Department of Cell Biology, Microbiology and Molecular Biology, University of South Florida, Tampa, FL, USA.
Eur J Immunol. 2012 Jul;42(7):1785-95. doi: 10.1002/eji.201142092.
We previously showed that germline or induced SHIP deficiency expands immuno-regulatory cell numbers in T lymphoid and myeloid lineages. We postulated these increases could be interrelated. Here, we show that myeloid-specific ablation of SHIP leads to the expansion of both myeloid-derived suppressor cell (MDSC) and regulatory T (Treg) cell numbers, indicating SHIP-dependent control of Treg-cell numbers by a myeloid cell type. Conversely, T-lineage specific ablation of SHIP leads to expansion of Treg-cell numbers, but not expansion of the MDSC compartment, indicating SHIP also has a lineage intrinsic role in limiting Treg-cell numbers. However, the SHIP-deficient myeloid cell that promotes MDSC and Treg-cell expansion is not an MDSC as they lack SHIP protein expression. Thus, regulation of MDSC numbers in vivo must be controlled in a cell-extrinsic fashion by another myeloid cell type. We had previously shown that G-CSF levels are profoundly increased in SHIP(-/-) mice, suggesting this myelopoietic growth factor could promote MDSC expansion in a cell-extrinsic fashion. Consistent with this hypothesis, we find that G-CSF is required for expansion of the MDSC splenic compartment in mice rendered SHIP-deficient as adults. Thus, SHIP controls MDSC numbers, in part, by limiting production of the myelopoietic growth factor G-CSF.
我们之前表明,SHIP 的种系或诱导缺失会增加 T 淋巴谱系和髓系中的免疫调节细胞数量。我们推测这些增加可能是相互关联的。在这里,我们表明髓系特异性敲除 SHIP 会导致髓源性抑制细胞 (MDSC) 和调节性 T (Treg) 细胞数量的扩张,表明 SHIP 通过一种髓样细胞类型控制 Treg 细胞数量。相反,T 谱系特异性敲除 SHIP 会导致 Treg 细胞数量的扩张,但不会导致 MDSC 区室的扩张,表明 SHIP 也在线粒体内在限制 Treg 细胞数量方面发挥作用。然而,促进 MDSC 和 Treg 细胞扩张的 SHIP 缺陷髓样细胞不是 MDSC,因为它们缺乏 SHIP 蛋白表达。因此,体内 MDSC 数量的调节必须以细胞外方式由另一种髓样细胞类型控制。我们之前表明,SHIP(-/-) 小鼠中的 G-CSF 水平显著增加,表明这种骨髓生成生长因子可以以细胞外方式促进 MDSC 扩张。与这一假设一致,我们发现 G-CSF 是成年后 SHIP 缺陷小鼠脾脏 MDSC 区室扩张所必需的。因此,SHIP 通过限制骨髓生成生长因子 G-CSF 的产生来控制 MDSC 数量,部分原因。
