Person: Hu, Dan
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Publication Identification of Cytolytic CD161(^−)CD56(^+) Regulatory CD8 T Cells in Human Peripheral Blood
(Public Library of Science, 2013) Hu, Dan; Weiner, Howard; Ritz, JeromeWe previously developed methods for establishing CD8 regulatory T cell (Treg) clones from normal human peripheral blood and demonstrated that these clones were capable of killing T cell receptor (TCR)-activated autologous CD4 T cells. Based on phenotypic and functional characterization of the CD8 Treg clones, we have identified a corresponding population of endogenous CD8 Treg in normal human peripheral blood. These cells appear morphologically as large lymphocytes with abundant cytoplasm and have the following unique phenotype: CD3(^+)CD8(^+)CD161(^−)CD56(^+). The majority of CD8 Treg express CD45RA and CD62L with low or negative expression of CD45RO, CD25, CD27, CD28 and CCR7. The expression of CD94 and NKG2a on CD8 Treg was elevated compared to conventional CD8 T cells. Following in vitro activation, this T cell subset is capable of killing TCR-activated CD4 T cells. These studies identify an endogenous CD8 Treg population in humans and it will now be possible to characterize these cells in a variety of clinical conditions.
Publication Transcriptional signature of human pro-inflammatory TH17 cells identifies reduced IL10 gene expression in multiple sclerosis
(Nature Publishing Group UK, 2017) Hu, Dan; Notarbartolo, Samuele; Croonenborghs, Tom; Patel, Bonny; Cialic, Ron; Yang, Tun-Hsiang; Aschenbrenner, Dominik; Andersson, Karin M.; Gattorno, Marco; Pham, Minh; Kivisakk, Pia; Pierre, Isabelle V.; Lee, Youjin; Kiani, Karun; Bokarewa, Maria; Tjon, Emily; Pochet, Nathalie; Sallusto, Federica; Kuchroo, Vijay; Weiner, HowardWe have previously reported the molecular signature of murine pathogenic TH17 cells that induce experimental autoimmune encephalomyelitis (EAE) in animals. Here we show that human peripheral blood IFN-γ+IL-17+ (TH1/17) and IFN-γ−IL-17+ (TH17) CD4+ T cells display distinct transcriptional profiles in high-throughput transcription analyses. Compared to TH17 cells, TH1/17 cells have gene signatures with marked similarity to mouse pathogenic TH17 cells. Assessing 15 representative signature genes in patients with multiple sclerosis, we find that TH1/17 cells have elevated expression of CXCR3 and reduced expression of IFNG, CCL3, CLL4, GZMB, and IL10 compared to healthy controls. Moreover, higher expression of IL10 in TH17 cells is found in clinically stable vs. active patients. Our results define the molecular signature of human pro-inflammatory TH17 cells, which can be used to both identify pathogenic TH17 cells and to measure the effect of treatment on TH17 cells in human autoimmune diseases.