Published in the journal Nature Communications on Aug 10, a joint study by the Institute of Biophysics (IBP) of the Chinese Academy of Sciences, and Tsinghua University has analyzed multiple high-resolution complex structures of the complete Eastern Equine Encephalitis virus (EEEV) virion-like particle and the full-length and truncated forms of the LDLR class A repeats (LAs) in the extracellular region of the human very low-density lipoprotein receptor (VLDLR), identifying two main receptor sequential binding modes, LA1-2 and LA3-5. This discovery updates the understanding of the interaction between alphaviruses and receptors.

EEEV, an alphavirus, can cause central nervous system infections leading to severe encephalitis, with a mortality rate of over 30%. VLDLR is a novel alphavirus receptor that binds to the glycoprotein on the alphavirus surface through its extracellular cysteine-rich repeat sequence domain, LAs. However, the specific binding mode and working mechanism remain unclear.

In this study, researchers found three distinct receptor binding sites on the surface of the alphavirus EEEV, all located on protrusions of the E1/E2 glycoprotein trimer far from the membrane surface. Furthermore, the LA domain binding of VLDLR at these three receptor binding sites is not completely fixed.

Through biochemical and cellular experiments, researchers identified the two main receptor sequential binding modes, LA1-2 and LA3-5. Both modes mediate the binding between the virus and cell surface receptors as well as subsequent virus internalization.

Interestingly, the key amino acid residue K206 at site C is not conserved in the EEEV virus. However, the vaccine strain EEEV-PE6 still contains K206 at site C, suggesting a potential risk associated with using the EEEV PE6 strain as a vaccine strain.

The authors further discovered that a mutation of the key binding site (W50A) in LA1 significantly reduces the virus's ability to adsorb on the cell surface. In contrast, a mutation of the key binding site (W132A) in LA3 enhances the virus's adsorption on the cell surface. Through structural and functional analysis, it was found that LA3 and LA1 may competitively bind at site A, and the W132A mutation drives the switch from the LA3-5 dominated binding mode to the LA1-2 dominated binding mode. Thus, introduction of the dysfunctional LA3 in VLDLR significantly enhances the attachment of EEEV to the cell.

Notably, the VLDLR-W132G mutation was identified in human genome and SNP sequences, indicating that individuals with the W132G mutation may be more susceptible to infection by the EEEV alphavirus.

This study systematically demonstrates the complex and varied receptor binding modes of the novel receptor VLDLR on the surface of the alphavirus EEEV. By revealing the different receptor recognition patterns of the novel receptors in various alphaviruses, it aids in understanding the transmission mechanisms of alphaviruses widely invading across multiple species.

Figure. Novel receptor recognition mechanism of VLDLR and alphavirus EEEV

（Image by ZHANG Xinzheng's group）

Article link: https://www.nature.com/articles/s41467-024-51293-x

Contact: ZHANG Xinzheng

Institute of Biophysics, Chinese Academy of Sciences

Beijing 100101, China

Email: xzzhang@ibp.ac.cn

（Reported by Prof. ZHANG Xinzheng's group）