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Expert Opinion on Drug Delivery Volume 17, 2020 - Issue 11
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Original Research

Co-delivery of a RanGTP inhibitory peptide and doxorubicin using dual-loaded liposomal carriers to combat chemotherapeutic resistance in breast cancer cells

Yusuf Haggaga Department of Pharmaceutical Technology, Faculty of Pharmacy, Tanta University, Tanta, Egypt
,
Bayan Abu Rasb School of Pharmacy and Clinical Sciences, University of Bradford, Bradford, UK
,
Yahia El-Tananib School of Pharmacy and Clinical Sciences, University of Bradford, Bradford, UK
,
Murtaza M. Tambuwalac School of Pharmacy and Pharmaceutical Sciences, Ulster University, UKORCID Iconhttps://orcid.org/0000-0001-8499-9891
ORCID Icon,
Paul McCarronc School of Pharmacy and Pharmaceutical Sciences, Ulster University, UK
,
Mohammed Isrebb School of Pharmacy and Clinical Sciences, University of Bradford, Bradford, UK
&
Mohamed El-Tananid Pharmacological and Diagnostic Research Centre, Faculty of Pharmacy, Al-Ahliyya Amman University, Amman, Jordan;e Institute of Cancer Therapeutics, Faculty of Life Sciences, University of Bradford, Bradford, UKCorrespondence[email protected]
 show all
Pages 1655-1669 | Received 19 May 2020, Accepted 19 Aug 2020, Published online: 15 Sep 2020
 
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ABSTRACT

Background

Multidrug resistance (MDR) limits the beneficial outcomes of conventional breast cancer chemotherapy. Ras-related nuclear protein (Ran-GTP) plays a key role in these resistance mechanisms, assisting cancer cells to repair damage to DNA. Herein, we investigate the co-delivery of Ran-RCC1 inhibitory peptide (RAN-IP) and doxorubicin (DOX) to breast cancer cells using liposomal nanocarriers.

Research design

A liposomal delivery system, co-encapsulating DOX, and RAN-IP, was prepared using a thin-film rehydration technique. Dual-loaded liposomes were optimized by systematic modification of formulation variables. Real-Time-Polymerase Chain Reaction was used to determine Ran-GTP mRNA expression. In vitro cell lines were used to evaluate the effect of loaded liposomes on the viability of breast and lung cancer cell lines. In vivo testing was performed on a murine Solid Ehrlich Carcinoma model.

Results

RAN-IP reversed the Ran-expression-mediated MDR by inhibiting the Ran DNA damage repair function. Co-administration of RAN-IP enhanced sensitivity of DOX in breast cancer cell lines. Finally, liposome-mediated co-delivery with RAN-IP improved the anti-tumor effect of DOX in tumor-bearing mice when compared to single therapy.

Conclusions

This study is the first to show the simultaneous delivery of RAN-IP and DOX using liposomes can be synergistic with DOX and lead to tumor regression in vitro and in vivo.

Declaration of interest

The authors have no other relevant affiliations or financial involvement with any organization or entity with a financial interest in or financial conflict with the subject matter or materials discussed in the manuscript apart from those disclosed.

Reviewer disclosures

Peer reviewers on this manuscript have no relevant financial or other relationships to disclose.

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