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The Pfs230 N-terminal fragment, Pfs230D1+: expression and characterization of a potential malaria transmission-blocking vaccine candidate.

Shwu-Maan LeeYimin WuJohn M HickeyKazutoyo MiuraNeal WhitakerSangeeta B JoshiDavid B VolkinC Richter KingJordan Plieskatt
Published in: Malaria journal (2019)
By elimination of an O-glycosylation site, a potential N-glycosylation site, and two proteolytic cleavage sites, an improved N-terminal Pfs230 fragment was produced, termed D1+, which is non-glycosylated, homogeneous, and biologically active. An intact protein at higher yield than that previously observed for the Pfs230C1 fragment was achieved. The results indicate that Pfs230D1+ protein produced in the baculovirus expression system is an attractive antigen for transmission-blocking vaccine development.
Keyphrases
  • poor prognosis
  • binding protein
  • protein protein
  • long non coding rna