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Establishing Mechanisms of Vitamin D Signaling Pathways

Jing Chen Project Advisor: Dr. Adrian F. Gombart Department of Biochemistry and Biophysics Linus Pauling Institute HHMI . Establishing Mechanisms of Vitamin D Signaling Pathways. Significance of Findings. Increase our understanding of the innate immune system in humans

JasminFlorian
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Establishing Mechanisms of Vitamin D Signaling Pathways

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  1. Jing Chen Project Advisor: Dr. Adrian F. Gombart Department of Biochemistry and Biophysics Linus Pauling Institute HHMI Establishing Mechanisms of Vitamin D Signaling Pathways

  2. Significance of Findings • Increase our understanding of the innate immune system in humans • Increase our understanding of how the VDR and CYP27B1 genes are involved in innate immunity • May lead to new treatments or medications for human diseases

  3. Background • Exposure to sunlight was historically known to cure tuberculosis • Sunlight stimulates the synthesis of vitamin D • Vitamin D stimulates the production of cathelicidin anti-microbial peptide (CAMP) to help fight infections

  4. Background continued Pathogen invades cell Vitamin D Signaling Pathway Toll-like receptor signaling activated Increased expression of VDR and CYP27B1 genes Activated vitamin D binds to VDR Vitamin D and VDR go to the nucleus and binds to the vitamin D response element (VDRE) Production of CAMP increases to fight microbes

  5. Background continued TLR = Toll-like receptor allows immune system to recognize microbes by looking at molecular patterns CYP27B1: a gene that encodes an enzyme to convert inactive vitamin D to active vitamin D VDR = Vitamin D Receptor Active vitamin D binds to VDR Active vitamin D Adams & Hewison (2008). Nature Clinical Practice Endocrinology & Metabolism, Volume 4, 80-90.

  6. Goal of Research Identify molecular mechanisms that regulate the expression of VDR and CYP27B1 genes in response to a pathogen

  7. Hypothesis • If toll-like receptor signaling is activated in a cell that encounters a pathogen, then the expression of VDR and CYP27B1 genes are induced by the NFκB transcription factor.

  8. NFκB • A transcription factor • Regulates immune response to infection • A target of TLR signaling

  9. Methods Overview • Establish a cell line that shows conservation of the vitamin D pathway • Target specific components of the TLR signaling pathway • Determine factors that are necessary for inducing VDR and CYP27B1 • Overexpress dominant negative factors to interfere with components of TLR pathway

  10. Using Dominant Negative Factors Source: Akira, S. J. Biol. Chem. 2003;278:38105-38108

  11. HaCat Cells • An adherent skin cell line • Keratinocyte • Skin is important in vitamin D synthesis

  12. Methods Treat Cells LPS: a TLR4 ligand, a component of cell walls in gram-negative bacteria FSL: a TLR2 ligand , a peptide in bacteria 25D3: inactive vitamin D LPS 1 ng/ml FSL-1 1:1000 Untreated 25D3 & FSL-1 1:1000 25D3 10-7 M

  13. Methods continued • Isolate total cellular mRNA from treated cells • Make cDNA from mRNA • Take cDNA samples and prepare a real-time PCR (RT-PCR) plate

  14. Methods continued Quantitative Real-time PCR • Amplifies and quantifies DNA samples • Measure the level of CAMP, VDR, and CYP27B1 in each sample • Strong induction of VDR and CYP27B1 genes will make it easier to detect decreases in levels

  15. Results * * = statistically significant

  16. Results continued * * * * = statistically significant

  17. Results continued * * * * = statistically significant

  18. Using Dominant Negative Factors Source: Akira, S. J. Biol. Chem. 2003;278:38105-38108

  19. Results continued Transfection of GFP-Ras into HaCat

  20. Discussion • CAMP, VDR, and CYP27B1 expression in HaCat cells increased after stimulation with vitamin D and a TLR ligand • Established a suitable cell line for transfection of dominant negative factors to interfere with TLR signaling pathway • Vitamin D and TLR signaling are important in a cell’s ability to respond to microbes

  21. Future Research • Use molecular mechanisms to interfere with TLR pathway components • Transfection using chemicals • Electroporation

  22. Acknowledgements • HHMI • URISC • NIH Grant 5R01AI065604 – 04 to A.F.G. • OSU Biochemistry and Biophysics Department • Linus Pauling Institute • Gombart Lab -Dr. Adrian F. Gombart -Dr. Tsuyako Saito -Dr. Malcolm Lowry -Mary Fantacone -Chunxiao Guo -Brian Sinnott -Yan Campbell -Jennifer Lam • Dr. Kevin Ahern

  23. References Adams, J.S. & Hewison, M. (2008). Unexpected actions of vitamin D: new perspectives on the regulation of innate and adaptive immunity. Nature Clinical Practice Endocrinology & Metabolism, 4, 80-90. Liu, P.T., Schenk, M., Walker, V.P., Dempsey, P.W., Kanchanapoomi, M., Wheelwright, M., et al. (2009). Convergence of IL-1β and VDR activation pathways in human TLR2/1-induced antimicrobial responses. PLoS One 4(6): e5810. doi: 10.1371/journal.pone.0005810. Schauber, J., Dorschner, R.A., Coda, A.B., Buchau, A.S., Liu, P.T., Kiken, D., et al. (2007). Injury enhances TLR2 function and antimicrobial peptide expression through a vitamin D-dependent mechanism. The Journal of Clinical Investigation, 117(3), 803-811. Segaert, S. & Simonart, T. (2008). The epidermal vitamin D system and innate immunity: some more light shed on this unique photoendocrine system? [Editorial]. Dermatology, 217: 7-11. doi: 10.1159/000118506. Stoffels, K., Overbergh, L., Guilietti, A., Verlinden, L., Bouillon, R., & Mathieu, C. (2006). Immune regulation of 25-hydroxyvitamin-D3-1-α-hydroxylase in human monocytes. Journal of Bone and Mineral Research , 21(1), 37-47.

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