Effect of Tyrosine-Derived Triblock Copolymer Compositions on Nanosphere Self-Assembly and Drug Delivery

Sheihet, Larisa; Piotrowska, Karolina; Dubin, Robert; Kohn, Joachim; Devore, David I.

doi:10.1021/bm060860t

Cited by 66 publications

(83 citation statements)

References 35 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…(21)(22)(23) In vivo efficacy of nanosphere-paclitaxel formulation exhibited anti-tumor activity in a breast cancer xenograft model that is similar to that of an equivalent dose of clinically used formulation of Cremophorpaclitaxel. (23,24) It is our believe, that this novel technology can potentially address the key military and civilian requirements for effective breast cancer chemotherapy: nontoxic administration, increased bioavailability, prolonged circulation and targeting cancer cells, leading to substantially greater drug efficacy and lower toxicity. Further exploration of the proposed multidisciplinary research, while potentially high risk, may result in the introduction of innovative, high impact treatments for breast cancer.…”

Section: Introduction Backgroundmentioning

confidence: 83%

“…The synthesis of desaminotyrosyl-tyrosine esters, DTR,(28) and triblock copolymers has been previously described. (22,23,29) Briefly, the triblock copolymers were synthesized in a one-pot reaction at 20 °C using in situ carbodiimide coupling of the PEG and oligo(DTR-XA) while reaction conditions such as monomer ratios, temperature and reaction time were kept constant for all compositions. We expect to identify an optimum ratio of triblock hydrophobicity/hydrophilicity, determined by the physical and chemical properties of the copolymer blocks, that provides for effective delivery of each selected drug.…”

Section: Copolymer Syntheses and Nanosphere Formulationmentioning

confidence: 99%

“…Tyrosine-derived triblock copolymers self-assemble into spherical structures with hydrodynamic diameters between 50 nm and 100 nm, thus providing particle size and surface chemical properties superior to conventional drug delivery designs. (21)(22)(23) In addition to their biocompatibility, biodegradability and lack of cellular toxicity, these nanospheres strongly bind and retain in vitro anti-tumor cytotoxicity of the hydrophobic chemotherapeutic agent, paclitaxel. (21)(22)(23) In vivo efficacy of nanosphere-paclitaxel formulation exhibited anti-tumor activity in a breast cancer xenograft model that is similar to that of an equivalent dose of clinically used formulation of Cremophorpaclitaxel.…”

Section: Introduction Backgroundmentioning

confidence: 99%

“…(21)(22)(23) In addition to their biocompatibility, biodegradability and lack of cellular toxicity, these nanospheres strongly bind and retain in vitro anti-tumor cytotoxicity of the hydrophobic chemotherapeutic agent, paclitaxel. (21)(22)(23) In vivo efficacy of nanosphere-paclitaxel formulation exhibited anti-tumor activity in a breast cancer xenograft model that is similar to that of an equivalent dose of clinically used formulation of Cremophorpaclitaxel. (23,24) It is our believe, that this novel technology can potentially address the key military and civilian requirements for effective breast cancer chemotherapy: nontoxic administration, increased bioavailability, prolonged circulation and targeting cancer cells, leading to substantially greater drug efficacy and lower toxicity.…”

Section: Introduction Backgroundmentioning

confidence: 99%

See 3 more Smart Citations

Nanospheric Chemotherapeutic and Chemoprotective Agents

Sheihet¹

2008

Self Cite

View full text Add to dashboard Cite

Public reporting burden for this collection of information is estimated to average 1 hour per response, including the time for reviewing instructions, searching existing data sources, gathering and maintaining the data needed, and completing and reviewing this collection of information. Send comments regarding this burden estimate or any other aspect of this collection of information, including suggestions for reducing this burden to Department of Defense, Washington Headquarters Services, Directorate for Information Operations and Reports (0704-0188), 1215 Jefferson Davis Highway, Suite 1204, Arlington, VA 22202-4302. Respondents should be aware that notwithstanding any other provision of law, no person shall be subject to any penalty for failing to comply with a collection of information if it does not display a currently valid OMB control number. PLEASE DO NOT RETURN YOUR FORM TO THE ABOVE ADDRESS. REPORT DATE (DD-MM-YYYY) ABSTRACTPurpose: Investigate the delivery of camptothecin in the presence of vitamin D3 with triblock copolymer-derived nanospheres that will increase the solubility of both of the drugs and provide protection to the camptothecin's lactone ring, resulting in its increased bioavailability to breast cancer cells. To date we have done the evaluation of two nanosphere formulations containing short alkyl pendent chain (DTB-SA/5K, Butyl) and/or benzyl ring (DTBn-SA/5K) Drug-binding efficiency of these nanospheres was evaluated for a constant quantity of the nanospheres with varying concentrations of the CPT and/or VD3. HPLC methods were developed and validated for quantitative determination of CPT and VD3 in the copolymer systems. To elucidate the synergistic effect of vitamin D3 on increasing the binding efficiency of CPT, different CPT to VD3 feed ratio were investigated. Results: The binding efficiency of VD3 in the presence of CPT. VD3 binding efficiency is not affected by the presence of the camptothecin, but is strongly affected by the nanospheres composition. Work was delayed by contract difficulties at Rutgers, but is now underway. SUBJECT TERMSNo subject terms were provided. I would like to bring to your attention that although this research project was awarded in August 2006 the actual award document was not issued until after April 2007. As a consequence, the actual research has begun just 3 month ago. We also applied for a one-year no-cost extension of funding that was accepted only on August 13, 2007. Thus, the below report is a summary of preliminary data obtained within 3.5 month of a research work. Introduction BackgroundSelf-assembling nanospheres offer a promising route to the delivery of pharmaceuticals that have poor bioavailability by improving the drugs' stability, circulation times in the body, and permeability through cell membranes, while reducing their toxicities.(1) Many drugs, including anti-tumor agents, anti-depressants and statins, are lipophilic and therefore require a solubilization process to enable their parenteral delivery. (2) Of the many alternative approac...

show abstract

Section: Introduction Backgroundmentioning

confidence: 83%

Section: Copolymer Syntheses and Nanosphere Formulationmentioning

confidence: 99%

Section: Introduction Backgroundmentioning

confidence: 99%

Section: Introduction Backgroundmentioning

confidence: 99%

See 2 more Smart Citations

Nanospheric Chemotherapeutic and Chemoprotective Agents

Sheihet¹

2008

Self Cite

View full text Add to dashboard Cite

show abstract

“…These comprise among others: small size, the ability to carry a wide variety of chemotherapeutic agents with sufficient drug space to meet the desired amount of biologically active drugs, the ability to release the drug at a predictable rate, biocompatibility, minimal antigenic properties, biodegradability , minimized toxicity of the breakdown products [6]. Liposomes, polysaccharides, nanocrystals, dendrimers, and polymeric, inorganic and modified nanoparticles meet all of these conditions [7][8][9][10][11][12][13][14][15][16]. Magnetic nanoparticles could be potentially used for drug delivery, as they can be easily handled by an external magnetic field and are preferentially taken up by the target tissue.…”

Section: Introductionmentioning

confidence: 99%

Synthesis and characterization of new functionalized polymer-Fe3O4 nanocomposite particles

Bukowska¹,

Bukowski²,

Hus³

et al. 2017

Express Polym. Lett.

View full text Add to dashboard Cite

Abstract. In this study, Fe 3 O 4 nanoparticles (NPs) were functionalized with copolymer or terpolymer bearing glycidyl methacrylate (GMA) moieties making them suitable for potential applications as drug delivery systems (DDS). For this purpose, the surface of magnetic nanoparticles was first coated with 3-(trimethoxysilyl) propyl methacrylate (MPS) by a silanization reaction to introduce reactive methacrylate groups onto the surface. Subsequently, monomers were grafted onto the surface of modified-MPS particles via two polymerization methods: seed emulsion (GMA, divinylbenzene, DVB, and styrene, S) and distillation -precipitation (GMA and DVB). The obtained nanocomposite particles were characterized by FTIR (Fourier transform infrared spectroscopy), DR UV-Vis (diffuse reflectance ultraviolet -visible spectroscopy), TEM (transmission electron microscopy) combined with EDS (energy dispersive X-ray spectroscopy) analysis and DLS (dynamic light scattering). FTIR spectroscopy showed that indeed a polymer -Fe 3 O 4 @MPS composite was obtained. TEM and EDS analysis showed that the seed emulsion method resulted in nanosized, 100 nm Fe 3 O 4 @MPS core/polymer shell NPs, forming long chains. On the contrary, the distillation -precipitation method caused the formation of an inverted structure, i.e. polymer core coated by a Fe 3 O 4 @MPS shell, which exhibited a very coarse size distribution varying from several hundreds to over 2 µm.

show abstract

Opportunities for biomaterials to address the challenges of COVID‐19

Chakhalian

Shultz

Miles

et al. 2020

J Biomedical Materials Res

View full text Add to dashboard Cite

The coronavirus disease 2019 (COVID‐19) pandemic has revealed major shortcomings in our ability to mitigate transmission of infectious viral disease and provide treatment to patients, resulting in a public health crisis. Within months of the first reported case in China, the virus has spread worldwide at an unprecedented rate. COVID‐19 illustrates that the biomaterials community was engaged in significant research efforts against bacteria and fungi with relatively little effort devoted to viruses. Accordingly, biomaterials scientists and engineers will have to participate in multidisciplinary antiviral research over the coming years. Although tissue engineering and regenerative medicine have historically dominated the field of biomaterials, current research holds promise for providing transformative solutions to viral outbreaks. To facilitate collaboration, it is imperative to establish a mutual language and adequate understanding between clinicians, industry partners, and research scientists. In this article, clinical perspectives are shared to clearly define emerging healthcare needs that can be met by biomaterials solutions. Strategies and opportunities for novel biomaterials intervention spanning diagnostics, treatment strategies, vaccines, and virus‐deactivating surface coatings are discussed. Ultimately this review serves as a call for the biomaterials community to become a leading contributor to the prevention and management of the current and future viral outbreaks.

show abstract

Effect of Tyrosine-Derived Triblock Copolymer Compositions on Nanosphere Self-Assembly and Drug Delivery

Cited by 66 publications

References 35 publications

Nanospheric Chemotherapeutic and Chemoprotective Agents

Nanospheric Chemotherapeutic and Chemoprotective Agents

Synthesis and characterization of new functionalized polymer-Fe3O4 nanocomposite particles

Opportunities for biomaterials to address the challenges of COVID‐19

Contact Info

Product

Resources

About