Glenn E. Nedwin scite author profile

When leukocytes are exposed to mitogens or antigens in vitro, they release bone-resorbing activity into the culture supernatants which can be detected by bioassay. Like many lymphocyte-monocyte products, this activity has been difficult to purify because of its low abundance in activated leukocyte cultures and the unwieldy bioassay required to detect biological activity. Partially purified preparations of this activity inhibit bone collagen synthesis in organ cultures of fetal rat calvariae. Recent data suggest that both activated lymphocytes and monocytes release factors which could contribute to this activity. Recently, monocyte-derived tumour necrosis factor alpha (TNF-alpha) and lymphocyte-derived tumour necrosis factor beta (TNF-beta) (previously called lymphotoxin), two multifunctional cytokines which have similar cytotoxic effects on neoplastic cell lines, have been purified to homogeneity and their complementary DNAs cloned and expressed in Escherichia coli. As both of these cytokines are likely to be present in activated leukocyte supernatants, we tested purified recombinant preparations for their effects on bone resorption and bone collagen synthesis in vitro, and report here that both cytokines at 10(-7) to 10(-9) M caused osteoclastic bone resorption and inhibited bone collagen synthesis. These data suggest that at least part of the bone-resorbing activity present in activated leukocyte culture supernatants may be due to these cytokines.

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Human Lymphotoxin and tumor necrosis factor genes: structure, homology and chromosomal localization

Nedwin¹,

et al. 1985

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Human Tumor Necrosis Factor and Lymphotoxin are cytotoxic proteins which have similar biological activities and share 30 percent amino acid homology. The single copy genes which encode these proteins share several structural features: each gene is approximately three kilobase pairs in length and is interrupted by three introns. In addition, these genes are closely linked and have been mapped to human chromosome 6. However, only the last exons of both genes, which code for more than 80 percent of each secreted protein, are significantly homologous (56 percent).

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Cloning and expression of cDNA for human lymphotoxin, a lymphokine with tumour necrosis activity

Gray¹,

Aggarwal²,

Benton³

et al. 1984

Nature

599

181

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Recombinant human β-galactoside binding lectin suppresses clinical and histological signs of experimental autoimmune encephalomyelitis

Offner

Celnik

Bringman

et al. 1990

Journal of Neuroimmunology

190

108

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Glenn E. Nedwin

Human tumour necrosis factor: precursor structure, expression and homology to lymphotoxin

Stimulation of bone resorption and inhibition of bone formation in vitro by human tumour necrosis factors

Human Lymphotoxin and tumor necrosis factor genes: structure, homology and chromosomal localization

Cloning and expression of cDNA for human lymphotoxin, a lymphokine with tumour necrosis activity

Recombinant human β-galactoside binding lectin suppresses clinical and histological signs of experimental autoimmune encephalomyelitis

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