Literature DB >> 7703852

Analysis of hydrophobicity in the alpha and beta chemokine families and its relevance to dimerization.

D G Covell1, G W Smythers, A M Gronenborn, G M Clore.   

Abstract

The chemokine family of chemotactic cytokines plays a key role in orchestrating the immune response. The family has been divided into 2 subfamilies, alpha and beta, based on the spacing of the first 2 cysteine residues, function, and chromosomal location. Members within each subfamily have 25-70% sequence identity, whereas the amino acid identity between members of the 2 subfamilies ranges from 20 to 40%. A quantitative analysis of the hydrophobic properties of 11 alpha and 9 beta chemokine sequences, based on the coordinates of the prototypic alpha and beta chemokines, interleukin-8 (IL-8), and human macrophage inflammatory protein-1 beta (hMIP-1 beta), respectively, is presented. The monomers of the alpha and beta chemokines have their strongest core hydrophobic cluster at equivalent positions, consistent with their similar tertiary structures. In contrast, the pattern of monomer surface hydrophobicity between the alpha and beta chemokines differs in a manner that is fully consistent with the observed differences in quaternary structure. The most hydrophobic surface clusters on the monomer subunits are located in very different regions of the alpha and beta chemokines and comprise in each case the amino acids that are buried at the interface of their respective dimers. The theoretical analysis of hydrophobicity strongly supports the hypothesis that the distinct dimers observed for IL-8 and hMIP-1 beta are preserved for all the alpha and beta chemokines, respectively. This provides a rational explanation for the lack of receptor crossbinding and reactivity between the alpha and beta chemokine subfamilies.

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Year:  1994        PMID: 7703852      PMCID: PMC2142647          DOI: 10.1002/pro.5560031119

Source DB:  PubMed          Journal:  Protein Sci        ISSN: 0961-8368            Impact factor:   6.725


  21 in total

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Journal:  Adv Immunol       Date:  1994       Impact factor: 3.543

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9.  Mapping the binding surface of interleukin-8 complexed with an N-terminal fragment of the type 1 human interleukin-8 receptor.

Authors:  R T Clubb; J G Omichinski; G M Clore; A M Gronenborn
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4.  Chemical modification of a variant of human MIP-1alpha; implications for dimer structure.

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5.  Novel dimeric interface and electrostatic recognition in bacterial Cu,Zn superoxide dismutase.

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  6 in total

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