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From: donpat	7/15/2011 1:12:28 PM
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Polymeric nanoparticles attack head and neck cancer [Encouraging use of a polymer targeted nanoparticle!] July 15, 2011 Head and neck cancer, the sixth most common cancer in the world, has remained one of the more difficult malignancies to treat, and even when treatment is successful, patients suffer severely from the available therapies. Now, researchers at the University of Michigan have developed a tumor-targeted nanoparticle that delivers high doses of anticancer agents directly to head and neck tumors. Tests in animals have shown that this novel formulation increases survival while triggering fewer side effects. Reporting its work in the Journal of Oral and Maxillofacial Surgery [ sciencedirect.com ], a team led by James R. Baker, Jr., created a spherical polymeric nanoparticle known as a dendrimer to deliver the drug methotrexate to head and neck tumors. To target the nanoparticle to those tumors, the investigators decorated the nanoparticle's surface with folic acid. Many tumors, but few healthy cells, produce excessive amounts of a folic acid receptor on their surfaces. Dr. Baker and his colleagues pioneered the use of dendrimers as targeted drug-delivery vehicles with funding from the National Cancer Institute's Alliance for Nanotechnology in Cancer. The researchers tested their dendrimer-based formulation in three different groups of mice. The control group had tumors grown from human head and neck tumors that did not produce the folic acid receptor. The two experimental groups had tumors grown from human head and neck tumors that expressed moderate and high levels of the folic acid receptor. Mice receiving the equivalent of three times the normally lethal dose of methotrexate, delivered on the dendrimer nanoparticle experienced none of the weight loss normally associated with methotrexate therapy. More importantly, dendrimer-delivered therapy produced marked gains in therapeutic response even in the mice whose tumors produced only moderate levels of folic acid receptor. This work, which is detailed in a paper titled, "Targeted Dendrimer Chemotherapy in an Animal Model for Head and Neck Squamous Cell Carcinoma," was supported in part by the NCI Alliance for Nanotechnology in Cancer, a comprehensive initiative designed to accelerate the application of nanotechnology to the prevention, diagnosis, and treatment of cancer. More information: doi:10.1016/j.joms.2010.12.041 dx.doi.org Provided by National Cancer Institute physorg.com

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From: donpat	7/15/2011 1:28:28 PM
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Nanoparticles working in harmony [The double whammy approach!] July 15, 2011 For decades, researchers have been working to develop nanoparticles that deliver cancer drugs directly to tumors, minimizing the toxic side effects of chemotherapy. However, even with the best of these nanoparticles, only about one percent of the drug typically reaches its intended target. Now, a team of researchers from MIT, the Sanford-Burnham Medical Research Institute, and the University of California at San Diego (UCSD) has designed a new type of delivery system in which a first wave of nanoparticles hones in on the tumor, then calls in a much larger second wave that dispenses the cancer drug. This communication between nanoparticles, enabled by the body's own biochemistry, boosted drug delivery to tumors by more than 40-fold in a mouse study. This new strategy could enhance the effectiveness of many drugs for cancer and other diseases, say the investigators. This multi-institutional team was led by MIT's Sangeeta Bhatia, who is also a member of the MIT-Harvard Center of Cancer Nanotechnology Excellence, part of the National Cancer Institute's Alliance for Nanotechnology in Cancer. This research is described in a paper published in the journal Nature Materials. Michael Sailor of UCSD and Erkki Ruoslahti of the Sanford Burnham Institute, both senior members of the Alliance for Nanotechnology in Cancer, also participated in this study. Dr. Bhatia and her collaborators drew their inspiration from complex biological systems in which many components work together to achieve a common goal. For example, the immune system works through highly orchestrated cooperation between many different types of cells. In this case, the team's approach is based on the blood coagulation cascade — a series of reactions that starts when the body detects injury to a blood vessel. Proteins in the blood known as clotting factors interact in a complex chain of steps to form strands of fibrin, which help seal the injury site and prevent blood loss. To harness the communication power of that cascade, the researchers needed two types of nanoparticles — signaling and receiving. Signaling particles, which make up the first wave, exit the bloodstream and arrive at the tumor site via tiny holes in the leaky blood vessels that typically surround tumors (this is the same way that most targeted nanoparticles reach their destination). Once at the tumor, this first wave of particles provokes the body into believing that an injury has occurred at a tumor site, either by emitting heat or by binding to a protein that sets off the coagulation cascade. Receiving particles are coated with proteins that bind to fibrin, which attracts them to the site of blood clotting. Those second-wave particles also carry a drug payload, which they release once they reach the tumor. In a study of mice, one system of communicating nanoparticle systems delivered 40 times more of the widely used anticancer agent doxorubicin than did non-communicating nanoparticles. The researchers also saw a correspondingly amplified therapeutic effect on the tumors of mice treated with communicating nanoparticles. To pave the path for potential clinical trials and regulatory approval, Dr. Bhatia and her colleagues are now exploring ways to replace components of these cooperative nanosystems with drugs already being tested in patients. For example, drugs that induce coagulation at tumor sites could replace the signaling particles tested in this study. This work, which is detailed in a paper titled, "Nanoparticles that communicate in vivo to amplify tumour targeting," was supported in part by the NCI Alliance for Nanotechnology in Cancer, a comprehensive initiative designed to accelerate the application of nanotechnology to the prevention, diagnosis, and treatment of cancer. Nanoparticles that communicate in vivo to amplify tumour targeting More information: doi:10.1038/nmat3049 dx.doi.org Provided by National Cancer Institute physorg.com

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From: donpat	7/15/2011 1:35:30 PM
	of 2500

Nanoparticles disguised as red blood cells deliver cancer-fighting drugs Posted: Jul 15th, 2011 (Nanowerk News) Researchers at the University of California, San Diego have developed a novel method of disguising nanoparticles as red blood cells, enabling the resulting nanoparticles to evade the body's immune system and deliver cancer-fighting drugs straight to a tumor. The method involves collecting the membrane from a red blood cell and wrapping it like a powerful camouflaging cloak around a biodegradable polymer nanoparticle stuffed with a cocktail of small molecule drugs. "This is the first work that combines the natural cell membrane with a synthetic nanoparticle for drug delivery applications," said Dr. Liangfang Zhang. "This nanoparticle platform will have little risk of immune response." Zhang and his collaborators published the results of their studies in the Proceedings of the National Academy of Sciences ("Erythrocyte membrane-camouflaged polymeric nanoparticles as a biomimetic delivery platform" [ dx.doi.org ]). Researchers have been working for years on developing drug delivery systems that mimic the body's natural behavior for more effective drug delivery. That means creating vehicles such as nanoparticles that can live and circulate in the body for extended periods without being attacked by the immune system. Red blood cells live in the body for up to 180 days and, as such, are nature's long-circulation delivery vehicle. Stealth nanoparticles are already used successfully in clinical cancer treatment to deliver chemotherapy drugs. They are coated in a synthetic material such as polyethylene glycol that creates a protection layer to suppress the immune system so that the nanoparticle has time to deliver its payload. Zhang said today's stealth nanoparticle drug delivery vehicles can circulate in the body for hours compared to the minutes a nanoparticle might survive without this special coating. But in Zhang's study, nanoparticles coated in the membranes of red blood cells circulated in the bodies of lab mice for nearly two days. Using the body's own red blood cells marks a significant shift in focus and a major breakthrough in the field of personalized drug delivery research. Trying to mimic the most important properties of a red blood cell in a synthetic coating requires an in-depth biological understanding of how all the proteins and lipids function on the surface of a cell. Instead, Zhang's team is just taking the whole surface membrane from an actual red blood cell. "We approached this problem from an engineering point of view and bypassed all of this fundamental biology," said Zhang. "If the red blood cell has such a feature and we know that it has something to do with the membrane—although we don't fully understand exactly what is going on at the protein level—we just take the whole membrane. You put the cloak on the nanoparticle, and the nanoparticle looks like a red blood cell." Using nanoparticles to deliver drugs also reduces the hours it takes to slowly drip chemotherapy drug solutions through an intravenous line to just a few minutes for a single injection of nanoparticle drugs. This significantly improves the patient's experience and compliance with the therapeutic plan. This particular breakthrough could lead to more personalized drug delivery wherein a small sample of a patient's own blood could produce enough of the essential membrane to disguise the nanoparticle, reducing the risk of immune response to almost nothing. Dr. Zhang said one of the next steps is to develop an approach for large-scale manufacturing of these biomimetic nanoparticles for clinical use, a project already underway. The investigators will also add a targeting molecule to the membrane that will enable the particle to seek and bind to cancer cells, and integrate the team's technology for loading drugs into the nanoparticle core so that multiple drugs can be delivered at the same time. Source: National Cancer Institute nanowerk.com

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From: donpat	7/15/2011 1:56:37 PM
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Harry Potter Director May Bring Stephen King Virus Novel to the Big Screen Jennifer Mishler @ 11:53 am Harry Potter director David Yates might soon be working on another book-turned-movie project. This time, it could be Stephen King‘s end of the world horror novel The Stand. Yates had directed four of the Harry Potter movies. The final film, Harry Potter and the Deathly Hallows: Part 2 is getting rave reviews. Now, Warner Bros. reportedly wants to continue working with Yates to turn The Stand into three movies. According to Cinema Blend, the director is very interested too. “Yates appears keen to tackle the story, reportedly flying out to meet with Warner executives and streaming through a copy of King’s story about survivors of a planet-cleansing virus who unite in a fight against the ultimate evil.” Stephen King is considered by many to be the “master of horror,” and several of his novels have been turned into successful movies including The Shawshank Redemption and The Green Mile. The Stand was previously made into a miniseries as well as a series of comic books from Marvel Comics. ecorazzi.com

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From: donpat	7/16/2011 10:54:35 AM
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Entry prohibited for AIDS viruses: Peptide triazole inhibitors disrupt cell-free HIV-1/Drexel U/Chaiken July 8, 2011 (PhysOrg.com) -- The initial entry of HIV-1 into host cells remains a compelling yet elusive target for the development of agents to prevent infection, a critical need in the fight against the global AIDS epidemic. A collaborative research effort led by Irwin Chaiken at Drexel University and Drexel University College of Medicine (Philadelphia, PA, USA) has demonstrated that modified peptide triazole inhibitors which specifically target the HIV-1 envelope (Env) protein gp120 can physically disrupt virus particles in the absence of host cells, and the results are reported in ChemMedChem. The Drexel team found that under conditions similar to those at which a newly designed peptide triazole (KR13) inhibits infection of host cells by an HIV-1 pseudovirus, it also causes virus rupture and release of an internal HIV-1 protein called gag p24 when incubated with virus alone. Both inhibition of cell infection and p24 release are enhanced substantially by the multivalent display of KR13 on gold nanoparticles. The novel antagonist design and reported characterization data could lead to the creation of a virucide to suppress initial HIV-1 infection, viremia in infected individuals, and the spread of infection between individuals. Such agents could be used for HIV-1 microbicides and therapeutics. These results also suggest that ligand-specific pathogen rupture may be possible for other viruses that contain metastable prefusion surface protein complexes, such as influenza, Ebola, and Dengue. More information: Irwin Chaiken, Cell-Free HIV-1 Virucidal Action by Modified Peptide Triazole Inhibitors of Env gp120, ChemMedChem 2011, 6, No. 8, wiley-vch.de physorg.com Virucides: The goal of this project is to test the hypothesis that a mature HIV particle is metastable against membrane poration due to a combination of virus spike protein metastability and high internal Laplace pressure. We seek molecular constructions that will bind simultaneously to virus spike and membrane, and disrupt membrane integrity sufficiently to cause irreversible leakage of viral contents, rendering the virus noninfectious. is.gd

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