Literature DB >> 9359703

A novel protein that participates in nonself discrimination of malignant cells by homologous complement.

M Matsumoto1, J Takeda, N Inoue, T Hara, M Hatanaka, K Takahashi, S Nagasawa, H Akedo, T Seya.   

Abstract

The human complement (C) system protects an individual against substances of nonself origin, including xenografts and microbial pathogens. Human cells express C-regulatory proteins, CD46 and CD55, thereby circumventing attack by C3, a major effector of C. Nevertheless, certain malignant cells, particularly those undergoing apoptotic stress, can activate homologous C, overcoming the regulatory actions of CD46 and/or CD55. The molecular mechanisms whereby malignant cells are tagged by homologous C3 remain largely unknown. We identified a novel gene product that converts human cells into targets for homologous complement. Only malignant cells and cell lines exposed to Fas or X-irradiation stimuli produced this protein, designated M161Ag, which was an unglycosylated 43-kDa protein. Analysis of cloned cDNAs indicated that this molecule was a secretory protein containing five amino acids encoded by TGA codons. Its functions were unique in that once secreted from the tumor cells, it bound back to the surface of these cells and activated homologous complement (C3) via the alternative pathway, allowing for C3 deposition on the membrane. This molecule may offer new insight into innate immunity; surveillance of tumor cells by complement is a common feature in the human immune system.

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Year:  1997        PMID: 9359703     DOI: 10.1038/nm1197-1266

Source DB:  PubMed          Journal:  Nat Med        ISSN: 1078-8956            Impact factor:   53.440


  10 in total

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Review 2.  Mycoplasma lipoproteins and Toll-like receptors.

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3.  Molecular cloning of a murine homologue of membrane cofactor protein (CD46): preferential expression in testicular germ cells.

Authors:  A Tsujimura; K Shida; M Kitamura; M Nomura; J Takeda; H Tanaka; M Matsumoto; K Matsumiya; A Okuyama; Y Nishimune; M Okabe; T Seya
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4.  Antibody-independent classical complement pathway activation and homologous C3 deposition in xeroderma pigmentosum cell lines.

Authors:  M Kurita; M Matsumoto; S Tsuji; M Kawakami; Y Suzuki; H Hayashi; K Toyoshima; T Seya
Journal:  Clin Exp Immunol       Date:  1999-06       Impact factor: 4.330

5.  Complement activation in Mycoplasma fermentans-induced mycoplasma clearance from infected cells: probing of the organism with monoclonal antibodies against M161Ag.

Authors:  S Kikkawa; M Matsumoto; T Sasaki; M Nishiguchi; K Tanaka; K Toyoshima; T Seya
Journal:  Infect Immun       Date:  2000-03       Impact factor: 3.441

6.  Differential posttranslational processing confers intraspecies variation of a major surface lipoprotein and a macrophage-activating lipopeptide of Mycoplasma fermentans.

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7.  Ascitic complement system in ovarian cancer.

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8.  CD59 Regulation by SOX2 Is Required for Epithelial Cancer Stem Cells to Evade Complement Surveillance.

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9.  Modulation of CD59 expression by restrictive silencer factor-derived peptides in cancer immunotherapy for neuroblastoma.

Authors:  Rossen M Donev; Lisa C Gray; Baalasubramanian Sivasankar; Timothy R Hughes; Carmen W van den Berg; B Paul Morgan
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10.  Use of cancer-specific yeast-secreted in vivo biotinylated recombinant antibodies for serum biomarker discovery.

Authors:  Nathalie Scholler; Jennifer A Gross; Barbara Garvik; Lance Wells; Yan Liu; Christian M Loch; Arturo B Ramirez; Martin W McIntosh; Paul D Lampe; Nicole Urban
Journal:  J Transl Med       Date:  2008-07-24       Impact factor: 5.531

  10 in total

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