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		<title>Approximately 16% of Worldwide Cancers Caused By Preventable Infections</title>
		<link>http://news.cancerconnect.com/approximately-16-of-worldwide-cancers-caused-by-preventable-infections/</link>
		<comments>http://news.cancerconnect.com/approximately-16-of-worldwide-cancers-caused-by-preventable-infections/#comments</comments>
		<pubDate>Thu, 17 May 2012 00:01:14 +0000</pubDate>
		<dc:creator>Cancerconnect</dc:creator>
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		<guid isPermaLink="false">http://news.cancerconnect.com/?p=59530</guid>
		<description><![CDATA[Two million cancer cases each year—or roughly 16 percent of cancers worldwide—are the result of preventable and treatable infections such as human papillomavirus (HPV) and Hepatitis C (HCV), according to the results of a study published in The Lancet Oncology.[1] Infections with certain viruses, bacteria, and parasites have been identified as strong risk factors for [...]]]></description>
			<content:encoded><![CDATA[<p>Two million cancer cases each year—or roughly 16 percent of cancers worldwide—are the result of preventable and treatable infections such as human papillomavirus (HPV) and Hepatitis C (HCV), according to the results of a study published in <em>The Lancet Oncology</em>.<a title="" href="#_edn1">[1]</a></p>
<p>Infections with certain viruses, bacteria, and parasites have been identified as strong risk factors for specific cancers. To examine the link between infections and cancer, researchers performed a systematic analysis of the proportion of cancer cases attributable to infection in 2008. They used data on cancer incidence from the GLOBOCAN project along with epidemiological data regarding the causal effects of infection on cancer. The data included information on 27 types of cancer from 182 countries.</p>
<p>They found that of the 12.7 million new cancer cases that occurred worldwide in 2008, 16 percent—or roughly two million—were attributable to infections. The rate of infection-related cancer was about three times higher in developing countries. For example, 3.3 percent of cancers in Australia and New Zealand were infection related, whereas 32.7 percent of cancers in sub-Saharan Africa were attributable to infections. The four main infections associated with cancer were human papillomavirus, hepatitis C, hepatitis B, and Helicobacter pylori. These infections were responsible for approximately 1.9 million cancer cases in 2008, mainly gastric, liver, and cervical cancers.</p>
<p>Cervical cancer accounted for about half of the infection-related cancers in women. Liver and gastric cancers accounted for more than 80 percent of the infection-related cancers in men.  About 30 percent of infection-related cancers occurred in people younger than 50 years. It’s important to note that it takes decades of chronic infection before an infection progresses to cancer.</p>
<p>Based on the statistics, the researchers noted that approximately two million cancer cases each year might be preventable with better public health methods for preventing infection. In an accompanying editorial, Dr. Goodarz Danaei, an assistant professor of global health at Harvard School of Public Medicine in Boston, noted that vaccines for HPV and hepatitis B are effective and that increasing their availability should be a priority for higher risk countries.<a title="" href="#_edn2">[2]</a> He suggests that increasing vaccine coverage could reduce the global burden of cancer.</p>
<p><strong>References:</strong></p>
<hr align="left" size="1" width="33%" />
<div>
<p><a title="" href="#_ednref1">[1]</a> de Martel C, Ferlay J, Franceschi S, et al. Global burden of cancers attributable to infections in 2008: a review and synthetic analysis. <em>The Lancet Oncology</em>. Published early online May 9, 2012. doi:10.1016/S1470-2045(12)70137-7</p>
</div>
<div>
<p><a title="" href="#_ednref2">[2]</a> Danaei G. Global burden of infection-related cancer revisited. <em>The Lancet Oncology</em>. Published early online May 9, 2012. doi:10.1016/S1470-2045(12)70176-6</p>
<p>&nbsp;</p>
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		<title>Men, Fertility, and Cancer</title>
		<link>http://news.cancerconnect.com/men-fertility-and-cancer/</link>
		<comments>http://news.cancerconnect.com/men-fertility-and-cancer/#comments</comments>
		<pubDate>Wed, 09 May 2012 00:01:02 +0000</pubDate>
		<dc:creator>Cancerconnect</dc:creator>
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		<guid isPermaLink="false">http://news.cancerconnect.com/?p=59454</guid>
		<description><![CDATA[Men who confront a cancer diagnosis before beginning or completing their families may have many questions about how cancer treatment will affect their ability to have children in the future. The good news is that an increasing amount of attention is being devoted to this topic, and there are steps that you may be able [...]]]></description>
			<content:encoded><![CDATA[<p>Men who confront a cancer diagnosis before beginning or completing their families may have many questions about how cancer treatment will affect their ability to have children in the future. The good news is that an increasing amount of attention is being devoted to this topic, and there are steps that you may be able to take to preserve your reproductive options. The best time to talk about this issue with your doctor is before cancer treatment begins.</p>
<p><strong>How does cancer treatment affect fertility in men?</strong></p>
<p><em>Chemotherapy:</em> Chemotherapy can temporarily—and in some cases, permanently—stop sperm production by the testes.<a title="" href="#_edn1">[1]</a> The extent to which chemotherapy affects sperm production depends on several factors, including the type and dose of chemotherapy.</p>
<p><em>Radiation:</em> Radiation to the abdomen or pelvis can also reduce or eliminate sperm production by the testes.</p>
<p><em>Surgery</em>: Surgery that involves the removal of both testicles (an option for some men with prostate cancer) eliminates sperm production, but other types of surgery can also affect a man’s fertility. Some types of pelvic surgery, for example, can change or eliminate ejaculation.</p>
<p><strong>Options for preserving fertility in men</strong></p>
<p>Although many men are able to conceive naturally after cancer treatment, others are not.</p>
<p>If possible, men should talk with their doctor about their future fertility before beginning cancer treatment. Some options for preserving fertility require that steps be taken before cancer treatment begins.</p>
<p>Sperm banking is the most well-established method of preserving fertility in men.<a title="" href="#_edn2">[2]</a> It involves the collection and storage of sperm, ideally before cancer treatment begins. The samples are kept frozen at a lab or sperm bank until they are needed. Sperm can be stored in this way for many years. After being thawed, the sperm can be used for intrauterine insemination (IUI) or in vitro fertilization (IVF). During IUI, sperm are placed directly into a woman’s uterus. During IVF, mature eggs are removed from a woman’s ovary and mixed with the sperm in the lab. Embryos that result from IVF can then be placed in a woman’s uterus or frozen for later use.</p>
<p>If a sample contains very few viable sperm (or if a man has already undergone cancer treatment and has a low sperm count), another approach may be used to fertilize an egg. Intracytoplasmic sperm injection (ICSI) requires only a small number of healthy sperm, along with mature eggs that have been collected from a woman’s ovary. A single sperm is injected directly into each egg. The embryos that develop can then be placed in a woman’s uterus or frozen for later use.</p>
<p>If it is not possible to collect sperm from ejaculate, it may in some cases be possible to collect sperm directly from the testicles. This approach is still investigational.</p>
<p>Finally, it may also be possible to modify some cancer treatments to minimize their effects on subsequent fertility. During radiation therapy, for example, it may be possible to shield the testes in order to preserve sperm production.</p>
<p><strong>Pregnancy after cancer</strong></p>
<p>In the event that your fertility is not affected by cancer treatment (or recovers quickly or unexpectedly), you and your partner should use birth control if you do not wish to have a child. If you are trying to conceive a child naturally, your doctor may advise you to wait for several months after treatment; this allows for the elimination of sperm that may have been damaged during treatment.</p>
<p>In general, the risk of birth defects in children born to cancer survivors appears to be similar to the risk in the general population.<a title="" href="#_edn3">[3]</a> If your cancer was due to a hereditary cancer syndrome, such as Lynch syndrome (hereditary nonpolyposis colorectal cancer), your children may inherit the gene mutation responsible for your family’s increased risk of cancer. Talking with a genetic counselor may be helpful.</p>
<p><strong>Other options for parenthood </strong></p>
<p>Not all men have the luxury of being able to explore their reproductive options before beginning cancer treatment, and not all men will find a fertility preservation option that meets their needs. But there are still ways to become a parent. Discussion of other routes to parenthood may be a painful topic for men who want to father a child but cannot. But as cancer survivors consider how best to build their families, methods such as adoption are important options.</p>
<p><em>Adoption:</em> Couples and individuals who wish to adopt have a range of options, including different types of domestic and international adoptions. You may wish to start by learning about the adoption laws in your state and by talking with other adoptive parents about the professionals and agencies they worked with. Before selecting an adoption agency, you may wish to talk with them about their attitudes toward placing a child with a cancer survivor. Many agencies will be receptive toward this, but it’s important to know before making a final decision.</p>
<p><em>Donor Sperm:</em> Donor sperm is readily available from sperm banks and can be used for either intrauterine insemination or in vitro fertilization.</p>
<p><strong>Individual decisions within a larger community</strong></p>
<p>The decisions that you make about building a family (or about coming to terms with not building a family) will be intensely personal, but know that you are part of a larger community of patients and healthcare providers who are grappling with these issues.  To think about future parenthood is to think about life after cancer. For many people with cancer, planning for the future may provide the motivation needed to get through treatment.</p>
<p><strong>More information? </strong></p>
<p>Discuss with others…. <a href="http://cancerconnect.com/groups/young-adults/topics/fertility-after-cancer-treatment">http://cancerconnect.com/groups/young-adults/topics/fertility-after-cancer-treatment</a></p>
<p>Fertile Hope (<a href="http://www.fertilehope.org/">www.fertilehope.org</a>) provides a range of fertility resources for people with cancer.</p>
<p><strong>References: </strong></p>
<div>
<p>&nbsp;</p>
<hr align="left" size="1" width="33%" />
<div>
<p><a title="" href="#_ednref1">[1]</a> Dohle. Male infertility in cancer patients: review of the literature. <em>International Journal of Urology</em>. 2010;17:327-331.</p>
</div>
<div>
<p><a title="" href="#_ednref2">[2]</a> Levine J, Canada A, Stern CJ. Fertility preservation in adolescents and young adults with cancer. <em>Journal of Clinical Oncology</em>. 2010;28:4831-4841.</p>
</div>
<div>
<p><a title="" href="#_ednref3">[3]</a> Knopman JM, Papadopoulos EB, Grifo JA, Fino ME, Noyes N. Surviving childhood cancer and reproductive-age malignancy: effects on fertility and future parenthood. <em>Lancet Oncology</em>. 2010;11:490-98.</p>
</div>
</div>
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		</item>
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		<title>Women, Fertility and Cancer</title>
		<link>http://news.cancerconnect.com/women-fertility-and-cancer-2/</link>
		<comments>http://news.cancerconnect.com/women-fertility-and-cancer-2/#comments</comments>
		<pubDate>Fri, 04 May 2012 00:01:01 +0000</pubDate>
		<dc:creator>Cancerconnect</dc:creator>
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		<guid isPermaLink="false">http://news.cancerconnect.com/?p=59452</guid>
		<description><![CDATA[Women who confront a cancer diagnosis before beginning or completing their families may have many questions about how cancer treatment will affect their ability to have children in the future. The good news is that an increasing amount of attention is being devoted to this topic, and there are steps that you may be able [...]]]></description>
			<content:encoded><![CDATA[<p>Women who confront a cancer diagnosis before beginning or completing their families may have many questions about how cancer treatment will affect their ability to have children in the future. The good news is that an increasing amount of attention is being devoted to this topic, and there are steps that you may be able to take to preserve your reproductive options. The best time to talk about these issues with your doctor is before cancer treatment begins.</p>
<p><strong>How does cancer treatment affect fertility in women?</strong></p>
<p><em>Chemotherapy:</em> Many chemotherapy drugs are toxic to the egg cells (oocytes) in the ovaries. If the number of remaining oocytes in the ovaries reaches a critically low point during treatment, women experience “acute ovarian failure.” This means that the ovaries stop functioning during or shortly after cancer treatment. If oocytes are lost during treatment but do not reach this critically low point, women are at risk for early menopause but may still be able to get pregnant for some time after treatment.</p>
<p><em>Radiation:</em> Radiation to the pelvis can also destroy oocytes. Radiation to the pelvis can also affect uterine growth and blood flow, particularly if received before puberty.<a title="" href="#_edn1">[1]</a> A poorly developed uterus may make a woman more likely to have a miscarriage, or more likely to have a preterm or low-birthweight infant.</p>
<p><em>Surgery</em>: Some cancers require surgical removal of the uterus, the ovaries, or both.</p>
<p>The effects of cancer treatment on fertility can vary substantially by age. Younger women, who have a larger pool of oocytes when they start cancer treatment, are more likely than older women to be able to get pregnant after treatment.<a title="" href="#_edn2">[2]</a></p>
<p><strong>Options for preserving fertility in women</strong></p>
<p>If possible, women should talk with their doctor about their future fertility before beginning cancer treatment. Some options for preserving fertility require that steps be taken before cancer treatment begins.</p>
<p>One of the most established approaches for preserving fertility among female cancer patients is embryo freezing.<a title="" href="#_edn3">[3]</a> Before starting cancer treatment, a woman would be given hormones to stimulate the development of eggs in her ovaries. Mature eggs would be removed and fertilized with the sperm of her husband, partner or a sperm donor. The embryos that result from these fertilized eggs would be frozen for later use.</p>
<p>Although embryo freezing is an established approach to helping women become pregnant after cancer, there are downsides. A woman may not currently have a male partner and may be unwilling to use an anonymous sperm donor. It’s also important to be aware that embryo freezing takes approximately two weeks after the start of a woman’s period. If a woman needs to begin cancer treatment immediately, she may not be able to go through this process. Finally, this approach is only an option for women of childbearing age; stimulating the ovaries to produce mature eggs is not an option for girls who develop cancer during childhood.</p>
<p>Several other options are still in the experimental phase. One approach being explored is the freezing of unfertilized eggs.3 Once again, the ovaries would be stimulated to produce mature eggs before cancer treatment begins. The eggs would then be frozen without being fertilized by sperm. Currently, freezing unfertilized eggs is less likely to result in pregnancy than freezing embryos, largely because unfertilized eggs are less likely than embryos to survive the process of freezing and thawing. Nevertheless, it may be an option for women who do not have a male partner at the time of their cancer diagnosis, and it avoids the difficult issue of what to do with unused embryos.</p>
<p>Another promising but still experimental approach is to freeze all or a part of an ovary before cancer treatment.<a title="" href="#_edn4">[4]</a> After treatment, the ovarian tissue is implanted either back in the woman’s pelvis or in another location (such as under her skin). If this process is successful, the ovarian tissue will begin producing eggs. A safety concern with this approach is the possibility of reintroducing cancer cells along with the ovarian tissue, and the tissue will need to be carefully screened for cancer before it is transplanted.4</p>
<p>Finally, it may also be possible to modify some cancer treatments to minimize their effects on subsequent fertility. For example, shielding the ovaries during radiation, or moving the ovaries out of the radiation field, may protect them from the effects of radiation. Scientists are also exploring whether using drugs to suppress the activity of the ovaries during chemotherapy will make the ovaries less susceptible to damage by chemotherapy.<a title="" href="#_edn5">[5]</a> For women with certain types of cervical or ovarian cancer, fertility-preserving surgery may also be an option.<a title="" href="#_edn6">[6]</a> It’s important to understand that only specific subsets of patients will be candidates for these approaches, and that some of the methods are still in the early stages of evaluation.</p>
<p><strong>Pregnancy after cancer</strong></p>
<p>In addition to having concerns about their ability to get pregnant, women may have concerns about whether pregnancy after cancer treatment will be safe for themselves and their children. While there is a limited amount of information about these topics, the news is generally good.</p>
<p>The risk of cancer recurrence during or after pregnancy has been most studied in women with breast cancer, and these studies generally have reported that pregnancy does not increase the risk of breast cancer recurrence. <a title="" href="#_edn7">[7]</a> Many doctors, however, suggest waiting for a period of time after treatment before becoming pregnant. <a title="" href="#_edn8">[8]</a></p>
<p>If chemotherapy or radiation therapy has damaged her heart or lungs, a woman may also have concerns about the strain that pregnancy will put on her body. Studies of breast cancer survivors suggest that long-term heart problems are uncommon after chemotherapy or radiation therapy, <a title="" href="#_edn9">[9]</a> but a woman may wish to talk with her doctor about her current health status and the likely effects of pregnancy.</p>
<p>Children born after their mother’s cancer treatment do not appear to be more likely than other children to have birth defects or cancer.<a title="" href="#_edn10">[10]</a> If a woman’s cancer was due to a hereditary cancer syndrome, such as Lynch syndrome (hereditary nonpolyposis colorectal cancer), her child may inherit the gene mutation responsible for her family’s increased risk of cancer. Talking with a genetic counselor may help clarify the child’s risk.</p>
<p>When planning for pregnancy, be aware that some cancer treatments may cause you to have an early menopause even if your periods resume after treatment. Also be aware that you may be capable of conceiving even if your periods do not resume; continue to use birth control if you do not wish to become pregnant.</p>
<p><strong>Other Options for Parenthood </strong></p>
<p>Not all women have the luxury of being able to explore their reproductive options before beginning cancer treatment, and not all women will find a fertility preservation option that meets their needs. But there are still ways to become a parent. Discussion of other routes to parenthood may be a painful topic for women who want to become pregnant and cannot. But as cancer survivors consider how best to build their families, methods such as adoption are important options.</p>
<p><em>Adoption:</em> Couples and individuals who wish to adopt have a range of options, including different types of domestic and international adoptions. You may wish to start by learning about the adoption laws in your state and by talking with other adoptive parents about the professionals and agencies they worked with. Before selecting an adoption agency, women may wish to talk with them about their attitudes toward placing a child with a cancer survivor. Many agencies will be receptive toward this, but it’s important to know before making a final decision.</p>
<p><em>Egg Donation:</em> Women who still have a uterus may be able to become pregnant using an egg donated by another woman. Through in vitro fertilization, the donated egg would be fertilized by the cancer survivor’s male partner or a sperm donor, and implanted in her uterus. Alternatively, another couple may donate a frozen embryo that could be implanted in her uterus.</p>
<p><em>Gestational Carrier or Surrogate:</em> Women who do not have a uterus, or who are otherwise unable to sustain a pregnancy, may be able to have another woman carry a pregnancy for them. If the cancer survivor has functioning ovaries, her own egg can be fertilized by her male partner’s sperm and transferred to the uterus of another woman. In this case, the woman who carries the pregnancy is known as a gestational carrier. If the cancer survivor does not have functioning ovaries, another woman can both donate an egg and carry the pregnancy. This is the arrangement traditionally known as surrogacy.</p>
<p><strong>Individual Decisions Within a Larger Community</strong></p>
<p>The decisions that you make about building a family (or about coming to terms with not building a family) will be intensely personal, but know that you are part of a larger community of patients and healthcare providers who are grappling with these issues.</p>
<p>To think about future parenthood is to think about life after cancer. For many people with cancer, planning for the future may provide the motivation needed to get through treatment.</p>
<p><strong>More Information? </strong></p>
<p>Discuss with others….. <a href="http://cancerconnect.com/groups/young-adults/topics/fertility-after-cancer-treatment">http://cancerconnect.com/groups/young-adults/topics/fertility-after-cancer-treatment</a></p>
<p>Fertile Hope (<a href="http://www.fertilehope.org/">www.fertilehope.org</a>) provides a range of fertility resources for people with cancer.</p>
<p><strong>References: </strong></p>
<div>
<hr align="left" size="1" width="33%" />
<div>
<p><a title="" href="#_ednref1">[1]</a> Critchley HOD, Wallace WHB. Impact of Cancer Treatment on Uterine Function. <em>Journal of the National Cancer Institute Monographs</em>. 2005;34:64-68.</p>
</div>
<div>
<p><a title="" href="#_ednref2">[2]</a> Sklar C. Maintenance of Ovarian Function and Risk of Premature Menopause Related to Cancer Treatment. <em>Journal of the National Cancer Institute Monographs</em>.2005;34:25-27.</p>
</div>
<div>
<p><a title="" href="#_ednref3">[3]</a> Lobo, RA. Potential Options for Preservation of Fertility in Women. <em>New England</em><em> Journal of Medicine</em>. 2005;353:64-73.</p>
</div>
<div>
<p><a title="" href="#_ednref4">[4]</a> Roberts JE, Oktay K. Fertility Preservation: a Comprehensive Approach to the Young Woman with Cancer. <em>Journal of the National Cancer Institute Monographs</em>. 2005;34:57-59.</p>
</div>
<div>
<p><a title="" href="#_ednref5">[5]</a> Blumenfeld Z, Eckman A. Preservation of Fertility and Ovarian Function and Minimization of Chemotherapy-Induced Gonadotoxicity in Young Women by GnRH-a. <em>Journal of the National Cancer Institute Monographs</em>. 2005;34:40-43.</p>
</div>
<div>
<p><a title="" href="#_ednref6">[6]</a> Gershenson DM. Fertility-Sparing Surgery for Malignancies in Women. <em>Journal of the National Cancer Institute Monographs</em>. 2005;34:43-7.</p>
</div>
<div>
<p><a title="" href="#_ednref7">[7]</a> Blakely LJ, Buzdarm AU, Lozada JA et al. Effects of Pregnancy After Treatment for Breast Carcinoma on Survival and Risk of Recurrence. <em>Cancer</em>. 2004;100:465-9.</p>
</div>
<div>
<p><a title="" href="#_ednref8">[8]</a> Simon B, Lee SJ, Partridge AH et al. Preserving Fertility After Cancer. <em>CA A Cancer Journal for Clinicians</em>. 2005;55:211-228.</p>
</div>
<div>
<p><a title="" href="#_ednref9">[9]</a> Shapiro CL, Recht A. Side Effects of Adjuvant Treatment of Breast Cancer. <em>New England</em><em> Journal of Medicine</em>. 2001;344:1997-2008.</p>
</div>
<div>
<p><a title="" href="#_ednref10">[10]</a> Nagarajan R, Robison LL. Pregnancy Outcomes in Survivors of Childhood Cancer. <em>Journal of the National Cancer Institute Monographs</em>. 2005;34:72-76.</p>
</div>
</div>
]]></content:encoded>
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		<title>Aspirin Continues to Look Promising for Cancer Prevention</title>
		<link>http://news.cancerconnect.com/aspirin-continues-to-look-promising-for-cancer-prevention/</link>
		<comments>http://news.cancerconnect.com/aspirin-continues-to-look-promising-for-cancer-prevention/#comments</comments>
		<pubDate>Mon, 26 Mar 2012 00:01:23 +0000</pubDate>
		<dc:creator>Cancerconnect</dc:creator>
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		<description><![CDATA[A combined analysis of 51 randomized trials found that daily aspirin use reduces the risk of new cancer diagnoses as well as the risk of cancer death. These results were published in The Lancet. A growing body of evidence suggests that aspirin may reduce the risk of several types of cancer, with particularly strong evidence [...]]]></description>
			<content:encoded><![CDATA[<p>A combined analysis of 51 randomized trials found that daily aspirin use reduces the risk of new cancer diagnoses as well as the risk of cancer death. These results were published in <em>The Lancet</em>.</p>
<p>A growing body of evidence suggests that aspirin may reduce the risk of several types of cancer, with particularly strong evidence for colorectal cancer. Not all studies have found a benefit, however, and any potential benefits of aspirin must be weighed against risks such as bleeding.</p>
<p>To further explore the relationships between daily aspirin and cancer, researchers conducted a combined analysis of 51 previous randomized trials.<a title="" href="#_edn1">[1]</a> The trials were originally designed to evaluate the effect of daily aspirin on outcomes such as heart disease, but information about cancer was also available.</p>
<ul>
<li>Daily aspirin reduced cancer deaths. After five years, aspirin users had a 37 percent reduction in risk of cancer death.</li>
<li>Aspirin also reduced the likelihood of developing cancer. From three years onward, aspirin users had a 24 percent reduction in the risk of being diagnosed with cancer.</li>
<li>As expected, aspirin carried a risk of major bleeding, but this risk appeared to diminish over time.</li>
</ul>
<p>Another study published in the same issue of <em>The Lancet</em> evaluated the effect of daily aspirin on cancer metastasis (the spread of cancer from its original site to other parts of the body). The study focused on 987 people who were diagnosed with cancer while participating in one of five trials of aspirin use. Those who were taking aspirin were less likely to have metastatic cancer than those who were not taking aspirin.<a title="" href="#_edn2">[2]</a></p>
<p>These results suggest that regular aspirin use may reduce cancer incidence and mortality, but concerns remain about the risks of regular aspirin use in healthy individuals. People who are considering using aspirin on a regular basis are advised to discuss the risks and benefits with their physician.</p>
<p>References:</p>
<div><br clear="all" /></p>
<hr align="left" size="1" width="33%" />
<div>
<p><a title="" href="#_ednref1">[1]</a> Rothwell PM, Price JF, Fowkes FGR et al. Short-term effects of daily aspirin on cancer incidence, mortality, and non-vascular death: analysis of the time course of risks and benefits n 51 randomised controlled trials. <em>Lancet</em>. Early online publication March 21, 2012.</p>
</div>
<div>
<p><a title="" href="#_ednref2">[2]</a> Rothwell PM, Wilson M, Price JF, Belch JFF, Meade TW, Mehta Z. Effect of daily aspirin on risk of cancer metastasis: a study of incident cancers during randomised controlled trials. <em>Lancet</em>. Early online publication March 21, 2012.</p>
</div>
</div>
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		<title>Erivedge Approved for Basal Cell Skin Cancer</title>
		<link>http://news.cancerconnect.com/erivedge-approved-for-basal-cell-skin-cancer/</link>
		<comments>http://news.cancerconnect.com/erivedge-approved-for-basal-cell-skin-cancer/#comments</comments>
		<pubDate>Wed, 01 Feb 2012 00:01:24 +0000</pubDate>
		<dc:creator>Cancerconnect</dc:creator>
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		<guid isPermaLink="false">http://news.cancerconnect.com/?p=57826</guid>
		<description><![CDATA[The US Food and Drug Administration (FDA) has approved the targeted therapy Erivedge™ (vismodegib) for the treatment basal cell carcinoma of the skin that has spread to other parts of the body or that is locally advanced and cannot be treated with surgery or radiation. Basal cell carcinoma is the most commonly diagnosed type of [...]]]></description>
			<content:encoded><![CDATA[<p>The US Food and Drug Administration (FDA) has approved the targeted therapy Erivedge™ (vismodegib) for the treatment basal cell carcinoma of the skin that has spread to other parts of the body or that is locally advanced and cannot be treated with surgery or radiation.</p>
<p>Basal cell carcinoma is the most commonly diagnosed type of skin cancer. Most cases can be treated with surgery or other types of local treatment and are not life-threatening, but the condition often occurs on the face and can be disfiguring. In the most severe cases, the cancer may be very large, may invade structures other than the skin, or may spread to other parts of the body. In these advanced cases, it may not be possible to surgically remove the cancer, and treatment options are limited.</p>
<p>Erivedge targets a specific biological pathway (the Hedgehog pathway) that is thought to play a role in more than 90% of cases of basal cell carcinoma. Taken orally, Erivedge inhibits the abnormal signaling in this pathway that contributes to cancer growth.</p>
<p>A study that contributed to the approval of Erivedge enrolled 104 adult patients with locally advanced or metastatic basal cell carcinoma. All study participants were treated with Erivedge. A reduction or elimination of detectable cancer was observed in 43% of patients with locally advanced basal cell carcinoma and 30% of patients with metastatic basal cell carcinoma.</p>
<p>Side effects of Erivedge include muscle spasms, hair loss, weight loss, fatigue, nausea, diarrhea, decreased appetite, constipation, joint pain, vomiting, and changes in taste. Erivedge may cause severe birth defects or fetal death if taken during pregnancy.</p>
<p>Erivedge is the first FDA-approved drug for metastatic basal cell carcinoma.</p>
<p>Reference: FDA News Release. FDA approves new treatment for most common type of skin cancer. January 30, 2012.</p>
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		<title>Homepage Video</title>
		<link>http://news.cancerconnect.com/homepage-video/</link>
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		<pubDate>Wed, 25 Jan 2012 08:19:22 +0000</pubDate>
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		<description><![CDATA[Dr. Richard Goldberg, a clinical researcher in Hematology and Oncology at UNC-Chapel Hill visits The Balancing Act studio to discuss Genomics and recent advances in the treatment of colon cancer.  ]]></description>
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		<title>Increased Skin Cancer Risk Among Those with Inflammatory Bowel Disease</title>
		<link>http://news.cancerconnect.com/increased-skin-cancer-risk-among-those-with-inflammatory-bowel-disease/</link>
		<comments>http://news.cancerconnect.com/increased-skin-cancer-risk-among-those-with-inflammatory-bowel-disease/#comments</comments>
		<pubDate>Tue, 29 Nov 2011 00:01:26 +0000</pubDate>
		<dc:creator>Cancerconnect</dc:creator>
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		<guid isPermaLink="false">http://news.cancerconnect.com/?p=56081</guid>
		<description><![CDATA[People with inflammatory bowel disease (IBD) may be at increased risk of non-melanoma skin cancer, particularly if they receive immune-suppressing medications such as thiopurines. These were the results of two studies published in Gastroenterology. Crohn’s disease and ulcerative colitis are the two major types of IBD. Ulcerative colitis involves inflammation of the lining of the [...]]]></description>
			<content:encoded><![CDATA[<p>People with inflammatory bowel disease (IBD) may be at increased risk of non-melanoma skin cancer, particularly if they receive immune-suppressing medications such as thiopurines. These were the results of two studies published in <em>Gastroenterology</em>.</p>
<p>Crohn’s disease and ulcerative colitis are the two major types of IBD. Ulcerative colitis involves inflammation of the lining of the large intestine, and Crohn’s disease involves inflammation of the lining and wall of the small or large intestine.<a href="#_edn1">[1]</a> Certain treatments for IBD act by suppressing the immune system, which could increase the risk for certain types of cancer. Immune-suppressing drugs include the thiopurines (e.g. azathioprine and mercaptopurine).</p>
<p>Non-melanoma skin cancer refers to skin cancers other than melanoma. The most common types of non-melanoma skin cancer are basal cell carcinoma and squamous cell carcinoma. These types of skin cancer are less likely than melanoma to be fatal (although some deaths do occur), but they can be disfiguring and invade nearby tissues.</p>
<p>Two studies published in the journal <em>Gastroenterology</em> evaluated the risk of non-melanoma skin cancer among people with IBD. The first study involved more than 9,600 IBD patients who had been identified from the University  of Manitoba IBD Epidemiology   Database. Risk of skin cancer in these patients was compared with the risk in a similar group of people without IBD.<a href="#_edn2">[2]</a></p>
<ul>
<li>People      with IBD were 20% more likely to develop basal cell carcinoma than people      without IBD.</li>
<li>Risk      of squamous cell carcinoma was increased among IBD patients who used      thiopurines.</li>
</ul>
<p>The second study was conducted in France and involved more than 19,000 people with IBD. <a href="#_edn3">[3]</a></p>
<ul>
<li>Current      and past users of thiopurines had an increased risk of non-melanoma skin      cancer. This increased risk was seen even among young patients (those      under the age of 50).</li>
</ul>
<p>These results suggest that people with IBD may have an increased risk of nonmelanoma skin cancer, particularly if they use thiopurines. As a precaution, people with IBD should protect their skin from the sun and monitor their skin for any changes. People with IBD may also wish to talk with their doctor about whether periodic skin exams would be appropriate.</p>
<p><strong>References:</strong></p>
<hr size="1" /><a href="#_ednref1">[1]</a> American Gastroenterological Association. Patient brochure: Inflammatory Bowel Disease. April 23, 2010.</p>
<p><a href="#_ednref2">[2]</a> Singh H, Nugent Z, Demers AA, Bernstein CN. Increased risk of nonmelanoma skin cancers among individuals with inflammatory bowel disease. <em>Gastroenterology.</em> 2011;141:1612-20.</p>
<p><a href="#_ednref3">[3]</a> Peyrin-Biroulet L, Khosrotehrani K, Carrat F et al. Increased risk for nonmelanoma skin cancers in patients who receive thiopurines for inflammatory bowel disease. <em>Gastroenterology.</em> 2011;141:1621-28.</p>
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		<title>CancerConnect Live Web Chat with Dr. Barrie Cassileth from Memorial Sloan-Kettering Cancer Center on Complementary Cancer Therapies on Thursday, November 17th at 6PM EST</title>
		<link>http://news.cancerconnect.com/do-complementary-therapies-work-ask-the-expert-about-herbs-acupuncture-and-other-complementary-therapies/</link>
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		<pubDate>Thu, 17 Nov 2011 00:02:39 +0000</pubDate>
		<dc:creator>Cancerconnect</dc:creator>
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		<description><![CDATA[Live Web Chat with Barrie R. Cassileth, PhD, Chief, Integrative Medicine Service; Laurance S. Rockefeller Chair Integrative Medicine, Memorial Sloan-Kettering Cancer Center (MSKCC), click here for Dr. Cassileth’s bio Dr. Cassileth is a world-renowned authority in integrative medicine. She is a researcher, educator, and planner who has worked in complementary (integrative) medicine and the psychosocial [...]]]></description>
			<content:encoded><![CDATA[<p><em>Live Web  Chat with </em><em>Barrie R. Cassileth, PhD, </em><em>Chief, Integrative Medicine Service; Laurance S. Rockefeller Chair  Integrative Medicine, </em><em>Memorial  Sloan-Kettering Cancer Center (MSKCC), <a href="http://www.mskcc.org/prg/prg/bios/525.cfm">click here</a></em><em> for Dr. Cassileth’s bio</em></p>
<p><img class="alignnone size-thumbnail wp-image-3709" title="Barrie C_a" src="http://cancerconnect.com/wp-content/uploads/2011/11/Barrie-C_a-150x150.jpg" alt="" width="150" height="150" align="left" /><a href="http://cancerconnect.com/dr-cassileth-webchat/"><img src="http://news.cancerconnect.com/wp-content/uploads/yellow3.jpg" alt="" title="yellow3" width="200" height="200" class="alignright size-full wp-image-55964" /></a>Dr. Cassileth is a world-renowned authority in integrative medicine. She is a  researcher, educator, and planner who has worked in complementary (integrative) medicine and the psychosocial aspects of cancer  care for more than 25 years.  She has  just released a new book,<em> <a href="http://www.cancercarestore.com/the-complete-guide-to-complementary-therapies-in-cancer-care-essential-information-for-patients-survivors-and-health-professionals/" target="blank">The Complete  Guide to Complementary Therapies in Cancer Care</a></em>. MSKCC’s Integrative  Medicine Service’s Web site, <a href="http://www.MSKCC.org" target="blank">www.MSKCC.org</a>, offers evidence-based information about herbs, vitamins, and  unproved cancer treatments at no charge to professionals and the public.</p>
<p>Integrative medicine  combines modern scientific treatment with complementary therapies that can  transform the physical, emotional, and spiritual lives of people living with  chronic or life-threatening illness. Complementary therapies such as touch  therapies, mind-body therapies, acupuncture, nutrition, and physical activity  are not substitutes for mainstream medical care. But when used in concert with  medical treatment, they alleviate stress; reduce pain, anxiety, and other  physical and emotional symptoms; and enhance quality of life.</p>
<p>On Thursday, November 17, 2011 at 6:00 PM EST  you’ll have the opportunity to hear a brief presentation and to ask the expert,  Dr. Barrie Cassileth, about helpful, evidence-based complementary  therapies. You’ll learn how to recognize bogus “treatments”  you will want to avoid.</p>
<p><a href="http://cancerconnect.com/dr-cassileth-webchat/">Click here</a> to submit a  question for the Q&amp;A portion of the Web Chat or to register for the Web  Chat. Please note, Dr. Cassileth will address as many questions as possible during  the 30-minute live Q&amp;A portion of the Web Chat. Thank you for your  participation.</p>
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		<title>Additional Evidence That Tanning Beds Increase Skin Cancer Risk</title>
		<link>http://news.cancerconnect.com/additional-evidence-that-tanning-beds-increase-skin-cancer-risk/</link>
		<comments>http://news.cancerconnect.com/additional-evidence-that-tanning-beds-increase-skin-cancer-risk/#comments</comments>
		<pubDate>Thu, 03 Nov 2011 00:01:36 +0000</pubDate>
		<dc:creator>Cancerconnect</dc:creator>
				<category><![CDATA[General Skin Cancer]]></category>
		<category><![CDATA[Health and Wellness]]></category>
		<category><![CDATA[Melanoma]]></category>
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		<category><![CDATA[Screening/Prevention Melanoma]]></category>
		<category><![CDATA[Skin Cancer]]></category>

		<guid isPermaLink="false">http://news.cancerconnect.com/?p=55816</guid>
		<description><![CDATA[According to a study of more than 73,000 women, use of tanning beds increases the risk of three common types of skin cancer: basal cell carcinoma, squamous cell carcinoma, and melanoma. These results were presented at the 10th AACR International Conference on Frontiers in Cancer Prevention Research. Sun exposure has long been linked with skin [...]]]></description>
			<content:encoded><![CDATA[<p>According to a study of more than 73,000 women, use of tanning beds increases the risk of three common types of skin cancer: basal cell carcinoma, squamous cell carcinoma, and melanoma. These results were presented at the 10<sup>th</sup> AACR International Conference on Frontiers in Cancer Prevention Research.</p>
<p>Sun exposure has long been linked with skin cancer, and a growing body of evidence indicates that tanning beds also increase risk. Exposure to sunlamps or tanning beds has been classified as “known to be a human carcinogen” by the National Toxicology Program of the U.S. Department of Health and Human Services.<a href="#_edn1">[1]</a></p>
<p>Basal cell carcinoma is the most commonly diagnosed type of skin cancer. Most cases can be treated with surgery or other types of local treatment and are not life-threatening, but the condition often occurs on the face and can be disfiguring. In the most severe cases, the cancer may be very large, may invade structures other than the skin, or may spread to other parts of the body. In these advanced cases, it may not be possible to surgically remove the cancer, and treatment is more challenging.</p>
<p>Squamous cell carcinoma is also very common and is usually treatable, although in some cases the cancer can metastasize (spread to other parts of the body) and become life-threatening.</p>
<p>Melanoma is less common than basal cell carcinoma or squamous cell carcinoma, but is also much more deadly. Each year in the United   States, there are more than 70,000 new diagnoses of melanoma and close to 9,000 deaths from the disease.</p>
<p>To evaluate how use of tanning beds affects risk of skin cancer, researchers assessed information from the Nurses’ Health Study II.<a href="#_edn2">[2]</a> The study enrolled more than 73,000 women. Study participants provided information about tanning bed use during high school and college and between the ages of 25 and 35.</p>
<p>The results indicated a dose-response effect with tanning bed use: women with higher exposure to tanning beds had a higher risk of skin cancer.</p>
<ul>
<li>For      each four visits per year to a tanning bed, risk of basal cell carcinoma      and squamous cell carcinoma increased by 15% and risk of melanoma      increased by 11%.</li>
<li>For      basal cell carcinoma, tanning bed use at younger ages (during high school      or college) had the strongest effect on risk.</li>
</ul>
<p>The results provide additional evidence that tanning beds increase the risk of several types of skin cancer, including melanoma.</p>
<p>References:</p>
<hr size="1" /><a href="#_ednref1">[1]</a> Report on Carcinogens, Eleventh Edition; U.S. Department of Health and Human Services, Public Health Service, National Toxicology Program.</p>
<p><a href="#_ednref2">[2]</a> Zhang M. I<strong>ndoor tanning use and incidence of skin cancer</strong><strong>. </strong><strong>Presented at the 10<sup>th</sup> AACR International Conference on Frontiers in Cancer Prevention Research. Boston, MA. Oct 22-25, 2011.</strong></p>
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		<title>What is Genomics?</title>
		<link>http://news.cancerconnect.com/what-is-genomics/</link>
		<comments>http://news.cancerconnect.com/what-is-genomics/#comments</comments>
		<pubDate>Thu, 06 Oct 2011 20:29:44 +0000</pubDate>
		<dc:creator>Cancerconnect</dc:creator>
				<category><![CDATA[All Cancer Types]]></category>
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		<description><![CDATA[You’ve probably heard of genetic testing for cancer susceptibility, but the more recent and broader field of genomics is also having a wide-reaching impact on patient care. To start with the more familiar term, genetics is the study of single genes and their effects.[1] For example, certain inherited mutations in the BRCA1 or BRCA2 genes [...]]]></description>
			<content:encoded><![CDATA[<p>You’ve probably heard of genetic testing for cancer susceptibility, but the more recent and broader field of genomics is also having a wide-reaching impact on patient care.</p>
<p>To start with the more familiar term, <em>genetics</em> is the study of single genes and their effects.<a href="#_edn1">[1]</a> For example, certain inherited mutations in the BRCA1 or BRCA2 genes greatly increase a woman’s risk of breast and ovarian cancer. Mutations in these genes can be passed down through either the mother’s or the father’s side of the family. If a woman tests positive for a BRCA mutation, there are steps that she can take to reduce her cancer risk or to detect cancer at an early stage.</p>
<p><em>Genomics</em> generally refers to the study of the study of the entire genome (all of the DNA in an organism). Genomics can consider multiple genes and how they interact with each other and the environment to affect health. Examples of genomic tests are the <a href="http://bit.ly/yWjUiz" target="blank">Oncotype DX</a> breast and colon cancer tests. The tests evaluate the activity of several genes in a sample of tumor tissue in order to assess the likelihood of cancer recurrence. Information about recurrence risk can affect treatment decisions.</p>
<p>Similarly, research that combines genomics with pharmacology (pharmacogenomics) is studying how genetic variation affects an individual’s response to particular medications. Variability in genes involved with drug metabolism can have a substantial effect on drug response and drug side effects. Progress in this area is likely to contribute to more individualized, more effective, and less toxic drug treatments.</p>
<p>In short, research in genomics is expanding at a rapid rate and will have a profound effect on many aspects of disease prevention, diagnosis, and treatment. Diseases such as cancer are remarkably complex; genomics provides researchers and physicians with tools to explore and address these complexities.</p>
<p>Reference:</p>
<hr size="1" /><a href="#_ednref1">[1]</a> Centers for Disease Control and Prevention website. Training: Genomics for Public Health Practitioners. Page last updated September 17, 2010.</p>
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