Mu, David

Mu, David
Close

Positions

Professor, Microbiology and Molecular Cell Biology

Contact Info

mud@evms.edu

EVMS Directory Profile

overview

Dr. David Mu received Ph.D. in Chemistry from the University of California at Berkeley under the guidance of Professor Judith P. Klinman. Subsequently, he conducted postdoctoral research in the laboratory of Professor Aziz Sancar at the University of North Carolina at Chapel Hill. His postdoctoral research of human Nucleotide Excision Repair mechanism attracted support from the Damon Runyon Cancer Research Fund. Following postdoctoral training, he joined the Cancer Genomics Division of Tularik Inc., using genomic tools to find novel cancer genes for drug discovery. Out of his desire to pursue research of his interest, he later returned to academia by joining the Cancer Genome Center of the Cold Spring Harbor Laboratory (CSHL), extending his cancer genomics research specifically in the realm of lung cancers. His research at CSHL culminated in the discovery of a recurrent lung cancer amplicon at 14q13 in which three genes (TTF-1, NKX2-8, and PAX9) are coamplified. Currently, Dr. Mu is dissecting the signaling mechanism of the amplified lung oncogenes at 14q13 by probing how the microRNA network is intertwined with the amplified lung oncogenes. In addition, he has a separate line of research that searches for new uses of old medications. Due to his past work experience in the biotech sector, he is keen in translating his scientific studies into practices that improve people's life.

selected publications

2019

Mechanistic Study of TTF-1 Modulation of Cellular Sensitivity to Cisplatin. SCIENTIFIC REPORTS. 9.
Full Text via DOI: 10.1038/s41598-019-44549-w PMID: 31142791
2018

Thyroid transcription factor 1 enhances cellular statin sensitivity via perturbing cholesterol metabolism. ONCOGENE. 37:3290-3300.
Full Text via DOI: 10.1038/s41388-018-0174-7 PMID: 29551766
2018

Roles of Thyroid Transcription Factor 1 in Lung Cancer Biology. THYROID HORMONE. 517-544.
Full Text via DOI: 10.1016/bs.vh.2017.05.007 PMID: 29407447
2016

Thyroid Transcription Factor 1 Reprograms Angiogenic Activities of Secretome. SCIENTIFIC REPORTS. 6.
Full Text via DOI: 10.1038/srep19857 PMID: 26912193
2014

Mnk2 Alternative Splicing Modulates the p38-MAPK Pathway and Impacts Ras-Induced Transformation. CELL REPORTS. 7:501-513.
Full Text via DOI: 10.1016/j.celrep.2014.03.041 PMID: 24726367
2013

The Complexity of Thyroid Transcription Factor 1 with Both Pro- and Anti-oncogenic Activities. JOURNAL OF BIOLOGICAL CHEMISTRY. 24992-25000.
Full Text via DOI: 10.1074/jbc.R113.491647 PMID: 23818522
2013

Tight junction proteins: From barrier to tumorigenesis. CANCER LETTERS. 41-48.
Full Text via DOI: 10.1016/j.canlet.2013.05.038 PMID: 23743355
2013

MicroRNA-33a Mediates the Regulation of High Mobility Group AT-Hook 2 Gene (HMGA2) by Thyroid Transcription Factor 1 (TTF-1/NKX2-1). JOURNAL OF BIOLOGICAL CHEMISTRY. 288:16348-16360.
Full Text via DOI: 10.1074/jbc.M113.474643 PMID: 23625920
2013

The splicing factor SRSF6 is amplified and is an oncoprotein in lung and colon cancers.. The Journal of pathology. 229:630-9.
Full Text via DOI: 10.1002/path.4129 PMID: 23132731
2013

Two Distinct Categories of Focal Deletions in Cancer Genomes.. PLOS ONE. 8:e66264.
Full Text via DOI: 10.1371/journal.pone.0066264 PMID: 23805207

research overview

Keywords: MicroRNA biology, Cancer Research, Lung cancer, Cancer genomics, Oncogene mechanism, Oncogenic signaling, Cancer cell metabolism, Cancer drugs, CRISPR-based gene targeting, exosome, extracellular vesicles.

I. Lung Cancer Signaling, MicroRNA, and Metabolism

Oncogenes activated via gene amplification have a proven track record of being amenable to drug discovery. We and others discovered a recurrent amplified region in lung cancer genomes. This amplicon contains the TTF-1 gene (thyroid transcription factor 1 or known as NKX2-1) which is essential for lung development and morphogenesis. We mapped the interconnection between TTF-1 and microRNAs to uncover novel entry points to investigate TTF-1-linked lung biology and discovered the two types of microRNAs interacting with TTF-1 - miR-365 that regulates TTF-1 and miR-33a that is regulated by TTF-1. Since miR-33a is a known regulator of cholesterol metabolism (CM), our finding suggests that TTF-1 may modulate CM in the lung. This represents a novel research direction regarding TTF-1 and we are actively pursuing it.

II. Cancer Secretome and Exosome

How a cell lineage gene such as TTF-1 may reprogram the function of secretome is poorly understood. To this end, we discovered that TTF-1 confers an antiangiogenic function to the secretome of lung cancer epithelial cells. This antiangiogenic activity is derived from TTF-1-promoted secretion of GM-CSF from the lung cancer epithelial cells which in turn induces endothelial cells to release the antiangiogenic soluble VEGF receptor 1. In view of this finding, we surmise that the exosomal cargo content in the secretome may also be subject to TTF-1 regulation. Indeed, we have shown that VEGF is a direct transcriptional target of TTF-1 and the exosomal VEGF cargo level is increased in the TTF-1+ lung cancer cells, suggesting that TTF-1 may reprogram the exosomal cargo content. We are interested in quantifying the extent of the TTF-1-dependent exosomal cargo reprogramming and the associated biological consequences.