Smart Release Nano-formulation of Cytochrome C and Hyaluronic Acid
Induces Apoptosis in Cancer Cells

Figueroa CM; Suárez BN; Molina AM; Fernández JC; Torres Z; Kai Griebenow

doi:10.4172/2157-7439.1000427

Awards Nomination 20+ Million Readerbase

PMC/PubMed Indexed Articles

Development of Secreted Protein and Acidic and Rich in Cysteine (SPARC) Targeted Nanoparticles for the Prognostic Molecular Imaging of Metastatic Prostate Cancer

The Highs and Lows of FAIMS: Predictions and Future Trends for High Field Asymmetric Waveform Ion Mobility Spectrometry

Google Scholar citation report

Citations : 8261

Journal of Nanomedicine & Nanotechnology received 8261 citations as per Google Scholar report

Journal of Nanomedicine & Nanotechnology peer review process verified at publons

25+ Million Website Visitors

Indexed In

Open J Gate
Genamics JournalSeek
Academic Keys
JournalTOCs
ResearchBible
China National Knowledge Infrastructure (CNKI)
Scimago
Ulrich's Periodicals Directory
Electronic Journals Library
RefSeek
Hamdard University
EBSCO A-Z
OCLC- WorldCat
SWB online catalog
Virtual Library of Biology (vifabio)
Publons
MIAR
Scientific Indexing Services (SIS)
Euro Pub
Google Scholar

Useful Links

Share This Page

Journal Flyer

Tweets by LONGDOM_JNMNT

Open Access Journals

Abstract

Smart Release Nano-formulation of Cytochrome C and Hyaluronic Acid Induces Apoptosis in Cancer Cells

Figueroa CM, Suárez BN, Molina AM, Fernández JC, Torres Z and Kai Griebenow

Herein we tested a nanosized cancer-cell targeted delivery system based on cytochrome c (Cyt c) and hyaluronic acid. Cyt c was chosen since it is a per se non-toxic protein but causes apoptosis when delivered to the cytoplasm of target cells. Hyaluronic acid was employed to create the nanosized delivery system with passive targeting capability in order to exploit the enhanced permeation and retention (EPR) effect and active targeting capability of hyaluronic acid. In addition, our goal was to incorporate a smart release strategy to only promote protein release upon reaching its target. Nanoparticles were formed by a simple yet precise nanoprecipitation process based on desolvation. They were physically characterized to select precipitation conditions leading to adequate size, shape, protein bioactivity, and protein loading to produce a feasible targeted cancer treatment. We synthesized nanoparticles of around 500 nm diameter with a 60% protein loading and more than 80% of protein bioactivity. In vitro, cumulative release of 92% of Cyt c was observed after 8 h under conditions mimicking the reductive intracellular environment, while under non-denaturing conditions only 20% was released. The nanoparticles displayed a selective cytotoxic effect on cancer cells. After 6 h of incubation with the nanoparticles, hyaluronic acid receptor over expressing A549 human lung adenocarcinoma cells showed a viability of ca. 20% at 0.16 mg/ml of Cyt c concentration. Only a negligible effect was observed on viability of COS-7 African green monkey kidney fibroblast, a normal cell line notoverexpressing the hyaluronic acid receptor. Confocal microscopy confirmed that the drug delivery system indeed delivered Cyt c to the cytoplasm of the target cells. We conclude that we were able to create a smart stimuli-responsive targeted drug delivery system with significant potential in cancer therapy.