Vaccination with prefusion-stabilized respiratory syncytial virus fusion protein induces genetically and antigenically diverse antibody responses

用融合前稳定的呼吸道合胞病毒融合蛋白进行疫苗接种可诱导产生遗传和抗原多样性的抗体反应。

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作者:Maryam Mukhamedova,Daniel Wrapp,Chen-Hsiang Shen,Morgan S A Gilman,Tracy J Ruckwardt,Chaim A Schramm,Larissa Ault,Lauren Chang,Alexandrine Derrien-Colemyn,Sarah A M Lucas,Amy Ransier,Samuel Darko,Emily Phung,Lingshu Wang,Yi Zhang,Scott A Rush,Bharat Madan,Guillaume B E Stewart-Jones,Pamela J Costner,LaSonji A Holman,Somia P Hickman,Nina M Berkowitz,Nicole A Doria-Rose,Kaitlyn M Morabito,Brandon J DeKosky,Martin R Gaudinski,Grace L Chen,Michelle C Crank,John Misasi,Nancy J Sullivan,Daniel C Douek,Peter D Kwong,Barney S Graham,Jason S McLellan,John R Mascola

Abstract

An effective vaccine for respiratory syncytial virus (RSV) is an unrealized public health goal. A single dose of the prefusion-stabilized fusion (F) glycoprotein subunit vaccine (DS-Cav1) substantially increases serum-neutralizing activity in healthy adults. We sought to determine whether DS-Cav1 vaccination induces a repertoire mirroring the pre-existing diversity from natural infection or whether antibody lineages targeting specific epitopes predominate. We evaluated RSV F-specific B cell responses before and after vaccination in six participants using complementary B cell sequencing methodologies and identified 555 clonal lineages. DS-Cav1-induced lineages recognized the prefusion conformation of F (pre-F) and were genetically diverse. Expressed antibodies recognized all six antigenic sites on the pre-F trimer. We identified 34 public clonotypes, and structural analysis of two antibodies from a predominant clonotype revealed a common mode of recognition. Thus, vaccination with DS-Cav1 generates a diverse polyclonal response targeting the antigenic sites on pre-F, supporting the development and advanced testing of pre-F-based vaccines against RSV.

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