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小鼠肥大细胞发育与迁移途径:追踪肥大细胞的起源与路径

Pathways of murine mast cell development and trafficking: tracking the roots and routes of the mast cell.

作者信息

Hallgren Jenny, Gurish Michael F

机构信息

Division of Rheumatology, Immunology and Allergy, Brigham and Women's Hospital, Boston, MA 02115, USA.

出版信息

Immunol Rev. 2007 Jun;217:8-18. doi: 10.1111/j.1600-065X.2007.00502.x.

DOI:10.1111/j.1600-065X.2007.00502.x
PMID:17498048
Abstract

The appreciation of the role of the mast cell (MC) in inflammatory processes has expanded dramatically during the last decade. Many of these processes, especially more prolonged responses, are accompanied by an increase in the number of MCs, and much of this increase is likely because of recruitment of immature progenitors with subsequent maturation under the control of the tissue microenvironment. We have begun to identify many of the cell-surface molecules that control this influx and have traced the development of these cells back to their hematopoietic roots. This development proceeds along the myelomonocytic pathway with distinct intermediates having been identified in both bone marrow and spleen. The expression of alpha4beta7 integrins has played a prominent role in this process, as it helped identify a bipotent basophil MC precursor in the spleens of C57BL/6 mice. This integrin also controls basal influx into the intestine and, along with alpha4beta1 integrins, plays a critical role in recruitment to inflamed lungs. Investigation of chemokines and chemokine receptors in these processes led to the identification of a dual role for the murine interleukin-8 receptor CXCR2. This alpha-chemokine receptor affects MC progenitor trafficking by its expression by MC progenitors and by its expression on stromal cells, likely endothelium, affecting trafficking to both intestine under basal conditions and lung during inflammatory recruitment.

摘要

在过去十年中,对肥大细胞(MC)在炎症过程中作用的认识有了显著扩展。许多这些过程,尤其是持续时间较长的反应,都伴随着肥大细胞数量的增加,而这种增加很大程度上可能是由于未成熟祖细胞的募集,随后在组织微环境的控制下成熟。我们已经开始识别许多控制这种流入的细胞表面分子,并将这些细胞的发育追溯到它们的造血根源。这种发育沿着髓单核细胞途径进行,在骨髓和脾脏中都已鉴定出不同的中间阶段。α4β7整合素的表达在这一过程中发挥了重要作用,因为它有助于在C57BL/6小鼠的脾脏中识别一种双能嗜碱性肥大细胞前体。这种整合素还控制着基础状态下进入肠道的细胞流入,并且与α4β1整合素一起,在募集到炎症肺部的过程中起关键作用。对这些过程中趋化因子和趋化因子受体的研究导致了对小鼠白细胞介素-8受体CXCR2双重作用的识别。这种α趋化因子受体通过肥大细胞前体的表达以及在基质细胞(可能是内皮细胞)上的表达来影响肥大细胞前体的运输,在基础状态下影响向肠道的运输,在炎症募集期间影响向肺部的运输。

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