Mechanistic insight into the bioactivity of prodigiosin-entrapped lipid nanoparticles against triple-negative breast, lung and colon cancer cell lines

This research investigates the potentials of prodigiosin PG derived from bacteria and its formulations against triple negative breast (TNB), lung, and colon cancer cells. The PG was extracted from using continuous batch culture, characterized, and formulated into lyophilized parenteral nanoparticles...

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Bibliographic Details
Published in:Heliyon 2023-06, Vol.9 (6), p.e16963-e16963
Main Authors: Gugu, Thaddeus H, Eze, Christopher O, Kenechukwu, Franklin C, Khumaini Mudhar Bintang, Muhammd A, Patil, Sanjay B, Basarkar, Ganesh D, Attama, Anthony A, Ibezim, Emmanuel C, Upasani, Chandrashekhar D, Srichana, Teerapol
Format: Article
Language:English
Subjects:
And colon cancer
Cancer cell lines
Lung cancer
Parenteral nanoparticles (PNPs)
Serratia marcescens, prodigiosin (PG)
Triple-negative breast cancer (TNBC)
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Summary:This research investigates the potentials of prodigiosin PG derived from bacteria and its formulations against triple negative breast (TNB), lung, and colon cancer cells. The PG was extracted from using continuous batch culture, characterized, and formulated into lyophilized parenteral nanoparticles (PNPs). The formulations were characterized with respect to entrapment efficiency (EE), DSC, FT-IR, TEM, and proton nuclear magnetic resonance (1H NMR) spectroscopy. drug release was evaluated in phosphate buffer (pH 7.4) while acute toxicity, hematological and histopathological studies were performed on rats. The cytotoxicity was evaluated against TNB (MCF-7), lung (A-549), and colon (HT-29) cancer cell lines. High EE (92.3 ± 12%) and drug release of up to 89.4% within 8 h were obtained. DSC thermograms of PG and PG-PNPs showed endothermic peaks indicating amorphous nature. The FT-IR spectrum of PG-PNPs revealed remarkable peaks of pure PG, indicating no strong chemical interaction between the drug and excipients. The TEM micrograph of the PG-PNPs showed nano-sized formulations (20-30 nm) whose particles were mostly lamellar and hexagonal structures. The 1H NMR result revealed the chemical structure of PG showing all assigned proton chemical shifts. Toxicity results of the PG and its formulation up to a concentration of 5000 mg/kg showed insignificant vacuolar changes of hepatocytes in the liver, with normal renal medulla and cortex in the kidney. The PG and PG-PNPs inhibited the growth of breast, lung, and colon cell lines. The nano-sized lipid formulation (PG-PNPs) showed potential in PG delivery and cancer treatments.
ISSN:2405-8440
2405-8440
DOI:10.1016/j.heliyon.2023.e16963