Adhesion molecule cross-linking and cytokine exposure modulate IgE- and non-IgE-dependent basophil activation

Kalm Frida; Mansouri Ladan; Russom Aman; Lundahl Joachim; Nopp Anna

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Adhesion molecule cross-linking and cytokine exposure modulate IgE- and non-IgE-dependent basophil activation

机译：粘附分子交联和细胞因子暴露调节IgE和非IgE依赖性嗜碱性泳泳池激活

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Basophils are known for their role in allergic inflammation, which makes them suitable targets in allergy diagnostics such as the basophil activation test (BAT) and the microfluidic immunoaffinity basophil activation test (miBAT). Beside their role in allergy, basophils have an immune modulatory role in both innate immunity and adaptive immunity. To accomplish this mission, basophils depend on the capability to migrate from blood to extravascular tissues, which includes interactions with endothelial cells, extracellular matrix and soluble mediators. Their receptor repertoire is well known, but less is known how these receptor-ligand interactions impact the degranulation process and the responsiveness to subsequent activation. As the consequences of these interactions are crucial to fully appreciate the role of basophils in immune modulation and to enable optimization of the miBAT, we explored how basophil activation status is regulated by cytokines and cross-linking of adhesion molecules. The expression of adhesion molecules and activation markers on basophils from healthy blood donors was analysed by flow cytometry. Cross-linking of CD203c, CD62L, CD11b and CD49d induced a significant upregulation of CD63 and CD203c. To mimic in vivo conditions, valid also for miBAT, CD62L and CD49d were cross-linked followed by IgE-dependent activation (anti-IgE), which caused a reduced CD63 expression compared with anti-IgE activation only. IL-3 and IL-33 priming caused increased CD63 expression after IgE-independent activation (fMLP). Together, our data suggest that mechanisms operational both in the microfluidic chip and in vivo during basophil adhesion may impact basophil anaphylactic and piecemeal degranulation procedures and hence their immune regulatory function.

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来源
《Immunology: An Official Journal of the British Society for Immunology》 |2021年第1期|共13页
作者
Kalm Frida; Mansouri Ladan; Russom Aman; Lundahl Joachim; Nopp Anna;
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作者单位

Karolinska Inst Dept Clin Sci &

Educ Sodersjukhuset SE-11883 Stockholm Sweden;

Karolinska Inst Dept Clin Sci &

Educ Sodersjukhuset SE-11883 Stockholm Sweden;

KTH Royal Inst Technol Div Nanobiotechnol Dept Prot Sci Sci Life Lab Stockholm Sweden;

Karolinska Inst Dept Clin Sci &

Educ Sodersjukhuset SE-11883 Stockholm Sweden;

Karolinska Inst Dept Clin Sci &

Educ Sodersjukhuset SE-11883 Stockholm Sweden;

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原文格式 PDF
正文语种 eng
中图分类医学免疫学;
关键词
CD203c; CD62L; degranulation; miBAT;

机译：CD203C;CD62L;脱粒;MIBAT;

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Adhesion molecule cross-linking and cytokine exposure modulate IgE- and non-IgE-dependent basophil activation

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