionmentioning

confidence: 99%

Microcephaly/Trigonocephaly, Intellectual Disability, Autism Spectrum Disorder, and Atypical Dysmorphic Features in a Boy with Xp22.31 Duplication

et al. 2018

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“…To induce oxidative stress, cells were treated with 0.5 mM arsenic trioxide (catalog number A1010, Sigma, St. Louis, MO) for 45 min as described previously [35]. Plasmids were transfected with Lipofectamine™ 2000 (Invitrogen) and siRNAs were transfected with Lipofectamine™ RNAiMAX (Invitrogen) according to the manufacturer's instructions.…”

Section: Methodsmentioning

confidence: 99%

The QKI-6 RNA Binding Protein Localizes with the MBP mRNAs in Stress Granules of Glial Cells

et al. 2010

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BackgroundThe quaking viable (qkv) mouse has several developmental defects that result in rapid tremors in the hind limbs. The qkI gene expresses three major alternatively spliced mRNAs (5, 6 and 7 kb) that encode the QKI-5, QKI-6 and QKI-7 RNA binding proteins that differ in their C-terminal 30 amino acids. The QKI isoforms are known to regulate RNA metabolism within oligodendrocytes, however, little is known about their roles during cellular stress.Methodology/Principal FindingsIn this study, we report an interaction between the QKI-6 isoform and a component of the RNA induced silencing complex (RISC), argonaute 2 (Ago2). We show in glial cells that QKI-6 co-localizes with Ago2 and the myelin basic protein mRNA in cytoplasmic stress granules.ConclusionsOur findings define the QKI isoforms as Ago2-interacting proteins. We also identify the QKI-6 isoform as a new component of stress granules in glial cells.

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“…Formation of neuronal networks enables successful communication between neurons via specific synaptic connections. Failure of normal neuritogenesis leads to morphological changes and abnormalities in brain function (17,19).…”

Section: Introductionmentioning

confidence: 99%

Bcl-xL Is Necessary for Neurite Outgrowth in Hippocampal Neurons

Park

Licznerski

Alavian

et al. 2015

Antioxidants & Redox Signaling

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Modulation of Neuritogenesis by a Protein Implicated in X-Linked Mental Retardation

Cited by 28 publications

References 39 publications

Microcephaly/Trigonocephaly, Intellectual Disability, Autism Spectrum Disorder, and Atypical Dysmorphic Features in a Boy with Xp22.31 Duplication

Microcephaly/Trigonocephaly, Intellectual Disability, Autism Spectrum Disorder, and Atypical Dysmorphic Features in a Boy with Xp22.31 Duplication

The QKI-6 RNA Binding Protein Localizes with the MBP mRNAs in Stress Granules of Glial Cells

Bcl-xL Is Necessary for Neurite Outgrowth in Hippocampal Neurons

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