Schepens Eye Research Institute and the Department of Ophthalmology Harvard Medical School, United States.
J Neuroimmunol. 2011 Mar;232(1-2):17-25. doi: 10.1016/j.jneuroim.2010.09.025. Epub 2010 Oct 20.
The functionality of immune cells is manipulated within the ocular microenvironment to protect the sensitive and non-regenerating light-gathering tissue from the collateral damage of inflammation. This is mediated partly by the constitutive presence of immunomodulating neuropeptides. Treating primary resting macrophages with soluble factors produced by the posterior eye induced co-expression of Arginase1 and NOS2. The neuropeptides alpha-melanocyte stimulating hormone and Neuropeptide Y alternatively activated the macrophages to co-express Arginase1 and NOS2 like myeloid suppressor cells. Similar co-expressing cells were found within healthy, but not in wounded retinas. Therefore, the healthy retina regulates macrophage functionality to the benefit of ocular immune privilege.
免疫细胞的功能在眼部微环境中受到调控,以保护敏感且不可再生的光收集组织免受炎症的附带损伤。这部分是通过免疫调节神经肽的固有存在来介导的。用眼后产生的可溶性因子处理原代静止巨噬细胞,诱导精氨酸酶 1 和 NOS2 的共表达。神经肽α-黑色素细胞刺激素和神经肽 Y 可交替激活巨噬细胞,使其像髓样抑制细胞一样共表达精氨酸酶 1 和 NOS2。在健康的视网膜中发现了类似的共表达细胞,但在受伤的视网膜中没有。因此,健康的视网膜调节巨噬细胞的功能,有利于眼部免疫特权。