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Immunology. 2006 Apr;117(4):494-501. doi: 10.1111/j.1365-2567.2006.02324.x.
2
Effective targeting of pathogens to neutrophils via chimeric surfactant protein D/anti-CD89 protein.通过嵌合表面活性蛋白D/抗CD89蛋白将病原体有效靶向至中性粒细胞。
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Bispecific molecules directed to the Fc receptor for IgA (Fc alpha RI, CD89) and tumor antigens efficiently promote cell-mediated cytotoxicity of tumor targets in whole blood.靶向IgA的Fc受体(FcαRI,CD89)和肿瘤抗原的双特异性分子可有效促进全血中肿瘤靶标的细胞介导细胞毒性。
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A recombinant bispecific single-chain fragment variable specific for HLA class II and Fc alpha RI (CD89) recruits polymorphonuclear neutrophils for efficient lysis of malignant B lymphoid cells.一种针对 HLA Ⅱ类和 FcαRI(CD89)的重组双特异性单链片段可变区,可募集多形核粒细胞,有效裂解恶性 B 淋巴细胞。
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Effective phagocytosis and killing of Candida albicans via targeting FcgammaRI (CD64) or FcalphaRI (CD89) on neutrophils.通过靶向中性粒细胞上的FcγRI(CD64)或FcαRI(CD89)有效吞噬和杀灭白色念珠菌。
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Human monocytes expressing a CEA-specific chimeric CD64 receptor specifically target CEA-expressing tumour cells in vitro and in vivo.表达癌胚抗原(CEA)特异性嵌合CD64受体的人单核细胞在体外和体内均可特异性靶向表达CEA的肿瘤细胞。
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[Regulation of Fc receptor expression by immune complexes on neutrophils and U937 cells].[免疫复合物对中性粒细胞和U937细胞上Fc受体表达的调节]
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Uptake of HLA Alloantigens via CD89 and CD206 Does Not Enhance Antigen Presentation by Indirect Allorecognition.通过 CD89 和 CD206 摄取 HLA 同种异体抗原不会增强间接同种异体识别的抗原呈递。
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本文引用的文献

1
Immature neutrophils mediate tumor cell killing via IgA but not IgG Fc receptors.未成熟中性粒细胞通过IgA而非IgG Fc受体介导肿瘤细胞杀伤。
J Immunol. 2005 May 1;174(9):5472-80. doi: 10.4049/jimmunol.174.9.5472.
2
Immunoregulatory functions of surfactant proteins.表面活性蛋白的免疫调节功能。
Nat Rev Immunol. 2005 Jan;5(1):58-68. doi: 10.1038/nri1528.
3
Protein kinase C-alpha and -delta are required for FcalphaR (CD89) trafficking to MHC class II compartments and FcalphaR-mediated antigen presentation.蛋白激酶C-α和-δ是FcalphaR(CD89)转运至MHC II类区室以及FcalphaR介导的抗原呈递所必需的。
Traffic. 2004 Aug;5(8):577-94. doi: 10.1111/j.1600-0854.2004.00202.x.
4
Effective targeting of pathogens to neutrophils via chimeric surfactant protein D/anti-CD89 protein.通过嵌合表面活性蛋白D/抗CD89蛋白将病原体有效靶向至中性粒细胞。
J Immunol. 2004 Apr 15;172(8):4934-40. doi: 10.4049/jimmunol.172.8.4934.
5
Surfactant proteins A and D inhibit the growth of Gram-negative bacteria by increasing membrane permeability.表面活性蛋白A和D通过增加膜通透性来抑制革兰氏阴性菌的生长。
J Clin Invest. 2003 May;111(10):1589-602. doi: 10.1172/JCI16889.
6
Collections and ficolins: humoral lectins of the innate immune defense.集落刺激因子和纤维胶凝蛋白:天然免疫防御的体液凝集素
Annu Rev Immunol. 2003;21:547-78. doi: 10.1146/annurev.immunol.21.120601.140954. Epub 2001 Dec 19.
7
Structural requirements for SP-D function in vitro and in vivo: therapeutic potential of recombinant SP-D.
Immunobiology. 2002 Sep;205(4-5):619-31. doi: 10.1078/0171-2985-00159.
8
HIV-1 down-modulates gamma signaling chain of Fc gamma R in human macrophages: a possible mechanism for inhibition of phagocytosis.HIV-1下调人类巨噬细胞中FcγR的γ信号链:一种抑制吞噬作用的可能机制。
J Immunol. 2002 Mar 15;168(6):2895-903. doi: 10.4049/jimmunol.168.6.2895.
9
Surfactant protein-D and pulmonary host defense.表面活性蛋白-D与肺部宿主防御
Respir Res. 2000;1(2):93-108. doi: 10.1186/rr19. Epub 2000 Aug 25.
10
Differential recruitment of accessory molecules by FcgammaRI during monocyte differentiation.FcγRI在单核细胞分化过程中对辅助分子的差异性募集。
Eur J Immunol. 2001 Sep;31(9):2718-25. doi: 10.1002/1521-4141(200109)31:9<2718::aid-immu2718>3.0.co;2-7.

表面活性蛋白D/抗Fc受体靶向单核细胞CD64或CD89介导细菌摄取。

Monocyte CD64 or CD89 targeting by surfactant protein D/anti-Fc receptor mediates bacterial uptake.

作者信息

Tacken Paul J, Batenburg Joseph J

机构信息

Department of Biochemistry and Cell Biology, Graduate School of Animal Health, Faculty of Veterinary Medicine, Utrecht University, Utrecht, the Netherlands.

出版信息

Immunology. 2006 Apr;117(4):494-501. doi: 10.1111/j.1365-2567.2006.02324.x.

DOI:10.1111/j.1365-2567.2006.02324.x
PMID:16556263
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1782248/
Abstract

We recently showed that a chimeric protein, consisting of a recombinant fragment of human surfactant protein D (rfSP-D) coupled to a Fab' fragment directed against the human Fcalpha receptor (CD89), effectively targets pathogens recognized by SP-D to human neutrophils. The present study evaluates the effectiveness of chimeric rfSP-D/anti-Fc receptor proteins targeting Escherichia coli to CD89 or to the Fcgamma receptor I (CD64) on monocytes. Both chimeric rfSP-D/anti-Fc receptor proteins increased internalization of E. coli by the human promonocytic cell line U937, but only after induction of monocytic differentiation, despite the fact that the expression levels of CD64 and CD89 on undifferentiated cells were at least as high as on differentiated cells. The two chimeric rfSP-D/anti-Fc receptor proteins did not enhance each other's effect on E. coli uptake. Targeting to differentiated U937 cells was inhibited by blocking the interaction either between the rfSP-D part of the chimeric molecule and E. coli, or between the anti-Fc receptor Fab' fragment and the Fc receptor on the U937 cell. In conclusion, both CD64 and CD89 on U937 cells prove to be suitable for targeting by rfSP-D/anti-Fc receptor proteins. However, in addition to mere Fc receptor expression, effective targeting requires monocytic differentiation.

摘要

我们最近发现,一种嵌合蛋白,由与人表面活性蛋白D的重组片段(rfSP-D)与针对人Fα受体(CD89)的Fab'片段偶联而成,能有效地将SP-D识别的病原体靶向人类中性粒细胞。本研究评估了将大肠杆菌靶向单核细胞上的CD89或Fcγ受体I(CD64)的嵌合rfSP-D/抗Fc受体蛋白的有效性。两种嵌合rfSP-D/抗Fc受体蛋白均增加了人原单核细胞系U937对大肠杆菌的内化,但仅在诱导单核细胞分化后才出现这种情况,尽管未分化细胞上CD64和CD89的表达水平至少与分化细胞上的一样高。这两种嵌合rfSP-D/抗Fc受体蛋白并未增强彼此对大肠杆菌摄取的影响。通过阻断嵌合分子的rfSP-D部分与大肠杆菌之间的相互作用,或抗Fc受体Fab'片段与U937细胞上的Fc受体之间的相互作用,可抑制对分化的U937细胞的靶向作用。总之,U937细胞上的CD64和CD89均被证明适用于rfSP-D/抗Fc受体蛋白的靶向作用。然而,除了单纯的Fc受体表达外,有效的靶向作用还需要单核细胞分化。