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Expression and regulation of Siglec-6 (CD327) on human mast cells and basophils

西格莱克 嗜碱性粒细胞 免疫学 免疫球蛋白E 抗原 CD14型 下调和上调 细胞因子 生物 细胞生物学 流式细胞术 抗体 生物化学 基因
作者
Dubravka Smiljkovic,Harald Herrmann,Irina Sadovnik,Susanne Gamperl,Daniela Berger,Gabriele Stefanzl,Gregor Eisenwort,Gregor Hoermann,Sonja Kopanja,Yulia Dorofeeva,Margarete Focke‐Tejkl,Péter Jaksch,Konrad Höetzenecker,Zsolt Szépfalusi,Rudolf Valenta,Michel Arock,Peter Valent
出处
期刊:The Journal of Allergy and Clinical Immunology [Elsevier BV]
卷期号:151 (1): 202-211 被引量:18
标识
DOI:10.1016/j.jaci.2022.07.018
摘要

BackgroundMast cells (MC) and basophils are effector cells of allergic reactions and display a number of activation-linked cell surface antigens. Of these antigens, however, only a few are functionally relevant and specifically expressed in these cells.ObjectiveWe sought to identify MC- and basophil-specific surface molecules and to study their cellular distribution and regulation during cytokine-induced and IgE-dependent activation.MethodsMulticolor flow cytometry was performed to recognize surface antigens and to determine changes in antigen expression upon activation.ResultsWe identified Siglec-6 (CD327) as a differentially regulated surface antigen on human MC and basophils. In the bone marrow, Siglec-6 was expressed abundantly on MC in patients with mastocytosis and in reactive states, but it was not detected on other myeloid cells, with the exception of basophils and monocytes. In healthy individuals, allergic patients, and patients with chronic myeloid leukemia (CML), Siglec-6 was identified on CD203c+ blood basophils, a subset of CD19+ B lymphocytes, and few CD14+ monocytes, but not on other blood leukocytes. CML basophils expressed higher levels of Siglec-6 than normal basophils. IL-3 promoted Siglec-6 expression on normal and CML basophils, and stem cell factor increased the expression of Siglec-6 on tissue MC. Unexpectedly, IgE-dependent activation resulted in downregulation of Siglec-6 in IL-3–primed basophils, whereas in MC, IgE-dependent activation augmented stem cell factor–induced upregulation of Siglec-6.ConclusionsSiglec-6 is a dynamically regulated marker of MC and basophils. Activated MC and basophils exhibit unique Siglec-6 responses, including cytokine-dependent upregulation and unique, cell-specific, responses to IgE-receptor cross-linking. Mast cells (MC) and basophils are effector cells of allergic reactions and display a number of activation-linked cell surface antigens. Of these antigens, however, only a few are functionally relevant and specifically expressed in these cells. We sought to identify MC- and basophil-specific surface molecules and to study their cellular distribution and regulation during cytokine-induced and IgE-dependent activation. Multicolor flow cytometry was performed to recognize surface antigens and to determine changes in antigen expression upon activation. We identified Siglec-6 (CD327) as a differentially regulated surface antigen on human MC and basophils. In the bone marrow, Siglec-6 was expressed abundantly on MC in patients with mastocytosis and in reactive states, but it was not detected on other myeloid cells, with the exception of basophils and monocytes. In healthy individuals, allergic patients, and patients with chronic myeloid leukemia (CML), Siglec-6 was identified on CD203c+ blood basophils, a subset of CD19+ B lymphocytes, and few CD14+ monocytes, but not on other blood leukocytes. CML basophils expressed higher levels of Siglec-6 than normal basophils. IL-3 promoted Siglec-6 expression on normal and CML basophils, and stem cell factor increased the expression of Siglec-6 on tissue MC. Unexpectedly, IgE-dependent activation resulted in downregulation of Siglec-6 in IL-3–primed basophils, whereas in MC, IgE-dependent activation augmented stem cell factor–induced upregulation of Siglec-6. Siglec-6 is a dynamically regulated marker of MC and basophils. Activated MC and basophils exhibit unique Siglec-6 responses, including cytokine-dependent upregulation and unique, cell-specific, responses to IgE-receptor cross-linking.

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