Preparation of ginsenoside compound-K mixed micelles with improved retention and antitumor efficacy

Jin, Xin; Yang, Qing; Cai, Ning

doi:10.2147/ijn.s167529

Cited by 19 publications

(18 citation statements)

References 42 publications

(45 reference statements)

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“…Likewise, CK ascorbyl palmitate (AP)/TPGS micelles enhanced solubility of CK and significantly inhibited P-gp-mediated efflux [ 37 ]. Similarly, the micellar system based on phosphatidylcholine (PC) and 1,2-distearoyl-sn-glycero-3-phosphoethanolamine polyethylene glycol 2000 (DP) showed improved solubility and continued release of CK [ 38 ]. The water solubility of the CK nanoparticles (NPs)/bovine serum albumin (BSA) and CK, was compared, and BSA was found to augment the water solubility of CK.…”

Section: Pharmacokinetics Metabolism and Safety Of Compound Kmentioning

confidence: 99%

“… K/γ-CyD and K/β-CyD K/γ-CyD at different ratios 1:1 and 1:3 and K/β-CyD at 1:1 Improved solubility at lower concentrations (<0.03 M) compared to higher (<0.06 M) ↑bioavailability ↑dissolution rate compared to CK and K/β-CyD Higher dissolution rate in 1:1 ratio compared to 1:3 [ 21 ] GCKT-liposomes Phospholipid and TPGS (7:3 ratio) ↑High CK loading capacity and solubility GCK EE% was of above 98.4 ± 2.3% Sustained discharge of GCK from GCKT-liposomes compared to GCK solution (in PBS) [ 33 ] CK-M PEG-PCL/TPGS mixed micelles at different ratios of 3:0. 3:1, 3:2, 3:3 ↑drug EE% in CK-M (94.6 ± 1.4) than CK-P (62.5 ± 1.6; PEG-PCL micelles) ↑CK concentration (107.3-times) in micelles (CK-M) than free CK ↑solubility of CK with higher TPGS [ 36 ] CK-AP/TPGS micelles AP/TPGS mixed micelles ↑solubility from 35.2 ± 4.3 to 1,463.2 ± 153.3 µg/mL of CK EE% = 91.3 ± 5.2% Inhibited P-gp mediated efflux [ 37 ] CK PC/DP micellar system CK, DP, and PC at ratios of 5:12:18 ↑water solubility (~66-fold) and long drug retention time [ 38 ] BSA-CK NPs BSA ↑water solubility [ 39 ] DCY51T-AuCKNps AuNPs synthesized using Lactobacillus kimchicus Drug loading efficiency-11.03% [ 40 ] …”

Section: Pharmacokinetics Metabolism and Safety Of Compound Kmentioning

confidence: 99%

“…Meanwhile, CK-M also displayed an improved tumor inhibitory effect in vivo [ 36 ]. The anti-lung cancer effects (in vitro and in vivo) of CK AP/TPGS mixed micelles [ 37 ] and CK PC/DP micellar system [ 38 ] have also been documented. Moreover, using in vitro models, BSA-CK NPs showed more significant cytotoxic effects in the liver carcinoma (HepG2), skin cell line (HaCaT), A549 cells, and colon cancer cell line (HT29) compared to monomer CK.…”

Section: Health-promoting Activitiesmentioning

confidence: 99%

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Ginsenoside Compound K: Insights into Recent Studies on Pharmacokinetics and Health-Promoting Activities

Sharma

Lee

2020

Biomolecules

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Ginseng (Panax ginseng) is an herb popular for its medicinal and health properties. Compound K (CK) is a secondary ginsenoside biotransformed from major ginsenosides. Compound K is more bioavailable and soluble than its parent ginsenosides and hence of immense importance. The review summarizes health-promoting in vitro and in vivo studies of CK between 2015 and 2020, including hepatoprotective, anti-inflammatory, anti-atherosclerosis, anti-diabetic, anti-cancer, neuroprotective, anti-aging/skin protective, and others. Clinical trial data are minimal and are primarily based on CK-rich fermented ginseng. Besides, numerous preclinical and clinical studies indicating the pharmacokinetic behavior of CK, its parent compound (Rb1), and processed ginseng extracts are also summarized. With the limited evidence available from animal and clinical studies, it can be stated that CK is safe and well-tolerated. However, lower water solubility, membrane permeability, and efflux significantly diminish the efficacy of CK and restrict its clinical application. We found that the use of nanocarriers and cyclodextrin for CK delivery could overcome these limitations as well as improve the health benefits associated with them. However, these derivatives have not been clinically evaluated, thus requiring a safety assessment for human therapy application. Future studies should be aimed at investigating clinical evidence of CK.

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Section: Pharmacokinetics Metabolism and Safety Of Compound Kmentioning

confidence: 99%

Section: Pharmacokinetics Metabolism and Safety Of Compound Kmentioning

confidence: 99%

Section: Health-promoting Activitiesmentioning

confidence: 99%

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Ginsenoside Compound K: Insights into Recent Studies on Pharmacokinetics and Health-Promoting Activities

Sharma

Lee

2020

Biomolecules

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“…Moreover, the compound K plasma concentrations increased or maintained at 2-4 h after sharply decreasing in the 0-2 h period, and then showed a slow decrease over the 4-48 h time period in both rats and mice ( Figure 7A,B). This pattern could be attributable to the continuous reabsorption of compound K. The lipophilicity (LogP value 3.85 for compound K; 5.53 for PPD) and moderate permeability (0.5-2 × 10 −6 cm/s for compound K; 1.15 × 10 −6 cm/s for PPD) of compound K and PPD in Caco-2 cells also support the possibility of compound K and PPD reabsorption [3,7,14,15].…”

Section: Discussionmentioning

confidence: 75%

“…Collectively, the proposed enterohepatic circulation of compound K and PPD ( Figure 10) could explain how compound K shows efficacy in vivo despite its fast and exclusive biliary excretion. The distribution of compound K into the liver could be a possible link to the hepatoprotective effect of compound K. However, the therapeutic use of compound K in other tissues and the oral administration of compound K and PPD may be limited because of poor aqueous solubility (33 µg/mL for compound K; <50 ng/mL for PPD) and P-gp-mediated efflux [4,14,15]. The use of nanocrystals for PPD formulation improved oral bioavailability and brain delivery [15].…”

Section: Discussionmentioning

confidence: 99%

Pharmacokinetics and Intestinal Metabolism of Compound K in Rats and Mice

et al. 2020

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We aimed to investigate the plasma concentration, tissue distribution, and elimination of compound K following the intravenous administration of compound K (2 mg/kg) in rats and mice. The plasma concentrations of compound K in mice were much higher (about five-fold) than those in rats. In both rats and mice, compound K was mainly distributed in the liver and underwent biliary excretion. There was 28.4% fecal recovery of compound K in mice and 13.8% in rats, whereas its renal recovery was less than 0.1% in both rats and mice. Relative quantification of compound K and its metabolite protopanaxadiol (PPD) in rat bile and intestinal feces indicated that the metabolism from compound K into PPD occurred in the intestine but not in the plasma. Therefore, PPD detected in the plasma samples could have been absorbed from the intestine after metabolism in control rats, while PPD could not be detected in the plasma samples from bile duct cannulated rats. In conclusion, mice and rats shared common features such as exclusive liver distribution, major excretion pathway via biliary route, and intestinal metabolism to PPD. However, there were significant differences between rats and mice in the plasma concentrations of compound K and the fecal recovery of compound K and PPD.

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Preparation of amentoflavone‐loaded DSPE‐PEG₂₀₀₀ micelles with improved bioavailability and in vitro antitumor efficacy

Yuan

Jin

Zhang

et al. 2023

Biomedical Chromatography

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To overcome the poor aqueous solubility and enhance the anticancer effects of amentoflavone (AF), a nontoxic and biodegradable amphiphilic copolymer, poly(ethyleneglycol)‐distearoylphosphatidylethanolamine (DSPE‐PEG2000), was introduced to prepare AF micelles using the thin‐film hydration method. Amentoflavone was successfully encapsulated into the core, achieving an encapsulation efficiency of 98.80 ± 0.24% and a drug loading efficiency of 2.96 ± 0.12%. The resulting micelles exhibited a spherical shape with a particle size of approximately 25.99 nm. The solubility of AF was significant improved by 412‐fold, and cumulative drug release studies showed that AF release was much faster from the micelles compared with the free drug. The release of AF was sustained over time and followed a degradation‐based kinetic model, similar to polymeric systems. After oral administration, the AF‐loaded micelles demonstrated an enhanced oral bioavailability, which was 3.79 times higher than that of free AF. In vitro evaluations of the micelles’ antitumor effects revealed a significantly greater efficacy compared with free AF. These findings highlight the tremendous potential of DSPE‐PEG2000 micelles as a drug delivery carrier for improving the solubility and therapeutic efficacy of AF.

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Preparation of ginsenoside compound-K mixed micelles with improved retention and antitumor efficacy

Cited by 19 publications

References 42 publications

Ginsenoside Compound K: Insights into Recent Studies on Pharmacokinetics and Health-Promoting Activities

Ginsenoside Compound K: Insights into Recent Studies on Pharmacokinetics and Health-Promoting Activities

Pharmacokinetics and Intestinal Metabolism of Compound K in Rats and Mice

Preparation of amentoflavone‐loaded DSPE‐PEG₂₀₀₀ micelles with improved bioavailability and in vitro antitumor efficacy

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Preparation of ginsenoside compound-K mixed micelles with improved retention and antitumor efficacy

Cited by 19 publications

References 42 publications

Ginsenoside Compound K: Insights into Recent Studies on Pharmacokinetics and Health-Promoting Activities

Ginsenoside Compound K: Insights into Recent Studies on Pharmacokinetics and Health-Promoting Activities

Pharmacokinetics and Intestinal Metabolism of Compound K in Rats and Mice

Preparation of amentoflavone‐loaded DSPE‐PEG2000 micelles with improved bioavailability and in vitro antitumor efficacy

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Preparation of amentoflavone‐loaded DSPE‐PEG₂₀₀₀ micelles with improved bioavailability and in vitro antitumor efficacy