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Cleavage-intermediate Lassa virus trimer elicits neutralizing responses, identifies neutralizing nanobodies, and reveals an apex-situated site-of-vulnerability.

Jason GormanCrystal Sao-Fong CheungZhijian DuanLi OuMaple WangXuejun ChenCheng ChengAndrea BijuYaping SunPengfei WangYongping YangBaoshan ZhangJeffrey C BoyingtonTatsiana BylundSam CharafSteven J ChenHaijuan DuAmy R HenryTracy LiuEdward K SarfoChaim A SchrammChen-Hsiang ShenTyler StephensI-Ting TengJohn-Paul ToddYaroslav TsybovskyRaffaello VerardiDanyi WangShuishu WangZhantong WangCheng-Yan ZhengTongqing ZhouDaniel C DouekJohn R MascolaDavid D HoMitchell HoPeter D Kwong
Published in: Nature communications (2024)
Lassa virus (LASV) infection is expanding outside its traditionally endemic areas in West Africa, posing a pandemic biothreat. LASV-neutralizing antibodies, moreover, have proven difficult to elicit. To gain insight into LASV neutralization, here we develop a prefusion-stabilized LASV glycoprotein trimer (GPC), pan it against phage libraries comprising single-domain antibodies (nanobodies) from shark and camel, and identify one, D5, which neutralizes LASV. Cryo-EM analyses reveal D5 to recognize a cleavage-dependent site-of-vulnerability at the trimer apex. The recognized site appears specific to GPC intermediates, with protomers lacking full cleavage between GP1 and GP2 subunits. Guinea pig immunizations with the prefusion-stabilized cleavage-intermediate LASV GPC, first as trimer and then as a nanoparticle, induce neutralizing responses, targeting multiple epitopes including that of D5; we identify a neutralizing antibody (GP23) from the immunized guinea pigs. Collectively, our findings define a prefusion-stabilized GPC trimer, reveal an apex-situated site-of-vulnerability, and demonstrate elicitation of LASV-neutralizing responses by a cleavage-intermediate LASV trimer.
Keyphrases
  • dengue virus
  • dna binding
  • climate change
  • zika virus
  • sars cov
  • pseudomonas aeruginosa
  • coronavirus disease
  • drug delivery
  • cystic fibrosis