Hepatocyte growth factor and met receptor signaling in nasopharyngeal carcinoma cell migration and invasion

溫啟峰, Wan, Kai-fung.

January 2007

published_or_final_version / abstract / Biological Sciences / Master / Master of Philosophy

Hepatocyte growth factor - Receptors.

Nasopharynx - Cancer.

Hepatocyte growth factor-met signaling in ovarian cancer progression

Zhou, Hongyan., 周紅艷.

January 2007

published_or_final_version / abstract / Zoology / Doctoral / Doctor of Philosophy

Hepatocyte growth factor - Receptors

Ovaries - Cancer - Genetic aspects.

Cytogenetics.

Expression of met receptor tyrosine kinase in hepatocellularcarcinoma

Cheung, Man-ting., 張敏婷.

January 2011

published_or_final_version / Pathology / Master / Master of Medical Sciences

Hepatocyte growth factor - Receptors.

Liver - Cancer - Genetic aspects.

Role of microRNA-709 in murine liver

Surendran, Sneha

January 2014

Indiana University-Purdue University Indianapolis (IUPUI) / MicroRNAs are small RNA molecules that regulate expression of genes involved in development, cell differentiation, proliferation and death. It has been estimated that in eukaryotes, approximately 0.5 to 1% of predicted genes encode a microRNA, which in humans, regulate at least 30% of genes at an average of 200 genes per miRNA. Some microRNAs are tissue-specific, while others are ubiquitously expressed. In liver, a few microRNAs have been identified that regulate specialized functions. The best known is miR-122, the most abundant liver-specific miRNA, which regulates cholesterol biosynthesis and other genes of fatty acid metabolism; it also regulates the cell cycle through inhibition of cyclin G1. To discover other miRNAs with relevant function in liver, we characterized miRNA profiles in normal tissue and identified miR-709. Our data indicates this is a highly abundant hepatic miRNA and is dysregulated in an animal model of type 2 diabetes. To understand its biological role, miR-709 gene targets were identified by analyzing the transcriptome of primary hepatocytes transfected with a miR-709 mimic. The genes identified fell within four main categories: cytoskeleton binding, extracellular matrix attachment, endosomal recycling and fatty acid metabolism. Thus, similar to miR-122, miR-709 downregulates genes from multiple pathways. This would be predicted, given the abundance of the miRNA and the fact that the estimated number of genes targeted by a miRNA is in the hundreds. In the case of miR-709, these suggested a coordinated response during cell proliferation, when cytoskeleton remodeling requires substantial changes in gene expression. Consistently, miR-709 was found significantly upregulated in an animal model of hepatocellular carcinoma. Likewise, in a mouse model of liver regeneration, mature miR-709 was increased. To study the consequences of depleting miR-709 in quiescent and proliferating cells, primary hepatocytes and hepatoma cells were cultured with antagomiRs (anti-miRs). The presence of anti-miR-709 caused cell death in proliferating cells. Quiescent primary hepatocytes responded by upregulating miR-709 and its host gene, Rfx1. These studies show that miR-709 targets genes relevant to cystokeleton structural genes. Thus, miR-709 and Rfx1 may be needed to facilitate cytoskeleton reorganization, a process that occurs after liver injury and repopulation, or during tumorigenesis.

Liver -- Regeneration

Gene expression -- Research

Liver -- Cancer -- Animal models

Hepatocyte growth factor -- Receptors

Mice as laboratory animals -- Research