Investigating in vitro and in vivo ?v?6 integrin receptor-targeting liposomal alendronate for combinatory ?? T cell immunotherapy.
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ABSTRACT: The ?v?6 integrin receptor has been shown to be overexpressed on many types of cancer cells, resulting in a more pro-invasive and aggressive phenotype, this makes it an attractive target for selective drug delivery. In tumours that over-express the ?v?6 receptor, cellular uptake of liposomes can be enhanced using ligand-targeted liposomes. It has previously been shown in both in vitro and in vivo studies that liposomal alendronate (L-ALD) can sensitise cancer cells to destruction by V?9V?2 T cells. It is hypothesised that by using the ?v?6-specific peptide A20FMDV2 as a targeting moiety for L-ALD, the therapeutic efficacy of this therapy can be increased in ?v?6 positive tumours. Targeted liposomes (t-L) were formulated and the targeting efficacy of targeted liposomes (t-L) was assessed by cell uptake and cytotoxicity studies in the ?v?6 positive cells line A375P?6. Bio-distribution of both L and t-L were carried out in ?v?6 positive (A375P?6 and PANC0403) and ?v?6 negative (A375Ppuro and PANC-1) subcutaneous tumour mouse models. Immuno-compromised mice bearing A375P?6 experimental metastatic lung tumours were treated with L-ALD or t-L-ALD as monotherapies or in combination with ex vivo-expanded V?9V?2 T cells. In vitro, ?v?6-dependant uptake of t-L was observed, with t-L-ALD being more effective than L-ALD at sensitising A375P?6 to ?? T cells. Interestingly, t-L-ALD led to slightly higher but not significant reduction in tumour growth compared to L-ALD, when used as monotherapy in vivo. Moreover, both L-ALD and t-L-ALD led to significant reductions in tumour growth when used in combination with ?? T cells in vivo but t-L-ALD offered no added advantage compared to L-ALD.
SUBMITTER: Hodgins NO
PROVIDER: S-EPMC5488751 | biostudies-literature | 2017 Jun
REPOSITORIES: biostudies-literature
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