AI Article Synopsis

  • Researchers developed a pre-erythrocytic vaccine candidate targeting the Plasmodium vivax circumsporozoite protein, creating two versions: a soluble protein (VMP001) and a particulate antigen (CSV-S,S) made using yeast.
  • Both vaccine types were tested in rhesus monkeys, showing they could elicit immune responses, but the CSV-S,S version generated higher antibody levels specific to the target protein.
  • The study found differences in immune cell responses based on the vaccine format, suggesting the need for more clinical trials to further evaluate the effectiveness of each type in providing immunity against malaria.

Article Abstract

We have designed a pre-erythrocytic vaccine candidate based on the Plasmodium vivax circumsporozoite (CSV) protein, which includes its N- and C-terminal parts and a truncated region containing repeat sequences from both the VK210 and the VK247 P. vivax subtypes. Two versions of this vaccine candidate were made: a soluble recombinant protein expressed in Escherichia coli, designated VMP001 and a particulate antigen expressed in Saccharomyces cerevisiae, designated CSV-S,S. The latter is composed of CSV-S, a fusion protein between VMP001 and hepatitis B surface antigen (HBsAg), and free HBsAg co-expressed in yeast and self-assembling into mixed particles. Both antigen versions, adjuvanted with AS01, were shown to be immunogenic in rhesus monkeys. CSV-S,S/AS01 induced higher levels of VMP001-specific antibodies than did VMP001/AS01. Antibody responses against the N- and C-terminal regions of CSV and the VK210 repeat motif were of a similar magnitude following immunization with either the soluble or the particulate antigen. However, antibodies against the AGDR region, a potentially protective B cell epitope, were only detected after immunization with CSV-S,S. Analysis of the induced CD4(+) T cells highlighted different cytokine profiles depending on the antigen form. These results warrant further clinical evaluation of these two vaccine candidates to assess the added value of a particulate versus soluble form of CSV, in terms of both immunogenicity and protective efficacy.

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http://dx.doi.org/10.1016/j.vaccine.2013.10.041DOI Listing

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