AI Article Synopsis

  • DNA vaccines using heat shock proteins (hsp) and chimeric peptides targeting tumor-associated antigens (TAA) like gp70 effectively stimulated protective CD8 T cell immunity against tumors.
  • Expression of gp70 was observed in various normal tissues, with notable levels in certain tumor cell lines, such as CT26.
  • Only hsp-capturing chimeric antigens were able to efficiently induce strong TAA-specific CD8 T cell responses, providing protection in tumor models.

Article Abstract

DNA vaccines encoding heat shock protein (hsp)-capturing, chimeric peptides containing antigenic determinants of the tumor-associated Ag (TAA) gp70 (an envelope protein of endogenous retrovirus) primed stable, specific, and tumor-protective CD8 T cell immunity. Expression of gp70 transcripts was detectable in most normal tissues but was particularly striking in some (but not all) tumor cell lines tested (including the adenocarcinoma cell line CT26). An approximately 200 residue gp70 fragment or its L(d)-binding antigenic AH1 peptide cloned in-frame behind an hsp-capturing (cT(272)) or noncapturing (T(60)) N-terminal large SV40 tumor Ag sequence was expressed as either hsp-binding or -nonbinding chimeric Ags. Only hsp-capturing, chimeric fusion proteins were expressed efficiently in transfected cell lines and primed TAA-specific CD8 T cell immunity. This immunity mediated protection in the CT26 and mKSA models. A vaccination strategy based on delivering antigenic, hsp-associated TAA fragments can thus prime protective CD8 T cell immunity even if these TAA are of low intrinsic immunogenicity.

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Source
http://dx.doi.org/10.4049/jimmunol.177.3.1534DOI Listing

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