Your search keyword '"Patrick Y. Kim"' showing total 3 results

1. High TDP43 expression is required for TRIM16-induced inhibition of cancer cell growth and correlated with good prognosis of neuroblastoma and breast cancer patients

Author

Owen Tan, Belamy B. Cheung, Toby Trahair, Bing Liu, Murray D. Norris, Michelle Haber, Glenn M. Marshall, Tao Liu, and Patrick Y. Kim

Subjects

0301 basic medicine, Cancer Research, Cell Survival, Ubiquitin-Protein Ligases, Two-hybrid screening, Breast Neoplasms, Cell Growth Processes, Biology, Transfection, Retinoblastoma Protein, law.invention, Tripartite Motif Proteins, Neuroblastoma, 03 medical and health sciences, Breast cancer, law, Cell Line, Tumor, medicine, Humans, E2F1, cDNA library, Binding protein, DNA, Prognosis, medicine.disease, DNA-Binding Proteins, 030104 developmental biology, Oncology, Cancer cell, MCF-7 Cells, Cancer research, Suppressor, Female, E2F1 Transcription Factor, Transcription Factors

Abstract

Tripartite Motif-containing protein 16 (TRIM16) is a member of a large family of tripartite motif (TRIM) proteins, that has been implicated in the pathogenesis of multiple cancers. However, the mechanism by which TRIM16 acts as a tumour suppressor is currently unknown. We used the versatile yeast two-hybrid assay on a cDNA library from human testes, which has relative high TRIM16 expression, to identify potential TRIM16-binding proteins. We identified transactive response DNA-binding protein 43 (TDP43) as a novel TRIM16 binding protein. Co-immunoprecipitation assay demonstrated that TDP43 bound TRIM16 in neuroblastoma and breast cancer cells. Enforced over-expression of TRIM16 increased the protein half-life of TDP43, through the inhibition of the proteosomal degradation pathway. High levels of TRIM16 and TDP43 are associated with good prognosis in both human neuroblastoma and breast cancer tissues. Importantly, we found TDP43 expression was required for TRIM16-induced inhibition of neuroblastoma and breast cancer cell growth and the repressive effect of TRIM16 on cell cycle regulatory proteins, E2F1 and pRb. Taken together, our data suggest that TRIM16 and TDP43 are both good prognosis indicators; also we showed that TRIM16 inhibits cancer cell viability by a novel mechanism involving interaction and stabilisation of TDP43 with consequent effects on E2F1 and pRb proteins.

Published

2016

2. Ectopic expression of anti-HIV-1 shRNAs protects CD8+ T cells modified with CD4ζ CAR from HIV-1 infection and alleviates impairment of cell proliferation

Author

Patrick Y. Kim, Otto O. Yang, Emiko Kranz, Masakazu Kamata, Sean M. O'connor, Gene-Errol Ringpis, Hwee L. Ng, Irvin S. Y. Chen, and Joshua Chan

Subjects

Biophysics, Gene Expression, HIV Infections, CD8-Positive T-Lymphocytes, Biochemistry, Article, Interleukin 21, Antigen, Humans, Cytotoxic T cell, IL-2 receptor, RNA, Small Interfering, Antigen-presenting cell, Cell Engineering, Molecular Biology, Cells, Cultured, Cell Proliferation, Interleukin 3, CD40, biology, virus diseases, Cell Biology, Virology, CD4 Antigens, HIV-1, biology.protein, Interleukin 12, Immunotherapy

Abstract

Chimeric antigen receptors (CARs) are artificially engineered receptors that confer a desired specificity to immune effector T cells. As an HIV-1-specific CAR, CD4ζ CAR has been extensively tested in vitro as well as in clinical trials. T cells modified with this CAR mediated highly potent anti-HIV-1 activities in vitro and were well-tolerated in vivo, but exerted limited effects on viral load and reservoir size due to poor survival and/or functionality of the transduced cells in patients. We hypothesize that ectopic expression of CD4ζ on CD8(+) T cells renders them susceptible to HIV-1 infection, resulting in poor survival of those cells. To test this possibility, highly purified CD8(+) T cells were genetically modified with a CD4ζ-encoding lentiviral vector and infected with HIV-1. CD8(+) T cells were vulnerable to HIV-1 infection upon expression of CD4ζ as evidenced by elevated levels of p24(Gag) in cells and culture supernatants. Concurrently, the number of CD4ζ-modified CD8(+) T cells was reduced relative to control cells upon HIV-1 infection. To protect these cells from HIV-1 infection, we co-expressed two anti-HIV-1 shRNAs previously developed by our group together with CD4ζ. This combination vector was able to suppress HIV-1 infection without impairing HIV-1-dependent effector activities of CD4ζ. In addition, the number of CD4ζ-modified CD8(+) T cells maintained similar levels to that of the control even under HIV-1 infection. These results suggest that protecting CD4ζ-modified CD8(+) T cells from HIV-1 infection is required for prolonged HIV-1-specific immune surveillance.

Published

2015

3. Identification of plasma Complement C3 as a potential biomarker for neuroblastoma using a quantitative proteomic approach

Author

Glenn M. Marshall, Toby Trahair, Owen Tan, Eric O. Sekerye, Sonya M. Diakiw, Valerie C. Wasinger, Patrick Y. Kim, Tao Liu, Lou Chesler, Maria Kavallaris, Alla Dolnikov, Murray D. Norris, Michelle Haber, Belamy B. Cheung, Daniel R. Carter, and Nai Kong Cheung

Subjects

Adult, Male, Zinc-alpha2-glycoprotein, Complement system, Transgene, Biophysics, Mice, Transgenic, Biology, Proteomics, Biochemistry, Germline, Mice, Neuroblastoma, medicine, Animals, Humans, TH-MYCN+/+, neoplasms, Infant, Newborn, Neoplasms, Experimental, Biomarker, Complement C3, medicine.disease, Blood proteins, Biomarker (cell), Child, Preschool, Immunology, Cancer cell, Cancer research, Female, Biomarkers

Abstract

The majority of patients diagnosed with neuroblastoma present with aggressive disease. Improved detection of neuroblastoma cancer cells following initial therapy may help in stratifying patient outcome and monitoring for relapse. To identify potential plasma biomarkers, we utilised a liquid chromatography tandem mass spectrometry-based proteomics approach to detect differentially-expressed proteins in serum from TH-MYCN mice. TH-MYCN mice carry multiple copies of the human MYCN oncogene in the germline and homozygous mice for the transgene develop neuroblastoma in a manner resembling the human disease. The abundance of plasma proteins was measured over the course of disease initiation and progression. A list of 86 candidate plasma biomarkers was generated. Pathway analysis identified significant association of these proteins with genes involved in the complement system. One candidate, complement C3 protein, was significantly enriched in the plasma of TH-MYCN+/+ mice at both 4 and 6 weeks of age, and was found to be elevated in a cohort of human neuroblastoma plasma samples, compared to healthy subjects. In conclusion, we have demonstrated the suitability of the TH-MYCN+/+ mouse model of neuroblastoma for identification of novel disease biomarkers in humans, and have identified Complement C3 as a candidate plasma biomarker for measuring disease state in neuroblastoma patients. Biological significance This study has utilised a unique murine model which develops neuroblastoma tumours that are biologically indistinguishable from human neuroblastoma. This animal model has effectively allowed the identification of plasma proteins which may serve as potential biomarkers of neuroblastoma. Furthermore, the label-free ion count quantitation technique which was used displays significant benefits as it is less labour intensive, feasible and accurate. We have been able to successfully validate this approach by confirming the differential abundance of two different plasma proteins. In addition, we have been able to confirm that the candidate biomarker Complement C3, is more abundant in the plasma of human neuroblastoma patient plasma samples when compared to healthy counterparts. Overall we have demonstrated that this approach can be potentially useful in the identification of biomarker candidates, and that further validation of the candidates may lead to the discovery of novel, clinically useful diagnostic tools in the detection of sub-clinical neuroblastoma. (C) 2013 The Authors. Published by Elsevier B.V. All rights reserved.

Published

2014