Drug Delivery to the Brain across the Blood–Brain Barrier Using Nanomaterials

Tsou, Yung Hao; Zhang, Xueqing; Zhu, He; Syed, Sahla; Xu, Xiaoyang

doi:10.1002/smll.201701921

Cited by 189 publications

(140 citation statements)

References 161 publications

(167 reference statements)

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“…The resonance multiplicity in the 1 H NMR spectra are described as “s” (singlet), “d” (doublet), “t” (triplet), and “m” (multiplet) and broad resonances are indicated by “b”. Residual protic solvent of CDCl 3 ( 1 H, δ 7.27 ppm; C, δ 77.0 ppm (central resonance of the triplet)), DMSO‐ d 6 ( 1 H, δ 2.50 ppm), and MeOD ( 1 H, δ 3.31 ppm and C, δ 49.0 ppm) were used for chemical shifts calibration.…”

Section: Methodsmentioning

confidence: 99%

“…Recently, the field of drug delivery has been revolutionized with a plethora of innovative nanotechnology‐based products which can effectively diffuse through the biological barricades within the body and deliver payloads of drugs, DNA, proteins or peptides to injured or diseased cells and tissues . Despite the significant growth in the field of nanotechnology, nanoparticles face challenges during clinical translation.…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Scalable synthesis and validation of PAMAM dendrimer‐N‐acetyl cysteine conjugate for potential translation

Sharma

Kambhampati

et al. 2018

Bioengineering & Transla Med

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Dendrimer‐N‐acetyl cysteine (D‐NAC) conjugate has shown significant promise in multiple preclinical models of brain injury and is undergoing clinical translation. D‐NAC is a generation‐4 hydroxyl‐polyamidoamine dendrimer conjugate where N‐acetyl cysteine (NAC) is covalently bound through disulfide linkages on the surface of the dendrimer. It has shown remarkable potential to selectively target and deliver NAC to activated microglia and astrocytes at the site of brain injury in several animal models, producing remarkable improvements in neurological outcomes at a fraction of the free drug dose. Here we present a highly efficient, scalable, greener, well‐defined route to the synthesis of D‐NAC, and validate the structure, stability and activity to define the benchmarks for this compound. This newly developed synthetic route has significantly reduced the synthesis time from three weeks to one week, uses industry‐friendly solvents/reagents, and involves simple purification procedures, potentially enabling efficient scale up.

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Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Scalable synthesis and validation of PAMAM dendrimer‐N‐acetyl cysteine conjugate for potential translation

Sharma

Kambhampati

et al. 2018

Bioengineering & Transla Med

View full text Add to dashboard Cite

show abstract

“…[ 4 ] It is reported that nearly 98% of small‐molecule drugs or contrast agents and most macromolecular drugs are routinely excluded from the brain, which makes the treatment and imaging of brain tumors extremely difficult. [ 5,6 ] Although the tight junctions of BBB at the late stage of brain tumors are disrupted to permit drug penetration into brain, the drug concentration in tumor sites is not sufficient to reach the therapeutic level. [ 7 ] More importantly, the treatment of the early stage of brain tumors is more challenging due to the presence of almost intact BBB.…”

Section: Introductionmentioning

confidence: 99%

“…[ 6,9 ] Nanoparticles conjugating a positively charged moiety, such as a cell penetrating peptide (CPP), can contact with the membrane surface of BBB (with negative charge) to traverse the BBB by AMT. [ 5,10 ] But the ability of such nanoparticles to traverse the BBB is relatively low because of limited affinity, lack of selectivity, and easy immune clearance. RMT is the most commonly adopted strategy, which involves the binding of target ligands conjugated onto the nanoparticle to corresponding receptors expressed on the surface of brain endothelial cells to improve the delivery of loaded therapeutic agents into the brain.…”

Section: Introductionmentioning

confidence: 99%

Camouflaging Nanoparticles with Brain Metastatic Tumor Cell Membranes: A New Strategy to Traverse Blood–Brain Barrier for Imaging and Therapy of Brain Tumors

Wang

et al. 2020

Adv Funct Materials

160

120

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Glioblastoma multiforme is one of the most fatal intracranial tumors with no effective treatment. The drug concentration in tumor sites is usually insufficient to reach therapeutic levels, due to poor blood–brain‐barrier (BBB) permeability and short biological half‐life. Inspired by the proneness of those malignant tumors to brain metastasis, a brain metastatic tumor cell membrane‐coated nanocarrier with core–shell structure is constructed to cross BBB for imaging and photothermal therapy of early brain tumors. The cell membranes as the shell are extracted from different metastatic tumor cells, which endow the nanoparticles with BBB‐crossing ability and long circulation. Indocyanine green (ICG)‐loaded polymeric nanoparticle as the core allows fluorescence imaging and phototherapy of brain tumors. The as‐prepared biomimetic nanoparticles display superb BBB penetration and effective suppression of tumor growth. These findings suggest the biomimetic nanotechnology provides a new insight for the design of BBB‐crossing nanomaterials and is promising to treat brain diseases.

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“…[ ][ ] One approach to reduce such side effects is through the use of nanosized drug delivery systems (DDS). Classic DDS are either composed of inorganic materials or made from self‐assembled soft matter . The latter are typically composed of amphiphilic molecules that can be loaded with various molecules of therapeutic interest .…”

Section: Introductionmentioning

confidence: 99%

Delivery of ROS Generating Anthraquinones Using Reduction‐Responsive Peptide‐Based Nanoparticles

Richard

Craciun

Gaitzsch

et al. 2018

Helvetica Chimica Acta

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In order to limit the side effects associated with antitumor drugs such as doxorubicin, nanosized drug‐delivery systems capable of selectively delivering and releasing the drug in the diseased tissue are required. We describe nanoparticles (NPs), self‐assembled from a reduction responsive amphiphilic peptide, capable of entrapping high amounts of a redox active anticancer drug candidate and releasing it in presence of a reducing agent. This system shows a high entrapment efficiency with up to 15 mg drug per gram of peptide (5.8 mol‐%). Treatment of the NPs with reducing agent results in the disassembly of the NPs and release of the drug molecules. A reduction in cell viability is observed at drug concentrations above 250 nm in HEK293T and HeLa cell lines. This drug delivery system has potential for targeting tumor sites via the EPR effect while taking advantage of the increased reduction potential in tumor microenvironment.

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Drug Delivery to the Brain across the Blood–Brain Barrier Using Nanomaterials

Cited by 189 publications

References 161 publications

Scalable synthesis and validation of PAMAM dendrimer‐N‐acetyl cysteine conjugate for potential translation

Scalable synthesis and validation of PAMAM dendrimer‐N‐acetyl cysteine conjugate for potential translation

Camouflaging Nanoparticles with Brain Metastatic Tumor Cell Membranes: A New Strategy to Traverse Blood–Brain Barrier for Imaging and Therapy of Brain Tumors

Delivery of ROS Generating Anthraquinones Using Reduction‐Responsive Peptide‐Based Nanoparticles

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