Quantitative and qualitative toxicological evaluation of thiol-ene "click" chemistry-based polyanhydrides and their degradation products

Quantitative and qualitative toxicological analyses of crosslinked, surface‐eroding polyanhydrides (PAHs) made from thiol‐ene “click” polymerizations are reported. The cytotoxicity of these PAHs was investigated against three skin‐based cell types; melanoma (A‐375), human dermal fibroblast adult (HD...

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Bibliographic Details
Published in:Journal of biomedical materials research. Part A 2016-08, Vol.104 (8), p.1936-1945
Main Authors: Mohammed, Halimatu S., Snyder, Brittany L., Samways, Damien S. K., Shipp, Devon A.
Format: Article
Language:English
Subjects:
3T3 Cells
Adult
Animals
Cell Death - drug effects
Cell Proliferation - drug effects
Cell Shape - drug effects
Cell Survival - drug effects
Click Chemistry - methods
Cross-Linking Reagents - chemistry
Crosslinking
cytotoxicity
Degradation
Dermis - cytology
Drug delivery systems
Fibroblasts
Fibroblasts - cytology
Fibroblasts - drug effects
Fluorescence
Humans
Imaging
Mice
Morphology
Polyallylamine hydrochloride
polyanhydrides
Polyanhydrides - chemistry
Polyanhydrides - toxicity
Polymerization
Sulfhydryl Compounds - chemistry
surface erosion
thiol-ene "click" polymerization
Toxicity Tests
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Summary:Quantitative and qualitative toxicological analyses of crosslinked, surface‐eroding polyanhydrides (PAHs) made from thiol‐ene “click” polymerizations are reported. The cytotoxicity of these PAHs was investigated against three skin‐based cell types; melanoma (A‐375), human dermal fibroblast adult (HDFa), and 3T3‐J2 (mouse fibroblast) cells, thus providing insight into the potential for these PAHs to be used in dermal drug delivery applications. Apoptosis was evaluated quantitatively and qualitatively using MTT assay and fluorescence microscopic imaging as indication of cytotoxicity. Upon exposure of A‐375 and HDFa cells to high concentrations (4000 mg/L) of crosslinked PAH, the respective morphologies remained relatively unchanged compared with nonexposed cells. The 3T3‐J2 cell type was more sensitive towards the PAH, exhibiting minimal deformation of cell morphology at 4000 mg/L. The MTT assay and fluorescence imaging revealed that this PAH and its degradation products are highly cytocompatible at high concentrations and cytotoxicity observed is dosage/time dependent. Further, the PAH did not induce inhibition of tested cells’ proliferation at high polymer concentration up to 2000 mg/L. The IC50 (concentration of the crosslinked PAH required to inhibit 50% cell viability) for HDFa and A‐375 cells was determined to be 4300 ± 70 and 8500 ± 50 mg/L, respectively. The high cytocompatibility of this type of crosslinked PAH, in addition to their degradation products, towards these skin cells (standard and cancer cell types) suggests that the polymer may be viable for dermal‐based drug delivery to normal and cancerous diseased tissues. © 2016 Wiley Periodicals, Inc. J Biomed Mater Res Part A: 104A: 1936–1945, 2016.
ISSN:1549-3296
1552-4965
DOI:10.1002/jbm.a.35724