Results of a completed phase I clinical trial of CYT-6091: A pegylated colloidal gold-TNF nanomedicine

Libutti, S. K.; Paciotti, Giulio F.; Myer, Lonnie D.; Haynes, R.; Gannon, William E.; Walker, Melissa; Seidel, G.; Byrnes, Adriana A.; Yuldasheva, N.; Tamarkin, Lawrence

doi:10.1200/jco.2009.27.15_suppl.3586

Cited by 28 publications

(14 citation statements)

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“…However, only a few examples of AuNPs currently are under investigation in clinical trials [161,162]. According to the literature, Aurimune CYT-6091 (Cytimmune) is the first tumor-targeted nanomedicine consisting of tumor necrosis factor-α (TNF) covalently linked to pegylated colloidal gold [163,164]. The conclusion after finishing the phase I clinical trial was that CYT-6091 targeted tumors in humans and was well tolerated at doses greater than maximum tolerated dose for native TNF.…”

Section: Perspective Recent Advances and Conclusionmentioning

confidence: 99%

Biocompatibility and Cytotoxicity of Gold Nanoparticles: Recent Advances in Methodologies and Regulations

Kus‐Liśkiewicz

Fickers

Tahar

2021

IJMS

125

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Recent advances in the synthesis of metal nanoparticles (MeNPs), and more specifically gold nanoparticles (AuNPs), have led to tremendous expansion of their potential applications in different fields, ranging from healthcare research to microelectronics and food packaging. The properties of functionalised MeNPs can be fine-tuned depending on their final application, and subsequently, these properties can strongly modulate their biological effects. In this review, we will firstly focus on the impact of MeNP characteristics (particularly of gold nanoparticles, AuNPs) such as shape, size, and aggregation on their biological activities. Moreover, we will detail different in vitro and in vivo assays to be performed when cytotoxicity and biocompatibility must be assessed. Due to the complex nature of nanomaterials, conflicting studies have led to different views on their safety, and it is clear that the definition of a standard biosafety label for AuNPs is difficult. In fact, AuNPs’ biocompatibility is strongly affected by the nanoparticles’ intrinsic characteristics, biological target, and methodology employed to evaluate their toxicity. In the last part of this review, the current legislation and requirements established by regulatory authorities, defining the main guidelines and standards to characterise new nanomaterials, will also be discussed, as this aspect has not been reviewed recently. It is clear that the lack of well-established safety regulations based on reliable, robust, and universal methodologies has hampered the development of MeNP applications in the healthcare field. Henceforth, the international community must make an effort to adopt specific and standard protocols for characterisation of these products.

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Section: Perspective Recent Advances and Conclusionmentioning

confidence: 99%

Biocompatibility and Cytotoxicity of Gold Nanoparticles: Recent Advances in Methodologies and Regulations

Kus‐Liśkiewicz

Fickers

Tahar

2021

IJMS

125

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“…A large number of gold compounds have been studied as anticancer and anti-HIV agents [1][2][3][4][5][6][7][8][9][10] and as drug delivery vehicles in the form of gold nanoparticles in therapeutics because of their bio-inertness and cellular imaging ability. 11 However, development of gold compounds and gold nanoparticles as therapeutics 12 are hampered by their unstable nature and lack of biocompatibility. 11,13 It has, therefore, become necessary to find both non-toxic and biocompatible ligands in order to produce gold compounds that would help overcome the above shortcomings.…”

Section: Introductionmentioning

confidence: 99%

Novel bio-friendly and non-toxic thiocarbohydrate stabilizers of gold nanoparticles

et al. 2015

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Several bio-friendly carbohydrate disulfides and thiocarbohydrates have been synthesized via the reaction of D-(+)-gluconic acid d-lactone with aminoalkylthiols, leading to n-gluconamidoalkyldisulfides (L3) and (2-gluconamidoethyl)thiol (L4)}. Acetylation of hydroxy groups in L1-L3 and subsequent reduction produced the following disulfides and thiols: acetylated di(2-gluconamidoethyl)disulfide (L5), acetylated di(3-gluconamidopropyl)disulfide (L6), acetylated di(4-gluconamidobutyl)disulfide (L7), acetylated di(2-gluconamidoethyl)thiol (L8), acetylated di(3-gluconamidopropyl)thiol (L9) and acetylated di(4-gluconamidobutyl)thiol (L10). Compounds L1-L10 were characterized by combination of NMR and infrared spectroscopy, microanalysis, mass spectrometry and in a selected case X-ray crystallographic data. These thiocarbohydrate compounds were used to stabilize gold nanoparticles to gold glyconanoparticles (AuNPs) of sizes in the range of ca. 2-9 nm. The thiocrabohydrates are non-toxic toward both cancer and normal cell lines and have IC 50 values generally Z200 mM.

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“…The protein tumor necrosis factor-a (TNF) is the prototypical member of a pro-apoptotic ligand family with substantial significance for cancer therapy. [1][2][3][4][5][6][7][8][9][10][11] Studies show that after binding with specific cytokine receptors (TNFR) on the tumor endothelial vascular lining, TNF is able to induce hemorrhagic necrosis of several types of tumors. 8,10 However, TNF is also a known pro-inflammatory cytokine that regulates immune response.…”

Section: Introductionmentioning

confidence: 99%

Tumor necrosis factor interaction with gold nanoparticles

Tsai¹,

Elzey²,

DelRio³

et al. 2012

Nanoscale

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We report on a systematic investigation of molecular conjugation of tumor necrosis factor-α (TNF) protein onto gold nanoparticles (AuNPs) and the subsequent binding behavior to its antibody (anti-TNF). We employ a combination of physical and spectroscopic characterization methods, including electrospray-differential mobility analysis, dynamic light scattering, polyacrylamide gel electrophoresis, attenuated total reflectance-Fourier transform infrared spectroscopy, fluorescence assay, and enzyme-linked immunosorbent assay. The native TNF used in this study exists in the active homotrimer configuration prior to conjugation. After binding to AuNPs, the maximum surface density of TNF is (0.09 ± 0.02) nm(-2) with a binding constant of 3 × 10(6) (mol L(-1))(-1). Dodecyl sulfate ions induce desorption of monomeric TNF from the AuNP surface, indicating a relatively weak intermolecular binding within the AuNP-bound TNF trimers. Anti-TNF binds to both TNF-conjugated and citrate-stabilized AuNPs, showing that non-specific binding is significant. Based on the number of anti-TNF molecules adsorbed, a substantially higher binding affinity was observed for the TNF-conjugated surface. The inclusion of thiolated polyethylene glycol (SH-PEG) on the AuNPs inhibits the binding of anti-TNF, and the amount of inhibition is related to the number ratio of surface bound SH-PEG to TNF and the way in which the ligands are introduced. This study highlights the challenges in quantitatively characterizing complex hybrid nanoscale conjugates, and provides insight on TNF-AuNP formation and activity.

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Results of a completed phase I clinical trial of CYT-6091: A pegylated colloidal gold-TNF nanomedicine

Cited by 28 publications

References 0 publications

Biocompatibility and Cytotoxicity of Gold Nanoparticles: Recent Advances in Methodologies and Regulations

Biocompatibility and Cytotoxicity of Gold Nanoparticles: Recent Advances in Methodologies and Regulations

Novel bio-friendly and non-toxic thiocarbohydrate stabilizers of gold nanoparticles

Tumor necrosis factor interaction with gold nanoparticles

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