Coordinated ASBT and EGFR Mechanisms for Optimized Liraglutide Nanoformulation Absorption in the GI Tract

Seho Kweon; Seong Jin Park; Ha Kyeong Lee; Seo Hee Kang; Kwan-Young Chang; Jeong Uk Choi; Jooho Park; Jung-Hyun Shim; Jin Woo Park; Youngro Byun

doi:10.2147/IJN.S442617

Coordinated ASBT and EGFR Mechanisms for Optimized Liraglutide Nanoformulation Absorption in the GI Tract

Int J Nanomedicine. 2024 Mar 23:19:2973-2992. doi: 10.2147/IJN.S442617. eCollection 2024.

Authors

Seho Kweon^{1

2}, Seong Jin Park³, Ha Kyeong Lee¹, Seo Hee Kang⁴, Kwan-Young Chang⁴, Jeong Uk Choi⁵, Jooho Park⁶, Jung-Hyun Shim⁷, Jin Woo Park⁷, Youngro Byun^{1

3}

Affiliations

¹ Department of Molecular Medicine and Biopharmaceutical Science, Graduate School of Convergence Science and Technology, Seoul National University, Seoul, 08826, Republic of Korea.
² College of Pharmacy, Chonnam National University, Gwangju, 61186, Republic of Korea.
³ College of Pharmacy, Seoul National University, Seoul, 08826, Republic of Korea.
⁴ Global R&D Center, IcureBNP, Seoul, 06170, Republic of Korea.
⁵ College of Pharmacy, Kyung Hee University, Seoul, 02447, Republic of Korea.
⁶ Department of Biomedical & Health Science, Konkuk University, Chungju, 27478, Republic of Korea.
⁷ College of Pharmacy and Biomedical and Healthcare Research Institute, Mokpo National University, Jeonnam, 58554, Republic of Korea.

Abstract

Background: For maintenance therapy in type 2 diabetes, glucagon-like peptide-1 agonist (GLP-1A), which exhibits low cardiovascular risk and high efficacy, is a promising peptide therapeutic. However, developing an oral GLP-1A presents challenges due to the analog's poor cellular permeability and gastrointestinal (GI) stability.

Methods: To mitigate such limitations, an oral nanoformulation of liraglutide (LG) was designed and achieved by combining LG with bile acid derivatives using the nanoprecipitation method. This strategy allowed the bile acid moieties to localize at the nanoparticle surface, enhancing the binding affinity for apical sodium-dependent bile acid transporter (ASBT) and improving GI stability. The in vitro characteristics, cellular permeability, and absorption mechanisms of the LG nanoformulation (LG/TD-NF) were thoroughly investigated. Furthermore, the in vivo oral absorption in rats and the glucose-lowering effects in a diabetic (db/db) mouse model were evaluated.

Results: The LG/TD-NF produced neutral nanoparticles with a diameter of 58.7 ± 4.3 nm and a zeta potential of 4.9 ± 0.4 mV. Notably, when exposed to simulated gastric fluid, 65.7 ± 3.6% of the LG/TD-NF remained stable over 120 min, while free LG was fully degraded. Relative to unformulated LG, the Caco-2 cellular permeability of the nanoformulation improved, measuring 10.9 ± 2.1 (× 10^-6 cm/s). The absorption mechanism prominently featured endocytosis simultaneously mediated by both ASBT and epidermal growth factor receptor (EGFR). The oral bioavailability of the LG/TD-NF was determined to be 3.62% at a dosage of 10 mg/kg, which is 45.3 times greater than that of free LG. In a diabetes model, LG/TD-NF at 10 mg/kg/day exhibited commendable glucose sensitivity and reduced HbA1c levels by 4.13% within 28 days, similar to that of subcutaneously administered LG at a dosage of 0.1 mg/kg/day.

Conclusion: The oral LG/TD-NF promotes ASBT/EGFR-mediated transcytosis and assures cellular permeability within the GI tract. This method holds promise for the development of oral GLP-1A peptides as an alternative to injections, potentially enhancing patient adherence to maintenance therapy.

Keywords: ASBT-mediated endocytosis; EGFR; nanoformulation of GLP-1A; oral liraglutide.

MeSH terms

Animals
Bile Acids and Salts
Caco-2 Cells
Diabetes Mellitus, Type 2* / drug therapy
ErbB Receptors
Gastrointestinal Tract / metabolism
Glucagon-Like Peptide 1 / therapeutic use
Glucose
Humans
Hypoglycemic Agents / pharmacology
Hypoglycemic Agents / therapeutic use
Liraglutide* / pharmacology
Mice
Rats

Substances

Liraglutide
Glucagon-Like Peptide 1
Bile Acids and Salts
Glucose
ErbB Receptors
Hypoglycemic Agents
EGFR protein, human