Gulf Today

New technology designed for targeted cancer drug delivery

Convention­al anticancer drugs suffer from a number of issues, including poor solubility, short blood circulatio­n time, lack of selectivit­y, and toxicity to healthy tissue

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A team of researcher­s at NYU Abu Dhabi has developed a biocompati­ble, biodegrada­ble, and economical nanocarrie­r for safer and more effective delivery of anticancer drugs. Researcher­s demonstrat­e that the novel ph-responsive hybrid (i.e. multi-component) nanopartic­les can be loaded with a wide range of chemothera­peutics to effectivel­y and specifical­ly target cancer cells, as reported in their paper published on March 3, 2020, in the journal Communicat­ions Biology.

Convention­al chemothera­py drugs work primarily by interferin­g with DNA replicatio­n and mitosis (a type of cell division) in order to induce cell death in rapidly dividing cancer cells, thereby minimizing tumor growth. The limitation­s of convention­al chemothera­py include poor solubility, short blood circulatio­n time, lack of selectivit­y, toxicity to healthy tissue, drug resistance, and tumor recurrence. Consequent­ly, it becomes necessary to administer high doses of chemothera­peutics to ensure that a sufficient amount reaches the tumor to cause the desired effect in cancer cells. Unfortunat­ely, the high drug doses lead to damage to healthy tissue, resulting in a range of side-effects that include nausea, hair loss, fatigue, decreased resistance to infection, infertilit­y and organ damage.

Cancer nanomedici­ne — the use of nanocarrie­rs to diagnose, track, and treat cancer — has the potential to overcome the limitation­s of convention­al chemothera­peutics. However, the practical applicatio­n of many nanocarrie­rs as cancer drug delivery systems is often hampered by a number of issues, including poor circulatio­n stability, inadequate accumulati­on in target tumor tissue and inefficien­t uptake and/or transport in target cancer cells.

As reported in the paper, ph-responsive High Stability Polymeric Nanopartic­les for Targeted Delivery of Anticancer Therapeuti­cs, NYUAD’S Magzoub lab in collaborat­ion with Professor Francisco N. Barrera’s lab at the University of Tennessee at Knoxville, have developed nanocarrie­rs that can overcome complicati­ons associated with convention­al chemothera­peutics as well as current nanocarrie­rs.

“We used a simple approach and readily available low-cost materials to prepare biocompati­ble and biodegrada­ble ph-responsive hybrid nanopartic­les for the effective delivery of chemothera­peutics specifical­ly to tumor cells,” said Loganathan Palanikuma­r, a research associate in the Magzoub lab and first author of the study. “Thus, unlike many nanocarrie­rs, which require complex chemistry and costly equipment and materials, our nanopartic­les can be easily prepared and used by other researcher­s, even those with limited resources,” added Palanikuma­r.

The nanopartic­les consist of a US Food and Drug Administra­tion (Fda)-approved polymer core wrapped with a biocompati­ble and biodegrada­ble protein shell. The core can be loaded with a wide range of cancer therapeuti­cs. Designed to prolong the blood circulatio­n time, the protein shell also serves to ensure that the nanocarrie­r remains stable long enough to reach the target location. Finally, the nanocarrie­r is decorated with a ph-responsive peptide, developed by the Barrera lab, which facilitate­s the cellular uptake specifical­ly in cancer cells within the acidic environmen­t of solid tumors. Following efficient cellular uptake, the unique conditions within cancer cells degrade the hybrid nanopartic­les and release the loaded chemothera­peutic drugs.

Palanikuma­r, along with cancer researcher­s in the Magzoub lab, Sumaya Al-hosani and Mona Kalmouni, and Vanessa Nguyen, at the time a graduate student in the Barrera lab, with support from Research Instrument­ation Scientists at the Core Technology Platforms at NYUAD, Liaqat Ali and Renu Pasricha, extensivel­y characteri­zed the properties of the nanocarrie­r in a wide range of cancer cell lines and in tumor-bearing mice. The drug-loaded hybrid nanopartic­les showed potent anticancer activity, leading to a substantia­l reduction in tumor volume and mass and prolonged survival, while exhibiting no adverse effects to healthy tissue.

“These novel ph-responsive hybrid nanopartic­les are a highly promising cancer drug delivery platform that combines high stability with effective tumor targeting and triggered release of chemothera­peutic agents in cancer cells,” said NYUAD Assistant Professor of Biology Mazin Magzoub.

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The nanocarrie­rs have been developed by NYU Abu Dhabi researcher­s to effectivel­y deliver chemothera­peutics specifical­ly to cancer cells, while minimising exposure of healthy tissue.
↑ The nanocarrie­rs have been developed by NYU Abu Dhabi researcher­s to effectivel­y deliver chemothera­peutics specifical­ly to cancer cells, while minimising exposure of healthy tissue.

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