Literature DB >> 31094367

Cell-penetrating peptide together with PEG-modified mesostructured silica nanoparticles promotes mucous permeation and oral delivery of therapeutic proteins and peptides.

Xinyi Tan1, Yan Zhang, Qian Wang, Tianyang Ren, Jingxin Gou, Wei Guo, Tian Yin, Haibing He, Yu Zhang, Xing Tang.   

Abstract

Poor permeation across intestinal mucous barriers often limits the oral delivery of prospective therapeutic proteins and peptides (TPPs). In order to address this issue, cell penetrating peptide (CPP) together with PEG modified and pore-enlarged mesostructured silica nanoparticle (NP) were constructed to form the mucus-penetrating electrostatic particle-complexes, CPP/TPP/NP. Alone, CPP and TPP often present with poor stability, and their traditional electrostatic complex shows reduced pharmacodynamics. To provide satisfactory protection, silica NPs were loaded with CPP and TPP (CPP@NP and TPP@NP), respectively, and then CPP@NP and TPP@NP could together form CPP/TPP/NP via electrostatic interaction. As a result, CPP involvement with PEG modification showed an 8.45-, 1.62- and 5.09-fold increase in cellular uptake, exocytosis and final transcellular permeation in mucous conditions, respectively. It was found that CPP involvement mainly affected transport and exocytosis, and the PEG polymer significantly influenced mucous penetration and cellular uptake, which could further promote CPP ability for uptake and exocytosis. Additionally, NP-mediated CPP/TPP/NP showed a similar uptake mechanism with supporting carriers (clathrin-mediated endocytosis), and could strengthen transcellular routes (the endoplasmic reticulum-Golgi apparatus pathway and the lysosome route). Utilizing recombinant growth hormone (RGH) as a model TPP, oral administration of the RGH-loaded CPP/TPP/LMSN-PEG10k with hydrophilic and electroneutral properties induced 5.41- and 4.91-fold increases in pharmacodynamics in vitro and in vivo, respectively. Thus, CPP/TPP/NP significantly promoted mucous permeation and shows promising potential for oral delivery of TPPs.

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Year:  2019        PMID: 31094367     DOI: 10.1039/c9bm00274j

Source DB:  PubMed          Journal:  Biomater Sci        ISSN: 2047-4830            Impact factor:   6.843


  9 in total

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Authors:  Jacob C McCright; Katharina Maisel
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Journal:  J Nanobiotechnology       Date:  2022-06-25       Impact factor: 9.429

3.  Macrophage-Engineered Vesicles for Therapeutic Delivery and Bidirectional Reprogramming of Immune Cell Polarization.

Authors:  Khaga R Neupane; J Robert McCorkle; Timothy J Kopper; Jourdan E Lakes; Surya P Aryal; Masud Abdullah; Aaron A Snell; John C Gensel; Jill Kolesar; Christopher I Richards
Journal:  ACS Omega       Date:  2021-01-26

Review 4.  Mesoporous Silica Nanoparticles: Properties and Strategies for Enhancing Clinical Effect.

Authors:  Alex N Frickenstein; Jordan M Hagood; Collin N Britten; Brandon S Abbott; Molly W McNally; Catherine A Vopat; Eian G Patterson; William M MacCuaig; Ajay Jain; Keisha B Walters; Lacey R McNally
Journal:  Pharmaceutics       Date:  2021-04-17       Impact factor: 6.321

5.  Extracellular Vesicles Mediate the Intercellular Exchange of Nanoparticles.

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Review 6.  Advances in oral peptide drug nanoparticles for diabetes mellitus treatment.

Authors:  Yan Li; Wen Zhang; Ruichen Zhao; Xin Zhang
Journal:  Bioact Mater       Date:  2022-02-28

Review 7.  Overcoming the cellular barriers and beyond: Recent progress on cell penetrating peptide modified nanomedicine in combating physiological and pathological barriers.

Authors:  Yingke Liu; Zhihe Zhao; Man Li
Journal:  Asian J Pharm Sci       Date:  2022-06-23       Impact factor: 9.273

Review 8.  Nanoparticles Modified with Cell-Penetrating Peptides: Conjugation Mechanisms, Physicochemical Properties, and Application in Cancer Diagnosis and Therapy.

Authors:  Isabel Gessner; Ines Neundorf
Journal:  Int J Mol Sci       Date:  2020-04-06       Impact factor: 5.923

9.  Peptide-Mucin Binding and Biosimilar Mucus-Permeating Properties.

Authors:  Xiaohong Sun; Raliat O Abioye; Ogadimma D Okagu; Chibuike C Udenigwe
Journal:  Gels       Date:  2021-12-21
  9 in total

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