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巨噬细胞半乳糖型C型凝集素-1缺陷小鼠胚胎发育中神经管内辐射诱导凋亡细胞清除的延迟。

Retardation of removal of radiation-induced apoptotic cells in developing neural tubes in macrophage galactose-type C-type lectin-1-deficient mouse embryos.

作者信息

Yuita Hiroshi, Tsuiji Makoto, Tajika Yuki, Matsumoto Yoshihisa, Hirano Kazuya, Suzuki Norio, Irimura Tatsuro

机构信息

Department of Radiation Oncology, University of Tokyo, Hongo 7-3-1, Bunkyo-ku, Tokyo 113-0033, Japan.

出版信息

Glycobiology. 2005 Dec;15(12):1368-75. doi: 10.1093/glycob/cwj028. Epub 2005 Aug 11.

DOI:10.1093/glycob/cwj028
PMID:16096344
Abstract

MGL1/CD301a is a C-type lectin that recognizes galactose and N-acetylgalactosamine as monosaccharides and is expressed on limited populations of macrophages and dendritic cells at least in adult mice. In this study, pregnant mice with Mgl1+/- genotype were mated with Mgl1+/- or Mgl1-/- genotype males, and the embryos were used to assess a hypothesis that this molecule plays an important role in the clearance of apoptotic cells. After X-ray irradiation at 1 Gy of developing embryos at 10.5 days post coitus (d.p.c.), the number of Mgl1-/- pups was significantly reduced as compared with Mgl1+/+ pups. Distributions of MGL1-positive cells, MGL2-positive cells, and apoptotic cells were histologically examined in irradiated Mgl1+/+ embryos. MGL1-positive cells were detected in the neural tube in which many cells undergo apoptosis, whereas MGL2-positive cells were not observed. Biotinylated recombinant MGL1 bound a significant portion of the apoptotic cells. When Mgl1+/+ and Mgl1-/- embryos were examined for the presence of apoptotic cells, similar numbers of apoptotic cells gave rise, but the clearance of these cells was slower in Mgl1-/- embryos than in Mgl1+/+ embryos. These results strongly suggest that MGL1/CD301a is involved in the clearance of apoptotic cells. This process should be essential in the repair and normal development of X-ray-irradiated embryos.

摘要

MGL1/CD301a是一种C型凝集素,可识别半乳糖和N-乙酰半乳糖胺作为单糖,至少在成年小鼠中表达于有限数量的巨噬细胞和树突状细胞上。在本研究中,将基因型为Mgl1+/-的怀孕小鼠与基因型为Mgl1+/-或Mgl1-/-的雄性小鼠交配,并使用胚胎来评估该分子在凋亡细胞清除中起重要作用的假说。在交配后10.5天(d.p.c.)对发育中的胚胎进行1 Gy的X射线照射后,与Mgl1+/+幼崽相比,Mgl1-/-幼崽的数量显著减少。对受照射的Mgl1+/+胚胎进行组织学检查,观察MGL1阳性细胞、MGL2阳性细胞和凋亡细胞的分布。在许多细胞发生凋亡的神经管中检测到MGL1阳性细胞,而未观察到MGL2阳性细胞。生物素化的重组MGL1结合了相当一部分凋亡细胞。当检查Mgl1+/+和Mgl1-/-胚胎中凋亡细胞的存在情况时,产生的凋亡细胞数量相似,但Mgl1-/-胚胎中这些细胞的清除速度比Mgl1+/+胚胎慢。这些结果强烈表明MGL1/CD301a参与凋亡细胞的清除。这一过程对于X射线照射胚胎的修复和正常发育应该是必不可少的。

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