Chronic Beryllium Disease: revealing the role of beryllium ion and small peptides binding to HLA-DP2.

PLoS One

Computational Biophysics and Bioinformatics, Physics Department, Clemson University, Clemson, South Carolina, United States of America.

Published: June 2015

AI Article Synopsis

  • Chronic Beryllium Disease (CBD) is a lung disorder caused by exposure to beryllium (Be) in individuals with the HLA-DP2 protein, which affects how peptides bind and interact with the immune system.
  • Recent in silico modeling indicates that Be binds to the HLA-DP2 protein first, inducing similar conformational changes for various peptides, although their binding strengths differ based on amino acid composition.
  • The changes in the HLA-DP2 protein caused by Be binding may mislead the immune signaling process, suggesting that CBD can result from any peptide in the presence of Be for those with the HLA-DP2*0201 allele.

Article Abstract

Chronic Beryllium (Be) Disease (CBD) is a granulomatous disorder that predominantly affects the lung. The CBD is caused by Be exposure of individuals carrying the HLA-DP2 protein of the major histocompatibility complex class II (MHCII). While the involvement of Be in the development of CBD is obvious and the binding site and the sequence of Be and peptide binding were recently experimentally revealed [1], the interplay between induced conformational changes and the changes of the peptide binding affinity in presence of Be were not investigated. Here we carry out in silico modeling and predict the Be binding to be within the acidic pocket (Glu26, Glu68 and Glu69) present on the HLA-DP2 protein in accordance with the experimental work [1]. In addition, the modeling indicates that the Be ion binds to the HLA-DP2 before the corresponding peptide is able to bind to it. Further analysis of the MD generated trajectories reveals that in the presence of the Be ion in the binding pocket of HLA-DP2, all the different types of peptides induce very similar conformational changes, but their binding affinities are quite different. Since these conformational changes are distinctly different from the changes caused by peptides normally found in the cell in the absence of Be, it can be speculated that CBD can be caused by any peptide in presence of Be ion. However, the affinities of peptides for Be loaded HLA-DP2 were found to depend of their amino acid composition and the peptides carrying acidic group at positions 4 and 7 are among the strongest binders. Thus, it is proposed that CBD is caused by the exposure of Be of an individual carrying the HLA-DP2*0201 allele and that the binding of Be to HLA-DP2 protein alters the conformational and ionization properties of HLA-DP2 such that the binding of a peptide triggers a wrong signaling cascade.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4219729PMC
http://journals.plos.org/plosone/article?id=10.1371/journal.pone.0111604PLOS

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