Function of
            <i>quaking</i>
            in myelination: Regulation of alternative splicing

Wu, Jiang; Reed, Robyn; Grabowski, Paula J.; Artzt, Karen

doi:10.1073/pnas.072090399

Cited by 178 publications

(226 citation statements)

References 34 publications

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“…The QKI gene product appears to function as an RNA-binding protein, interacting through KH domains with numerous transcripts controlling oligodendrocyte fate specification and myelin component metabolism. 38 Following on a recent description of genetic association at the QKI locus, 39 two studies have gone on to document significant and widespread reductions in QKI expression (both global and transcript specific) in schizophrenia patients compared with controls and in regions overlapping with those studied here (BA44 and BA46). 40,41 This raises the intriguing possibility that a deficit in QKI common to multiple psychiatric disorders may lead to aberrant oligodendroglial development.…”

Section: Discussionmentioning

confidence: 89%

Altered expression of genes involved in ATP biosynthesis and GABAergic neurotransmission in the ventral prefrontal cortex of suicides with and without major depression

et al. 2007

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The prefrontal cortex is believed to play a major role in depression and suicidal behavior through regulation of cognition, memory, recognition of emotion, and anxiety-like states, with numerous post-mortem studies documenting a prefrontal serotonergic dysregulation considered to be characteristic of depressive psychopathology. This study was carried out to detect changes in gene expression associated with both suicide and major depression using oligonucleotide microarrays (Affymetrix HG-U133 chip set) summarizing expression patterns in primarily ventral regions of the prefrontal cortex (BA44, 45, 46 and 47). A total of 37 male subjects were included in this study, of which 24 were suicides (depressed suicides = 16, nondepressed suicides = 8) and 13 were matched controls. All subjects were clinically characterized by means of psychological autopsies using structured interviews. Unique patterns of differential expression were validated in each of the cortical regions evaluated, with group-specific changes highlighting the involvement of several key neurobiological pathways that have been implicated in both suicide and depression. An overrepresentation of factors involved in cell cycle control and cell division (BA44), transcription (BA44 and 47) and myelination (BA46) was seen in gene ontology analysis of differentially expressed genes, which also highlights changes in the expression of genes involved in ATP biosynthesis and utilization across all areas. Gene misexpression in BA46 was most pronounced between the two suicide groups, with many significant genes involved in GABAergic neurotransmission. The pronounced misexpression of genes central to GABAergic signaling and astrocyte/ oligodendrocyte function provides further support for a central glial pathology in depression and suicidal behavior.

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Section: Discussionmentioning

confidence: 89%

Altered expression of genes involved in ATP biosynthesis and GABAergic neurotransmission in the ventral prefrontal cortex of suicides with and without major depression

et al. 2007

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“…The qk gene, which encodes for RNA binding proteins involved in posttranscriptional mRNA regulation (6,7), is in close proximity to the proximal deletion breakpoint of qk v (8). The qk v deficiency affects the region upstream of the qk gene to reduce the expression of qk mRNAs in oligodendrocytes, resulting in the CNS myelination defect (9,10).…”

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confidence: 99%

Deletion of the Parkin coregulated gene causes male sterility in the quaking ^viable mouse mutant

Lorenzetti

Bishop

Justice

2004

Proc. Natl. Acad. Sci. U.S.A.

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Quaking viable (qk v ) is a recessive neurological mouse mutation with severe dysmyelination of the CNS and spermiogenesis failure. The molecular lesion in the qk v mutant is a deletion of Ϸ1 Mb on mouse chromosome 17 that alters the expression of the qk gene in oligodendrocytes. Complementation analysis between the qk v mutation and qk mutant alleles generated through chemical mutagenesis showed that the male sterility is a distinctive feature of the qk v allele. This observation suggested that the sperm differentiation defect in qk v is due to the deletion of a gene(s) distinct from qk. Here, we demonstrate that the deletion of Pacrg is the cause of male sterility in the qk v mutant. Pacrg is the mouse homologue of the human PARKIN-coregulated gene (PACRG), which encodes for a protein whose biochemical function remains unclear. We show that Pacrg is highly expressed in the testes in both mice and humans. In addition, the expression pattern of Pacrg during spermiogenesis suggests that it plays a role in sperm differentiation. In support of this hypothesis, we show that transgenic expression of Pacrg in testes restores spermiogenesis and fertility in qk v males. This finding provides the first in vivo evidence, to our knowledge, for the function of Pacrg in a model organism. Immunolocalization experiments on isolated spermatozoa show that the Pacrg protein is present in mature sperm. Remarkably, the mammalian Pacrg protein shares significant sequence similarities with gene products from flagellated protozoans, suggesting that Pacrg may be necessary for proper flagellar formation in many organisms.

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“…The Qki gene contains an RNA-binding domain (KH domain) that binds directly to cellular RNA (8). Several different sequence motifs have been identified as targets for the Qki protein (9)(10)(11)(12). One of these Qki response elements (QREs) consists of a bipartite consensus sequence that has been shown to bind the Qki protein in vivo in at least 23 different mouse mRNA species (9).…”

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confidence: 99%

“…One of these Qki response elements (QREs) consists of a bipartite consensus sequence that has been shown to bind the Qki protein in vivo in at least 23 different mouse mRNA species (9). This mouse protein directly regulates the expression of at least one myelin-specific gene, e.g., myelin basic protein (Mbp) (1), and controls the alternative splicing of the myelin-associated glycoprotein (Mag) (12). In addition, Qki protein regulates the cell cycle inhibitor cyclin-dependent kinase inhibitor 1B (Cdkn1b) (10), which is involved in the terminal differentiation of oligodendrocytes (13).…”

mentioning

confidence: 99%

Human QKI, a potential regulator of mRNA expression of human oligodendrocyte-related genes involved in schizophrenia

Åberg

Saetre

Jareborg

et al. 2006

Proc. Natl. Acad. Sci. U.S.A.

190

159

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The quaking viable mouse mutation (qk v ) is a deletion including the 5 regulatory region of the quaking gene (Qki), which causes body tremor and severe dysmyelination in mouse. The function of the human quaking gene, called quaking homolog KH domain RNAbinding (mouse) (QKI), is not well known. We have previously shown that QKI is a new candidate gene for schizophrenia. Here we show that human QKI mRNA levels can account for a high proportion (47%) of normal interindividual mRNA expression variation (and covariation) of six oligodendrocyte-related genes (PLP1, MAG, MBP, TF, SOX10, and CDKN1B) in 55 human brain autopsy samples from individuals without psychiatric diagnoses. In addition, the tightly coexpressed myelin-related genes (PLP1, MAG, and TF) have decreased mRNA levels in 55 schizophrenic patients, as compared with 55 control individuals, and most of this difference (68 -96%) can be explained by variation in the relative mRNA levels of QKI-7kb, the same QKI splice variant previously shown to be down-regulated in patients with schizophrenia. Taken together, our results suggest that QKI levels may regulate oligodendrocyte differentiation and maturation in human brain, in a similar way as in mouse. Moreover, we hypothesize that previously observed decreased activity of myelin-related genes in schizophrenia might be caused by disturbed QKI splicing.myelin ͉ quaking ͉ splice variant

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Function of quaking in myelination: Regulation of alternative splicing

Cited by 178 publications

References 34 publications

Altered expression of genes involved in ATP biosynthesis and GABAergic neurotransmission in the ventral prefrontal cortex of suicides with and without major depression

Altered expression of genes involved in ATP biosynthesis and GABAergic neurotransmission in the ventral prefrontal cortex of suicides with and without major depression

Deletion of the Parkin coregulated gene causes male sterility in the quaking ^viable mouse mutant

Human QKI, a potential regulator of mRNA expression of human oligodendrocyte-related genes involved in schizophrenia

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Function of quaking in myelination: Regulation of alternative splicing

Cited by 178 publications

References 34 publications

Altered expression of genes involved in ATP biosynthesis and GABAergic neurotransmission in the ventral prefrontal cortex of suicides with and without major depression

Altered expression of genes involved in ATP biosynthesis and GABAergic neurotransmission in the ventral prefrontal cortex of suicides with and without major depression

Deletion of the Parkin coregulated gene causes male sterility in the quaking viable mouse mutant

Human QKI, a potential regulator of mRNA expression of human oligodendrocyte-related genes involved in schizophrenia

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Deletion of the Parkin coregulated gene causes male sterility in the quaking ^viable mouse mutant