Extending Half Life of H-Ferritin Nanoparticle by Fusing Albumin Binding Domain for Doxorubicin Encapsulation

Wang, Chunyue; Zhang, Chun; Li, Zenglan; Yin, Shaowu; Wang, Qi; Guo, Fangxia; Zhang, Yao; Yu, Rong; Liu, Yongdong; Su, Zhiguo

doi:10.1021/acs.biomac.7b01545

Cited by 50 publications

(46 citation statements)

References 35 publications

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“…Cheng and co-workers recently constructed a nanosystem based on coumarin-anchored low generation dendrimers, which could self-assembly into nanostructures in aqueous solution via hydrophobic interactions. [82] 5-Fluorouracil (5-Fu) as an anticancer drug and plasmid DNA for encoding tumor necrosis factor-related apoptosis-inducing ligand (TRAIL) were efficiently loaded into the nanostructures. After cross-linking the coumarin substitutes upon irradiation with 365 nm UV light, the obtained nanomaterials possessed low toxicity, improved DNA binding, and gene transfection efficacy as well as high cellular uptake.…”

Section: Photoinduced Cross-linking/decross-linking Systemsmentioning

confidence: 99%

Remote Light‐Responsive Nanocarriers for Controlled Drug Delivery: Advances and Perspectives

Zhao

Wang

et al. 2019

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Engineering of smart photoactivated nanomaterials for targeted drug delivery systems (DDS) has recently attracted considerable research interest as light enables precise and accurate controlled release of drug molecules in specific diseased cells and/or tissues in a highly spatial and temporal manner. In general, the development of appropriate light‐triggered DDS relies on processes of photolysis, photoisomerization, photo‐cross‐linking/un‐cross‐linking, and photoreduction, which are normally sensitive to ultraviolet (UV) or visible (Vis) light irradiation. Considering the issues of poor tissue penetration and high phototoxicity of these high‐energy photons of UV/Vis light, recently nanocarriers have been developed based on light‐response to low‐energy photon irradiation, in particular for the light wavelengths located in the near infrared (NIR) range. NIR light‐triggered drug release systems are normally achieved by using two‐photon absorption and photon upconversion processes. Herein, recent advances of light‐responsive nanoplatforms for controlled drug release are reviewed, covering the mechanism of light responsive small molecules and polymers, UV and Vis light responsive nanocarriers, and NIR light responsive nanocarriers. NIR‐light triggered drug delivery by two‐photon excitation and upconversion luminescence strategies is also included. In addition, the challenges and future perspectives for the development of light triggered DDS are highlighted.

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Section: Photoinduced Cross-linking/decross-linking Systemsmentioning

confidence: 99%

Remote Light‐Responsive Nanocarriers for Controlled Drug Delivery: Advances and Perspectives

Zhao

Wang

et al. 2019

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192

115

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“…In a similar study, ferritin was genetically modified to display a serum albumin-binding domain (from the streptococcal protein G) on its external surface (ABD–Hfn), enabling the facile non-covalent attachment of serum albumin coatings upon entering the blood plasma [26]. ABD–Hfn was loaded with DOX as a drug model and fluorescent reporter in pharmacokinetic studies performed in mice.…”

Section: Engineering Pnps As Nddsmentioning

confidence: 99%

Developing Protein-Based Nanoparticles as Versatile Delivery Systems for Cancer Therapy and Imaging

et al. 2019

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In recent years, it has become apparent that cancer nanomedicine’s reliance on synthetic nanoparticles as drug delivery systems has resulted in limited clinical outcomes. This is mostly due to a poor understanding of their “bio–nano” interactions. Protein-based nanoparticles (PNPs) are rapidly emerging as versatile vehicles for the delivery of therapeutic and diagnostic agents, offering a potential alternative to synthetic nanoparticles. PNPs are abundant in nature, genetically and chemically modifiable, monodisperse, biocompatible, and biodegradable. To harness their full clinical potential, it is important for PNPs to be accurately designed and engineered. In this review, we outline the recent advancements and applications of PNPs in cancer nanomedicine. We also discuss the future directions for PNP research and what challenges must be overcome to ensure their translation into the clinic.

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“…Another interesting property of HSA is its exceptional long half-life in serum (≈18-19 days). Therefore, from a drug delivery perspective, this protein is an ideal carrier because of its combination of longevity and stability [32][33][34][35][36]. In addition, it has been reported that albumin-binding receptors (e.g., SPARC and gp60) are overexpressed on tumor cells and tumor vessel endothelium to increase the uptake of nutrients necessary for growth [37,38].…”

Section: Introductionmentioning

confidence: 99%

“…In addition, it has been reported that albumin-binding receptors (e.g., SPARC and gp60) are overexpressed on tumor cells and tumor vessel endothelium to increase the uptake of nutrients necessary for growth [37,38]. In consequence, HSA can act as a molecular carrier to selectively transport and accumulate anticancer drugs in target tumor tissues and cells [32][33][34][35]39].…”

Section: Introductionmentioning

confidence: 99%

The Interaction of Temozolomide with Blood Components Suggests the Potential Use of Human Serum Albumin as a Biomimetic Carrier for the Drug

et al. 2020

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The interaction of temozolomide (TMZ) (the main chemotherapeutic agent for brain tumors) with blood components has not been studied at the molecular level to date, even though such information is essential in the design of dosage forms for optimal therapy. This work explores the binding of TMZ to human serum albumin (HSA) and alpha-1-acid glycoprotein (AGP), as well as to blood cell-mimicking membrane systems. Absorption and fluorescence experiments with model membranes indicate that TMZ does not penetrate into the lipid bilayer, but binds to the membrane surface with very low affinity. Fluorescence experiments performed with the plasma proteins suggest that in human plasma, most of the bound TMZ is attached to HSA rather than to AGP. This interaction is moderate and likely mediated by hydrogen-bonding and hydrophobic forces, which increase the hydrolytic stability of the drug. These experiments are supported by docking and molecular dynamics simulations, which reveal that TMZ is mainly inserted in the subdomain IIA of HSA, establishing π-stacking interactions with the tryptophan residue. Considering the overexpression of albumin receptors in tumor cells, our results propose that part of the administered TMZ may reach its target bound to plasma albumin and suggest that HSA-based nanocarriers are suitable candidates for designing biomimetic delivery systems that selectively transport TMZ to tumor cells.

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Extending Half Life of H-Ferritin Nanoparticle by Fusing Albumin Binding Domain for Doxorubicin Encapsulation

Cited by 50 publications

References 35 publications

Remote Light‐Responsive Nanocarriers for Controlled Drug Delivery: Advances and Perspectives

Remote Light‐Responsive Nanocarriers for Controlled Drug Delivery: Advances and Perspectives

Developing Protein-Based Nanoparticles as Versatile Delivery Systems for Cancer Therapy and Imaging

The Interaction of Temozolomide with Blood Components Suggests the Potential Use of Human Serum Albumin as a Biomimetic Carrier for the Drug

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