<i>In Vivo</i> Mechanism of Action of Sodium Caprate for Improving the Intestinal Absorption of a GLP1/GIP Coagonist Peptide

Tran, Huyen; Aihara, Eitaro; Mohammed, Faiz Ahmad; Qu, Haiyan; Riley, Andrew M.; Yuan, Shuai; Lai, Xianyin; Huang, Siyuan; Aburub, Aktham; Chen, Jack Jia Hua; Vitale, Olivia Hope; Lao, Yanbin; Estwick, Selina; Qi, Zhonghua; El-Sayed, Mohamed

doi:10.1021/acs.molpharmaceut.2c00443

Cited by 8 publications

(6 citation statements)

References 45 publications

(99 reference statements)

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“…After utilizing confocal in vivo imaging for observation, the highest bioavailability could reach 2%. [42] It has also been noted that the bioavailability of peptides coadministered with osmotic enhancers remains low and highly variable after oral administration, and investigators have developed an enteral administration device that promotes intestinal absorption of the peptide MEDI7219 and the osmotic enhancer, sodium adipate, as an example of the use of osmotic enhancers to augment the enteral administration of peptide drugs. [43] There are also a large number of studies showing [44][45][46][47] that the effect of CS as an osmotic enhancer is potentially promising (Table 1).…”

Section: Permeation Enhancers For Enhanced Oral Deliverymentioning

confidence: 99%

“…In addition to its properties of permeability, nontoxicity, biocompatibility and biodegradability, CS, and its derivatives have shown good ability to enhance the permeation of drugs through mucosal absorption in recent years, making it a promising and safe mucosal osmotic enhancer. [35] Taking oral delivery of insulin as an example, a large number of studies [42,44,45,[48][49][50][51][52][53] have used a variety of osmotic enhancers in the design of insulin oral delivery systems, and from the results, unprotected insulin is still at risk of hydrolysis, but the simultaneous application of NPs and osmotic enhancers can be effective in enhancing the bioavailability of insulin for oral administration. In general, PEs exhibit notable efficacy in enhancing drug permeation, particularly for biomolecules such as peptides and proteins.…”

Section: Permeation Enhancers For Enhanced Oral Deliverymentioning

confidence: 99%

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Micro/Nanomotors for Oral Delivery of Drugs: From Design to Application

Xie,

Luo,

Zhang

et al. 2023

Advanced NanoBiomed Research

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Oral administration, as a traditional approach of taking therapeutic drugs, is easily accepted by patients due to its convenience and compliance. However, the harsh digestive environment and mucosa‐epithelial cell barriers limit the absorption of drugs through the oral route, particularly for biomacromolecules such as protein, peptide, or nucleic acid drugs. To address this issue, active carriers such as micro/nanomotors and mechanical devices have been engineered as novel delivery systems that are capable of converting various energy into mechanical force. The active delivery of these carriers holds promise for overcoming absorptive barriers and improving drug delivery efficiency, making them an attractive option for precision medicine applications that include drug delivery, gene and cell therapy, biopsy, tissue penetration, intracellular delivery, and biosensing. This article presents an overview of the progress and challenges associated with orally delivering macromolecular drugs, as well as strategies to enhance drug absorption. Additionally, it discusses recent developments and potential applications of active carriers in drug delivery and related fields, which may provide inspiration for future research.

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Section: Permeation Enhancers For Enhanced Oral Deliverymentioning

confidence: 99%

Section: Permeation Enhancers For Enhanced Oral Deliverymentioning

confidence: 99%

Micro/Nanomotors for Oral Delivery of Drugs: From Design to Application

Xie,

Luo,

Zhang

et al. 2023

Advanced NanoBiomed Research

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“…In vitro methods range from using artificial membranes and Caco-2 cell monolayers to isolated tissue mounted in an Ussing chamber or set up as inverted sacs , The physiological similarities in the gastrointestinal tract of humans and larger animals like dogs and pigs make them good models to test and evaluate the oral absorption of such drug formulations . Nevertheless, there is an increased need in pharmaceutical research to promote the “3Rs” framework (reduce, replace, and refine the use of in vivo studies) and keep the use of in vivo studies to an acceptable minimum. , …”

Section: Introductionmentioning

confidence: 99%

“…The highest studied concentration of 300 mM mimics the scenario, where the entire dosage form dissolves in one intestinal fluid pocket, with the lowest concentration of 50 mM mimicking the scenario, where the dosage form dissolves in the total resting small-bowel volume (typical volume of 43–105 mL) . For in vitro studies presented in the manuscript, C10 solutions were formulated to 25–150 mM (or less for Caco-2 investigations to be aligned with what has previously been published). ,, …”

Section: Introductionmentioning

confidence: 99%

“…19 For in vitro studies presented in the manuscript, C10 solutions were formulated to 25−150 mM (or less for Caco-2 investigations to be aligned with what has previously been published). 12,20,21 This paper aims to share our experience and observations gained from using various in vitro and in vivo methods to evaluate C10 as a permeation enhancer in our quest to improve the oral bioavailability of macromolecules. Animal models and administration strategies that were applied in this study were endoscopic administration to the small intestine in the pig and intestinal bolus administration in the rat.…”

Section: ■ Introductionmentioning

confidence: 99%

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Experiences and Translatability of In Vitro and In Vivo Models to Evaluate Caprate as a Permeation Enhancer

Emeh,

Breitholtz,

Berg

et al. 2023

Mol. Pharmaceutics

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Transient permeation enhancers (PEs) have been widely used to improve the oral absorption of macromolecules. During pharmaceutical development, the correct selection of the macromolecule, PE, and the combination needs to be made to maximize oral bioavailability and ensure successful clinical development. Various in vitro and in vivo methods have been investigated to optimize this selection. In vitro methods are generally preferred by the pharmaceutical industry to reduce the use of animals according to the "replacement, reduction, and refinement" principle commonly termed "3Rs," and in vitro methods typically have a higher throughput. This paper compares two in vitro methods that are commonly used within the pharmaceutical industry, being Caco-2 and an Ussing chamber, to two in vivo models, being in situ intestinal instillation to rats and in vivo administration via an endoscope to pigs. All studies use solution formulation of sodium caprate, which has been widely used as a PE, and two macromolecules, being FITC−dextran 4000 Da and MEDI7219, a GLP-1 receptor agonist peptide. The paper shares our experiences of using these models and the challenges with the in vitro models in mimicking the processes occurring in vivo. The paper highlights the need to consider these differences when translating data generated using these in vitro models for evaluating macromolecules, PE, and combinations thereof for enabling oral delivery.

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