4.7 Article

Nonameric Peptide Orchestrates Signal Transduction in the Activating HLA-E/NKG2C/CD94 Immune Complex as Revealed by All-Atom Simulations

Journal

Publisher

MDPI
DOI: 10.3390/ijms22136670

Keywords

immune complex; molecular dynamics; immunology; NK cell; signal transduction

Funding

  1. Javna Agencija za Raziskovalno Dejavnost Republike Slovenije (ARRS
  2. Slovenian Research Agency) [P1-0017, P1-0012, 39011]

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NK cells exert their cytolytic function against tumors and virally infected cells through interactions with specific ligands on target cells, which involve complex molecular events and signal transduction mechanisms.
The innate immune system's natural killer (NK) cells exert their cytolytic function against a variety of pathological challenges, including tumors and virally infected cells. Their activation depends on net signaling mediated via inhibitory and activating receptors that interact with specific ligands displayed on the surfaces of target cells. The CD94/NKG2C heterodimer is one of the NK activating receptors and performs its function by interacting with the trimeric ligand comprised of the HLA-E/beta 2m/nonameric peptide complex. Here, simulations of the all-atom multi-microsecond molecular dynamics in five immune complexes provide atomistic insights into the receptor-ligand molecular recognition, as well as the molecular events that facilitate the NK cell activation. We identify NKG2C, the HLA-E-alpha 2 domain, and the nonameric peptide as the key elements involved in the molecular machinery of signal transduction via an intertwined hydrogen bond network. Overall, the study addresses the complex intricacies that are necessary to understand the mechanisms of the innate immune system.

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