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Arginine-Coated Nanoglobules for the Nasal Delivery of Insulin

Multiple daily injections via subcutaneous route are the primary modes of insulin delivery for patients with Diabetes Mellitus. While this process is invasive, painful and may cause patients to develop lipohypertrophy at injection site, the perception of fear surrounding this process causes patients...

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Autores principales: Das, Atanu, Vartak, Richa, Islam, Md Asrarul, Kumar, Sunil, Shao, Jun, Patel, Ketan
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9965127/
https://www.ncbi.nlm.nih.gov/pubmed/36839674
http://dx.doi.org/10.3390/pharmaceutics15020353
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author Das, Atanu
Vartak, Richa
Islam, Md Asrarul
Kumar, Sunil
Shao, Jun
Patel, Ketan
author_facet Das, Atanu
Vartak, Richa
Islam, Md Asrarul
Kumar, Sunil
Shao, Jun
Patel, Ketan
author_sort Das, Atanu
collection PubMed
description Multiple daily injections via subcutaneous route are the primary modes of insulin delivery for patients with Diabetes Mellitus. While this process is invasive, painful and may cause patients to develop lipohypertrophy at injection site, the perception of fear surrounding this process causes patients to delay in initiation and remain persistent with insulin therapy over time. Moreover, poor glycemic control may often lead to acute complications, such as severe hypoglycemia and nocturnal hypoglycemia, especially in older patients with diabetes. To address the imperative need for a patient-convenient non-invasive insulin therapy, an insulin-loaded arginine-coated self-emulsifying nanoglobule system (INS-LANano) was developed for nasal delivery of insulin with a biodegradable cationic surfactant—Lauroyl Ethyl Arginate (LAE). Incorporation of LAE resulted in formation of positively charged nanoglobules with L-arginine oriented on the surface. LANano enabled binding of insulin molecules on the surface of nanoglobules via an electrostatic interaction between negatively charged α-helix and LAE molecules at physiological pH. INS-LANano showed a hydrodynamic diameter of 23.38 nm with a surface charge of +0.118 mV. The binding efficiency of insulin on LANano globules was confirmed by zeta potential, circular dichroism (CD) spectroscopy and centrifugal ultrafiltration studies. The attachment of insulin with permeation-enhancing nanoglobules demonstrated significantly higher in vitro permeability of insulin of 15.2% compared to insulin solution across human airway epithelial cell (Calu-3) monolayer. Upon intranasal administration of INS-LANano to diabetic rats at 2 IU/kg insulin dose, a rapid absorption of insulin with significantly higher Cmax of 14.3 mU/L and relative bioavailability (BA) of 23.3% was observed. Therefore, the INS-LANano formulation significant translational potential for intranasal delivery of insulin
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spelling pubmed-99651272023-02-26 Arginine-Coated Nanoglobules for the Nasal Delivery of Insulin Das, Atanu Vartak, Richa Islam, Md Asrarul Kumar, Sunil Shao, Jun Patel, Ketan Pharmaceutics Article Multiple daily injections via subcutaneous route are the primary modes of insulin delivery for patients with Diabetes Mellitus. While this process is invasive, painful and may cause patients to develop lipohypertrophy at injection site, the perception of fear surrounding this process causes patients to delay in initiation and remain persistent with insulin therapy over time. Moreover, poor glycemic control may often lead to acute complications, such as severe hypoglycemia and nocturnal hypoglycemia, especially in older patients with diabetes. To address the imperative need for a patient-convenient non-invasive insulin therapy, an insulin-loaded arginine-coated self-emulsifying nanoglobule system (INS-LANano) was developed for nasal delivery of insulin with a biodegradable cationic surfactant—Lauroyl Ethyl Arginate (LAE). Incorporation of LAE resulted in formation of positively charged nanoglobules with L-arginine oriented on the surface. LANano enabled binding of insulin molecules on the surface of nanoglobules via an electrostatic interaction between negatively charged α-helix and LAE molecules at physiological pH. INS-LANano showed a hydrodynamic diameter of 23.38 nm with a surface charge of +0.118 mV. The binding efficiency of insulin on LANano globules was confirmed by zeta potential, circular dichroism (CD) spectroscopy and centrifugal ultrafiltration studies. The attachment of insulin with permeation-enhancing nanoglobules demonstrated significantly higher in vitro permeability of insulin of 15.2% compared to insulin solution across human airway epithelial cell (Calu-3) monolayer. Upon intranasal administration of INS-LANano to diabetic rats at 2 IU/kg insulin dose, a rapid absorption of insulin with significantly higher Cmax of 14.3 mU/L and relative bioavailability (BA) of 23.3% was observed. Therefore, the INS-LANano formulation significant translational potential for intranasal delivery of insulin MDPI 2023-01-20 /pmc/articles/PMC9965127/ /pubmed/36839674 http://dx.doi.org/10.3390/pharmaceutics15020353 Text en © 2023 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Das, Atanu
Vartak, Richa
Islam, Md Asrarul
Kumar, Sunil
Shao, Jun
Patel, Ketan
Arginine-Coated Nanoglobules for the Nasal Delivery of Insulin
title Arginine-Coated Nanoglobules for the Nasal Delivery of Insulin
title_full Arginine-Coated Nanoglobules for the Nasal Delivery of Insulin
title_fullStr Arginine-Coated Nanoglobules for the Nasal Delivery of Insulin
title_full_unstemmed Arginine-Coated Nanoglobules for the Nasal Delivery of Insulin
title_short Arginine-Coated Nanoglobules for the Nasal Delivery of Insulin
title_sort arginine-coated nanoglobules for the nasal delivery of insulin
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9965127/
https://www.ncbi.nlm.nih.gov/pubmed/36839674
http://dx.doi.org/10.3390/pharmaceutics15020353
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