Intracellular Sequestration of the NKG2D Ligand MIC B by Species F Adenovirus

Overview

Journal Viruses

Publisher MDPI

Specialty Microbiology

Date 2021 Aug 10

PMID 34372495

Citations 2

Authors

Edson R A Oliveira

Lenong Li

Marlene Bouvier

Affiliations

Soon will be listed here.

Abstract

The enteric human adenoviruses of species F (HAdVs-F), which comprise HAdV-F40 and HAdV-F41, are significant pathogens that cause acute gastroenteritis in children worldwide. The early transcription unit 3 (E3) of HAdVs-F is markedly different from that of all other HAdV species. To date, the E3 proteins unique to HAdVs-F have not been characterized and the mechanism by which HAdVs-F evade immune defenses in the gastrointestinal (GI) tract is poorly understood. Here, we show that HAdV-F41 infection of human intestinal HCT116 cells upregulated the expression of MHC class I-related chain A (MIC A) and MIC B relative to uninfected cells. Our results also showed that, for MIC B, this response did not however result in a significant increase of MIC B on the cell surface. Instead, MIC B was largely sequestered intracellularly. Thus, although HAdV-F41 infection of HCT116 cells upregulated MIC B expression, the ligand remained inside infected cells. A similar observation could not be made for MIC A in these cells. Our preliminary findings represent a novel function of HAdVs-F that may enable these viruses to evade immune surveillance by natural killer (NK) cells in the infected gut, thereby paving the way for the future investigation of their unique E3 proteins.

Citing Articles

Pediatric adenovirus pneumonia: clinical practice and current treatment.

Zhang J, Zhu Y, Zhou Y, Gao F, Qiu X, Li J Front Med (Lausanne). 2023; 10:1207568.

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Multiplex MinION sequencing suggests enteric adenovirus F41 genetic diversity comparable to pre-COVID-19 era.

Maes M, Khokhar F, Wilkinson S, Smith A, Kovalenko G, Dougan G Microb Genom. 2023; 9(1).

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