Evolutionary, Structural and Functional Interplay of the IκB Family Members

Shaherin Basith,Vijayakumar Gosu,Balachandran Manavalan,Sangdun Choi,Vladimir N. Uversky

doi:10.1371/journal.pone.0054178

Abstract

A primary level of control for nuclear factor kappa B (NF-κB) is effected through its interactions with the inhibitor protein, inhibitor of kappa B (IκB). Several lines of evidence confirm the existence of multiple forms of IκB that appear to regulate NF-κB by distinct mechanisms. Therefore, we performed a comprehensive bioinformatics analysis to understand the evolutionary history and intrinsic functional diversity of IκB family members. Phylogenetic relationships were constructed to trace the evolution of the IκB family genes. Our phylogenetic analysis revealed 10 IκB subfamily members that clustered into 5 major clades. Since the ankyrin (ANK) domain appears to be more ancient than the Rel homology domain (RHD), our phylogenetic analysis suggests that some undefined ancestral set of ANK repeats acquired an RHD before any duplication and was later duplicated and then diverged into the different IκB subfamilies. Functional analysis identified several functionally divergent sites in the ANK repeat domains (ARDs) and revealed that this region has undergone strong purifying selection, suggesting its functional importance in IκB genes. Structural analysis showed that the major variations in the number of ANK repeats and high conformational changes in the finger loop ARD region contribute to the differing binding partner specificities, thereby leading to distinct IκB functions. In summary, our study has provided useful information about the phylogeny and structural and functional divergence of the IκB family. Additionally, we identified a number of amino acid sites that contribute to the predicted functional divergence of these proteins.

Highlights

Nuclear factor kappa B (NF-kB) proteins comprise a family of structurally related and evolutionarily conserved transcription factors that are involved in the control of a large number of normal cellular and organismal processes such as immune and inflammatory responses, developmental processes, cellular growth and apoptosis
All inhibitor of kappa B (IkB) proteins possess common domain architecture, such as an N-terminal region followed by a Cterminal ANK repeat domains (ARDs)
NF-kB proteins have C-terminal IkB-like inhibitory domains consisting of ANK repeats, which must be removed for their activation

Summary

Introduction

Nuclear factor kappa B (NF-kB) proteins comprise a family of structurally related and evolutionarily conserved transcription factors that are involved in the control of a large number of normal cellular and organismal processes such as immune and inflammatory responses, developmental processes, cellular growth and apoptosis. The 5 members of the mammalian NF-kB transcription factor family are p65 (RelA), RelB, c-Rel, NF-kB1 (p50 and its precursor p105), and NF-kB2 (p52 and its precursor p100), which associate with each other to form various transcriptionally active homo- and heterodimeric complexes [1,2]. Studies carried out by Baltimore et al led to the discovery that NF-kB is regulated through its interaction with inhibitor of kappa B (IkB) proteins [3]. The primary function of IkBs was originally thought to be the suppression of NF-kB activity; recent studies have revealed that IkBs are not simple inhibitors of NF-kB activity, but rather pleiotropic NF-kB cofactors and more complex regulators of gene expression [6,7]

Methods

Results

Conclusion