Abstract

Measles is a highly contagious disease that causes temporary and severe immunosuppression in patients. Signaling lymphocyte activation molecule (SLAM) expressed on cells of the immune system functions as a receptor for measles virus (MV). In addition to SLAM, vaccine strains of MV also use a ubiquitously expressed complement regulatory protein, CD46, as a receptor, whereas wild-type (wt) MV strains do not use this receptor. However, recent studies have indicated that SLAM is not the sole receptor for wt MV strains. These strains have an intrinsic ability to enter both immune and epithelial cells using distinct receptor binding sites in their hemagglutinin (H) protein. Recently, a clear answer was obtained through the identification of an epithelial MV receptor, nectin4, expressed at adherens junctions, thereby greatly improving our knowledge of MV receptors. It is now clear that MV specifically targets two cell types, immune cells and epithelial cells, using SLAM and nectin4, respectively. MV loses the ability to use either SLAM or nectin4 when it possesses specific mutations in the H protein. However, nectin4-blind MV still infects SLAM-positive immune cells efficiently (SLAM-tropic), and conversely, SLAM-blind MV infects nectin4-positive epithelial cells efficiently (nectin4-tropic). In this regard, MV is intrinsically dual-tropic to immune cells and epithelial cells. Although many aspects and molecular mechanisms underlying immunosuppressive effects and a highly contagious nature of MV still remain to be elucidated, analyses of physiological functions of these two receptors would provide deep insights into MV pathogenesis.

Highlights

  • MEASLES VIRUS Measles is a highly contagious acute viral disease characterized by high fever, malaise, coryza, conjunctivitis, cough, and a maculopapular rash (Griffin, 2007)

  • It remained difficult to make a final conclusion that Signaling lymphocyte activation molecule (SLAM)/CD150 is the sole receptor for wt measles virus (MV), because histopathological examinations of measles patients and monkeys infected with MV have revealed considerable levels of MV protein expression in the epithelia of various organs, and histopathological changes are evident in these epithelia (Nii et al, 1964; Lightwood and Nolan, 1970; Olding-Stenkvist and Bjorvatn, 1976; Moench et al, 1988; Craighead, 2000; Figure 1)

  • Nectin4 is a possible candidate for an MV receptor in the central nervous system (CNS), no nectin4 expression was observed in the CNS in humans (Reymond et al, 2001; Brancati et al, 2010), and some MV strains derived from sclerosing panencephalitis (SSPE) patients are likely to use nectin4 inefficiently (Seki et al, 2011)

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Summary

Introduction

MEASLES VIRUS Measles is a highly contagious acute viral disease characterized by high fever, malaise, coryza, conjunctivitis, cough, and a maculopapular rash (Griffin, 2007). This receptor is signaling lymphocyte activation molecule, known as CD150 (SLAM/CD150), which is expressed on cells of the immune system (Tatsuo et al, 2000). The SLAM-family receptors are type I transmembrane proteins that typically possess an extracellular region with two Ig-like domains (an amino-terminal variable (V)-like domain and a carboxy-terminal constant-2 (C2)-like domain), a transmembrane region, and a cytoplasmic region that harbors multiple tyrosine-based motifs (Detre et al, 2010; Veillette, 2010; Cannons et al, 2011; Ma and Deenick, 2011).

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