4.7 Article

Uniaxial and Coaxial Nanofibers PCL/Alginate or PCL/Gelatine Transport and Release Tamoxifen and Curcumin Affecting the Viability of MCF7 Cell Line

期刊

NANOMATERIALS
卷 12, 期 19, 页码 -

出版社

MDPI
DOI: 10.3390/nano12193348

关键词

nanofiber; curcumin; tamoxifen; breast cancer; electrospinning; MCF-7

资金

  1. Minciencias Bogota Colombia MINCIENCIAS [FP44842-07-2018, 122277657905]
  2. Departamento de Fisica, Grupo de Materiales Nanoestructurados y sus Aplicaciones, Universidad Nacional de Colombia-Colombia, Bogota-Colombia
  3. CAPES
  4. FAPEMIG
  5. CNPq
  6. Center of Microscopy at UFMG

向作者/读者索取更多资源

Breast cancer is the second leading cause of cancer death in women worldwide. Researchers are exploring therapeutic and preventive alternatives, including the use of synthetic drug tamoxifen citrate and natural compound curcumin. To enhance effectiveness and reduce side effects, a controlled release system utilizing nanoscale materials was developed. The system demonstrated high toxicity to breast cancer cells and minimal toxicity to healthy cells.
Breast cancer is the second cause of cancer death in women worldwide. The search for therapeutic and preventive alternatives has increased in recent years. One synthetic drug for patients with hormone receptor-positive tumours is tamoxifen citrate (TMX). Curcumin (Cur) is a natural compound that is being tested. Both were coupled with nanoscale-controlled and sustained release systems to increase the effectiveness of the treatment and reduce adverse effects. We produced a controlled release system based on uniaxial and coaxial polymeric nanofibers of polycaprolactone (PCL), alginate (Alg) and gelatine (Gel) for the transport and release of TMX and Cur, as a new alternative to breast cancer treatment. Nanofibers combining PCL-Alg and PCL-Gel were fabricated by the electrospinning technique and physicochemically characterised by thermal analysis, absorption spectroscopy in the infrared region and X-ray diffraction. Morphology and size were studied by scanning electron microscopy. Additionally, the release profile of TMX and Cur was obtained by UV-Vis spectroscopy. Additionally, the cytotoxic effect on breast cancer cell line MCF7 and peripheral-blood mononuclear cells (PBMCs) from a healthy donor were evaluated by a Resazurin reduction assay. These assays showed that PCL-TMX nanofiber was highly toxic to both cell types, while PCL-Cur was less toxic.

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