Challenges in developing a cross-serotype rhinovirus vaccine

Alper; Appleyard; Ashraf; Barclay; Bartlett; Beale; Blanco; Bochkov; Bochkov; Buscho; Cate; Contoli; Cooney; Cooney; Doggett; Edlmayr; Fleet; Gern; Glanville; Grissell; Hamory; Hamparian; Hastings; Iwasaki; Iwasaki; Jackson; Jackson; Katpally; Lee; Mallia; Martin; McCray; McLean; Message; Mitchison; Niespodziana; Palmenberg; Palmenberg; Papi; Perkins; Richter; Sherry; Sridhar; Taylor-Robinson; Turner; Waman; Wilkinson

Challenges in developing a cross-serotype rhinovirus vaccine

Authors: Alper
Appleyard
Ashraf
Barclay
Bartlett
Beale
Blanco
Bochkov
Bochkov
Buscho
Cate
Contoli
Cooney
Cooney
Doggett
Edlmayr
Fleet
Gern
Glanville
Grissell
Hamory
Hamparian
Hastings
Iwasaki
Iwasaki
Jackson
Jackson
Katpally
Lee
Mallia
Martin
McCray
McLean
Message
Mitchison
Niespodziana
Palmenberg
Palmenberg
Papi
Perkins
Richter
Sherry
Sridhar
Taylor-Robinson
Turner
Waman
Wilkinson
Publication date: 29 March 2015
Publisher: 'Elsevier BV'
Doi

Abstract

A great burden of disease is attributable to human rhinovirus (HRV) infections which are the major cause of the common cold, exacerbations of both asthma and chronic obstructive pulmonary disease (COPD), and are associated with asthma development. Despite this there is currently no vaccine for HRV. The first vaccine studies showed some promise in terms of serotype-specific protection against cold symptoms, but antigenic heterogeneity amongst the >150 HRVs has been regarded as a major barrier to effective vaccine development and has resulted in little progress over 50 years. Here we review those vaccine studies conducted to date, discuss the difficulties posed by antigenic heterogeneity and describe some recent advances in generating cross-reactive antibodies and T cell responses using peptide immunogens