Literature DB >> 28676380

Investigation of the biodistribution, breakdown and excretion of delta inulin adjuvant.

Lixin Wang1, Thomas Barclay1, Yunmei Song1, Paul Joyce2, Isaac G Sakala3, Nikolai Petrovsky3, Sanjay Garg4.   

Abstract

Insoluble, nanostructured delta inulin particles enhance the immunogenicity of co-administered protein antigens and consequently are used as a vaccine adjuvant (Advax™). To better understand their immunomodulatory properties, the in vitro hydrolysis and in vivo distribution of delta inulin particles were investigated. Delta inulin particle hydrolysis under bio-relevant acidic conditions resulted in no observable change to the bulk morphology using SEM, and HPLC results showed that only 6.1% of the inulin was hydrolysed over 21days. However, 65% of the terminal glucose groups were released, showing that acid hydrolysis relatively rapidly releases surface bound chemistries. This was used to explain in vivo biodistribution results in which delta inulin particles surface-labelled with fluorescein-5-thiosemicabizide were administered to mice using intramuscular (I.M.) or subcutaneous (S.C.) routes. Comparison analysis of the fluorescence of soluble inulin in the supernatants of homogenised tissues maintained at room temperature or heated to 100°C to solubilise particulate inulin was used to distinguish between fluorescent probe on soluble inulin and probe bound to inulin within particles. Following both I.M. and S.C. injection delta inulin exhibited a depot behaviour with local injection site residence for several weeks. Over this time, as injection site inulin reduced, there was measurable transport of intact delta inulin particles by macrophages to secondary lymphoid organs and the liver. Ultimately, the injected delta inulin became solubilised resulting in its detection in the plasma and in the urine. Thus injected delta inulin particles are initially taken up by macrophages at the site of injection, trafficked to secondary lymphoid tissue and the liver, and hydrolysed resulting in their becoming soluble and diffusing into the blood stream, from whence they are glomerularly filtered and excreted into the urine. These results provide important insights into the biodistribution of I.M. or S.C. injected delta inulin particles when used as vaccine adjuvants and their method of excretion.
Copyright © 2017 Elsevier Ltd. All rights reserved.

Entities:  

Keywords:  Biodistribution; Carbohydrate hydrolysis; Delta inulin; Vaccine adjuvant

Mesh:

Substances:

Year:  2017        PMID: 28676380     DOI: 10.1016/j.vaccine.2017.06.045

Source DB:  PubMed          Journal:  Vaccine        ISSN: 0264-410X            Impact factor:   3.641


  6 in total

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Journal:  Pharmacol Rep       Date:  2022-09-20       Impact factor: 3.919

3.  Randomized controlled trial demonstrating the benefits of delta inulin adjuvanted immunotherapy in patients with bee venom allergy.

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Authors:  Jasmine Tomar; Harshad P Patil; Gustavo Bracho; Wouter F Tonnis; Henderik W Frijlink; Nikolai Petrovsky; Rita Vanbever; Anke Huckriede; Wouter L J Hinrichs
Journal:  J Control Release       Date:  2018-09-12       Impact factor: 9.776

5.  Doxorubicin-Loaded Delta Inulin Conjugates for Controlled and Targeted Drug Delivery: Development, Characterization, and In Vitro Evaluation.

Authors:  Lixin Wang; Yunmei Song; Ankit Parikh; Paul Joyce; Rosa Chung; Liang Liu; Franklin Afinjuomo; John D Hayball; Nikolai Petrovsky; Thomas G Barclay; Sanjay Garg
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6.  Synthesis and Characterization of pH-Sensitive Inulin Conjugate of Isoniazid for Monocyte-Targeted Delivery.

Authors:  Franklin Afinjuomo; Thomas G Barclay; Ankit Parikh; Rosa Chung; Yunmei Song; Gayathri Nagalingam; Jamie Triccas; Lixin Wang; Liang Liu; John D Hayball; Nikolai Petrovsky; Sanjay Garg
Journal:  Pharmaceutics       Date:  2019-10-28       Impact factor: 6.321

  6 in total

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