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'Pro-choice Community' Should Find New 'Way Of Talking About Reproductive Freedom,' Opinion Piece Says
"Most of the push-back" from antiabortion-rights advocates to a recent e-mail message from author Judy Blume on behalf of Planned Parenthood -- which asked mailing list subscribers for donations -- was generated by an article in the antiabortion-rights publication LifeNews, columnist Meghan Daum writes in a Los Angeles Times opinion piece. The article put a "heavy, misrepresentative spin" on Blume"s message, which urged donors to "do all [they] can to support" the increasing number of women turning to Planned Parenthood centers for health care during the economic downturn.The LifeNews article said, "Blume notes how more women are seeking abortions from Planned Parenthood because of the difficult economy, and she urges readers of the e-mail to use that as a reason to support the abortion business." According to Daum, "this is just the kind of thing that makes abortion-rights advocates apoplectic," noting that abortion-rights advocates "fired-back" in the "blogosphere ... imparting the statistic about abortion making up only 3% of Planned Parenthood"s services and pointing out that many of the women being yelled at by picketers in clinic parking lots aren"t even pregnant but, rather, trying to avoid getting pregnant." Daum continues that the organization, much like Blume, "occupies a clear position on the post-Roe cultural map," adding, "Generally speaking, if you"re on board with abortion rights, you"re on board with Planned Parenthood." In addition, if you are against abortion rights, the "organization is the headquarters of Godlessness," she adds. Daum writes that it is not difficult to see why Planned Parenthood enlisted Blume -- an "icon of 1970s-era feminism and its efforts on behalf of sex education and women"s health" -- because she conjures "nostalgia for the early days of the fight that makes pro-choicers want to keep fighting today."Daum writes that as she watched this "saga unfold in [her] inbox," she was "struck by a troubling question. Even though Blume may not be associated with abortion in and of itself … is there something about her persona that signals a lack of dispassion about its ramifications? Is she reminding people of a time when, in the relief of Roe being decided, there was a cultural perception that abortion was a simple procedure that needn"t come with attendant emotional baggage?"Daum adds that there is "no denying that the language and overall tone around abortion has changed. Despite what many pro-life groups seem to think, most abortion-rights advocates prefer "safe, legal and rare" to "no big deal."" According to Daum, President Obama, "pro-choice though he is, is hardly strident -- and even a little evasive -- on the issue." She adds that Obama favors language about reducing the need for abortions and "finding common ground with the other side." Daum notes that the pop cultural arena "has become downright allergic to the issue" of abortion, with a recent movie coining the term "shmashmortion" because the characters "can"t even get the word out." Daum adds that although Blume "was undoubtedly effective" at bringing in funding for Planned Parenthood, perhaps what might have been "even more radical is if the pro-choice community could find a way of talking about reproductive freedom that neither reverts to the perceived casualness of the 1970s nor panders to the "shmashmortion" dialect of today. "Safe, legal and rare" comes close. But "safe, legal, rare and a big deal" might be even better" (Daum, Los Angeles Times, 5/14).

Is There Any Association Between COX2 And Colon Cancer?
Non-steroidal anti-inflammatory drugs (NSAIDs), which are known to reduce the risk of colon cancer, act directly on cyclooxygenase-2 (COX2) and reduce its activity. Population studies have found an association of inherited variations in the COX2 gene with colon cancer risk, but others were unable to replicate this finding. Similarly, variations in the uridine diphosphate glucuronosyltransferase 1A6 (UGT1A6) gene, which is also known to be key in the metabolism of NSAIDs, have been shown to modify the effect of NSAIDs on developing colon polyps, a precursor of colon cancer, but these modifications of NSAID effects have not been observed in risk of colon cancer.
News of the day
Response Genetics To Present New Data On Lung Cancer Supporting The Use Of Gene Expression To Help Personalize Cancer Therapy Selection
Response Genetics Inc. (Nasdaq: RGDX), a company focused on the development and sale of molecular diagnostic tests for cancer, will announce the results of separate analyses of KRAS gene mutations and TS and RRM1 gene expression in non-small cell lung cancer (NSCLC) during the 13th World Conference on Lung Cancer, which will be held July 31 to August 4. Results will provide insights into which patient subtypes are most likely to benefit from the commonly prescribed chemotherapies pemetrexed and gemcitabine.
Diagnostics

Could Science Use The Common Cold To Cure Cystic Fibrosis?

In 1989 scientists identified the gene mutation that causes cystic fibrosis (CF), which led to the hope that CF lung disease could be "cured" using gene therapy. The premise of gene therapy is that modified viruses or other gene-based systems could be used to deliver a corrected version of a gene into affected tissues. However, the projected cure has been hampered by the natural ability of the lung to limit the introduction of foreign genes into its cells. Now, University of North Carolina at Chapel Hill School of Medicine scientists have found what may be the most efficient way to deliver a corrected gene to lung cells derived from CF patients, renewing hope that gene therapy for CF lung disease could be a successful future treatment. While Cystic Fibrosis is a multiple organ disease, it most devastatingly affects the lung. In people with CF the airways are clogged with mucus that is dehydrated and thicker than normal. The inability to clear mucus from the lung increases the susceptibility of CF patients to lung infections, which results in lung damage. Over the last two decades scientists have developed a variety of viral and non-viral vector systems suitable for delivering a corrected CF gene back into lung cells grown in the laboratory. Several of these vectors systems have been tested in human clinical trials. However, the efficiency of gene delivery achieved in the laboratory has not borne out in the clinical studies, suggesting that the cell models used in the laboratory do not represent the status of the cells in patients" lungs. Scientists have since developed laboratory models of human lung cells derived from CF patients that recapitulate the architecture and function of the cells present in the human lung. Studies using such cell models have revealed that previously used vector systems cannot deliver the corrected CF gene to enough lung cells to be of clinical benefit to CF patients. In this new study reported today in PLoS Biology, UNC scientists took a different approach and used parainfluenza virus, a virus known to infect human lung cells and to cause common colds. The UNC scientists engineered this virus to contain the corrected CF gene and found that it could deliver this gene to 60-70% of lung cells although only 25% of cells needed to be targeted to restore normal function back to the tissue model. "This is the first demonstration in which we"ve been able to execute delivery in an efficient manner to a tissue that resembles what is present in the lung," said Ray Pickles, Ph.D., associate professor of Microbiology and Immunology at the Cystic Fibrosis Research and Treatment Center and the Department of Microbiology and Immunology. "When you consider that in past gene therapy clinical trials, the targeting efficiency has been somewhere around 0.1 percent of cells at best, you can see this is a giant leap forward." "We discovered that if you take a virus that has evolved to infect the human airways, and you engineer a normal CF gene into it, you can use this virus to correct hallmark CF features in the model system that we used," he said. For instance, the experiment restored the cells" ability to hydrate and transport mucus secretions making the CF cells function essentially like normal cells. Now the researchers must work to ensure the safety of the delivery system. In a pleasant surprise, simply adding the CF gene to the virus significantly attenuated it, potentially reducing its ability to cause an inflammatory reaction. But the scientists may need to alter the virus further. "We haven"t generated a vector that we can go out and give to patients right now," Pickles said, "but we are slowly but surely moving forward towards this goal" Pickles says. "It is going to require a long term commitment from the CF gene therapy field that has achieved so much this far and it"s only a matter of time until we understand how to do this reproducibly and safely". Funding: This work was funded by the National Institutes of Health (NIH) and Cystic Fibrosis Foundation (CFF) grants NIH R01 HL77844 (RP), NIH P01 HL051818 (RP); NIH Molecular Therapy Core Center P30 DK065988 (RB, SG, RP); CFF ZHAN03I0 (LZ), GABRIE04G1 (SG) and GABRIE05P0 (SG); and the NIAID Intramural Research Program (MS, LV, PC). The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript. Competing interests statement: The authors declare that no competing interests exist. Citation: "CFTR Delivery to 25% of Surface Epithelial Cells Restores Normal Rates of Mucus Transport to Human Cystic Fibrosis Airway Epithelium." Zhang L, Button B, Gabriel SE, Burkett S, Yan Y, et al. (2009) PLoS Biol 7(7): e1000155.doi:10.1371/journal.pbio.1000155 PLoS Biology


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