Department of Biomedical Sciences, SNU
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Kim, hye-young

Ph.D. / Professor
Laboratory of mucosal immunity
TEL +82-2-740-8970
E-MAIL hykim11@snu.ac.kr
WEBSITE http://mucosimmunolab.com

Research

Research Field
The main research interests of our laboratory are the host defense and innate immune responses of mucosal tissues such as the lung, skin, and intestine. We are trying to understand 1) how innate immune circuits detect and respond to allergen/pathogen challenges in mucosal tissues, and 2) how the innate immune system contributes to tissue homeostasis or harmful inflammatory responses in the various organs.
In particular, we are studying with great interest innate lymphocyte cells (ILCs), which are a group of lymphocytes that lack specific antigen receptors but can rapidly respond to external stimuli. We investigate the role of ILCs in animal models of various diseases such as asthma, atopic dermatitis, colitis, and lupus nephritis. We also try to translate the data in human disease and discover the potential roles of ILCs as biomarkers in the diagnosis and/or future therapeutic targets.
Research Themes
1.Induction and regulation of innate immune cells in the mucosal tissue
2.ILCs-immune cell interactions in various disease
3.Epigenetic control of activation or inhibition of ILCs
4.Finding potential biomarker of allergic disease
Pure Link
https://snucm.elsevierpure.com/en/persons/hye-young-kim
Keyword
Mucosal immunology, Innate immunity, Inflammatory diseases
Intensive Major
# Immune
# Molecular cell

Education

  • 1997- 2001 B.S. in Biology, Ewha Womans University)
  • 2001 - 2003 M.S in Genetics, Seoul National University
  • 2003 - 2006 Ph.D. in Immunology, Seoul National University College of Medicine

Career

  • 2006-2011. Research fellow, Harvard Medical School/BCH
  • 2011-2013 Instructor (Research Associate), Harvard Medical School/BCH
  • 2014-2020 Associate professor, Seoul National University College of Medicine,
  • 2021-present Professor, Seoul National University College of Medicine,

Publication

  1. [1] Ham JH, Kim JH, Shon KH, Park IW, Choi BW, Chung DH, Cho SH, Kang HR, Jung JW*, Kim HY*. Cigarette smoke aggravates asthma by inducing memory-like type 3 innate lymphoid cells (Nat Commun. 2022 Jul 4;13(1):3852. doi: 10.1038/s41467-022-31491-1. IF 17.694)
  2. [2] Ryu SW, Shin JW, Kwon S, Lee J, Kim YC, Bae YS, Bas YS, Kim DK, Kim YS, Yang SH*, Kim HY*. Siglec-F-expressing neutrophils are essential for creating a 3 pro-fibrotic microenvironment in the renal fibrosis (J Clin Invest. 2022. https://doi.org/10.1172/JCI156876 IF 19.456)
  3. [3] Ko YG, Kim, MH, Park JY, Gil CH, Kim TS, Choi JY, Chung DH, Kim HK, Kim DY*, Kim HY*. Chronic rhinosinusitis endotypes associate with distinct local cytokine milieus that shape the distribution of innate lymphoid cells. (Allergy. 2022 Mar 31. doi: 10.1111/all.15300 IF 14.710)
  4. [4] Shin JW, Kim, JH, Ham S, Choi, SM, Lee CH, Lee JC, Kim JH, Cho SH, Kang HR, Kim YM, Chung DH, Chung Y, Bae YS, Bae YS, Roh TY, Kim T, Kim HY*. A unique population of neutrophils generated by air pollutant-induced lung damage exacerbates airway inflammation (J Allergy Clin Immunol 2021 Oct 12;S0091-6749(21)01520-7 IF 14.29).
  5. [5] Kim JH, Shin JW, Lee HJ, Kim JH, Choi SM, Lee CH, Kang HR, Park SH, Bae YS, Chung DH, Kim HY*. Serum amyloid A promotes emphysema by triggering the reciprocal activation of neutrophils and ILC3s. (Clin Transl Med. 2021 Dec;11(12):e637. doi: 10.1002/ctm2.637. IF 11.492)
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