Crimean-Congo haemorrhagic fever virus uses LDLR to bind and enter host cells.
Vanessa M MonteilShane C WrightMatheus DyczynskiMax J KellnerSofia K AppelbergSebastian Wolfgang PlatzerAhmed IbrahimHyesoo KwonIoannis PittarokoilisMattia MirandolaGeorg MichlitsStéphanie DevignotElizabeth G ElderSamir AbdurahmanSándor BereczkyBinnur BagciSonia YouhannaTeodor AastrupVolker Martin LauschkeCristiano SalataNazif ElaldiFriedemann WeberNuria MontserratDavid W HawmanHeinrich FeldmannMoritz HornJosef M PenningerAli MirazimiPublished in: Nature microbiology (2024)
Climate change and population densities accelerated transmission of highly pathogenic viruses to humans, including the Crimean-Congo haemorrhagic fever virus (CCHFV). Here we report that the Low Density Lipoprotein Receptor (LDLR) is a critical receptor for CCHFV cell entry, playing a vital role in CCHFV infection in cell culture and blood vessel organoids. The interaction between CCHFV and LDLR is highly specific, with other members of the LDLR protein family failing to bind to or neutralize the virus. Biosensor experiments demonstrate that LDLR specifically binds the surface glycoproteins of CCHFV. Importantly, mice lacking LDLR exhibit a delay in CCHFV-induced disease. Furthermore, we identified the presence of Apolipoprotein E (ApoE) on CCHFV particles. Our findings highlight the essential role of LDLR in CCHFV infection, irrespective of ApoE presence, when the virus is produced in tick cells. This discovery holds profound implications for the development of future therapies against CCHFV.