The quantum chemical causality of pMHC-TCR biological avidity: Peptide atomic coordination data and the electronic state of agonist N termini

The quantum state of functional avidity of the synapse formed between a peptide-Major Histocompatibility Complex (pMHC) and a T cell receptor (TCR) is a subject not previously touched upon. Here we present atomic pair correlation meta-data based on crystalized tertiary structures of the Tax (HTLV-1)...

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Published inData in brief Vol. 3; no. C; pp. 180 - 184
Main Authors Antipas, Georgios S.E., Germenis, Anastasios E.
Format Journal Article
LanguageEnglish
Published Netherlands Elsevier Inc 01.06.2015
Elsevier
Subjects
agonists
ammonium
antagonists
Biochemistry
CD8
Class I MHC
Cytotoxic Lymphocytes
Data
data collection
density functional theory
humans
Immunology
major histocompatibility complex
Materials Science
metadata
peptides
Protein–protein interactions
protonation
Quantum Chemistry
quantum mechanics
synapse
T-lymphocytes
Materials Science
Quantum Chemistry
Immunology
Protein–protein interactions
CD8
Biochemistry
Class I MHC
Cytotoxic Lymphocytes
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ISSN2352-3409
2352-3409
DOI10.1016/j.dib.2015.02.021

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Summary:The quantum state of functional avidity of the synapse formed between a peptide-Major Histocompatibility Complex (pMHC) and a T cell receptor (TCR) is a subject not previously touched upon. Here we present atomic pair correlation meta-data based on crystalized tertiary structures of the Tax (HTLV-1) peptide along with three artificially altered variants, all of which were presented by the (Class I) HLA-A201 protein in complexation with the human (CD8+) A6TCR. The meta-data reveal the existence of a direct relationship between pMHC-TCR functional avidity (agonist/antagonist) and peptide pair distribution function (PDF). In this context, antagonist peptides are consistently under-coordinated in respect to Tax. Moreover, Density Functional Theory (DFT) datasets in the BLYP/TZ2P level of theory resulting from relaxation of the H species on peptide tertiary structures reveal that the coordination requirement of agonist peptides is also expressed as a physical observable of the protonation state of their N termini: agonistic peptides are always found to retain a stable ammonium (NH3+) terminal group while antagonist peptides are not.
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ISSN:2352-3409
2352-3409
DOI:10.1016/j.dib.2015.02.021