Solid Lipid Nanoparticles for Duodenum Targeted Oral Delivery of Tilmicosin

Zhou, Kaixiang; Yan, Yuanyuan; Chen, Dongmei; Huang, Lingli; Li, Chao; Meng, Kuiyu; Wang, Shuge; Algharib, Samah Attia; Zhang, Yuan; Xie, Shuyu

doi:10.3390/pharmaceutics12080731

Cited by 19 publications

(18 citation statements)

References 46 publications

(62 reference statements)

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“… Chitosan and Eudragit L-100 Insulin Oral insulin delivery system 130 43. Acrylic acid and methacrylic Rifampicin Sustained release and mucoadhesive delivery 131 44. Poloxamer 188, polyvinyl alcohol, and polyacryl resin II Tilmicosin Prevent gastrointestinal degradation 132 …”

Section: Enteric-coated Nanoparticle Formulations For Non-colorectal mentioning

confidence: 99%

<p>Enteric-Coated Strategies in Colorectal Cancer Nanoparticle Drug Delivery System</p>

Wathoni

Nguyen

Rusdin

et al. 2020

DDDT

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Colorectal cancer is one of the most common cancer diseases with the increase of cases prevalence >5% every year. Multidrug resistance mechanisms and non-localized therapy become primary problems of chemotherapy drugs for curing colorectal cancer disease. Therefore, the enteric-coated nanoparticle system has been studied and proved to be able to resolve those problems with good performance for colorectal cancer. The highlight of our review aims to summarize and discuss the enteric-coated nanoparticle drug delivery system specific for colorectal cancer disease. The main and supporting literatures were collected from published research articles of journals indexed in Scopus and PubMed databases. In the oral route of administration, Eudragit pH-sensitive copolymer as a coating agent prevents the degradation of the nanoparticle system from the gastric fluid and releases drug to intestinal-colon track. Therefore, it provides a colon-specific targeting ability. Impressively, enteric-coated nanoparticles having a sustained release profile significantly increase the cytotoxic effect of chemotherapeutic drugs and achieve cell-specific target delivery. The enteric-coated nanoparticle drug delivery system represents an excellent modification to improve the effectiveness and performance of anticancer drugs for colorectal cancer disease in terms of the oral route of administration.

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Section: Enteric-coated Nanoparticle Formulations For Non-colorectal mentioning

confidence: 99%

<p>Enteric-Coated Strategies in Colorectal Cancer Nanoparticle Drug Delivery System</p>

Wathoni

Nguyen

Rusdin

et al. 2020

DDDT

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“… 20 − 23 Zhou et al prepared TIM-loaded nanoparticles by hot melting with the ultrasonic emulsification method. 24 In addition, TIM-loaded lipid nanocarriers prepared through the high shear method display excellent storage and gastrointestinal stability and consequently enhanced oral absorption in broilers. 3 , 4 Zhou et al found that TIM-loaded in alginate-chitosan nanogels shows stronger sustained drug release compared with the injection of pure TIM.…”

Section: Introductionmentioning

confidence: 99%

Facile Preparation of Tilmicosin-Loaded Polymeric Nanoparticle with Controlled Properties and Functions

Wang

Bhutto

et al. 2020

ACS Omega

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As one of the effective broad-spectrum antimicrobial and anti-inflammatory drugs, tilmicosin (TIM) is applied extensively in a wide range of veterinary treatments. However, the low bioavailability typically leads to overuse of TIM in practical applications, which can cause residual accumulation in the environment and contamination of foodstuffs. Here, we report a precipitation method that allows us to prepare TIM-loaded poly(methyl methacrylate- co -methacrylic acid) (P(MMA- co -MAA)) nanoparticles. Specifically, TIM and biocompatible P(MMA- co -MAA) are dissolved in methanol and then water is introduced as an antisolvent, which triggers the co-precipitation and leads to well-controlled nanoparticles. Depending on the drug/polymer mass ratio and the total concentration of drug and polymer, the formed nanoparticles display a tunable radius from 27 to 80 nm with a narrow size distribution, a high drug loading content, and a controlled release of TIM. The encapsulation does not interrupt the antibacterial function of TIM while reducing its cytotoxicity enormously. Moreover, the formed nanoparticles could be dried to powder through freeze-drying, and the redispersion of the particles hardly disturbs the particle size, size distribution, and drug loading content. Our study developed a facile and robust precipitation method for the controlled construction of TIM-loaded polymeric nanoparticles with tunable properties and functions, as well as improved biocompatibility, which shall improve the bioavailability of TIM and enhance the practical applications.

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“…This improved the in vivo anti-inflammatory efficacy of the formulation to rats with indomethacin-induced intestinal lesions, significantly reducing the ulcer index and the histological intestinal damage [ 212 ]. The ability of Tween 80 (polysorbate) to inhibit Pgp has also shown a promising role in the bioavailability enhancement of Pgp substrates [ 149 , 156 , 213 ]. In this line, Goo et al observed 4.1-fold permeation enhancement of valsartan, a Pgp substrate, through rat jejunum by its encapsulation in SNEDDS stabilized by Tween 80, as well as a 470% increase in its oral bioavailability in rats.…”

Section: Inhibition Of P-glycoproteinmentioning

confidence: 99%

“…Similarly, Zhou et al have recently exploited the potential of polysorbate-80 to inhibit drug efflux. These authors reported higher intestinal permeability of tilmicosin-loaded solid lipid nanoparticles when polysorbate-80 was added as Pgp inhibitor [ 213 ].…”

Section: Inhibition Of P-glycoproteinmentioning

confidence: 99%

Current approaches in lipid-based nanocarriers for oral drug delivery

Plaza-Oliver

Santander-Ortega

Lozano

2021

Drug Deliv. and Transl. Res.

102

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Graphical abstract Lipid-based nanocarriers have gained much interest as carriers of drugs with poor oral bioavailability because of their remarkable advantages like low toxicity, affordable scale-up manufacture, strong biocompatibility or high drug loading efficiency. The potential of these nanocarriers lies in their ability to improve the gastrointestinal stability, solubility and permeability of their cargo drugs. However, achieving efficient oral drug delivery through lipid-based nanocarriers is a challenging task, since they encounter multiple physicochemical barriers along the gastrointestinal tract, e.g. the gastric acidic content, the intestinal mucus layer or the enzymatic degradation, that they must surmount to reach their target. These limitations may be turned into opportunities through a rational design of lipid-based nanocarriers. For that purpose, this review focuses on the main challenges of the oral route indicating the strategies undertaken for lipid-based nanocarriers in order to overcome them. Understanding their shortcomings and identifying their strengths will determine the future clinical success of lipid-based nanocarriers.

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Solid Lipid Nanoparticles for Duodenum Targeted Oral Delivery of Tilmicosin

Cited by 19 publications

References 46 publications

<p>Enteric-Coated Strategies in Colorectal Cancer Nanoparticle Drug Delivery System</p>

<p>Enteric-Coated Strategies in Colorectal Cancer Nanoparticle Drug Delivery System</p>

Facile Preparation of Tilmicosin-Loaded Polymeric Nanoparticle with Controlled Properties and Functions

Current approaches in lipid-based nanocarriers for oral drug delivery

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