Your search keyword '"Siu, V"' showing total 9 results

1. Differential brain region‐specific expression of MeCP2 and BDNF in Rett Syndrome patients: a distinct grey‐white matter variation.

Author

Pejhan, S., Siu, V. M., Ang, L. C., Del Bigio, M. R., and Rastegar, M.

Subjects

RETT syndrome, GLIAL fibrillary acidic protein, MYELIN basic protein, GENETIC mutation, BRAIN

Abstract

Introduction and objectives: Rett Syndrome (RTT) is a neurodevelopmental disorder caused by Methyl CpG Binding Protein 2 (MECP2) gene mutations. Previous studies of MeCP2 in the human brain showed variable and inconsistent mosaic‐pattern immunolabelling, which has been interpreted as a reflection of activation‐state variability. We aimed to study post mortem MeCP2 and BDNF (MeCP2 target) degradation and brain region‐specific detection in relation to RTT pathophysiology. Methods: We investigated MeCP2 and BDNF stabilities in non‐RTT human brains by immunohistochemical labelling and compared them in three brain regions of RTT and controls. Results: In surgically excised samples of human hippocampus and cerebellum, MeCP2 was universally detected. There was no significantly obvious difference between males and females. However, post mortem delay in autopsy samples had substantial influence on MeCP2 detection. Immunohistochemistry studies in RTT patients showed lower MeCP2 detection in glial cells of the white matter. Glial fibrillary acidic protein (GFAP) expression was also reduced in RTT brain samples without obvious change in myelin basic protein (MBP). Neurons did not show any noticeable decrease in MeCP2 detection. BDNF immunohistochemical detection showed an astroglial/endothelial pattern without noticeable difference between RTT and controls. Conclusions: Our findings indicate that MeCP2 protein is widely expressed in mature human brain cells at all ages. However, our data points towards a possible white matter abnormality in RTT and highlights the importance of studying human RTT brain tissues in parallel with research on animal and cell models of RTT. [ABSTRACT FROM AUTHOR]

Published

2020

2. Biochemical and Hematologic Manifestations of Gastric Intrinsic Factor (GIF) Deficiency: A Treatable Cause of B12 Deficiency in the Old Order Mennonite Population of Southwestern Ontario.

Author

Ferrand, A., Siu, V. M., Rupar, C. A., Napier, M. P., Al-Dirbashi, O. Y., Chakraborty, P., and Prasad, C.

Published

2015

3. Is there a correlation between the proportion of cells with isodicentric Yp at amniocentesis and phenotypic sex?

Author

Xu, Jie and Siu, V. M.

Abstract

Objectives (1) To present a case with prenatally detected idic Yp. (2) To review literature to assess if there is a correlation between the proportion of amniocytes with idic Yp and phenotypic sex. Methods Seventeen cases were reviewed. Results Amniocentesis was done due to positive integrated prenatal screening result. Interphase FISH was normal for chromosomes 13, 18, and 21, but mosaic for cell lines with 1 X and 0 to 2 copies of DYZ3, SRY, or DYZ1(Yq12). Amniocytes had 45,X[28]/46,X,idic(Y)(q11.2)[2].ish idic(Y)(DYZ3 + +, SRY + +). An apparently normal female was born at 37 weeks. The umbilical cord had 45,X[50], but cord blood had 45,X[17]/46,X,idic(Y)[31]/47,X,idic(Y)x2[2]. Review of 17 cases showed that 13 cases with 20 to 100% cells with idic Yp all had a male phenotype. Two cases with 3 and 7% of idic Yp cells had a female phenotype. Two cases with 45,X only at prenatal diagnosis but idic Yp detected postnatally were phenotypic male. Conclusion (1) We present the first report of prenatally detected idic Yp and Yq12 resulting in an apparently normal female at birth. (2) Finding of > 20% of G-banded amniocytes with idic Yp in the absence of other indicators of foetal structural anomalies seems to correlate with phenotypically normal male in most cases. Copyright © 2010 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]

Published

2010

4. DRR drives brain cancer invasion by regulating cytoskeletal-focal adhesion dynamics.

Author

Le, P U, Angers-Loustau, A, de Oliveira, R M W, Ajlan, A, Brassard, C L, Dudley, A, Brent, H, Siu, V, Trinh, G, Mölenkamp, G, Wang, J, Seyed Sadr, M, Bedell, B, Del Maestro, R F, and Petrecca, K

Subjects

TREATMENT of brain cancer, RENAL cell carcinoma, NEUROGLIA, ACTIN, CYTOSKELETON

Abstract

Malignant glioma invasion is a primary cause of brain cancer treatment failure, yet the molecular mechanisms underlying its regulation remain elusive. We developed a novel functional-screening strategy and identified downregulated in renal cell carcinoma (DRR) as a regulator of invasion. We show that DRR drives invasion in vitro and in vivo. We found that while DRR is not expressed in normal glial cells, it is highly expressed in the invasive component of gliomas. Exploring underlying mechanisms, we show that DRR associates with and organizes the actin and microtubular cytoskeletons and that these associations are essential for focal adhesion (FA) disassembly and cell invasion. These findings identify DRR as a new cytoskeletal crosslinker that regulates FA dynamics and cell movement. [ABSTRACT FROM AUTHOR]

Published

2010

5. An interstitial deletion of the long arm of chromosome 21 in a case of a first episode of psychosis.

Author

Takhar, J., Malla, Ashok K., Siu, V., MacPherson, Colin, Fan, Y. S., and Townsend, L.

Subjects

CHROMOSOMES, PSYCHOSES, GENETICS

Abstract

Objective: Case of an interstitial deletion of the long arm of chromosome 21 presenting with first episode of psychosis. Method: A case report. Results: A 16-year-high school student of Somalian origin presented with a first episode of psychosis, mild mental retardation and dysmorphic features. Chromosome analysis revealed an interstitial deletion in the long arm of chromosome 21, described as 46, XX del (21) (q21q22.1). Conclusion: First episode of psychosis occurred in combination with neurobiological vulnerability and a complex genetic inheritance. The occurrence of psychosis in our case may be attributable to genes located within the region 21q21q22.1. The possibility that other loci exist on chromosome 21, which predispose to schizophrenia has to be considered. Identification of susceptibility genes will greatly facilitate investigation of factors that contribute to the disease process and may lead to early intervention and prevention. [ABSTRACT FROM AUTHOR]

Published

2002

6. A gene for Hirschsprung disease maps to the proximal long arm of chromosome 10.

Author

Lyonnet, S., Bolino, A., Pelet, A., Abel, L., Nihoul-Fékété, C., Briard, M. L., Mok-Siu, V., Kaariainen, H., Martucciello, G., Lerone, M., Puliti, A., Luo, Yin, Weissenbach, J., Devoto, M., Munnich, A., and Romeo, G.

Published

1993

7. Hazards of microwave ovens.

Author

Siu, Victoria, Kissoon, Niranjan, Siu, V, and Kissoon, N

Published

1987

8. Evaluation of the electromagnetic hazard of intense THz pulses on neural cells.

Author

Peccianti, M., Seyed Sadr, M., Sabau, C., Sharma, G., Blanchard, F., Razzari, L., Maret, D., Seyed Sadr, E., Alshami, J., Siu, V., Gobbi, G., Ozaki, T., Del Maestro, R., and Morandotti, R.

Published

2010

9. Perianal fibroadenoma.

Author

Grube-Pagola, P., Gámez-Siu, V., Maldonado-Barrón, R., Remes-Troche, J. M., and Alderete-Vázquez, G.

Subjects

CASE studies, ANAL cancer, ADENOMA, PAIN, WOMEN, PERIODIC health examinations

Abstract

The article presents a case study of a 28-year-old woman complaining pain in the anal canal. It states that physical examination detected a pediculated, hard tumour covered by unaltered perianal skin, wherein the stroma was composed of compressed elongated collagen bundles and anastomosing ducts. It also discusses the occurrence of anogenital fibroadenomas predominately in the vulva of women.

Published

2012