10.3389/fimmu.2018.01352.s001 Wojciech Baran Wojciech Baran Stephanie Oehrl Stephanie Oehrl Fareed Ahmad Fareed Ahmad Thomas Döbel Thomas Döbel Christina Alt Christina Alt Angelika Buske-Kirschbaum Angelika Buske-Kirschbaum Marc Schmitz Marc Schmitz Knut Schäkel Knut Schäkel data_sheet_1_Phenotype, Function, and Mobilization of 6-Sulfo LacNAc-Expressing Monocytes in Atopic Dermatitis.docx Frontiers 2018 atopic dermatitis dendritic cells 6-sulfo LacNAc-expressing monocytes immunology inflammation IL-12 CD86 2018-06-21 09:23:01 Dataset https://frontiersin.figshare.com/articles/dataset/data_sheet_1_Phenotype_Function_and_Mobilization_of_6-Sulfo_LacNAc-Expressing_Monocytes_in_Atopic_Dermatitis_docx/6632447 <p>Mononuclear phagocytes (MPs) are important immune regulatory cells in atopic dermatitis (AD). We previously identified 6-sulfo LacNAc-expressing monocytes (slanMo) as TNF-α- and IL-23-producing cells in psoriatic skin lesions and as inducers of IFN-γ-, IL-17-, and IL-22-producing T cells. These cytokines are also upregulated in AD and normalize with treatment, as recently shown for dupilumab-treated patients. We here asked for the role of slanMo in AD. Increased numbers of slanMo were found in AD skin lesions. In difference to other MPs in AD, slanMo lacked expression of FcɛRI, CD1a, CD14, and CD163. slanMo from blood of patients with AD expressed increased levels of CD86 and produced IL-12 and TNF-α at higher amounts than CD14<sup>+</sup> monocytes and myeloid dendritic cells. While CD14<sup>+</sup> monocytes from patients with AD revealed a reduced IL-12 production, we observed no difference in the cytokine production comparing slanMo in AD and healthy controls. Interestingly, experimentally induced mental stress, a common trigger of flares in patients with AD, rapidly mobilized slanMo which retained their high TNF-α-producing capacity. This study identifies slanMo as a distinct population of inflammatory cells in skin lesions and as proinflammatory blood cells in patients with AD. slanMo may, therefore, represent a potent future target for treatment of AD.</p>