4.7 Article

In Vivo Antitumor and Antimetastatic Efficacy of a Polyacetal-Based Paclitaxel Conjugate for Prostate Cancer Therapy

ADVANCED HEALTHCARE MATERIALS (2022)

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Journal

ADVANCED HEALTHCARE MATERIALS
Volume 11, Issue 7, Pages -

Publisher

WILEY
DOI: 10.1002/adhm.202101544

Keywords

antitumor efficacy; nanomedicines; paclitaxel; pH-responsiveness; polyacetals; polymer-drug conjugates; prostate cancer

Categories

Engineering, Biomedical Nanoscience & Nanotechnology Materials Science, Biomaterials

Funding

  1. Fondo de Investigaciones Sanitarias - Instituto de Salud Carlos III (FIS-ISCIII) [PI14/02079]
  2. Spanish Ministry of Science and Innovation (MICINN) [IPT-090000-2010-0001, IPT-2012-0712-010000]
  3. MINECO [SAF2013-44848-R, SAF2016-80427-R, PID2019-108806RB-I00]
  4. Valencian Council for Innovation, Universities, Science and Digital Society [PROMETEO/2016/103]
  5. FEDER
  6. ASEICA
  7. Fundacio Marato TV3 [337/C/2013]
  8. SGR [2017 SGR 00638]
  9. Spanish Ministry of Science and Innovation [PTA2013-8431-I, PTA2013-8849-I]
  10. Science and Technology Facilities Council (STFC) [9-13-504]
  11. EC, European Nanomedicine Characterisation Laboratory (EUNCL) H2020 project [654190]
  12. Generalitat Valenciana
  13. FEDER funds (PO FEDER of Comunitat Valenciana 2014-2020)

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The study demonstrates that tert-Ser-PTX conjugate can provide sustained release of PTX in a pH-responsive manner over 2 weeks, along with epimerization of PTX to 7-epi-PTX. Serum proteins can stabilize tert-Ser-PTX, showing enhanced stability in human serum compared to PBS. While in vitro efficacy assessments in PCa cells showed IC50 values higher than the free form of PTX, in vivo tolerability assays revealed that tert-Ser-PTX significantly reduces systemic toxicities associated with free PTX treatment.
Prostate cancer (PCa), one of the leading causes of cancer-related deaths, currently lacks effective treatment for advanced-stage disease. Paclitaxel (PTX) is a highly active chemotherapeutic drug and the first-line treatment for PCa; however, conventional PTX formulation causes severe hypersensitivity reactions and limits PTX use at high concentrations. In the pursuit of high molecular weight, biodegradable, and pH-responsive polymeric carriers, one conjugates PTX to a polyacetal-based nanocarrier to yield a tert-Ser-PTX polyacetal conjugate. tert-Ser-PTX conjugate provides sustained release of PTX over 2 weeks in a pH-responsive manner while also obtaining a degree of epimerization of PTX to 7-epi-PTX. Serum proteins stabilize tert-Ser-PTX, with enhanced stability in human serum versus PBS (pH 7.4). In vitro efficacy assessments in PCa cells demonstrate IC50 values above those for the free form of PTX due to the differential cell trafficking modes; however, in vivo tolerability assays demonstrate that tert-Ser-PTX significantly reduces the systemic toxicities associated with free PTX treatment. tert-Ser-PTX also effectively inhibits primary tumor growth and hematologic, lymphatic, and coelomic dissemination, as confirmed by in vivo and ex vivo bioluminescence imaging and histopathological evaluations in mice carrying orthotopic LNCaP tumors. Overall, the results suggest the application of tert-Ser-PTX as a robust antitumor/antimetastatic treatment for PCa.

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