KE108-conjugated unimolecular micelles loaded with a novel HDAC inhibitor thailandepsin-A for targeted neuroendocrine cancer therapy

Chen, Guojun; Jaskula-Sztul, Renata; Harrison, April D.; Dammalapati, Ajitha; Xu, Wenjin; C, Yi; Chen, Herbert; Gong, Shaoqin

doi:10.1016/j.biomaterials.2016.04.029

Cited by 43 publications

(41 citation statements)

References 52 publications

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“…The s27 primer sequences were as follows: forward, 5′-TCTTTAGCCATGCACAAACG-3′ and reverse, 5′-TTTCAGTGCTGCTTCCTCCT-3′. The mRNA expression levels of the SSTRs in MZ–CRC–1 cells were measured following a similar procedure 34 . Both TT and MZ–CRC–1 are human MTC cell lines.…”

Section: Methodsmentioning

confidence: 99%

“…KE108 peptide is a somatostatin analog displaying strong binding affinities to all five subtypes of SSTRs. Our recent report demonstrated, for the first time, that KE108, a true pansomatostatin synthetic nonapeptide, can be used as an efficient SSTR-targeting ligand for targeted carcinoid cancer therapy 34 . In this study, we aimed to develop multifunctional unimolecular micelles for targeted MTC treatment (Figure 1 (A)).…”

Section: Introductionmentioning

confidence: 99%

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AB3-loaded and tumor-targeted unimolecular micelles for medullary thyroid cancer treatment

et al. 2017

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Medullary thyroid cancer (MTC) is often resistant to standard therapies, emphasizing the need for the development of other treatments. A new histone deacetylase inhibitor, AB3, can effectively inhibit MTC cell proliferation in vitro. However, its poor aqueous solubility and stability, fast clearance, and lack of tumor targeting ability limit its in vivo application. Therefore, multifunctional unimolecular micelles were developed for targeted delivery of AB3 for MTC therapy. The unimolecular micelles exhibited a spherical core–shell structure, uniform size distribution, and excellent stability. AB3 was encapsulated into the hydrophobic core of the unimolecular micelles, thus significantly enhancing its aqueous solubility and stability. KE108, a somatostatin analog possessing high affinity to all five subtypes of SSTR, was used as an MTC-targeting ligand. In vitro cellular uptake analyses demonstrated that the KE108 exhibited superior targeting ability in MTC cells compared to octreotide, the first clinically used somatostatin analog. Moreover, the AB3-loaded and KE108-conjugated unimolecular micelles exhibited the best efficacy in suppressing MTC cell growth and tumor marker expression in vitro. Furthermore, AB3-loaded, KE108-conjugated micelles demonstrated the best anticancer efficacy in vivo without any apparent systemic toxicity, thereby offering a promising approach for targeted MTC therapy.

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Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

AB3-loaded and tumor-targeted unimolecular micelles for medullary thyroid cancer treatment

et al. 2017

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“…IL-2 was more specific than any marker other than Ki-67 in detecting gastroenteropancreatic NE tumors 235, even though some other targeting markers were promising for use in clinical treatment. Novel TDP-A-loaded and KE108-conjugated unimolecular micelles exhibited the best potential in suppressing NE cancer cell growth both in vitro and in vivo 236. There also have also been some achievements in the fields of prostate, lung, pancreas, and gastrointestinal tracts.…”

Section: Neuroendocrine Cellmentioning

confidence: 99%

Role of tumor microenvironment in tumorigenesis

et al. 2017

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Tumorigenesis is a complex and dynamic process, consisting of three stages: initiation, progression, and metastasis. Tumors are encircled by extracellular matrix (ECM) and stromal cells, and the physiological state of the tumor microenvironment (TME) is closely connected to every step of tumorigenesis. Evidence suggests that the vital components of the TME are fibroblasts and myofibroblasts, neuroendocrine cells, adipose cells, immune and inflammatory cells, the blood and lymphatic vascular networks, and ECM. This manuscript, based on the current studies of the TME, offers a more comprehensive overview of the primary functions of each component of the TME in cancer initiation, progression, and invasion. The manuscript also includes primary therapeutic targeting markers for each player, which may be helpful in treating tumors.

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“…Cy5, a commonly used near-infrared dye, was encapsulated into various microemulsions for visualization of distribution in vivo. 25,26 At 8 h post-intragastric administration of free Cy5, the fluorescence signal of HepG2 tumor-bearing mice mainly accumulated in the intestinal tract and was eliminated rapidly from 8 to 24 h. Due to nanoparticle-mediated EPR effect, Cy5/C-MEs presented a potential of tumor targeting after crossing the enterocytes, especially at the initial 4 h. In sharp contrast, Cy5/ Gal(oct)-C-MEs displayed the most obvious fluorescence signal in the tumor site, which was retained for 48 h ( Figure 6A). For further confirming the accumulation of the tumor, ex vivo imaging was observed immediately after harvest of the tumor tissues from HepG2 tumor-bearing mice.…”

Section: Tumor Targeting In Vivo and Pharmacokineticsmentioning

confidence: 99%

Octanoyl galactose ester-modified microemulsion system self-assembled by coix seed components to enhance tumor targeting and hepatoma therapy

Qu¹,

Liu²,

Huang³

et al. 2017

IJN

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A nanosized drug delivery platform with a combination of rational components and tumor targeting is significant for enhancement of anticancer therapy and reduction of side effects. In this study, we developed a octanoyl galactose ester-modified microemulsion system self-assembled by coix seed components (Gal(oct)-C-MEs), which improved the tumor accumulation through asialoglycoprotein receptor-mediated endocytosis and promoted the antitumor efficacy through multicomponent-mediated synergistic effect. Octanoyl galactose ester (Gal(oct)) with a yield of 82.3% was synthesized through a green enzymatic reaction and multidimensional characterization. Gal(oct)-C-MEs with a spherical shape had a small and uniform particle size (58.49±1.03 nm), narrow polydispersity index (0.09±0.01) and neutral surface charge (−5.82±0.57 mV). In the cellular uptake studies, the internalized Gal(oct)-C-ME was 2.28-fold higher relative to that of coix seed component-based microemulsions (C-MEs). The half-maximal inhibitory concentration of Gal(oct)-C-MEs against HepG2 cells was 46.5±2.4 μg/mL, which was notably higher than that of C-MEs. Importantly, the intratumor fluorescence of HepG2 xenograft-bearing nude mice treated with Cy5/Gal(oct)-C-MEs was 1.9-fold higher relative to treatment with Cy5/C-MEs. In the study of antitumor efficacy in vivo, HepG2 xenograft-bearing nude mice intragastrically administered Gal(oct)-C-MEs for 14 days exhibited the strongest inhibition of tumor growth and the lowest toxicity against liver and kidney among all the treatments. In summary, Gal(oct)-C-ME, as a highly effective and safe anticancer drug delivery system, showed promising potential for hepatoma therapy.

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KE108-conjugated unimolecular micelles loaded with a novel HDAC inhibitor thailandepsin-A for targeted neuroendocrine cancer therapy

Cited by 43 publications

References 52 publications

AB3-loaded and tumor-targeted unimolecular micelles for medullary thyroid cancer treatment

AB3-loaded and tumor-targeted unimolecular micelles for medullary thyroid cancer treatment

Role of tumor microenvironment in tumorigenesis

Octanoyl galactose ester-modified microemulsion system self-assembled by coix seed components to enhance tumor targeting and hepatoma therapy

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