IDENTIFICATION OF CYTOKINE-INDUCED NEUTROPHIL CHEMOATTRACTANTS (CINC), RAT GRO/CINC-2-ALPHA AND CINC-2-BETA, PRODUCED BY GRANULATION-TISSUE IN CULTURE - PURIFICATION, COMPLETE AMINO-ACID-SEQUENCES AND CHARACTERIZATION

被引:124
作者
NAKAGAWA, H [1 ]
KOMORITA, N [1 ]
SHIBATA, F [1 ]
IKESUE, A [1 ]
KONISHI, K [1 ]
FUJIOKA, M [1 ]
KATO, H [1 ]
机构
[1] TOYAMA MED & PHARMACEUT UNIV,FAC MED,SUGITANI,TOYAMA 93001,JAPAN
来源
BIOCHEMICAL JOURNAL | 1994年 / 301卷
关键词
D O I
10.1042/bj3010545
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Four basic neutrophil chemotactic factors (chemokines) have been purified from conditioned medium of granulation tissue obtained from carrageenin-induced inflammation in the rat. On the basis of their N-terminal amino acid sequences, one of the chemokines was identical with rat GRO/cytokine-induced neutrophil chemoattractant (CINC) which we reported previously, and another was identical with rat macrophage inflammatory protein-2 (MIP-2). Two other chemokines were novel chemoattractants related to MIP-2. The novel chemokines are referred to as rat GRO/CINC-2 alpha and CINC-2 beta, and consequently CINC and rat MIP-2 are renamed rat GRO/CINC-1 and CINC-3 respectively. The complete amino acid sequences of purified CINC-2 alpha and CINC-3 were determined by analysis of the fragments isolated from proteinase V8-treated CINCs. The cDNA for CINC-2 beta was cloned by reverse transcription/PCR amplification using specific primers starting with total RNA extracted from lipopolysaccharide-stimulated rat macrophages. A comparison of the amino acid sequence encoded by the cDNA with the N-terminal amino acid sequence of purified CINC-2 beta revealed that mature CINC-2 beta is a 68-residue chemoattractant produced by cleavage of a 32-residue signal peptide. The difference in amino acid sequences between CINC-2 alpha and CINC-2 beta consisted of only three C-terminal residues. Rat GRO/CINC-2 alpha is a major chemokine, and the four purified chemokines have similar chemotactic activity, suggesting that they contribute to neutrophil infiltration into inflammatory sites in rats.
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页码:545 / 550
页数:6
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