Your search keyword '"Thangaveloo, Moogaambikai"' showing total 2 results

1. Connexin 43 upregulation in burns promotes burn conversion through spread of apoptotic death signals.

Author

Feng, Jiajun, Thangaveloo, Moogaambikai, Ong, Yee Siang, Chong, Si Jack, Joethy, Janna-Vale, and Becker, David L.

Subjects

*CONNEXIN 43, *HEAT shock proteins, *APOPTOSIS, *PROTEIN expression, *PROTEIN metabolism, *DISEASE progression, *RESEARCH, *FIBROBLASTS, *BURNS & scalds, *CELL membranes, *RESEARCH methodology, *CELL physiology, *MEDICAL cooperation, *EVALUATION research, *COMPARATIVE studies, *DERMIS, *MEMBRANE proteins

Abstract

Background: Burn wounds continue to worsen after initial injury in a process known as burn conversion, which lasts about 3-5 days. It causes burn wounds to enlarge and deepen, leading to greater morbidity. Apoptosis is one of the factors contributing to the conversion of the zone of stasis into the zone of coagulation. Suppression of apoptosis has been associated with reducing burn conversion. Connexin 43 (Cx43) gap junctions facilitate the spread of apoptotic signals from dying cells to healthy neighbouring cells in injured tissues through the bystander effect.Objectives: The study is to understand the role of Cx43 in burn conversion.Methods: In our study, 15 burn tissue samples were arranged into three groups as early (beginning of burn conversion), intermediate (extensive burn conversion) and late (established burn conversion) burns.Results: We found a striking increase in the amount of Cx43 protein expressed in the dermal fibroblasts (identified with heat shock protein 47 (HSP47) staining) in the zone of stasis in early and intermediate burns. These dermal fibroblasts also express high levels of cleaved-Caspase 3 indicating on-going apoptosis.Conclusions: Our findings suggest that elevation of Cx43 may play an active role in burn conversion spreading apoptosis in the early and intermediate burn wound. [ABSTRACT FROM AUTHOR]

Published

2020

2. ST3GAL1-Associated Transcriptomic Program in Glioblastoma Tumor Growth, Invasion, and Prognosis.

Author

Yuk Kien Chong, Sandanaraj, Edwin, Koh, Lynnette W. H., Thangaveloo, Moogaambikai, Tan, Melanie S. Y., Koh, Geraldene R. H., Toh, Tan Boon, Lim, Grace G. Y., Holbrook, Joanna D., Oi Lian Kon, Nadarajah, Mahendran, Ivan Ng, Wai Hoe Ng, Nguan Soon Tan, Kah Leong Lim, Carol Tang, Beng Ti Ang, Chong, Yuk Kien, Kon, Oi Lian, and Ng, Ivan

Subjects

PROTEIN metabolism, ANIMAL experimentation, BIOCHEMISTRY, BRAIN tumors, CANCER invasiveness, CELL physiology, CELLULAR signal transduction, GENES, GENETIC techniques, GLIOMAS, GROWTH factors, PHENOMENOLOGY, MICE, PROGNOSIS, TRANSFERASES, XENOGRAFTS, GENE expression profiling, KAPLAN-Meier estimator, COLONY-forming units assay

Abstract

Background: Cell surface sialylation is associated with tumor cell invasiveness in many cancers. Glioblastoma is the most malignant primary brain tumor and is highly infiltrative. ST3GAL1 sialyltransferase gene is amplified in a subclass of glioblastomas, and its role in tumor cell self-renewal remains unexplored. Methods: Self-renewal of patient glioma cells was evaluated using clonogenic, viability, and invasiveness assays. ST3GAL1 was identified from differentially expressed genes in Peanut Agglutinin-stained cells and validated in REMBRANDT (n = 390) and Gravendeel (n = 276) clinical databases. Gene set enrichment analysis revealed upstream processes. TGFβ signaling on ST3GAL1 transcription was assessed using chromatin immunoprecipitation. Transcriptome analysis of ST3GAL1 knockdown cells was done to identify downstream pathways. A constitutively active FoxM1 mutant lacking critical anaphase-promoting complex/cyclosome ([APC/C]-Cdh1) binding sites was used to evaluate ST3Gal1-mediated regulation of FoxM1 protein. Finally, the prognostic role of ST3Gal1 was determined using an orthotopic xenograft model (3 mice groups comprising nontargeting and 2 clones of ST3GAL1 knockdown in NNI-11 [8 per group] and NNI-21 [6 per group]), and the correlation with patient clinical information. All statistical tests on patients' data were two-sided; other P values below are one-sided. Results: High ST3GAL1 expression defines an invasive subfraction with self-renewal capacity; its loss of function prolongs survival in a mouse model established from mesenchymal NNI-11 (P < .001; groups of 8 in 3 arms: nontargeting, C1, and C2 clones of ST3GAL1 knockdown). ST3GAL1 transcriptomic program stratifies patient survival (hazard ratio [HR] = 2.47, 95% confidence interval [CI] = 1.72 to 3.55, REMBRANDT P = 1.92 x 10⁻⁸; HR = 2.89, 95% CI = 1.94 to 4.30, Gravendeel P = 1.05 x 10⁻¹¹), independent of age and histology, and associates with higher tumor grade and T2 volume (P = 1.46 x 10⁻⁴). TGFβ signaling, elevated in mesenchymal patients, correlates with high ST3GAL1 (REMBRANDT gliomacor = 0.31, P = 2.29 x 10⁻¹⁰; Gravendeel gliomacor = 0.50, P = 3.63 x 10⁻²⁰). The transcriptomic program upon ST3GAL1 knockdown enriches for mitotic cell cycle processes. FoxM1 was identified as a statistically significantly modulated gene (P = 2.25 x 10⁻⁵) and mediates ST3Gal1 signaling via the (APC/C)-Cdh1 complex. Conclusions: The ST3GAL1-associated transcriptomic program portends poor prognosis in glioma patients and enriches for higher tumor grades of the mesenchymal molecular classification. We show that ST3Gal1-regulated self-renewal traits are crucial to the sustenance of glioblastoma multiforme growth. [ABSTRACT FROM AUTHOR]

Published

2016