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. 2025 Nov;10(11):2781-2796.
doi: 10.1038/s41564-025-02126-0. Epub 2025 Sep 26.

Epstein-Barr virus exploits desmocollin 2 as the principal epithelial cell entry receptor

Hongbo Wang  1 Zongjun Mou  2 Yao Yu Yeo  3 Qianyun Ge  4 Xiang Liu  5 Yohei Narita  6 Zhixuan Li  6 Chong Wang  6 Wanyu Li  7 Katelyn Rs Zhao  6 Jenny Li  8 Wei Bu  9 Benjamin Gewurz  6 Jeffrey I Cohen  9 Mingxiang Teng  5 Xinghong Dai  2 Xuefeng Liu  8 Sizun Jiang  10   11 Bo Zhao  12
Affiliations

Epstein-Barr virus exploits desmocollin 2 as the principal epithelial cell entry receptor

Hongbo Wang et al. Nat Microbiol. 2025 Nov.

Abstract

Epstein-Barr virus (EBV) infects B and epithelial cells, causing various lymphomas and epithelial malignancies. Although cell-free infection of epithelial cells is inefficient, direct B-epithelial cell contact infection is highly efficient and probably the dominant route. To identify mechanisms of contact-mediated infection, we implemented a genome-wide CRISPR screen and uncovered desmocollin 2 (DSC2) as an EBV epithelial receptor and DSC3 as a co-factor for infection. DSC2 and DSC3 double knockout significantly inhibited both cell-free and cell-cell contact EBV infection of normal oral keratinocytes, while their overexpression permitted infection in receptor-negative cells. Antibodies to DSC2 blocked infection across normal oral keratinocytes, primary oral keratinocytes, and head and neck epithelial organoids. Combining DSC2 and DSC3 antibodies efficiently blocked cell-cell contact infection. Mechanistically, DSC2 interacted with the EBV gH/gL glycoprotein and facilitated epithelial fusion. Notably, EphA2 overexpression failed to restore infection in DSC2/3-deficient cells, indicating its dependence on DSC2/3. Our findings establish DSC2 as a principal EBV entry receptor and target for vaccine and therapeutic development.

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Conflict of interest statement

Competing interests: S.J. is a co-founder of Elucidate Bio Inc. and has received research support from Roche and Novartis, both unrelated to this work. All other authors declare that they have no competing financial interests.

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