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Mac-1 的抑制作用可使人类巨噬细胞在 ICAM-1 上沿剪切流的方向迁移。

Inhibition of Mac-1 allows human macrophages to migrate against the direction of shear flow on ICAM-1.

机构信息

Department of Biomedical Engineering, New Jersey Institute of Technology, Newark, NJ 07103.

Department of Bioengineering, University of Pennsylvania, Philadelphia, PA 19104.

出版信息

Mol Biol Cell. 2024 Oct 1;35(10):br18. doi: 10.1091/mbc.E24-03-0114. Epub 2024 Aug 21.

Abstract

All immune cells must transit from the blood to distal sites such as the lymph nodes, bone marrow, or sites of infection. Blood borne monocytes traffic to the site of inflammation by adhering to the endothelial surface and migrating along endothelial intracellular adhesion molecule 1 (ICAM-1) by their ligand's macrophage 1 antigen (Mac-1) and lymphocyte functional antigen 1 (LFA-1) to transmigrate through the endothelium. Poor patient prognoses in chronic inflammation and tumors have been attributed to the hyper recruitment of certain types of macrophages. Therefore, targeting the binding of ICAM-1 to its respective ligands provides a novel approach to targeting the recruitment of macrophages. To that end, we determined whether the loss of Mac-1 expression could induce this upstream migration behavior by using blocking antibodies against Mac-1 to examine the effects of hydrodynamic flow on the migration of the human macrophage cell line U-937 on ICAM-1 surfaces. Blocking Mac-1 on U-937 cells led to upstream migration against the direction of shear flow on ICAM-1 surfaces. In sum, the ability of macrophages to migrate upstream when Mac-1 is blocked represents a new avenue to precisely control the differentiation, migration, and trafficking of macrophages.

摘要

所有免疫细胞都必须从血液转移到远处的部位,如淋巴结、骨髓或感染部位。血液来源的单核细胞通过黏附在内皮表面并沿着内皮细胞间黏附分子 1(ICAM-1)迁移,通过其配体巨噬细胞 1 抗原(Mac-1)和淋巴细胞功能抗原 1(LFA-1)来穿越内皮细胞,从而转移到炎症部位。慢性炎症和肿瘤中患者预后不良归因于某些类型的巨噬细胞的过度募集。因此,针对 ICAM-1 与其各自配体的结合提供了一种靶向募集巨噬细胞的新方法。为此,我们通过使用针对 Mac-1 的阻断抗体来确定 Mac-1 表达的丧失是否可以诱导这种上游迁移行为,以检查水力流对人巨噬细胞系 U-937 在 ICAM-1 表面上迁移的影响。在 U-937 细胞上阻断 Mac-1 导致在 ICAM-1 表面上沿剪切流的方向发生上游迁移。总之,当 Mac-1 被阻断时,巨噬细胞向上游迁移的能力代表了一种精确控制巨噬细胞分化、迁移和运输的新途径。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/00d5/11481704/e335ba52fedc/mbc-35-br18-g001.jpg

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