Investigation of polymeric drug delivery systems to improve therapeutic efficiency for breast cancer

This project was lead by:

Dr. Yongmei Zhao (Graduated)

Thesis: “Investigation of polymeric drug delivery systems to improve therapeutic efficiency for breast cancer

Pursuing a tenure track position at Nantong University in China.

Former PhD Student – Thurecht Group, University of Queensland

Thesis

Summary

Paper 1 Abstract:

Theranostics is a strategy that combines multiple functions such as targeting, stimulus-responsive drug release, and diagnostic imaging into a single platform, often with the aim of developing personalized medicine.1,2 Based on this concept, several well-established hyperbranched polymeric theranostic nanoparticles were synthesized and characterized as model nanomedicines to investigate how their properties affect the distribution of loaded drugs at both the cell and whole animal levels. An 8-mer peptide aptamer was covalently bound to the periphery of the nanoparticles to achieve both targeting and potential chemosensitization functionality against heat shock protein 70 (Hsp70). Doxorubicin was also bound to the polymeric carrier as a model chemotherapeutic drug through a degradable hydrazone bond, enabling pH-controlled release under the mildly acid conditions that are found in the intracellular compartments of tumor cells. In order to track the nanoparticles, cyanine-5 (Cy5) was incorporated into the polymer as an optical imaging agent. In vitro cellular uptake was assessed for the hyperbranched polymer containing both doxorubicin (DOX) and Hsp70 targeted peptide aptamer in live MDA-MB-468 cells, and was found to be greater than that of either the untargeted, DOX-loaded polymer or polymer alone due to the specific affinity of the peptide aptamer for the breast cancer cells. This was also validated in vivo with the targeted polymers showing much higher accumulation within the tumor 48 h postinjection than the untargeted analogue. More detailed assessment of the nanomedicine distribution was achieved by directly following the polymeric carrier and the doxorubicin at both the in vitro cellular level via compartmental analysis of confocal images of live cells and in whole tumors ex vivo using confocal imaging to visualize the distribution of the drug in tumor tissue as a function of distance from blood vessels. Our results indicate that this polymeric carrier shows promise as a cancer theranostic, demonstrating active targeting to tumor cells with the capability for simultaneous drug release.

Paper 2 Abstract:

Targeted nanomedicines offer many advantages over macromolecular therapeutics that rely only on passive accumulation within the tumour environment. The aim of this work was to investigate the in vivo anticancer efficiency of polymeric nanomedicines that were conjugated with peptide aptamers that show high affinity for receptors on many cancer cells. In order to assess the ability for the nanomedicine to treat cancer and investigate how structure affected the behavior of the nanomedicine, three imaging modalities were utilized, including in vivo optical imaging, multispectral optoacoustic tomography (MSOT) and ex vivo confocal microscopy. An 8-mer (A8) or 13-mer (A13) peptide aptamer that have been shown to exhibit high affinity for heat shock protein 70 (HSP70) was covalently-bound to hyperbranched polymer (HBP) nanoparticles with the purpose of both cellular targeting, as well as the potential to impart some level of chemo-sensitization to the cells. Furthermore, doxorubicin was bound to the polymeric carrier as the anticancer drug, and Cyanine-5.5 (Cy5.5) was incorporated into the polymer as a monomeric fluorophore to aid in monitoring the behavior of the nanomedicine. Enhanced tumour regression was observed in nude mice bearing MDA-MB-468 xenografts when the nanocarriers were targeted using the peptide ligands, compared to control groups treated with free DOX or HBP without aptamer. The accumulated DOX level in solid tumours was 5.5 times higher in mice treated with the targeted therapeutic, than mice treated with free DOX, and 2.6 times higher than the untargeted nanomedicine that relied only on passive accumulation. The results suggest that aptamer-targeted therapeutics have great potential for improving accumulation of nanomedicines in tumours for therapy.

Paper 3 Abstract:

An ideal nanotherapeutic should enhance therapeutic efficacy of the drug while reducing side effects. This work reports development of a nanotherapeutic utilising hyperbranched polymers as a platform for conjugating doxorubicin (DOX) and camptothecin (CPT) as potential synergistic therapies. The carrier also includes cyanine-5 (Cy5) as an imaging tracer to monitor distribution and efficacy of the therapeutic, and a bispecific antibody (BsAb) as a cell targeting agent to increase accumulation and specificity for tumour tissue. The synergism of this drug combination was investigated by utilising both redox- and hydrolytic release mechanisms of CPT and DOX, respectively. Drug release and cellular uptake studies confirmed the proposed delivery mechanisms and subsequent intracellular trafficking of the drugs. In this particular case, a super-additive effect was observed in vitro for the two drugs when delivered by nanocarrier. This was enhanced when the carrier was targeted to epidermal growth factor receptor (EGFR) that is upregulated in the tumours. Moreover, tumour regression studies showed that the synergistic therapeutic effect of combination nanocarriers have greater inhibition of xenograft tumour growth compared to treatments that deliver DOX or CPT alone, suggesting that co-delivery of dual therapeutics using modular hyperbranched polymer carriers offers unique potential to regulate tumour growth.

People

This project is a PhD project for Yongmei Zhao, for which I was a co-supervisor. People other than Yongmei and myself who are involved in the project are listed below with their roles and affiliations (see affiliations by superscript below).

  • Liyu Chen1,2,3 – Optical imaging and haematology
  • Nicholas L. Fletcher1,2,3 – Optical imaging and animal work
  • Adrian V. Fuchs1,2,3 – Materials prepration supervision
  • Anna Gemmell1,2,3 – Photoacoustic imaging
  • Joshua D. Simpson1,2,3 – Confocal microscopy
  • Michelle Tianqing5 – Spheroid work and microscopy
  • Idriss Blakey1,2 – Co-supervisor and polymer chemist
  • Kristofer J. Thurecht1,2,3,4 – Primary supervisor

Affiliations

  1. Centre for Advanced Imaging, The University of Queensland, St Lucia, QLD 4072, Australia.
  2. Australian Institute for Bioengineering and Nanotechnology, The University of Queensland, St Lucia, QLD 4072, Australia.
  3. ARC Centre of Excellence in Convergent BioNano Science and Technology, The University of Queensland, St Lucia, QLD 4072, Australia
  4. ARC Training Centre for Innovation in Biomedical Imaging Technology, The University of Queensland, St Lucia, QLD 4072, Australia
  5. QIMR Berghofer Medical Research Institute, 300 Herston Road, Brisbane, QLD, 4006, Australia

Outputs

Investigation of the Therapeutic Potential of a Synergistic Delivery System through Dual Controlled Release of Camptothecin–Doxorubicin

Journal Article
Zhao, Yongmei and Fletcher, Nicholas L. and Gemmell, Anna and Houston, Zachary H. and Howard, Christopher B. and Blakey, Idriss and Liu, Tianqing and Thurecht, Kristofer J.
Advanced Therapeutics, 2020, doi:10.1002/adtp.201900202
Publication year: 2020

In vivo therapeutic evaluation of polymeric nanomedicines: effect of different targeting peptides on therapeutic efficacy against breast cancer

Journal Article
Zhao, Y. and Fletcher, N. L. and Liu, T. and Gemmell, A. C. and Houston, Z. H. and Blakey, I. and Thurecht, K. J.
Nanotheranostics{booktitle}, 2018
Publication year: 2018

Using Peptide Aptamer Targeted Polymers as a Model Nanomedicine for Investigating Drug Distribution in Cancer Nanotheranostics

Journal Article
Zhao, Y. and Houston, Z. H. and Simpson, J. D. and Chen, L. and Fletcher, N. L. and Fuchs, A. V. and Blakey, I. and Thurecht, K. J.
Mol Pharm{booktitle}, 2017
Publication year: 2017