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Characterization of receptors for human tumour necrosis factor and their regulation by γ-interferon
Tumour necrosis factors, TNF- α and TNF- β (previously called lymphotoxin), are the products of activated monocytes and lymphocytes, respectively, and both have recently been purified, sequenced and cloned by recombinant DNA methods 1–5 , revealing 35% identity and 50% homology in the amino-acid seq...
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Published in: | Nature (London) 1985-12, Vol.318 (6047), p.665-667 |
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Main Authors: | , , |
Format: | Article |
Language: | English |
Subjects: | |
Citations: | Items that this one cites Items that cite this one |
Online Access: | Get full text |
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Summary: | Tumour necrosis factors, TNF-
α
and TNF-
β
(previously called lymphotoxin), are the products of activated monocytes and lymphocytes, respectively, and both have recently been purified, sequenced and cloned by recombinant DNA methods
1–5
, revealing 35% identity and 50% homology in the amino-acid sequence. Both proteins have been found to be specifically toxic to many tumour cells. Furthermore, it has been reported that various interferons are synergistic with TNF for anti-tumour effects
in vitro
6–8
, while activities attributed to the two proteins have also been shown to necrotize various tumours
in vivo
2,3,9
. We have now prepared
125
I-labelled highly purified recombinant human TNF-
α
to study in detail its binding to the human cervical carcinoma cell line ME-180. Our results indicate that there is a single class of specific high-affinity receptors for TNF on this cell line which has a K
d
of about 0.2 nM and an average of 2,000 receptor sites per cell. The binding of labelled TNF-
α
to these cells can be inhibited by both TNF-
α
and TNF-
β
but not by
γ
-interferon (IFN-
γ
). However, preincubation of cells with IFN-
γ
increases the total number of TNF receptors two to threefold without any significant change in the affinity constant. This is the first report that TNF-
α
and -
β
share a common receptor and that the receptors can be up-regulated by interferon. Our results may explain previous observations regarding similar biological activities observed for these two cytotoxic proteins and also their synergistic action with interferons. |
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ISSN: | 0028-0836 1476-4687 |
DOI: | 10.1038/318665a0 |