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Loosing the Breast Cancer War Part 3

March 2nd, 2009 by admin | No Comments | Filed in Uncategorized

According to the World Health Organisation, more than 1.2 million people were diagnosed with worldwide in 2005. In the United States, it is said that every two minutes one woman is diagnosed with . In 2005, it was estimated that there were 212,0000 new cases of and out of which 40,000 or about 19%, died from the disease. In the city-state of Singapore, it is said that every day three women are being diagnosed with . In Malaysia 3,738 cases were reported in 2003. This means that one in twenty women in Malaysia will get .

Despite extensive research, the exact cause of is not known. Medicine has all along been about treating , not about preventing it. Most often, women with are subjected to a “package” of standard treatments – surgery, , radiotherapy and hormonal therapy. The most important question that patients ask after undergoing all these treatments is: “Am I cured? Or, is there truly a cure for ?”

According to Silvia Dellapasqua et al. (in: J. Clinical Oncol. 23:1736-1749) the “prognosis of in young women is generally considered to be unfavourable. Young pre-menopausal patients treated with adjuvant CMF had higher risk of relapse and death than older pre-menopausal patients.” Martin Piccart-Gebhart (in J. Clinical Oncol. 23:1611-1613) wrote: “Chemotherapy has long been considered our most efficient weapon in the fight against … where this dream, unfortunately, did not materialize.”

One sad example of such crashed dream was a case of Mei (not real name), a 34-year old female nurse. Mei was diagnosed with carcinoma of the right breast. She underwent a right and axillary clearance in August 2003. This was followed by six cycles of using FAC (5-FU, andriamycin and cyclophosphamide). From 1 March to 19 March 2004, Mei received radiotherapy on her right chest wall. When the treatments were completed,she was started on tamoxifen.

Barely eight months after the completion of her treatments, in November 2004, Mei had a 3 x 3 cm soft tissue mass associated with bony destruction in her sternum. In addition, there were multiple nodules scattered in both her lungs. Sadly, the cancer recurred and spread within this short period of time.

Mei underwent again, using Taxol. After five cycles, the use of Taxol was terminated because it was not effective resulting in disease progression. The lymph nodes in her right collarbone seemed to have been infected. Mei was given another round of using Navelbine. But unfortunately after the first treatment, this was abandoned due to severe side effects.

In April 2005, Mei was given an oral drug Arimidex (anastrozole). From 25 May to 31 May 2005, she was on radiotherapy again, as the sternal mass was increasing in size. In spite of this treatment, the swelling of the right collarbone grew bigger. The use of Arimidex was discontinued and was replaced with Xeloda.

Mei decided to stop further . On 23 June 2005, she developed right pleural effusion (fluid in the lung). The doctor tapped out 5.5 liters of fluid from her lung and she felt better. On 23 July 2005, I received a fax asking for help. Unfortunately, Mei died a month later — much too late to help her in any way.

According to Mei’s sister, upon diagnosis of , Mei’s boss, who is a doctor, handed her my book (Cancer Yet They Live) and said: “Read this, and if you believe in what the author said, go and see him. But don’t tell people that I give you this book.” Mei was a nurse. Her training had placed her in a “box” with a fixed mindset that only modern medicine has all the answers to cancer. To her the only right way is surgery, , radiotherapy and follow-up drugs. Other ways are hocus pocus.

Dr. Alan Levin, professor of immunology at the University of California Medical School, was quoted to have said: “Most cancer patients … die of . Chemotherapy does not eliminate breast, colon or lung cancers. Women with are likely to die faster with than without it.”

Dr. Hardin Jones, professor of medical physics at the University of California, Berkeley, analysed cancer survival statistics for twenty-five years. In 1969 at the American Cancer Society meeting, he was quoted to have said: “Untreated patients … in many cases live longer (they) do not die sooner than patients receiving orthodox treatment.”

Dr. Lai Gi-ming, Taiwan Cooperative Oncology Group, National Research Institute wrote: “The thing that most frustrates modern doctors is that, after surgery, and radiotherapy, all they can do is keep chasing and chasing the cancer!”

How much of what were said by these experts apply to Mei’s case?

For more information about complementary cancer therapy visit:
cacare.com cacare.com
NaturalHealingForYou.com NaturalHealingForYou.com
BookOnCancer.com BookOnCancer.com

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Cancer - To See A Doctor Is To Be Told When You Are Going To Die

February 27th, 2009 by admin | No Comments | Filed in Uncategorized

Eddy from Indonesia came to our centre on 18 June 2007. He brought his father-in-law who suffer from to see us. This was Eddy’s second visit here. His first visit was on 22 April 2005 when he came with a colleague to seek our help regarding his colleague’s father, Sugi, who had . During this June 2007 visit, I enquired from Eddy about Sugi’s health – is he still alive? The answer was: “Sure, he is doing well.” I was indeed surprised and was really happy with this wonderful news. I searched out Sugi’s file to write this almost forgotten story.

Sugi (not real name) is a non-smoker. He was 67 years old in August 2003, when he suffered from sores in his mouth and had jaundice. He went to see a doctor who did a CT scan and found cancer in his lungs. The doctor told Sugi that he only had six months to live, in spite of the fact that Sugi appeared healthy. Someone told Sugi about CA Care and he decided to take our herbs: Capsule A, Lung 1 and Lung 2 teas. Sugi took the herbs for eight months but his jaundice still persisted. He lost faith in our therapy and decided to take herbs from other sources. But Sugi did not receive any medical treatment.

On 22 April 2005, Sugi’s son came to Penang and seek our help. He told us that Sugi went to see a doctor again two weeks before this visit and the doctor again told Sugi that he only had four months to live. Sugi’s son said: “In the first visit to the doctor, my father was told that he only had six months to live and now it has been two years and he is still alive. Last two weeks, the doctor told my father he only had four months to live. The doctor suggested that my father do an operation to remove the tumours but my father refused.”

After updating Sugi’s condition, we suggested that Sugi take Capsule A, Lung 1 and Lung 2, C-tea, T & E, and S & M teas.

On 1 July 2005, we received an e-mail from Sugi’s son with the following message:

“After visiting you last April 2005, I would like to share with you about my dad’s . My dad has been recovering significantly in terms of increased weight (from 54 kg to 61 kg). Visually he looked better and he felt better too. I sincerely thank you and appreciate all your kind advices and herbs.”

I e-mailed Sugi’s son requesting for an update of his father’s health. On 2 July 2007, I received his reply (original text in Bahasa Indonesia).

Hello, Dr. Chris,

It has been a long time since I last wrote you about my father’s condition. We are indeed grateful to the Almighty God for through Dr. Chris’s hands, that my father is able to remain alive up to this day. Currently, my father is able to do what he wanted to do as a normal person.

Let me answer your questions:
a) How is your father’s health currently? Can eat? Can sleep? Can move without any problems?

My father’s health, based on visual appearance is very good. His appetite is very good and he is still observing the diet restriction as written by Dr. Chris in his book: Food & Cancer. Every morning, my father walks for three km to keep fit. He sleeps very well. He is mobile without any problem.

b) After you and Eddy came to see me in Penang until now, has your father ever gone to see any doctor?

My father went to see his doctor only once. He received an injection to increase his immunity. After that, my father has been receiving this injection every month. This therapy seems to be good but I don’t know about its effect on his cancer.

c) Was your father on any other herbs besides our CA Care herbs?

He was on your herbs only. But since the past three months, my father stopped taking your herbs. I guessed he was bored with the herbs.

Comments

This is one case which almost slipped out of our records. Sugi come from Central Java and when he started taking herbs he did not come to see us personally. So there was not much communication between us. It was unfortunate that in the first instance his jaundice did not go away after taking the herbs. The reason is obvious – he was not given any Jaundice Tea to take. Our experience shows that Jaundice Heat or Jaundice Cold tea, is effective for such condition. Though Sugi suffered from jaundice, it was surprising that the doctor indicated that his liver was in good health.

This story highlighted one sad aspect about scientific medicine. When patients are diagnosed with (or for that matter any cancer), some doctors invariable try to play God and give their prognosis. “You have three months to live” or “You have six months to live.” Such comment is indeed very destructive. I wonder what purpose such negative comment serves. Is this a way of putting “fear and terror” into patients? When patients are reduced to a state of “helplessness and hopelessness” they become more compliant with whatever treatments suggested. To the doctors, surgery, and radiotherapy are the only ways to deal with cancer – other ways are “hocus pocus” and unproven.

Unfortunately this story proves otherwise. Without these evasive treatments, Sugi was and is better off. He maintained his good health and well-being – physically, emotionally and financially. It has been almost four years since Sugi was diagnosed with . Let us pray that Sugi will continue to live many more years to come. Sugi’s success defies medical logic, if you believe that there is such a thing as logic!

For more information about complementary cancer therapy visit: cacare.com cacare.com, NaturalHealingForYou.com NaturalHealingForYou.com, BookOnCancer.com BookOnCancer.com

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Tumor Markers

February 25th, 2009 by admin | No Comments | Filed in Uncategorized

Due to progress in medical and biotechnological studies in the recent years scientists have focused on tumors not only within macroscopic or pharmacological perspectives, but also within molecular and cytogenic ones. Molecular epidemiology, a new area of medical knowledge has been singled out. It is currently oriented at the search for biomedical markers which not only signal the early phase of cancer, often undetected in accessible imaging methods, but also indicate higher risk of incidence and they may be used in so-called groups of high-risk. In addition, research is little invasive, as biomarkers are easily accessible in the cellular material or biological liquids.

However, molecular epidemiology cannot replace traditional epidemiology but is a tool enabling its supplementation. Namely, traditional epidemiology studies affiliation between exposure factors (for instance geography, diet, exposure to a given chemical, physical, biological factors) and cancer incidence rate; molecular epidemiology studies, on the other hand, the analysis of factors found in the vast niche between the two (the level of cancer gene, its metabolites or adducts from DNA, mutations, genes’ activations and deactivations and finally the level of cells proliferation stimulation – neoplasis. Nowadays, using tumor markers is not only about early diagnosis, but also about forecasting and monitoring the therapy. Some of them work well in the screening tests. Unfortunately, apart from a quarter million of publications on markers, it is not clear whether substantially changed level of a determined factor in the serum is sufficient to define the cancer recurrences.

Measurement of adducts. the measurement of adducts, which generate cancer genes or their DNA metabolites, seems to be the best biomarker as far as defining the level of exposure to cancer diseases. It creates s the possibility to pick up persons substantially at risk from the population, but it may also already determine the degree of the genome damage by mutations. Research has also been conducted, which pointed to the fact that the measurement of adducts may be important in monitoring therapies using pharmaceuticals (CDDP, alkalizing factors).

Taking into consideration the epidemiological factors, a division of biomarkers has been proposed, which may reflect in its scheme the scope of molecular epidemiology. Biomarkers of exposure to cancer genes substances. Two groups have been distinguished in this category. The first one comprises the biomarkers which may be found in soil, water and air, the second – those found in living organisms. In the latter one, internal doses of biomarkers are classified (determination based on the amount of cancerogenic chemical substance or its metabolite, which penetrated the organism; mutagenic activity detected thanks to laboratory tests taking advantage of cancerogenic substance interaction or its bacteria DNA metabolite – Ames test or DNA of other cells) and doses of biologically effective biomarkers (the level of cancer gene adducts, most often from DNA).

correlation between the number of smoked cigarettes and the type of acetylation and the incidence rate of urinary bladder cancer. It has been proven that among slow acetilators the level of adduct 4-aminobifenyl (a substance found in the nicotine smoke) hemoglobin is higher than among the fast ones and that the number of smoked cigarettes does not have a significant influence. It binds the level of adduct with the features of metabolic predispositions of a given person and it may suggest the fact that in some cases persons with a higher genetic predisposition may have a higher incidence rate as for given types of tumors even if the exposure to cancer genes is lower.

The connection between the consumption of aflatoxine B1 and the liver cancer incidence rate. The level of an adduct which aflatoxine B1 creates with DNA (aflatoxine-N7-guanine) is higher in the urine of persons exposed to this cancerogenic mykotoxine. A correlation has been found between the level of aflatoxine-N7-guanine in the urine and the liver cancer incidence rate. It is the example of DNA cancer genes adducts released during repair processes. In this example what focuses our attention is the simplicity and accessibility of biological material while it is ambiguous whether aflatoxine-N7-guanine solely comes from DNA or also from RNA.

A connection between the length of exposure to cancer genes and the number of DNA-protein crosslinks. One of the results of DNA-protein crosslinks creation may be the inactivation of 53p gene. Shaham showed the correlation between the years of exposure to formaldehyd in conditions of risk and the number of crosslinks. It is suspected that other permeable cancer genes such as chrome, nickel, alkalizing factors, cisplatine or UV radiation give similar results.

Biomarkers of health results induced by cancer genes and their metabolites. They provide information about biological and biochemical changes that took place in the organism’s cells as a result of an interaction of cancerogenic substances or their metabolites on them. Here the attention is focused on mutations, genes’ activations and deactivations, changes in chromosomes, oncoproteins and antioncoproteins presence.

A connection between the appearance of detectable changes in chromosomes and the amount of cancer gene dose, and the time of exposure. Peripheral blood lymphocytes are most often the research material (as in the majority of biomarkers of health results determination) which with a certain probability reflect changes in all the chromosomes of the target tissue cells which is very often inaccessible for examination purposes. The frequency of SCE (sister chromatides exchange) may serve as an example in five days after acute exposure to ethylene oxide. Using cytogenetic examination (e.g. SCE or CA chromosome aberrations) as a biomarker cannot be treated as sufficient to get decisive results.

The accumulation of genetic irregularities in many genes clinically supersedes the appearance of the disease. Mutations in p53 gene and in the race gene appear in the saliva of the examined group already about a year before the clinical appearance of . What is more, a specific place of the sequence change seems to correspond to the presence of a given mutagenic factor.

Determining oncoproteins in the biological material (or mutated antioncoprotein) may supersede the appearance of the disease for a few years. The research that highlights it is not, however randomized and many times it is the description of given cases, therefore its results should be carefully analyzed. Among others, the race oncoprotein p21, oncoprotein fes or beta - the transforming growth factor - are brought into discussion while exposed to asbestos, benzopirene (polycyclic aromatic carbohydrates) or polichlorised bifenyls. There is not doubt that the presence of p53 protein in the examined material indicates its mutation (half-life of mutated p53 protein equals to 12 hours whereas the one not modified up to 20 minutes), however, taking into consideration not fully clear and undefined role of the “genome guard” sequence change in the process of tumor transformation one should not draw snap conclusions.

Biomarkers determining individual sensitivity towards cancerogenic substances activity. They examine individual differentiation in response to the activity of cancerogenic factors. This group reflects genetic or acquired factors which influence the character and the extent of cells’ responses to the exposure. They identify those in the population who are genetically, or in an acquired manner, more at risk as for cancer disease when we take into consideration a given exposure to cancer gene.

For years, in order to determine biomarkers of sensitivity, tests have been used that examined the level of medicine in the serum and clearance of its metabolized derivative in the urine, as determining the polymorphism of enzyme which was to be defined. Currently the PCR reaction is used to achieve this, which directly defines changes in the nucleotides’ sequence that codes a given enzyme. Thanks to these methods genotypes of such enzymes that metabolize cancer genes as transferase S-glutatione, cytochrome CYP1A1 and CYP2D6 or N- acethylotransferase were found.

Another group of sensitivity biomarkers are those, which determine the level of genetic differentiation influencing repair processes activity. This group is crucial as it allows detection of the presence of mutated genes inherited after parents in the offspring, such as APC gene or BRCA 1. In such situations the early stages of cancerogenesis are omitted, therefore one should not doubt the arguments for the research in this direction.

Biomarkers specificity depending on the location and the type of the tumor:

Sex cells tumors. Alpha-fetoprotein (AFP), human chorionic gonadotropine (hCG) and LHD are sex cells tumors markers known for 20 years. Because of their diagnostic properties, they are unconditionally recommended already to diagnose diseases, as well as to define the level of progression, forecast, monitor treatment and define the presence of recurrence. No useful values were found for screening. In the case of testis seminoma determining the level of placenta-alkalic phosphatase, which is ectopically released in 80% of cases (the remaining 20% is released by hCG) was found useful. AFP, hCG and LDH are the indicators of tumor progression level recommended by AJCC (the American Joint Committee on Cancer).

Monitoring their concentration in the serum completely entitles to state whether there are metastases or defining the level of response to the . The fall of the level of AFP and hCG after orchidectomy should be correlated with the normal time of half-life of these compounds (for AFP 7 days, hCG – 3 days). Rapidity of changes during first six weeks of the cycle may indicate contingency of recurrences in the first month after it has been finished, that is why the measurement of AFP, hCG and LDH concentration is recommended every week. Undoubtedly, it is one of the greatest achievements of medical studies in a de facto multidisciplinary area of oncology and a lot of research is done in the direction of similar achievements. Norms [12]: AFP in serum: more than 12U/ml (pregnant women 38 – 160 U/ml), waiting for the results: 1 – 2 days; LDH in serum: adults 240 – 480 U/l. Tumors of the lower part of alimentary tract (colon, rectum)

CEA (carcinoembryonic antigen) is present in the prevailing majority of cases in the blood serum. However, it does not justify using it to determine it in screening or for early diagnosis purposes but it is important in forecasting and defining the level of progression. It is a preoperative test recommended by American Cancer Society as an aid to define the histopathological progression of an ulcer and to determine the scope of resection. In the aftersurgery monitoring after resection of isolated metastases to liver CEA should be determined every 2 – 3 months in the two first years since the surgery. Its higher level leads towards metastatic disease. Similarly, when solely a tumor is due to resection, a higher CEA level in at least 2 tests taken in the same frequency may suggest the progression of the disease. In conclusion, determining CEA is helpful while monitoring the therapy but its character and specificity is insufficient to diagnose colon and rectum tumors. Norms: Tumor – foetal antigene (carcinoembryonic) in serum: smoking persons below 5.0 ng/ml, non-smokers below 3.0 ng/ml, results in 2 – 3 days. Breast cancer.

A basic examination recommended by many centers involves determining the level of estrogen and progesterone receptors in all women (in the pre- and post- menopausal age) as an indicator of responses to the hormonal therapy. In the case when the presence of metastases is confirmed determining the level of receptors is used only if its results have influence on the further treatment. There are also no doubts about determining the level of over expression HER-2 / neu (c-erbB-2) while qualifying to a trastuzbam therapy. CA 15-3 and BR 27.29 are definitely the best breast tumors markers to determine in the serum but because of small specificity, low sensitivity in the early phase of the disease and controversial application while bringing therapeutical benefits they are not recommended in the early detection, to screening or staging. Both CA 15-3 and BR 27.29 have the recommendation of Food and Drug Administration to monitor therapy in advanced . However, as the benefits after monitoring remain controversial, the appropriateness for determining these markers remains unclear. They may be helpful while defining the failure of the treatment (when clinical changes indicate it) and monitoring the clinical course of , which may raise some ethical doubts. Determining CEA level is not either applied in the early disease detection, screening, determining the level of progression or forecasting in the cases. Some American centers accept the possibility to use it to monitor the therapy, however due to its small specificity it should closely correlate with the clinical picture.

Norms: Tumor antigene Ca 15-3 in serum : over 30U/ml, results in 2 – 3 days. Ovary cancer CA 125 is definitely the best marker for an early diagnosis of ovary cancer (or even screening) provided women have a positive family history. It helps to differentiate the tumors found in the pelvis on benign and malignant among women in their postmenopausal age. A fall of CA 125 level is discernible after ovaries resection or after cytotoxical . It does not play a significant role in staging, therefore the results cannot be based on TNM classification. It has not been precisely defined whether and how often the concentration of this marker in the serum should be determined, it is suggested to do it once every 2-3 weeks (in the case of its level being doubled a pelvis computer tomography is advised). One should remember that a progression of tumor changes may take place without a substantially changed level of CA 125. Norms: Tumor antigene Ca 125 in serum: above 35U/ml, results in 2 – 3 days. Prostate cancer.

PSA (prostate specific antigen) has been the best known and the most useful tumor marker. Its application begins with screening. Together with per rectum examination or DRE (digital rectal examination) it gives a strong correlation and it is an indication for biopsy with taking a segment of prostate, which is the best diagnostic tool of changes occuring around prostate. Its role in staging has been proven, although due to the lack of official recommendations only auxiliary significance can be ascribed to it. Undoubtedly, the level of PSA is useful in monitoring therapy, however one cannot focus on these measurements solely. There have been cases when the result of determining the PSA level biochemically indicated the presence of metastatic changes, whereas no such changes occurred in fact. Nevertheless, one cannot undermine the importance of PSA concentration test in serum and one has to bear in mind that together with the clinical picture it constitutes a powerful diagnostic tool. Norms: PSA in serum – total: Age 40 - 49: < 2.5 ng/ml, 50 - 59: < 3.5 ng/ml, 60 - 69: < 4.5 ng/ml, 70 - 79: < 6.5 ng/ml; PSA in serum – free fraction: norm up to 0.9 ng/ml. Free PSA/total PSA below 0.1 – high probability of ; free PSA/total PSA above 0.25 – high probability of no tumor changes. Results in: 2 - 3 days. Lung cancer.

The measurement of the level of tumor markers is not often found in the cases of . Out of a few applied, NSE level measurement is used when differentiating small celled . Its serial measurement after the first therapy of this type of a tumor (resection, ) may be helpful in determining usually asymptomatic course of the early recurrence or resection completeness. Tumors of neuroendocrinal organs

Tumors of neuroendocrinal organs are rare. Determining the biomarkers may contribute to their differentiation, among all neuroblastomy and pheochromocytomy. In such cases the level of catecholamines, vanillymandelic acid and/or vanillic acid in the urine are determined. Thyroid cancer.

The level of thyreoglobulin is helpful while diagnosing and monitoring the . A correlation has been proven also when measuring the concentration of calcitonine and the appearance of medullary .

Markers’ prevalence, data verification, benefits and limits. Determining the level of tumor markers in the serum usually depends strictly on clinical needs. As the treatment algorithms are due to constant modification and the development of biotechnology takes advantage of modern technologies and finds more precise pictures of clinical state, the use of tumor markers also gains in popularity. As it has been mentioned several times, the analysis of the laboratory results has to closely correlate with the features presented in the clinic and it cannot be a sole confirmation of diagnostic presumptions. Obviously, it does not change the fact that they are essential and valuable in the doctor’s activity. Together with doctor’s practical skills they become a powerful tool supporting his or her work. It is worth bearing in mind some essential cues, such as the latency period, which has to take place since implementing the mode of action (e.g. surgerical or pharmacological) for laboratory markers to be a valuable source of information about the patient’s state and not introducing unnecessary confusion.

Being acquainted with the mechanisms of biomarkers concentration changes substantially influences the multidisciplinary image of the patient’s care and, despite the fact that many questions remain unanswered, one should hope that the progress of medical studies will provide the answers in the years to come.

Radoslaw Pilarski is a PhD candidate working on anticancer properties of Uncaria tomentosa - uncariatomentosa.com uncariatomentosa.com - at PAS, Poland. mLingua Worldwide Translations, Ltd. - mlingua.pl mlingua.pl - provides professional language translations.

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Your Cancer Resource

February 25th, 2009 by admin | No Comments | Filed in Uncategorized

It seems the news has become virtually unwatchable and the print media, too painful to read. With death, sickness and disease plastered across most nightly news programs, it may be unavoidable. One of the worst of the worst is a horrible disease that we call cancer. Our collective knowledge of this disease is scarce to say the least. This is why it’s important to acquire cancer facts from a reliable cancer resource. In the best resource you have right now is at your fingertips, your computer.

Have you ever has it that need for a solid and cancer resource? There is a plethora of valuable information that is available to us. The most important resource is also the most convenient as a cancer resource. I’m talking about the Internet. Cancer is so prevalent that I believe we should all take the time to learn a little, and by doing so we may educate ourselves and how to avoid getting cancer.

Are you aware that cancer is a genetic condition in many cases? It’s true; while most individuals people don’t realize this, they nevertheless are susceptible to cancer like the rest of us. But just because there are cancer genes with MS doesn’t mean we have to succumb to them. To start, our diets play a big role in our health.

That’s why it is so important that we take care of ourselves by heating right and exercising. When you subject yourself to poor eating habits and gaining extra pounds, you in turn better your chances of acquiring some kind of illness. We must play an active role in protecting our bodies from those agents that may do us harm.

Are you watching your diet? You can certainly turn to a credible cancer resource such as the Internet to learn more about eating right and avoiding processed foods. And of course it goes without saying that cancer can be avoided in many cases by simply not smoking. By now, virtually all of us should know and understand the negative effects of smoking and what it does to our lungs. Although I personally know someone that smokes who was in denial of this fact. If you are a heavy smoker, then you may want to get online and browse a few websites that deal with .

In this day and age it’s definitely not difficult to find a cancer resource. We would all be well served to become better educated in this area. There are numerous types of cancer that can affect different areas of the body. It may very well be impossible to completely , but at the same time there are plenty of things that we can do to protect ourselves from contracting it to begin with. Having a quality cancer resource at your disposal is an excellent first step in battling this hideous disease.

Morgan Hamilton offers expert advice and great tips regarding all aspects concerning men’s health. Get the information you are seeking now by visiting

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Finding Valuable Cancer Information

February 23rd, 2009 by admin | No Comments | Filed in Uncategorized

Cancer, as everything else, has been largely discussed on the Internet. There are many sites dedicated to cancer diseases, to people suffering from cancers, to their friends and families. The Internet is a good source of valuable cancer information, but there is more to it than that. It is a means to integrate the suffering into a network of virtual friends and supporters, which doesn’t let them feel isolated and alone.

The Internet helps friends and families of deceased people to realize that they are not alone with their pain, and that many people are going through the same terrible plot. One of the best traits of cancer information sites is that they unite people and help them overcome their grief.

There are a variety of forums and online discussions meant to bring people together. Cancer is a topic of great interest for many people. Anyone can read and respond to, there are options for instant messages with fellow cancer patients, cancer survivors, and cancer supporters.

One useful site for friends and family members of ill patients is Cancer and Careers.com’s “What You Can Do as a Friend”. It props you up with information about what your behavior in front of the ill friend should be. You shouldn’t talk about certain things, neither be too optimistic, nor be too negative in your expectations.

Your main duty as a friend should be supportive and encouraging. This cancer information is very helpful at the beginning. Another essential book for friends may be Facing Cancer Together: How to Help Your Friend or Loved One by Pamela N. Brown. It can help a lot in guiding your attitude towards your ill friend.

Valuable cancer information can be found at cancernews.com. There is a large list of directories meant to give orientation to people for any local cancer support groups. Most of them can also be found at the Cancer Information Network. There are many organizations supporting cancer hotlines— one of them is The National Cancer Institute, their site being reached at cancer.gov, others are Y-ME National Breast Cancer Organization (Their site is: y-me.org/hotline), the RA Bloch Cancer Foundation Cancer Hotline (1-800-433-0464), and the Lung Cancer Alliance Toll-free Hotline (1-800-298-2436).

There are also a lot of specific information sites about different types of cancers: see Mesothelioma-net ( a site, designed to offer cancer information on the specific types of , its treatment, and coping strategies and so on). Another site which presents you a list of all cancers is The Cancer Information Network (at cancerlinksusa.com); and, of course, The American Cancer Society (cancer.org). The latter one gives you information on everything from prevention and early detection strategies, as well as treatment and cancer information by type. There are great statistics and investigations included, which offer you information from the past 100 years.

Morgan Hamilton offers expert advice and great tips regarding all aspects concerning health and research. Learn more at

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