Hua Huang, MD, PhD

Special Interests

Research Interests

My lab studies transcriptional and epigenetic regulation of genes that control immune effector cell development and regulate cytokine and chemokine gene expression. We investigate how super-enhancers and their associated transcription factors integrate signals triggered by various external stimuli, such as antigenic stimulation, infection, cytokine and metabolic products, to generate gene transcription outputs. We also determine the contribution of genetic variants to enhancer activity, gene expression and disease severity. We utilize various cutting-edge technologies, including next-generation sequencing, bioinformatics, enhancer library and CRISPR to address significant research problems in inflammation and allergic immune responses.

View more about our current lab projects.

Education

Education

1995 - 1999

Leukemia Society Fellow and Postdoctoral fellow, The Laboratory of Immunology, NIAID, NIH, Immunology

1993 - 1995

Leukemia Society Fellow, The Department of Molecular Biology, Princeton University, Stem Cell Biology

1984

Sun Yat-Sen University School of Medicine, Guangzhou, P. R. China, MD

1991

University of Wisconsin-Madison, MS, Immunology

1993

University of Wisconsin-Madison, PhD, Developmental Biology

Awards & Recognition

Visiting professor at Fudan University, Sichuan University and Sun Yat-sen University
The Lydia Schweppe Immunology Career Development Award
NIH K22 Research Career Award
Leukemia Society of America Fellowship
Visiting Scholarship awarded by the Radiation Effects Research Foundation (Japan)

Professional Memberships

American Association of Immunology

Publications

Li YL, Gao JF, Zhao DZ, Guan XY, Morris SC, Finkelman FD, Huang H. The GC box at the proximal enhancer of the Hdc gene is critical for Hdc gene transcription and histamine-mediated anaphylaxis. (BioRxiv 495950) [Preprint], available from: https://doi.org/10.1101/2022.06.13.495950. J Allergy Clin Immunol, published online Feb. 23, 2023, 10.1016/j.jaci.2023.01.031.

Li, Y., Gao, J. F., Kamran, M. Harmacek, L., Danhorn, T., Leach, S. M., O'Connor, B. P., Hagman, J. R., Huang H. GATA2 regulates mast cell identity and responsiveness to antigenic stimulation by promoting chromatin remodeling at super-enhancers. Nat Commun 12, 494 (2021). https://doi.org/10.1038/s41467-020-20766-0

Kamran, M.*, Liang, J.Y., 2*, Liu, B., Li, Y., Gao, J.F. Keating, A., Mohamed, F., Dai S.D., Reinhardt, R., Yang, J., Wu, Z.D., Huang H. The Clusters of Transcription Factors NFATC2, STAT5, GATA2, AP1, RUNX1 and EGR2 Binding Sites at the Induced Il13 Enhancers Mediate Il13 Gene Transcription in Response to Antigenic Stimulation. J Immunol, Nov, 13, 2020, 10.4049/jimmunol.2000985.

Li Y, Qi X, Liu B, and Huang H.  The STAT5-GATA2 Pathway Is Critical in Basophil and Mast Cell Differentiation and Maintenance. J Immunol. 2015, 194: 4328-38. (Also see Editorial in “In This Issue”)

Qi X, L. Chaves, Y.H. Zhuang, Y. Chen, D. Wang, J. Chahon, B. Graham, K. Ohmori, and Huang H.  Antagonistic regulation by transcription factors C/EBPa and MITF specifies basophil and mast cell fates.  Immunity, 2013, 39, 97-110.

A complete list of my publications can be found on ORCID https://ORCID.org/0000-0001-7317-8983

Academic Affiliations

Professor, Department of Immunology & Microbiology, University of Colorado School of Medicine

Teaching & Professional Positions

Faculty member in the Medical Scientist Training Program and Regenerative Medicine and Stem Cell Biology Program, CU School of Medicine

Website Information

Department of Immunology & Microbiology Colorado University School of Medicine