Sunday, 30 June 2013

Do you have the 3Ps to success?

If success sometime seems like a terribly long reach, it might be time to get back to prosperity basics.
P 1
PATIENCE: Prosperity is a process of growth, development and self-learning, and patience is often the key to allowing that growth.  Be patient with myself and allow at least 3 years of consistent efforts before anticipating major and permanent changes in my level of success, prosperity and my inner state of life to strengthen.
P 2
PERSISTENCE: By apply this P, I can only know what I know at each step in my journey to prosperity, I am always making adjustments and corrections in direction and scope. These adjustments and deviations in the path aren’t failures; they are simply a required part of the path I am journeying. Staying persistent always, even stubbornly determined, in the face of any obstacles will keep me moving swiftly towards success and eventually towards prosperity.
P 3
PLEASURE: Finally, to reach prosperity, I must have to take real pleasure in what I am creating and manifesting. Pleasure and joy are the emotions that can move manifestation along at warp speed. So whatever I choose as my route to prosperity, I must enjoy the journey as well as anticipating my prosperous destination!
Whenever I am down and out, these 3Ps of Success can lift my spirit and remind me of my aims and my mission in life. Constantly check whether I am short on patience, persistence or pleasure to get myself back on the road to success, victory, prosperity and happiness.
CS



Wednesday, 6 March 2013

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Tuesday, 26 February 2013

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Wednesday, 20 February 2013

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Monday, 18 February 2013

Method to Personalize Chemo Drug Selection

In laboratory studies, scientists at the Johns Hopkins Kimmel Cancer Center have developed a way to personalize chemotherapy drug selection for cancer patients by using cell lines created from their own tumors.
If the technique is successful in further studies, it could replace current laboratory tests to optimize drug selection that have proven technically challenging, of limited use, and slow, the researchers say.
Oncologists typically choose anticancer drugs based on the affected organs' location and/or the appearance and activity of cancer cells when viewed under a microscope. Some companies offer commercial tests on surgically removed tumors using a small number of anticancer drugs.  But Anirban Maitra, MBBS, professor of pathology and oncology at the Johns Hopkins University School of Medicine, says the tissue samples used in such tests may have been injured by anesthetic drugs or shipping to a lab, compromising test results.
By contrast, he says "our cell lines better and more accurately represent the tumors, and can be tested against any drug library in the world to see if the cancer is responsive."
The Johns Hopkins scientists developed their test-worthy cell lines by injecting human pancreatic and ovarian tumor cells into mice genetically engineered to favor tumor growth. Once tumors grew to one centimeter in diameter in the mice, the scientists transferred the tumors to culture flasks for additional studies and tests with anticancer drugs.
In one experiment, they successfully pinpointed the two anticancer drugs from among more than 3,000 that were the most effective in killing cells in one of the pancreatic cancer cell lines. A report on the success was published online Jan. 22 in the journal Clinical Cancer Research.
The new method was designed to overcome one of the central problems of growing human tumor cell lines in a laboratory dish -- namely the tendency of noncancerous cells in a tumor to overgrow cancerous ones, says James Eshleman, M.D., Ph.D., professor of pathology and oncology and associate director of the Molecular Diagnostics Laboratory at Johns Hopkins. As a consequence, it has not been possible to conventionally grow cell lines for some cancers.  Still other cell lines, Eshleman says, don't reflect the full spectrum of disease.
To solve the problem of overcrowding by noncancerous cells, Maitra and Eshleman bred genetically engineered mice that replace the noncancerous cells with mouse cells that can be destroyed by chemicals, leaving pure human tumor cells for study.
"Our technique allows us to produce cell lines where they don't now exist, where more lines are needed, or where there is a particularly rare or biologically distinctive patient we want to study," says Eshleman.
In its proof of concept research, the Johns Hopkins team created three pancreatic ductal adenocarcinoma cell lines and one ovarian cancer cell line. They then tested one of the pancreatic cancer cell lines (called Panc502) against the Johns Hopkins Drug Library of 3,131 drugs, identifying tumor cells most responsive to the anticancer drugs digitoxin and nogalamycin.
For 30 days, they watched the effects in living mice of the two drugs and a control medicine on tumors grown from implanted cells derived from Panc502 and an additional pancreatic cell line, Panc410. They measured the size of tumors twice a week. Both drugs demonstrated more activity in reducing the tumor appearance and size in Panc502 than in Panc410, supporting the notion that the cell line technology may better predict sensitivity to the two drugs.
The investigators have given one type of their genetically engineered mice to The Jackson Laboratory in Bar Harbor, ME, a mouse genetics research facility, for breeding and distribution to other laboratories and are looking to partner with a company to distribute two other types.
Study co-authors were Hirohiko Kamiyama, Sherri Rauenzahn, Joong Sup Shim, Collins A. Karikari, Georg Feldmann, Li Hua, Mihoko Kamiyama, F. William Schuler, Ming-Tseh Lin, Robert M. Beaty, Balasubramanyam Karanam, Hong Liang, Michael E. Mullendore, Guanglan Mo, Manuel Hidalgo, Elizabeth Jaffee, Ralph H. Hruban, Richard B. S. Roden, Antonio Jimeno, and Jun O. Liu, of Hopkins; and H. A. Jinnah of Emory University School of Medicine in Atlanta.
The work was supported by the National Institutes of Health, National Cancer Institute (CA130938, CA62924 and CA122581), the Sol Goldman Pancreatic Cancer Research Center, the Stewart Trust Fund, the Lustgarten Foundation, the Mary Lou Wootton Pancreatic Pancreatic Cancer Research Fund, the Michael Rolfe Pancreatic Cancer Foundation and the HERA Foundation.
Rauenzahn, Maitra and Eshleman may receive royalty payments if the mice are licensed, and Eshleman is an advisory board member for Roche Molecular Diagnostics. These relationships have been disclosed and are under the management of the Johns Hopkins University School of Medicine Conflict of Interest Committee.

On the Web:
www.hopkinskimmelcancercenter.org


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'Quality of Life' Therapy Improves Health During Cancer Treatment, Mayo Clinic Finds

Therapy to ease stress, fatigue and other quality of life issues significantly improves patients' sense of well-being during cancer treatment, new Mayo Clinic research shows. Patients who kept to their standard routines showed a decline in quality of life measures, the study found. The findings are published this month in Cancer.
Mayo cancer care specialists created a six-session program to address cognitive, physical, emotional, social and spiritual well-being. Each session includes physical therapy exercises to improve fatigue, discussions of topics such as developing coping strategies or addressing spiritual concerns, and deep breathing or guided imagery to reduce stress.
For people with cancer, fighting the disease understandably takes highest priority. But other factors - including stressfatigue, pain, and spiritual uncertainty - can severely diminish patients' quality of life during and after treatment, says the study's lead author, psychologist Matthew M. Clark, Ph.D., of the Mayo Clinic Department. Many studies have tested strategies to improve patients' experience, but most approaches have focused on only one quality of life issue at a time and typically after cancer treatment, he says.
In the randomized trial, researchers studied a group of 113 patients with advanced cancer; 63 percent were male, mostly in their late 50s. All were receiving radiation therapy at the Mayo Clinic Cancer Center. Family members caring for cancer patients also often experience a lower quality of life, and the study included them. While half of participants stayed with their usual psychosocial routine during treatment (for instance, seeing their own therapists, counselors or clergy), the other half attended the formal, 90-minute program three days a week.
"Much of the success may be that the program is active and engaged, and patients participated in the sessions as part of a group. They received support and encouragement to go home and practice things like physical activity, spirituality and relaxation," Dr. Clark says.
While the study showed that the intervention can improve quality of life for cancer patients, Dr. Clark says there were two surprising results. Researchers found the program did not improve quality of life for caregivers during the treatment time period.
"We were hoping the program would also help caregivers who tend to experience significant emotional and physical fatigue," he says. "We still have to find ways to help them."
In addition, in a follow-up questionnaire conducted six months after treatment, the patients who took part in the program showed a lack of improvement in quality-of-life measures over time.
"The intervention is helpful at a critical time, but doesn't have a lasting continuous enhancing effect," Dr. Clark says. "Our hope is to develop strategies to help people maintain and then improve their quality of life throughout survivorship."
The study was funded by the Linse Bock Foundation and Mayo Clinic.

###

About Mayo Clinic

Mayo Clinic is the first and largest integrated, not-for-profit group practice in the world. Doctors from every medical specialty work together to care for patients, joined by common systems and a philosophy of "the needs of the patient come first." More than 3,700 physicians, scientists and researchers, and 50,100 allied health staff work at Mayo Clinic, which has campuses in Rochester, Minn; Jacksonville, Fla; and Scottsdale/Phoenix, Ariz.; and community-based providers in more than 70 locations in southern Minnesota., western Wisconsin and northeast Iowa. These locations treat more than half a million people each year. To obtain the latest news releases from Mayo Clinic, go to www.mayoclinic.org/news. For information about research and education, visit www.mayo.eduMayoClinic.com (www.mayoclinic.com)
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Monday, 28 January 2013

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