Intertumoral and intratumoral barriers as approaches for drug delivery and theranostics to solid tumors using stimuli-responsive materials

Karim Khanmohammadi Chenab, Haniyeh Malektaj, Ali Akbar Ranjbari Nadinlooie, Sedigheh Mohammadi, Mohammad-Reza Zamani-Meymian

Research output: Contribution to journalReview articlepeer-review

4 Citations (Scopus)

Abstract

The solid tumors provide a series of biological barriers in cellular microenvironment for designing drug delivery methods based on advanced stimuli-responsive materials. These intertumoral and intratumoral barriers consist of perforated endotheliums, tumor cell crowding, vascularity, lymphatic drainage blocking effect, extracellular matrix (ECM) proteins, hypoxia, and acidosis. Triggering opportunities have been drawn for solid tumor therapies based on single and dual stimuli-responsive drug delivery systems (DDSs) that not only improved drug targeting in deeper sites of the tumor microenvironments, but also facilitated the antitumor drug release efficiency. Single and dual stimuli-responsive materials which are known for their lowest side effects can be categorized in 17 main groups which involve to internal and external stimuli anticancer drug carriers in proportion to microenvironments of targeted solid tumors. Development of such drug carriers can circumvent barriers in clinical trial studies based on their superior capabilities in penetrating into more inaccessible sites of the tumor tissues. In recent designs, key characteristics of these DDSs such as fast response to intracellular and extracellular factors, effective cytotoxicity with minimum side effect, efficient permeability, and rate and location of drug release have been discussed as core concerns of designing paradigms of these materials.

Original languageEnglish
Article number541
JournalMicrochimica Acta
Volume191
Issue number9
Number of pages51
DOIs
Publication statusPublished - Sept 2024

Keywords

  • Liposome
  • Smart drug delivery
  • Solid tumor
  • Stimuli-responsive
  • Targeting cancer cells
  • Theranostics

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