30 Lecture 30 Stem Cells Cloning 2
By: tawkaw OpenCourseWare
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30 Lecture 30 Stem Cells Cloning 2 - Video
Posted: May 26, 2014 at 6:09 pm
30 Lecture 30 Stem Cells Cloning 2
By: tawkaw OpenCourseWare
Continue reading here:
30 Lecture 30 Stem Cells Cloning 2 - Video
Posted: May 26, 2014 at 5:52 pm
Dr. J Off Air - SVF Stem Cell Therapy Informational Video
http://www.innovationsstemcellcenter.com Call: 214.420.7970 If you are considering stem cell therapy, you need to watch this video prior to your consultation. Facebook: https://www.facebook.com/i...
By: dallasdrj
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Dr. J Off Air - SVF Stem Cell Therapy Informational Video - Video
Posted: May 26, 2014 at 6:43 am
Stem cell therapy | biopen Copy
http://www.arthritistreatmentcenter.com I #39;m in Australia again... to report on a fascinating new concept when it comes to stem cells. Surgeons 3D print stem cells and repair bone with biopen...
By: Nathan Wei
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Stem cell therapy | biopen Copy - Video
Posted: May 26, 2014 at 2:43 am
Stem cell therapy | biopen Copy
http://www.arthritistreatmentcenter.com I #39;m in Australia again... to report on a fascinating new concept when it comes to stem cells. Surgeons 3D print stem cells and repair bone with biopen...
By: Nathan Wei
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Stem cell therapy | biopen Copy - Video
Posted: May 25, 2014 at 7:47 pm
"Ive felt a big difference. It hasnt cured my knee but its certainly helped it out": Trent Hodkinson. Photo: Getty Images
A $10,000 experimental medical procedure has helped saved the careers of two NSW players.
Stem cells placed into the knees of Trent Hodkinson and Aaron Woods have helped resurrect their careers and has allowed them to leap into the representative arena. They both had severe knee problems which could have forced them into early retirement.Hodkinson had the procedure in 2012, Woods at the end of last season.
Former long-term Wests Tigers doctor Donald Kuah performed the Regeneus HiQ procedure on Woods where a persons own fat tissue via liposuction is injected into an affected joint or tendon.
Grateful: Aaron Woods. Photo: Getty Images
The aim is to accelerate the regeneration of damaged cartilage.Kuah had no doubt Woods would have been forced into premature retirement had the operation failed.He probably mightve had cortisone injections which would last six weeks or so at a time, Kuah said. To be honest, he might be able to do one season and then he probably would have had to retire at the end of that.
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"He started last season strong but as the season went on he wasnt getting the miles in his legs because he couldnt train with the team.Players seem to get symptom relief [from the stem cells operation]. I dont think it cures them as such but it buys them some time and it can reverse some of the damages to their knee.
Kuah described the surgery as experimental. It costs about $10,000 and is not covered by Medicare or private health insurance.
Woods said the surgery had given his life back after battling through the pain last year. Both he and Hodkinson said they could barely walk up stairs and Woods spent a large chunk of time icing and treating the knee after games.My knee would swell up on the outside, thats where I hurt the lateral meniscus, Woods said. I would have to get 50 millilitres of yellow fluid drained from my knee because the knee was in so much stress.Now I have nothing, no pain at all. I couldnt believe it when I started to run pain free.
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Stem cells give new life to Blues pair
Posted: May 25, 2014 at 7:40 am
The Koyal Group InfoMag News: Why so Much Fake, Unduplicable Stem Cell Research?
Hi. I am Art Caplan, from the NYU Langone Medical Center, Division of Medical Ethics. What is going on in the field of regenerative medicine with respect to ...
By: Margaret Koyal
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The Koyal Group InfoMag News: Why so Much Fake, Unduplicable Stem Cell Research? - Video
Posted: May 25, 2014 at 7:40 am
Stem Cell Research Diabetes
http://www.living-healthy-with-diabetes.com/stem-cell-research-diabetes.html Advances in stem cell research diabetes have led to exciting breakthroughs in tr...
By: living-healthy-with-diabetes.com
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Stem Cell Research Diabetes - Video
Posted: May 24, 2014 at 6:46 pm
The world has great expectations that stem cell research one day will revolutionize medicine. But in order to exploit the potential of stem cells, we need to understand how their development is regulated. Now researchers from University of Southern Denmark offer new insight.
Stem cells are cells that are able to develop into different specialized cell types with specific functions in the body. In adult humans these cells play an important role in tissue regeneration. The potential to act as repair cells can be exploited for disease control of e.g. Parkinson's or diabetes, which are diseases caused by the death of specialized cells. By manipulating the stem cells, they can be directed to develop into various specialized cell types. This however, requires knowledge of the processes that regulate their development.
Now Danish researchers from University of Southern Denmark report a new discovery that provides valuable insight into basic mechanisms of stem cell differentiation. The discovery could lead to new ways of making stem cells develop into exactly the type of cells that a physician may need for treating a disease.
"We have discovered that proteins called transcription factors work together in a new and complex way to reprogram the DNA strand when a stem cell develops into a specific cell type. Until now we thought that only a few transcription factors were responsible for this reprogramming, but that is not the case," explain postdoc Rasmus Siersbaek, Professor Susanne Mandrup and ph.d. Atefeh Rabiee from Department of Biochemistry and Molecular Biology at the University of Southern Denmark.
"An incredibly complex and previously unknown interplay between transcription factors takes place at specific locations in the cell's DNA, which we call 'hotspots'. This interplay at 'hotspots' appears to be of great importance for the development of stem cells. In the future it will therefore be very important to explore these 'hotspots' and the interplay between transcription factors in these regions in order to better understand the mechanisms that control the development of stem cells," explains Rasmus Siersbaek.
"When we understand these mechanisms, we have much better tools to make a stem cell develop in the direction we wish," he says.
Siersbaek, Mandrup and their colleagues made the discovery while studying how stem cells develop into fat cells. The Mandrup research group is interested in this differentiation process, because fundamental understanding of this will allow researchers to manipulate fat cell formation.
"We know that there are two types of fat cells; brown and white. The white fat cells store fat, while brown fat cells actually increase combustion of fat. Brown fat cells are found in especially infants, but adults also have varying amounts of these cells.
"If we manage to find ways to make stem cells develop into brown rather than white fat cells, it may be possible to reduce the development of obesity. Our findings open new possibilities to do this by focusing on the specific sites on the DNA where proteins work together," the researchers explain.
Details of the study
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Stem cell development: Experts offer insight into basic mechanisms of stem cell differentiation
Posted: May 24, 2014 at 12:53 pm
PUBLIC RELEASE DATE:
22-May-2014
Contact: Shawna Williams shawna@jhmi.edu 410-955-8236 Johns Hopkins Medicine
Working with mice, Johns Hopkins researchers report they have identified chemical signals that certain breast cancers use to recruit two types of normal cells needed for the cancers' spread. A description of the findings appears in the online early May edition of the Proceedings of the National Academy of Sciences.
"Blocking one of these cell-recruiting signals in a mouse's tumor made it much less likely to metastasize or spread," says Gregg Semenza, M.D., Ph.D., a professor and director of the Vascular Biology Program in the Johns Hopkins University School of Medicine's Institute for Cell Engineering. "If a drug can be found that safely blocks the same signal in humans, it could be a very useful addition to current breast cancer treatment particularly for patients with chemotherapy-resistant tumors."
Semenza's research group studies a chemical signal called hypoxia-inducible factor 1 (HIF-1), which cells release to help them cope with low-oxygen conditions. Earlier, the group determined that HIF-1 helps breast tumor cells survive the low-oxygen conditions in which they often live, and spread to other parts of the body such as the lungs. "In breast cancer, it's not the original tumor that kills patients, but the metastases," says Semenza.
Also in a previous study, Semenza's group found that HIF-1 induced adult stem cells called mesenchymal stem cells release a signal to nearby breast cancer cells, which made them more likely to spread. The researchers suspected this communication might run both ways and that the stem cells' presence might also help the cancer to recruit the host animal's white blood cells. Breast cancers need the support of several types of host cells in order to metastasize, including mesenchymal stem cells and one type of white blood cell, Semenza notes.
Studying tumor cells grown in a dish, Semenza's team used chemicals that blocked the functions of various proteins to map a web of signals flying among breast cancer cells, menenchymal stem cells and white blood cells. One positive feedback loop brought mesenchymal stem cells close in to the breast cancer cells. A separate loop of signals between the stem cells and cancer cells caused the cancer cells to release a chemical "beacon" that drew in white blood cells. The concentrations of all the signals in the web were increased by the presence of HIF-1 and ultimately, by low-oxygen conditions.
The team then used genetic engineering to reduce the levels of the cell-recruiting signals in breast cancer cells and implanted those cells into female mice. Compared with unaltered breast cancer cells, those with reduced recruiting power grew into similar-sized tumors, Semenza says, but were much less likely to spread.
All of the breast cancer cells used in the study were so-called triple-negative, meaning they lack receptors for estrogen, progesterone and human epidermal growth factor receptor 2, so they do not respond to therapies that target those receptors. In people, triple-negative breast cancers also tend to be more deadly than other breast cancers because they contain more HIF-1, Semenza says. "This study adds to the evidence that a HIF-1 inhibitor drug could be an effective addition to chemotherapy regimens, especially for triple-negative breast cancers," he says. Several potential drugs of this kind are now in the early stages of development, he notes.
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Signals found that recruit host animals' cells, enabling breast cancer metastasis
Posted: May 23, 2014 at 7:41 pm
Paving the Way to New Liver Cancer Treatments
Research on liver cancer stem cells and cell signalling pathways by HKU academics offers insight into understanding liver cancer development and can help identify potential targets in novel...
By: ResearchatHKU