Recently,
there has been an increasing interest for utilizing the host immune
system to fight against cancer. Moreover, cancer vaccines, which can
stimulate the host immune system to respond to cancer in the long
term, are being investigated as a promising approach to induce tumor-specific
immunity. In this work, we prepared an effective cancer vaccine (denoted
as “vacosome”) by reconstructing the cancer cell membrane,
monophosphoryl lipid A as a toll-like receptor 4 agonist, and egg
phosphatidylcholine. The vacosome triggered and enhanced bone marrow
dendritic cell maturation as well as stimulated the antitumor response
against breast cancer 4T1 cells
in vitro
. Furthermore,
an immune memory was established in BALB/c mice after three-time preimmunization
with the vacosome. After that, the immunized mice showed inhibited
tumor growth and prolonged survival period (longer than 50 days).
Overall, our results demonstrate that the vacosome can be a potential
candidate for clinical translation as a cancer vaccine.
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