Efficacy of a novel LyP-1-containing self-microemulsifying drug delivery system (SMEDDS) for active targeting to breast cancer
Tarih
2019Yazar
Timur, Selin S. and Yoyen-Ermis, Digdem and Esendagli, Guldal and Yonat,
Selcen and Horzum, Utku and Esendagli, Gunes and Gursoy, R. Neslihan
Üst veri
Tüm öğe kaydını gösterÖzet
An ideal cancer therapy targets the tumor cells selectively without
damaging healthy tissues. Even though the tumor-specific markers are
limited, these molecules can be used for the delivery of anti-cancer
drugs as an active targeting strategy. Since the lymphatic system plays
a critical role in the dissemination of cancer cells, the drugs directed
through lymphatics can feasibly reach to the sites of metastasis. LyP-1
is a peptide that binds to the p32 receptor which is highly expressed
not only on the lymphatic endothelium but also on the malignant cells;
thus, making this peptide ligand a preferable candidate to mediate
active targeting of lymphatics and cancer cells. In this study,
different formulations of LyP-1 containing lipid-based nanophannaceutics
so-called self-microemulsifying drug delivery systems (SMEDDS) were
developed and tested for their efficacy in targeting breast cancer.
Following the selection of non-toxic formulation, doxorubicin
hydrochloride and LyP-1 were co-administered in the SMEDDS, which
resulted in a significant increase in in vitro cytotoxicity in
p32-expressing breast cancer cells, 4T1 and MDA-MB-231. Accordingly, the
uptake of LyP-1 in the SMEDDS by the cancer cells was demonstrated. The
expression of p32 was detected in the 4T1 tumor tissues which were
efficiently targeted with LyP-1 in the SMEDDS. When doxorubicin was
co-administrated with LyP-1 in SMEDDS via intraperitonial
administration, tumor growth and metastasis were significantly reduced.
In conclusion, a novel and efficacious SMEDDS formulation containing
LyP-1 with a droplet size less than 100 nm was developed for the
lymphatic targeting of breast cancer.
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