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ImmunoVaccine Technologies Partners With FIT Biotech To Advance A Therapeutic HIV Vaccine
ImmunoVaccine Technologies Inc. (IVT), a Canadian vaccine development
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California Govenor Outlines Cuts To Address State's Budget Deficit Problems
California Gov. Arnold Schwarzenegger (R) outlined two budget proposals to address the state"s budget problems, and both plans would affect health care, the Los Angeles Times reports. The first proposal addresses the situation if California voters approve a set of special ballot measures intended to provide funds for fiscal year 2009-2010. The state would still face a $15.4 billion budget deficit even if voters approve the measures, and the second proposal addresses that scenario (Rothfeld, Los Angeles Times, 5/15). The governor proposed $750 million in cuts to Medi-Cal, the state"s Medicaid program, that would reduce eligibility and provider rates. The state would need to seek a federal waiver to implement the cuts. The governor also proposed eliminating eligibility for non-emergency Medi-Cal benefits for documented immigrants (Colliver, San Francisco Chronicle, 5/15). Spending for centers that provide services to people with developmental disabilities would be cut by $234 million (Zapler, San Jose Mercury News, 5/14).If voters do not approve three ballot measures, Schwarzenegger outlined $800 million in additional cuts to health and human services programs, including a proposal to eliminate Healthy Families coverage for about 225,000 children. Healthy Families is California"s CHIP (Yi et al., San Francisco Chronicle, 5/15).
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Teens' Risk Factors For Heart Disease, Diabetes Reduced By Lap Band Weight Loss Surgery
In teenagers, laparoscopic gastric banding surgery for treatment of extreme obesity can significantly improve and even reverse the metabolic syndrome, a new study found. The results were presented at The Endocrine Society"s 91st Annual Meeting in Washington, D.C.
Oncology

Derivative Of Red Sea Coral Products Fight Skin

Scientists at South Dakota State University are exploring the mechanisms by which a substance derived ultimately from Red Sea coral could help treat skin cancer. The study built on earlier work by SDSU distinguished professor Chandradhar Dwivedi"s lab looking at the chemopreventive effects of sarcophine-diol, made from a substance called sarcophine that can be isolated from soft coral found in the Red Sea. The new study carried the work beyond looking at sarcophine-diol"s possible use in prevention of skin cancer to consider its potential as a tool in therapies to actually treat skin cancer. "We are finding that sarcophine-diol could be used both for chemoprevention and as a chemotherapeutic agent," Dwivedi said. Specifically, the new SDSU research explored sarcophine-diol"s potential to inhibit cell growth of cancers, and also its potential to induce orderly, programmed cell death of skin cancer cells. The scientists published their research findings in March 2009 in the academic journal Translational Oncology. Dwivedi, head of SDSU"s Department of Pharmaceutical Sciences, directed the study by departmental graduate student researcher Xiaoying Zhang. Other researchers involved included Ajay Bommareddy of the University of Pittsburgh Cancer Institute, a former graduate student in Dwivedi"s laboratory; SDSU graduate student Wei Chen of the Department of Pharmaceutical Sciences; Sherief Khalifa of Misr International University in Cairo, Egypt; assistant professor Radhey Kaushik, who has a joint appointment in SDSU"s Department of Veterinary Sciences and the Department of Biology and Microbiology; and associate professor Hesham Fahmy of the SDSU Department of Pharmaceutical Sciences. SDSU researchers found that treating human skin cancer cells with different concentrations of sarcophine-diol for different lengths of time reduced the viability of cancer cells in each case. Related work showed that sarcophine-diol also inhibited the proliferation or uncontrolled growth of cancer cells. The SDSU study also showed that sarcophine-diol induced apoptosis, or programmed cell death, in cancer cells. The extent of apoptosis observed in different treatments in the study was correlated to the level of sarcophine-diol used, Dwivedi said. However, sarcophine-diol did not induce what scientists call necrosis, or the premature death of healthy cells. Dwivedi said that is an important finding because it suggests sarcophine-diol could be used in treatments that specifically target cancer cells without damaging nearby healthy cells. The SDSU experiment also looked at whether sarcophine-diol treatments could increase what is called DNA fragmentation, considered a biochemical hallmark of apoptosis an indication that the cell is committed to die, in other words. At lower concentrations, sarcophine-diol didn"t significantly induce DNA fragmentation in skin tumor cells, but higher levels of sarcophine-diol did. Finally, the SDSU study found that treatments with higher concentrations of sarcophine-diol induced higher level of so-called "executioner" proteins that have a role in apoptosis, or programmed cell death compared to a control group. Importantly, the SDSU research found that sarcophine-diol did not significantly increase the level of the "executioner" proteins in normal cells. Sarcophine-diol had some effect on viability of healthy cells, but the results suggest sarcophine-diol is considerably more toxic to skin tumor cells than to healthy cells. "Further investigations of sarcophine-diol in experimental models and in cell culture studies are needed to explore its mechanisms of action," Dwivedi said. "Sarcophine-diol has excellent potential to be a potent chemotherapeutic agent that can be further investigated for use against nonmelanoma skin cancer development." South Dakota State University


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