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QRxPharma Initiates Comparative Phase 2 Proof-of-Concept Study For MoxDuo(TM) IV Pain Therapy
QRxPharma Limited (Pink Sheets: QRXPY; ASX: QRX) announced the initiation of a Phase 2 comparative proof-of-concept study to evaluate the efficacy and safety of MoxDuo(TM) IV (intravenous morphine and oxycodone) versus IV morphine alone for the treatment of moderate to severe post-operative pain in patients following hip replacement surgery. Data from this study will serve as a significant predictor of MoxDuo(TM) IV"s clinical benefits and provide guidance for the design of further clinical trials leading to submission of an NDA to the US Food and Drug Administration (FDA) within the next three years.

HUD To Distribute $310M In Housing Assistance Grants For People Living With HIV/AIDS
The U.S. Department of Housing and Urban Development (HUD) on Wednesday announced that it will provide several housing assistance grants to help low-income families living with HIV/AIDS, the Boston Globe reports (7/23). "A record $310 million will assist 58,000 U.S. households annually, officials said," KITV.com reports. The grants were distributed based on the number of AIDS cases reported nationwide. The Gregory House Programs of Honolulu, a nonprofit that provides housing assistance, substance use and other services, will receive $1.3 million (KITV.com, 7/22). The Frannie Peabody Center in Portland, Maine, will receive $1.3 million; the city of Portland will receive $1.4; New Hampshire will receive over $716,000; and the Burlington Housing Authority in Vermont will receive over $392,000, the Globe reports (7/23).
News of the day
With Health Reform Uncertain, Maryland Hospitals Consolidate
"Facing difficult economic times and the uncertainties of national health care reform, some Maryland hospitals are choosing to be swallowed up by larger medical systems, with an unusual string of mergers over the past 16 months and more likely on the way," The Baltimore Sun reports. The consolidations could offer benefits to all those involved. Small hospitals gain "the hope of safe harbor from whatever financial storms are on the horizon, hospital chains "get footholds in new areas, where they can build market share and increase the number of patients they serve," and patients may "gain access to large networks of top-notch doctors, even if the patients live many miles from a major medical institution."
Medical Devices

No Evidence That WHO-recommended Treatment For Insecticide Poisoning Improves Survival

A study published this week in the open access journal PLoS Medicine finds no evidence to suggest that a controversial antidote recommended by the World Health Organisation (WHO) to treat patients poisoned with highly toxic insecticides improves their chance of survival. The results may even add weight to existing concerns about pralidoxime, the treatment recommended by the WHO, by suggesting that it could be harmful in patients who have deliberately poisoned themselves with insecticides. Poisoning with organophosphorous pesticides - toxic chemicals commonly used in agriculture in developing countries is a global public health problem causing an estimated 200,000 deaths a year. Deliberate self-poisoning with pesticides is a common method of suicide in some countries - in Sri Lanka, more than 50% of fatal suicide attempts are a result of pesticide poisoning. Michael Eddleston, from the University of Edinburgh, and colleagues conducted a clinical trial to study the effects of WHO-recommended pralidoxime treatment in patients who had been admitted to two hospitals in Sri Lanka for insecticide self-poisoning. If ingested by humans the pesticides disrupt the communication between the brain and body, inhibiting the activity of a neurotransmitter called acetylcholine, which plays a crucial role in the central nervous system and the control of breathing. To treat organophosphate poisoning, the WHO recommends that in addition to atropine, an antidote that is known to reverse some but not all of the effects of the poisoning, a regimen of pralidoxime should be used to reactivate acetylcholine activity. As the authors of this study mention, few randomized clinical trials have been conducted into its use, meaning that there is a lack of evidence for its effectiveness, in particular relating to dosage. The researchers enrolled 235 patients at two Sri Lankan hospitals who had self-poisoned with organophosphate insecticides, determining how much, and which, pesticide each patient had been exposed to, and randomly allocating them to receive either the WHO-recommended regimen of pralidoxime or a salt water placebo. However, the trial was stopped early and did not reach its intended study size owing to discussions surrounding the results of another trial of pralidoxime therapy, carried out in India at the same timewhich led to a fall-off in recruitment of patients. In the Sri Lankan trial, published in PLoS Medicine, more patients in the pralidoxime arm died than in the placebo arm, despite the fact that pralidoxime was shown to aid acetylcholine activity. Whilst the difference in mortality between arms was not statistically significant, it is suggestive of a higher mortality rate resulting from pralidoxime treatment. Acknowledging the difficult situation that clinicians now face when deciding whether or not to administer pralidoxime to patients poisoned with organophosphorous pesticides, the authors conclude that there is no consistent clinical evidence for the use of pralidoxime in patients who have self-poisoned with organophosphorous pesticides. They argue that further trials are needed to explore the risks and benefits of oximes and dosing regimens. Funding: ME is a Wellcome Trust Career Development Fellow. This work was funded by grant 063560 from the Wellcome Trust"s Tropical Interest Group to ME. The South Asian Clinical Toxicology Research Collaboration is funded by a Wellcome Trust/National Health and Medical Research Council International Collaborative Research Grant 071669. The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript. Citation: " Pralidoxime in Acute Organophosphorus Insecticide Poisoning-A Randomised Controlled Trial." Eddleston M, Eyer P, Worek F, Juszczak E, Alder N, et al. (2009) PLoS Med 6(6): e1000104. doi:10.1371/journal.pmed.1000104 PLoS Medicine


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