Your search keyword '"Wong, Albert"' showing total 12 results

1. The glucocorticoid receptor-FKBP51 complex contributes to fear conditioning and posttraumatic stress disorder

Author

Li, Haiyin, Su, Ping, Lai, Terence K.Y., Jiang, Anlong, Liu, Jing, Zhai, Dongxu, Campbell, Charlie T.G., Lee, Frankie H.F., Yong, WeiDong, Pasricha, Suvercha, Li, Shupeng, Wong, Albert H.C., Ressler, Kerry J., and Liu, Fang

Subjects

Protein binding -- Comparative analysis, Peptides -- Comparative analysis, Glucocorticoids -- Comparative analysis, Animal experimentation -- Comparative analysis, Post-traumatic stress disorder -- Comparative analysis, Genes, Time, Major depressive disorder, Depression (Mood disorder), Health care industry, University of Toronto. Centre for Addiction and Mental Health

Abstract

Posttraumatic stress disorder (PTSD) can develop after exposure to severe psychological trauma, leaving patients with disabling anxiety, nightmares, and flashbacks. Current treatments are only partially effective, and development of better treatments is hampered by limited knowledge of molecular mechanisms underlying PTSD. We have discovered that the glucocorticoid receptor (GR) and FK506 binding protein 51 (FKBP51) form a protein complex that is elevated in PTSD patients compared with unaffected control subjects, subjects exposed to trauma without PTSD, and patients with major depressive disorder (MDD). The GR-FKBP51 complex is also elevated in fear-conditioned mice, an aversive learning paradigm that models some aspects of PTSD. Both PTSD patients and fear-conditioned mice had decreased GR phosphorylation, decreased nuclear GR, and lower expression of 14-3-3[epsilon], a gene regulated by GR. We created a peptide that disrupts GR-FKBP51 binding and reverses behavioral and molecular changes induced by fear conditioning. This peptide reduces freezing time and increases GR phosphorylation, GR-FKBP52 binding, GR nuclear translocation, and 14-3-3[epsilon] expression in fear-conditioned mice. These experiments demonstrate a molecular mechanism contributing to PTSD and suggest that the GR-FKBP51 complex may be a diagnostic biomarker and a potential therapeutic target for preventing or treating PTSD., Introduction Posttraumatic stress disorder (PTSD) was originally described in soldiers exposed to horrific battlefield events, but the conception of psychological trauma has since been expanded to include any life- or [...]

Published

2020

2. Proteolytic Release of CD44 Intracellular Domain and Its Role in the CD44 Signaling Pathway

Author

Okamoto, Isamu, Kawano, Yoshiaki, Murakami, Daizo, Sasayama, Takashi, Araki, Norie, Miki, Toru, Wong, Albert J., and Saya, Hideyuki

Published

2001

3. Dopamine Receptor Genetics in Neuropsychiatric Disorders

Author

Lee, Frankie H.F., Wong, Albert H.C., and Neve, Kim A., Series Editor

Published

2010

4. Gene Amplification of c-myc and N-myc in Small Cell Carcinoma of the Lung

Author

Wong, Albert J., Ruppert, John M., Eggleston, Joseph, Hamilton, Stanley R., Baylin, Stephen B., and Vogelstein, Bert

Published

1986

5. Identification of an Amplified, Highly Expressed Gene in a Human Glioma

Author

Kinzler, Kenneth W., Bigner, Sandra H., Bigner, Darell D., Trent, Jeffrey M., Law, Martha L., O'Brien, Stephen J., Wong, Albert J., and Vogelstein, Bert

Published

1987

6. Increased Expression of the Epidermal Growth Factor Receptor Gene in Malignant Gliomas is Invariably Associated with Gene Amplification

Author

Wong, Albert J., Bigner, Sandra H., Bigner, Darell D., Kinzler, Kenneth W., Hamilton, Stanley R., and Vogelstein, Bert

Published

1987

7. Genetic modification of PIN genes induces causal mechanisms of stay-green drought adaptation phenotype.

Author

Borrell, Andrew K, Wong, Albert C S, George-Jaeggli, Barbara, Oosterom, Erik J van, Mace, Emma S, Godwin, Ian D, Liu, Guoquan, Mullet, John E, Klein, Patricia E, Hammer, Graeme L, McLean, Greg, Hunt, Colleen, and Jordan, David R

Subjects

*SORGHUM, *PHENOTYPIC plasticity, *LOCUS (Genetics), *PERSONAL identification numbers, *DROUGHTS, *GENES

Abstract

The stay-green trait is recognized as a key drought adaptation mechanism in cereals worldwide. Stay-green sorghum plants exhibit delayed senescence of leaves and stems, leading to prolonged growth, a reduced risk of lodging, and higher grain yield under end-of-season drought stress. More than 45 quantitative trait loci (QTL) associated with stay-green have been identified, including two major QTL (Stg1 and Stg2). However, the contributing genes that regulate functional stay-green are not known. Here we show that the PIN FORMED family of auxin efflux carrier genes induce some of the causal mechanisms driving the stay-green phenotype in sorghum, with SbPIN4 and SbPIN2 located in Stg1 and Stg2 , respectively. We found that nine of 11 sorghum PIN genes aligned with known stay-green QTL. In transgenic studies, we demonstrated that PIN genes located within the Stg1 (SbPIN4), Stg2 (SbPIN2), and Stg3b (SbPIN1) QTL regions acted pleiotropically to modulate canopy development, root architecture, and panicle growth in sorghum, with SbPIN1 , SbPIN2 , and SbPIN4 differentially expressed in various organs relative to the non-stay-green control. The emergent consequence of such modifications in canopy and root architecture is a stay-green phenotype. Crop simulation modelling shows that the SbPIN2 phenotype can increase grain yield under drought. [ABSTRACT FROM AUTHOR]

Published

2022

8. 5-hmC in the brain is abundant in synaptic genes and shows differences at the exon-intron boundary.

Author

Khare, Tarang, Pai, Shraddha, Koncevicius, Karolis, Pal, Mrinal, Kriukiene, Edita, Liutkeviciute, Zita, Irimia, Manuel, Jia, Peixin, Ptak, Carolyn, Xia, Menghang, Tice, Raymond, Tochigi, Mamoru, Moréra, Solange, Nazarians, Anaies, Belsham, Denise, Wong, Albert H C, Blencowe, Benjamin J, Wang, Sun Chong, Kapranov, Philipp, and Kustra, Rafal

Subjects

BRAIN physiology, GENES, EXONS (Genetics), METHYLCYTOSINE, LABORATORY mice, DNA, RNA splicing

Abstract

The 5-methylcytosine (5-mC) derivative 5-hydroxymethylcytosine (5-hmC) is abundant in the brain for unknown reasons. Here we characterize the genomic distribution of 5-hmC and 5-mC in human and mouse tissues. We assayed 5-hmC by using glucosylation coupled with restriction-enzyme digestion and microarray analysis. We detected 5-hmC enrichment in genes with synapse-related functions in both human and mouse brain. We also identified substantial tissue-specific differential distributions of these DNA modifications at the exon-intron boundary in human and mouse. This boundary change was mainly due to 5-hmC in the brain but due to 5-mC in non-neural contexts. This pattern was replicated in multiple independent data sets and with single-molecule sequencing. Moreover, in human frontal cortex, constitutive exons contained higher levels of 5-hmC relative to alternatively spliced exons. Our study suggests a new role for 5-hmC in RNA splicing and synaptic function in the brain. [ABSTRACT FROM AUTHOR]

Published

2012

9. Disc1 Point Mutations in Mice Affect Development of the Cerebral Cortex.

Author

Lee, Frankie H. F., Fadel, Marc P., Preston-Maher, Kate, Cordes, Sabine P., Clapcote, Steven J., Price, David J., Roder, John C., and Wong, Albert H. C.

Subjects

GENETIC mutation, CEREBRAL cortex, GENES, SCHIZOPHRENIA, MENTAL illness, LABORATORY mice

Abstract

Disrupted-in-Schizophrenia 1 (DISC1) is a strong candidate gene for schizophrenia and other mental disorders. DISC1 regulates neurodevelopmental processes including neurogenesis, neuronal migration, neurite outgrowth, and neurotransmitter signaling. Abnormal neuronal morphology and cortical architecture are seen in human postmortem brain from patients with schizophrenia. However, the etiology and development of these histological abnormalities remain unclear. We analyzed the histology of two Disc1 mutant mice with point mutations (Q31L and L100P) and found a relative reduction in neuron number, decreased neurogenesis, and altered neuron distribution compared to wild-type littermates. Frontal cortical neurons have shorter dendrites and decreased surface area and spine density. Overall, the histology of Disc1 mutant mouse cortex is reminiscent of the findings in schizophrenia. These results provide further evidence that Disc1 participates in cortical development, including neurogenesis and neuron migration. [ABSTRACT FROM AUTHOR]

Published

2011

10. Cortical gene expression in the neonatal ventral-hippocampal lesion rat model

Author

Wong, Albert H.C., Lipska, Barbara K., Likhodi, Olga, Boffa, Ernie, Weinberger, Daniel R., Kennedy, James L., and Van Tol, Hubert H.M.

Subjects

*SCHIZOPHRENIA, *MESSENGER RNA, *GENE expression, *MOLECULAR genetics, *RNA metabolism, *ANALYSIS of variance, *ANIMAL experimentation, *ANIMAL populations, *BIOLOGICAL models, *COMPARATIVE studies, *FRONTAL lobe, *GENES, *HIPPOCAMPUS (Brain), *RESEARCH methodology, *MEDICAL cooperation, *RATS, *RESEARCH, *RNA, *TEMPORAL lobe, *EVALUATION research, *HALOPERIDOL, *OLIGONUCLEOTIDE arrays, *PHARMACODYNAMICS

Abstract

Abstract: Schizophrenia is a chronic, debilitating psychotic illness of unknown etiology that has been the subject of many genetic studies. We studied the neonatal ventral-hippocampal lesioned rat as an animal model of schizophrenia in order to identify novel candidate genes for schizophrenia. Temporal and frontal cortices were assessed using cDNA microarrays for differences in mRNA expression associated with the lesion, haloperidol treatment and in two rat strains with differential sensitivity to the behavioural effects of the lesion. Genes that had altered expression levels as a result of the lesion, that were normalized by haloperidol treatment, and that differed between rat strains were selected. The pattern of differential transcription was confirmed with quantitative PCR for all six candidate genes: large conductance calcium-activated potassium channel, subfamily M, beta member 1 (Kcnmb1); doublecortex (dcx); adenylyl cyclase-associated protein 1 (CAP1); adenosine monophosphate deaminase 2-isoform L (AMPD2); malic enzyme 3, NADP(+)-dependent, mitochondrial (Me3); and aspartylglucosaminidase (AGA). None of these genes has been extensively studied in schizophrenia, and further work with post-mortem tissue and genetic studies are ongoing. [Copyright &y& Elsevier]

Published

2005

11. Association between schizophrenia and the syntaxin 1A gene

Author

Wong, Albert H.C., Trakalo, Joseph, Likhodi, Olga, Yusuf, Muneeb, Macedo, Antonio, Azevedo, Maria-Helena, Klempan, Tim, Pato, Michele T., Honer, William G., Pato, Carlos N., Van Tol, Hubert H.M., and Kennedy, James L.

Subjects

*GENETICS of schizophrenia, *PSYCHOSES, *GENES, *GENETIC polymorphisms, *GENETICS

Abstract

Background: Both microarray and candidate molecule studies have demonstrated that protein and mRNA expression of syntaxin and other genes involved in synaptic function are altered in the cerebral cortex of patients with schizophrenia.Methods: Genetic association between polymorphic markers in the syntaxin 1A gene and schizophrenia was assessed in a matched case-control sample of 192 pairs, and in an independent sample of 238 nuclear families.Results: In the family-based sample, a significant genetic association was found between schizophrenia and one of the four single nucleotide polymorphisms (SNPs) tested: an intron 7 SNP (transmission disequilibrium test [TDT] χ2 = 5.898; df = 1; p = .015, family-based association test [FBAT] z = 2.280, p = .023). When the results for the TDT and case-control analyses were combined, the association was stronger (n = 430; zc = 2.859; p = .004). Haplotype analysis supported the association with several significant values that appear to be driven by the intron 7 SNP.Conclusions: The results should be treated with caution until replicated, but this is the first report of a genetic association between syntaxin 1A and schizophrenia. [Copyright &y& Elsevier]

Published

2004

12. Epidermal Growth Factor Receptor Variant III Contributes to Cancer Stem Cell Phenotypes in Invasive Breast Carcinoma.

Author

Vecchio, Catherine A. Del, Jensen, Kristin C., Nitta, Ryan T., Shain, A. Hunter, Giacomini, Craig P., and Wong, Albert J.

Subjects

*EPIDERMAL growth factor, *GROWTH factors, *TUMORS, *BREAST cancer, *GENES, *REVERSE transcriptase

Abstract

EGFRvIII is a tumor-specific variant of the epidermal growth factor receptor (EGFR). Although EGFRvIII is most commonly found in glioblastoma, its expression in other tumor types remains controversial. In this study, we investigated EGFRvIII expression and amplification in primary breast carcinoma. Our analyses confirmed the presence of EGFRvIII, but in the absence of amplification or rearrangement of the EGFR locus. Nested reverse transcriptase PCR and flow cytometry were used to detect a higher percentage of positive cases. EGFRvIII-positive cells showed increased expression of genes associated with self-renewal and epithelial-mesenchymal transition along with a higher percentage of stem-like cells. EGFRvIII also increased in vitro sphere formation and in vivo tumor formation. Mechanistically, EGFRvIII mediated its effects through the Wnt/β-catenin pathway, leading to increased β-catenin target gene expression. Inhibition of this pathway reversed the observed effects on cancer stem cell (CSC) phenotypes. Together, our findings show that EGFRvIII is expressed in primary breast tumors and contributes to CSC phenotypes in breast cancer cell lines through the Wnt pathway. These data suggest a novel function for EGFRvIII in breast tumorigenesis. [ABSTRACT FROM AUTHOR]

Published

2012