Archive for the ‘Skin Stem Cells’ Category

E Dermastamp at La Belle Forme in Glasgow
If you #39;re interested in the latest treatments aimed at treating fine lines, wrinkles, acne scars, stretch marks and damage caused by the sun, the E-Dermastam...

By: labelleformeglasgow

Read more here:
E Dermastamp at La Belle Forme in Glasgow - Video

LONDON In a north London hospital, scientists are growing noses, ears and blood vessels in the laboratory in a bold attempt to make body parts using stem cells.

It is among several labs around the world, including in the US, that are working on the futuristic idea of growing custom-made organs in the lab.

While only a handful of patients have received the British lab-made organs so far including tear ducts, blood vessels and windpipes researchers hope they will soon be able to transplant more types of body parts into patients, including what would be the worlds first nose made partly from stem cells.

Its like making a cake, said Alexander Seifalian at University College London, the scientist leading the effort. We just use a different kind of oven.

Dr. Michelle Griffin, a plastic surgery research fellow, holds a synthetic polymer ear.Photo: AP

During a recent visit to his lab, Seifalian showed off a sophisticated machine used to make molds from a polymer material for various organs.

Last year, he and his team made a nose for a British man who lost his to cancer. Scientists added a salt and sugar solution to the mold of the nose to mimic the somewhat sponge-like texture of the real thing. Stem cells were taken from the patients fat and grown in the lab for two weeks before being used to cover the nose scaffold. Later, the nose was implanted into the mans forearm so that skin would grow to cover it.

Seifalian said he and his team are waiting for approval from regulatory authorities to transfer the nose onto the patients face but couldnt say when that might happen.

The potential applications of lab-made organs appear so promising, even the city of London is getting involved: Seifalians work is being showcased on Tuesday as Mayor Boris Johnson announces a new initiative to attract investment to Britains health and science sectors so spin-off companies can spur commercial development of the pioneering research.

The polymer material Seifalian uses for his organ scaffolds has been patented and hes also applied for patents for their blood vessels, tear ducts and windpipe. He and his team are creating other organs including coronary arteries and ears. Later this year, a trial is scheduled to start in India and London to test lab-made ears for people born without them.

More here:
Sci-fi meets reality as stem cells are turned into noses, ears

Professor Alexander Seifalian poses for photographs with a synthetic polymer nose at his research facility in the Royal Free Hospital in London, Monday, March 31, 2014. In a north London hospital, scientists are growing noses, ears and blood vessels in the laboratory in a bold attempt to make body parts using stem cells. AP

In a north London hospital, scientists are growing noses, ears and blood vessels in the laboratory in a bold attempt to make body parts using stem cells.

It is among several labs around the world, including in the U.S., that are working on the futuristic idea of growing custom-made organs in the lab.

5 Photos

In a north London hospital, scientists are growing noses, ears and blood vessels in attempt to make body parts using stem cells

"It's like making a cake," said Alexander Seifalian at University College London, the scientist leading the effort. "We just use a different kind of oven."

During a recent visit to his lab, Seifalian showed off a sophisticated machine used to make molds from a polymer material for various organs.

Last year, he and his team made a nose for a British man who lost his to cancer. Scientists added a salt and sugar solution to the mold of the nose to mimic the somewhat sponge-like texture of the real thing. Stem cells were taken from the patient's fat and grown in the lab for two weeks before being used to cover the nose scaffold. Later, the nose was implanted into the man's forearm so that skin would grow to cover it.

Seifalian said he and his team are waiting for approval from regulatory authorities to transfer the nose onto the patient's face but couldn't say when that might happen

The potential applications of lab-made organs appear so promising even the city of London is getting involved: Seifalian's work is being showcased on Tuesday as Mayor Boris Johnson announces a new initiative to attract investment to Britain's health and science sectors so spin-off companies can spur commercial development of the pioneering research.

Go here to read the rest:
Ears, noses grown from stem cells in lab dishes

London's Royal Free hospital is among several in the world that are working on the futuristic idea of growing custom-made organs in the lab Few have received the lab-made organs so far - including ears and windpipes - but researchers hope they will soon transplant more They hope to transplant world's first nose made partly from stem cells

By Associated Press and Ellie Zolfagharifard

Published: 05:38 EST, 8 April 2014 | Updated: 10:51 EST, 8 April 2014

101 shares

17

View comments

At London's Royal Free hospital, scientists are growing noses, ears and blood vessels in the laboratory in a bold attempt to make body parts using stem cells.

It is among several labs around the world, including in the U.S., that are working on the futuristic idea of growing custom-made organs in the lab.

Only a handful of patients have received the British lab-made organs so far - including tear ducts, blood vessels and windpipes.

But researchers hope they will soon be able to transplant more types of body parts into patients, including what would be the world's first nose made partly from stem cells.

Read the original:
British scientists make custom-made body parts using stem cells

AP Photo/Matt Dunham Dr Michelle Griffin, a plastic research fellow, poses for photographs with a synthetic polymer ear at her research facility in the Royal Free Hospital in London, Monday, March 31, 2014. In a north London hospital, scientists are growing noses, ears and blood vessels in the laboratory in a bold attempt to make body parts using stem cells.

By MARIA CHENG/AP Medical Writer/April 8, 2014

LONDON (AP) In a north London hospital, scientists are growing noses, ears and blood vessels in a bold attempt to make body parts in the laboratory.

Its far from the only lab in the world that is pursuing the futuristic idea of growing organs for transplant. But the London work was showcased Tuesday as Mayor Boris Johnson announced a plan to attract more labs to do cutting-edge health and science research in the area.

While only a handful of patients have received the British lab-made organs so far including tear ducts, blood vessels and windpipes researchers hope they will soon be able to transplant more types of body parts into patients, including what would be the worlds first nose made partly from stem cells.

Its like making a cake, said Alexander Seifalian at University College London, the scientist leading the effort. We just use a different kind of oven.

British authorities have invested nearly 4 million pounds ($6.7 million) in the plan to stimulate research in the London-Oxford-Cambridge area. It aims to attract companies to the area to foster collaboration and promote research and manufacturing. A major center for biological research will open in London next year.

University College London is a partner in the campaign. During a recent visit to his lab there, Seifalian showed off a sophisticated machine used to make molds from a polymer material for various organs.

Last year, he and his team used that material to mold a nose for a British man who lost his to cancer. Then they added a salt and sugar solution to the mold to mimic the somewhat sponge-like texture of a natural nose. Stem cells were taken from the patients fat and grown in the lab for two weeks before being used to cover the nose scaffold. Later, the nose was implanted into the mans forearm so that skin would grow to cover it.

Seifalian said he and his team are waiting for approval from regulatory authorities to transfer the nose onto the patients face but couldnt say when that might happen.

Read more:
UK scientists make body parts in lab

Jeunesse Luminesce Ultimate Lifting Masque
How would you like to do something once a week that will change your life and make you look and feel better about yourself? Well, this is what you do. You si...

By: allen hookens

Continued here:
Jeunesse Luminesce Ultimate Lifting Masque - Video

Irvine, CA (PRWEB) April 03, 2014

DrSkinSpa.com is a top-tier skin care web-retail store. It places its primary focus on bringing clinically tested skin care creations that are manufactured using naturally derived ingredients. The company proudly markets an extensive line of natural and effective anti wrinkle cream skin products. Skin care rejuvenators are just one of the many categories of beauty products sold here and DrSkinSpa.com has just added Eminence Bamboo Firming Fluid, 1.2 oz. to its extensive line.

The organic skin care product that is Eminence Bamboo Firming Fluid, 1.2 oz., contains an abundance of plant ingredients, essential oils, and anti-aging Swiss Green Apple Stem Cells. When placed together in this anti aging products, wrinkles and lines are smoothed, hydrated, and the skin is firmed up for a younger appearance.

The key ingredients in Eminence Bamboo Firming Fluid, 1.2 oz. include bamboo, both coconut oil and water, a natural retinol alternative complex with chicory root and tara tree, Swiss Green Apple Stem Cells, and monoi, a fragrant and firming Tahitian oil.

Bamboo has both soluble and insoluble fiber, free-radical fighting antioxidants, proteins, skin-enriching vitamins and minerals to help firm and anti age skin. Coconut oil is included in Eminence Bamboo Firming Fluid, 1.2 oz., for its moisturizing effects, which also help restore skins natural moisture barrier. This oil also works as an antioxidant. The coconut water in this serum balances the skins pH, returning moisture to skin; it also tones the complexion. Coconut water has natural reserves of Vitamin C, electrolytes, calcium, potassium and phosphorous, all plusses for both skin and body.

The Natural Retinol Alternative Complex in Eminence Bamboo Firming Fluid, 1.2 oz., is a combination of chicory root natural sugars (oligosaccharides) and tara tree. The sugars from chicory root firm up loose and sagging skin with immediate activity. It also increases collagen synthesis. Tara tree provides long-lasting moisture.

Dr. Farid Mostamand, owner of DrSkinSpa.com, says, Eminence Bamboo Firming Fluid, 1.2 oz., contains the patented PhytoCellTec. These are the Swiss Green Apple Stem Cells concentrate formula that has been clinically shown to reduce and prevent signs of aging.

DrSkinSpa.com is doctor operated and owned. The company studies and choosesfor sale only the finest products, with clinically proven and natural ingredients. DrSkinSpa.com extends to customers a two-week money-back guarantee for every product sold on their web site. The site also provides customers with a 120% price protection warranty in addition to no cost shipping. Complimentaryaesthetician consultations are also available. DrSkinSpa.com is owned by Crescent Health Center and is based in Anaheim, California.

Link:
DrSkinSpa.com Announces the Addition of Eminence Bamboo Firming Fluid, 1.2 oz.

A genetic tweak can make light work of some nervous disorders. Using flashes of light to stimulate modified neurons can restore movement to paralysed muscles. A study demonstrating this, carried out in mice, lays the path for using such "optogenetic" approaches to treat nerve disorders ranging from spinal cord injury to epilepsy and motor neuron disease.

Optogenetics has been hailed as one of the most significant recent developments in neuroscience. It involves genetically modifying neurons so they produce a light-sensitive protein, which makes them "fire", sending an electrical signal, when exposed to light.

So far optogenetics has mainly been used to explore how the brain works, but some groups are exploring using it as therapy. One stumbling block has been fears about irreversibly genetically manipulating the brain.

In the latest study, a team led by Linda Greensmith of University College London altered mouse stem cells in the lab before transplanting them into nerves in the leg this means they would be easier to remove if something went wrong.

"It's a very exciting approach that has a lot of potential," says Ziv Williams of Harvard Medical School in Boston.

Greensmith's team inserted an algal gene that codes for a light-responsive protein into mouse embryonic stem cells. They then added signalling molecules to make the stem cells develop into motor neurons, the cells that carry signals to and from the spinal cord to the rest of the body. They implanted these into the sciatic nerve which runs from the spinal cord to the lower limbs of mice whose original nerves had been cut.

After waiting five weeks for the implanted neurons to integrate with the muscle, Greensmith's team anaesthetised the mice, cut open their skin and shone pulses of blue light on the nerve. The leg muscles contracted in response. "We were surprised at how well this worked," says Greensmith.

Most current approaches being investigated to help people who are paralysed involve electrically stimulating their nerves or muscles. But this can be painful because they may still have working pain neurons. Plus, the electricity makes the muscles contract too forcefully, making them tire quickly.

Using the optogenetic approach, however, allows the muscle fibres to be stimulated more gently, because the light level can be increased with each pulse. "It gives a very smooth contraction," says Greensmith.

To make the technique practical for use in people, the researchers are developing a light-emitting diode in the form of a cuff that would go around the nerve, which could be connected to a miniature battery pack under the skin.

Original post:
Muscle paralysis eased by light-sensitive stem cells

Just weeks after invalidating a groundbreaking paper describing a simple technique for generating pluripotent stem cells, professor Kenneth Ka Ho Lee now believes he has identified the correct approach.

Lee, chief of stem cell research at the Chinese University of Hong, spoke to Wired.co.uk in March about his tentative excitement when he read the Nature study in question, published at the start of the year. The proposed Stap cells (stimulus-triggered acquisition of pluripotency) in it were a revelation, because they suggested there was a simple way to generate embryonic-like stem cells that could potentially be used in the treatment of diseases such as Parkinson's. The method involved reprogramming a donor's own adult blood and skin cells (in this case, mice) by exposing them to extreme trauma, such as an acid bath.

Lee could see its potential, but like the rest of the community he had his doubts. While reports circulated that the images published in the Nature study also featured in older papers penned by lead researcher Haruko Obokata of Japan's Riken Centre, Lee set about trying to replicate the experiment himself.

It didn't work.

Since then the Riken Centre has launched an investigation into the legitimacy of the trial, and that investigation today revealed Obokata had indeed falsified information, including results and images of DNA fragments used.

"Actions like this completely destroy data credibility," commented Shunsuke Ishii, head of the investigative committee and a Riken molecular geneticist, at a press conference. "There is no doubt that she was fully aware of this danger. We've therefore concluded this was an act of research misconduct involving fabrication." Obokata has denied the allegations, but Riken says its own research team will be the one to verify the results and carry out the experiment again.

In the interim however, a coauthor on the paper at the centre of the debacle,Charles Vacanti published yet another protocol for the Stap technique, fairly different from the original. Vacanti, of ear-on-a-mouse fame, is a professor at Harvard Medical School and published online what he said was found to be "an effective protocol for generating Stap cells in our lab, regardless of the cell type being studied". It was a combination of the two approaches mentioned in the Naturepaper -- the acid bath, and the trituration process (the application of pressure on the cells using pipettes to induce stress). He describes the latter process as being exerted with force, more so than in the original paper, and over a lengthy period -- twice a day for the first week.

Nature had already rejected Lee's version of experiments for publication last month. Undeterred, he set about applying Vacanti's technique. Liveblogging the experiments on ResearchGate, the open source platform where Lee had published his first set of experiments, the Hong Kong researcher immediately saw the excess stress was leading to rapid cell death among the lung fibroblast cells used.

"The Vacanti protocol put a deal of emphasis on mechanically passing the cells through narrow bore glass pipettes for 30 minutes before acid treatment and then growing the cells on non-adhesive culture plates," Lee told Wired.co.uk. "We conducted these experiments, but it did not induce expression of the pluripotent stem cell markers (Oct4, Sox2 and Nanog)."

Nevertheless, things appeared to turn around. In his preliminary studies Lee has concluded that it could be the extreme stress through trituration, and not the acid bath, that was responsible for creating the Stap cells.

Continue reading here:
'Fabricated' stem cell paper technique may yet be proven valid

I WAS a bit apprehensive when asked to test the La Mer lifting and firming mask. The first time I tried a La Mer product the Lifting Contour Serum it did not give good results.

This was a high-end sculpting serum for face and neck, said to give skin a tighter feel and visibly define and re-shape contours as well as redefine the appearance of the skin.

It is claimed that after using the serum for four weeks, the contours of the jaw line would look more lifted and skin appear firm and more defined.

Unfortunately, I did not get the promised results. In fact, after using it for four days, my skin turned red. I felt a stinging sensation when I applied the serum. Then my skin started to peel, especially on my forehead and cheeks. There was also a small red patch near my right eye. Clearly, some ingredients in the serum did not react well with my skin.

Worried that it would turn worse, I stopped using the serum. La Mer consultant education manager Carina Choo wanted to find out what was wrong.

TOO DRY After discussing my skincare regime, she thought it could be that my skin was dry. The serum tried to repair my skin cells which resulted in the peeling and a stinging sensation.

Well, I do have dry skin. For the past few years, I have been using a moisturiser during the day to ease the problem. Choo said while it is good to do so, it is more important to use skincare products at night.

Our skin is repaired between 10pm and 2am. This is why we need to go to sleep before 10pm so that our skin can get enough rest. Before that, it is important to wash the face, use a toner and apply moisturiser that does not have a sun protection factor.

She suggested that I try the lifting and firming mask which works to repair skin at night. It is a sleep-on mask and works well at night to repair skin.

Choo said the mask boosts skin energy and encourages cell renewal for more radiant and retexturised skin. So, you literally wake up to beautiful skin.

View original post here:
TRIED & TESTED: Wake up to beautiful skin

Just weeks after invalidating a groundbreaking paper describing a simple technique for generating pluripotent stem cells, professor Kenneth Ka Ho Lee now believes he has identified the correct approach.

Lee, chief of stem cell research at the Chinese University of Hong, spoke to Wired.co.uk in March about his tentative excitement when he read the Nature study in question, published at the start of the year. The proposed Stap cells (stimulus-triggered acquisition of pluripotency) in it were a revelation, because they suggested there was a simple way to generate embryonic-like stem cells that could potentially be used in the treatment of diseases such as Parkinson's. The method involved reprogramming a donor's own adult blood and skin cells (in this case, mice) by exposing them to extreme trauma, such as an acid bath.

Lee could see its potential, but like the rest of the community he had his doubts. While reports circulated that the images published in the Nature study also featured in older papers penned by lead researcher Haruko Obokata of Japan's Riken Centre, Lee set about trying to replicate the experiment himself.

It didn't work.

Since then the Riken Centre has launched an investigation into the legitimacy of the trial, and that investigation today revealed Obokata had indeed falsified information, including results and images of DNA fragments used.

"Actions like this completely destroy data credibility," commented Shunsuke Ishii, head of the investigative committee and a Riken molecular geneticist, at a press conference. "There is no doubt that she was fully aware of this danger. We've therefore concluded this was an act of research misconduct involving fabrication." Obokata has denied the allegations, but Riken says its own research team will be the one to verify the results and carry out the experiment again.

In the interim however, a coauthor on the paper at the centre of the debacle,Charles Vacanti published yet another protocol for the Stap technique. Vacanti, of ear-on-a-mouse fame, is a professor at Harvard Medical School and published online what he said was found to be "an effective protocol for generating Stap cells in our lab, regardless of the cell type being studied". It was a combination of the two approaches mentioned in the Naturepaper -- the acid bath, and the trituration process (the application of pressure on the cells using pipettes to induce stress). He describes the latter process as being exerted with force, more so than in the original paper, and over a lengthy period -- twice a day for the first week.

Nature had already rejected Lee's version of experiments for publication last month. Undeterred, he set about applying Vacanti's technique. Liveblogging the experiments on ResearchGate, the open source platform where Lee had published his first set of experiments, the Hong Kong researcher immediately saw the excess stress was leading to rapid cell death among the lung fibroblast cells used.

"We estimated that there was a 50 percent decrease in cell number," Lee wrote four days ago on the blog. "In the original paper reported in Nature, such decrease in cell count was reported for day two, which is inline with our current experiment. Day three will be critical as this was the time Oct4-GFP expression [an indication that stem cells are generating] was reported for Stap cells. If we find that the cell number decreased even more drastically in our cultures, we will harvest some of the cultures and use them directly for qPCR analysis [quantitative polymerase chain reaction,a screening technique for stem cells]."

Nevertheless, things appeared to turn around. In his preliminary studies Lee has concluded that it could be the extreme stress through trituration, and not the acid bath, that was responsible for creating the Stap cells. "I am shocked and amazed by the qPCR results for the three-day-old control and Stap cultures," he wrote on ResearchGate, alongside a graph of the results. "Totally speechless!"

See more here:
'Fabricated' stem cell paper may have just been proven valid

St. Petersburg, FL (PRWEB) April 01, 2014

Sublime Beauty has recently introduced its newest serum which makes a positive impact on aging skin within 30 days.

Cell Renewal | Fibroblast Serum is discounted 35% for 2 days only at the company webstore, SublimeBeautyShop with coupon code CELLRENEW35.

"A key ingredient is Human Fibroblast Conditioned Media, rich in proteins and growth factors, that instruct the skin's fibroblasts to product collagen," says Kathy Heshelow, founder of Sublime Beauty. "The non-embryonic stem cells are powerful indeed - no fillers are used."

The company offers a free brochure about the ingredients on the product page. "We find that our customers want to know about ingredients in the product, what they do and what to expect." says Heshelow. "We offer lots of education on our products."

Sublime Beauty focuses on anti-aging and healthy-skin oriented products, from Skin Brushing and collagen boosters to organic products for the skin. It specializes in serums.

The company offers free standard shipping within the continental U.S and a Sublime Beauty VIP Club. Interested clients can sign up for secret deals and deep discounts as well.

The 35% off sale ends Wednesday at midnight.

Excerpt from:
The New Scientific Serum That Helps Skin Become Younger and Healthier on Sale at Sublime Beauty Now

These neurons derived from stem cells made from the skin of people with bipolar disorder communicated with one another differently than neurons made from the skin of people without bipolar disorder.(Credit: University of Michigan)

Bipolar disorder is known to run in families, but scientists have yet to pinpoint the genes involved. Now they have a powerful new tool in the hunt: stem cells.

In a first-of-its-kind procedure, researchers from the University of Michigan have created stem cells from the skin of people with bipolar disorder, and then coaxed the cells into neurons. This has allowed scientists, for the first time, to directly measure cellular differences between people with bipolar disorder and people without.

In the future the cells could provide a greater understanding of what causes the disease, and allow for the development of personalized medications specific to each patients cells.

The team from Michigan took skin cell samples from 22 people with bipolar disorder and 10 people without the disorder. Under carefully controlled conditions, they coaxed adult skin cells into an embryonic stem cell-like state. These cells, called induced pluripotent stem cells, then had the potential to transform into any type of cell. With further coaxing, the cells became neurons.

This gives us a model that we can use to examine how cells behave as they develop into neurons. Already, we see that cells from people with bipolar disorder are different in how often they express certain genes, how they differentiate into neurons, how they communicate, and how they respond to lithium, study co-leader Sue OShea said in a news release.

Researchers published their findings Wednesday in the journalTranslational Psychiatry.

The research team discovered intriguing differences between stem cellsand neuronsfrom bipolar individuals and those from healthy people.

For one thing, bipolar stem cells expressed more genes associated with receiving calcium signals in the brain. Calcium signals play an important role in neuron development and function. Therefore, the new findings support the idea that genetic differences expressed early in life may contribute to the development of bipolar disorder later in life.

Once the stem cells turned into neurons, researchers tested how they reacted to lithium, a typical treatment for the disorder. The tests showed that lithium normalized the behavior of neurons from bipolar patients by altering their calcium signalingfurther confirmation that this cellular pathway should be of key interest in future studies of the disease.

View original post here:
Stem Cells Shed Light on Treatments for Bipolar Disorder

TUESDAY, March 25, 2014 (HealthDay News) -- Brain cells of patients with bipolar disorder act differently than those of people without the mental illness, according to scientists who conducted a stem cell study of the condition.

The investigators said their research might one day lead to a better understanding of bipolar disorder and new treatments for the disease, which causes extreme emotional highs and lows. About 200 million people worldwide have bipolar disorder.

"We're very excited about these findings. But we're only just beginning to understand what we can do with these cells to help answer the many unanswered questions in bipolar disorder's origins and treatment," said study co-leader Dr. Melvin McInnis, a professor of bipolar disorder and depression at the University of Michigan Medical School.

The study authors took skin stem cells from people with and without bipolar disorder and transformed them into neurons similar to brain cells. It's the first time that stem cell lines specific to bipolar disorder have been created, the researchers said.

They discovered distinct differences in how the two sets of neurons behave and communicate with each other. The cells also differed in their response to lithium, the most widely used treatment for bipolar disorder.

The study was published online March 25 in the journal Translational Psychiatry.

"This gives us a model that we can use to examine how cells behave as they develop into neurons," study co-leader Sue O'Shea, a professor in the department of cell and developmental biology and director of the University of Michigan Pluripotent Stem Cell Research Lab, said in a university news release.

"Already, we see that cells from people with bipolar disorder are different in how often they express certain genes, how they differentiate into neurons, how they communicate, and how they respond to lithium," O'Shea said.

McInnis said it's possible the research could lead to new types of drug trials. If it becomes possible to test new drug candidates in these cells, patients would be spared the current trial-and-error approach that leaves many with uncontrolled symptoms, he said.

More information

Here is the original post:
Scientists use stem cells to study bipolar disorder

By Liisa Vexler

University of Michigan scientists have managed to create brain cells from embryonic-like stem cells that they have grown from individuals with bipolar disorder, and these brain cells are providing insight into some of the mysteries of the psychiatric condition. The new cells, which maintain the specific genetic information from the patients own cells, show different characteristics and behaviors than those from individuals without bipolar disorder.

Already, we see that cells from people with bipolar disorder are different in how often they express certain genes, how they differentiate into neurons, how they communicate, and how they respond to lithium," said lead scientist Sue O'Shea. The study published in Translational Psychiatry is one of the first to use stem cell research to examine a patients own cells to learn more about his or her medical condition.

Diseases of the mind are some of the hardest to study since the living brain is still such an enigma. Trying to create mental illness in laboratory animal experiments is difficult since determining presence of the disease is not specific.

In this study, researchers looked at induced pluripotent stem cells, also known as iPS cells. These cells are transformed from ordinary human skin cells into their state as just-conceived embryonic cells. The Michigan research team demonstrated differences in cell behavior between the cells taken from patients with bipolar disorder and those without the disorder. The cells they used became pluripotent, which means they can be transformed or tricked into becoming any type of cell. In this case, they were turned into neurons, a type of brain cell. This gives us a model that we can use to examine how cells behave as they develop into neurons, OShea explained.

Bipolar disorder, known as manic-depression in the past, affects approximately three percent of the worlds population. It is hereditary and is distinguished by distinct mood swings from depression to elation. According to the National Institute on Mental Health, in about 50% of cases, bipolar disorder takes hold before the patient turns 25. Existing treatments are still hit and missand include lithium, antidepressants and antipsychotics.

Go here to read the rest:
Bipolar Disorder Benefits from Stem Cell Research

Contact Information

Available for logged-in reporters only

Newswise Scientists at University of California, San Diego School of Medicine and Sanford-Burnham Medical Research Institute have shown that by encapsulating immature pancreatic cells derived from human embryonic stem cells (hESC), and implanting them under the skin of diabetic mouse models, sufficient insulin is produced to maintain glucose levels without unwanted potential trade-offs of the technology.

The research, published online in Stem Cell Research, suggests that encapsulated hESC-derived insulin-producing cells may be an effective and safe cell replacement therapy for insulin dependent-diabetes.

Our study critically evaluates some of the potential pitfalls of using stem cells to treat insulin dependent-diabetes, said Pamela Itkin-Ansari, PhD, assistant project scientist in the UC San Diego Department of Pediatrics and adjunct assistant professor in Development, Aging and Regenerative program at Sanford-Burnham.

We have shown that encapsulated hESC-derived insulin-producing cells are able to produce insulin in response to elevated glucose without an increase in the mass or their escape from the capsule, said Itkin-Ansari. These results are important because it means that the encapsulated cells are both fully functional and retrievable.

Previous attempts to replace insulin producing cells, called beta cells, have met with significant challenges. For example, researchers have tried treating diabetics with mature beta cells, but because these cells are fragile and scarce, the method is fraught with problems. Moreover, since the cells come from organ donors, they may be recognized as foreign by the recipients immune system requiring patients to take immunosuppressive drugs to prevent their immune system from attacking the donors cells, ultimately leaving patients vulnerable to infections, tumors and other adverse events.

Encapsulation technology was developed to protect donor cells from exposure to the immune system and has proven extremely successful in preclinical studies.

Itkin-Ansari and her research team previously made an important contribution to the encapsulation approach by showing that pancreatic islet progenitor cells are an optimal cell type for encapsulation. They found that progenitor cells were more robust than mature beta cells to encapsulate, and while encapsulated, they matured into insulin-producing cells that secreted insulin only when needed.

In the study, Itkin-Ansari and her team used bioluminescent imaging to determine if encapsulated cells stay in the capsule after implantation.

View post:
Stem Cell-Derived Beta Cells Under Skin Replace Insulin

Researchers have grown embryonic-like stem cells from patients with bipolar disorder and transformed them into brain cells that are already answering questions about the condition.

The cells, which carry the precisely tailored genetic instructions from the patients own cells, behave differently than cells taken from people without the disorder, the researchers report.

Already, we see that cells from people with bipolar disorder are different in how often they express certain genes, how they differentiate into neurons, how they communicate, and how they respond to lithium," Sue O'Shea, a stem cell specialist at the University of Michigan who led the study, said in a statement.

The work, described in the journal Translational Psychiatry, helps fulfill one of the big promises of stem cells research using a patients own cells to study his or her disease.

Mental illness is especially hard to study. Getting into a living persons brain is almost impossible, and scientists cant deliberately cause it in people in order to study it.

Creating animals such as mice with what looks like human mental illness is imprecise at best.

The University of Michigan team turned instead to what are called induced pluripotent stem cells, or iPS cells. These are ordinary skin cells taken from a patient and tricked into turning back into the state of a just-conceived embryo.

These cells, grown from skin cells taken from people with bipolar disorder, arose from stem cells and were coaxed to become neural progenitor cells -- the kind that can become any sort of nervous system cell. The research showed differences in cell behavior compared with cells grown from people without bipolar disorder.

They are pluripotent, meaning they can become any type of cell there is. In this case, the Michigan team redirected the cells to become neurons the cells that make up much of the brain. "This gives us a model that we can use to examine how cells behave as they develop into neurons, OShea said.

Bipolar disorder, once called manic-depression, is very common, affecting an estimated 3 percent of the population globally. It runs in families, suggesting a strong genetic cause, and is marked by mood swings from depression to feelings of euphoria and creativity thats considered the manic phase.

Continue reading here:
Stem Cells Shed Light on Bipolar Disorder

Researchers have grown embryonic-like stem cells from patients with bipolar disorder and transformed them into brain cells that are already answering questions about the condition.

The cells, which carry the precisely tailored genetic instructions from the patients own cells, behave differently than cells taken from people without the disorder, the researchers report.

Already, we see that cells from people with bipolar disorder are different in how often they express certain genes, how they differentiate into neurons, how they communicate, and how they respond to lithium," Sue O'Shea, a stem cell specialist at the University of Michigan who led the study, said in a statement.

The work, described in the journal Translational Psychiatry, helps fulfill one of the big promises of stem cells research using a patients own cells to study his or her disease.

Mental illness is especially hard to study. Getting into a living persons brain is almost impossible, and scientists cant deliberately cause it in people in order to study it.

Creating animals such as mice with what looks like human mental illness is imprecise at best.

The University of Michigan team turned instead to what are called induced pluripotent stem cells, or iPS cells. These are ordinary skin cells taken from a patient and tricked into turning back into the state of a just-conceived embryo.

These cells, grown from skin cells taken from people with bipolar disorder, arose from stem cells and were coaxed to become neural progenitor cells -- the kind that can become any sort of nervous system cell. The research showed differences in cell behavior compared with cells grown from people without bipolar disorder.

They are pluripotent, meaning they can become any type of cell there is. In this case, the Michigan team redirected the cells to become neurons the cells that make up much of the brain. "This gives us a model that we can use to examine how cells behave as they develop into neurons, OShea said.

Bipolar disorder, once called manic-depression, is very common, affecting an estimated 3 percent of the population globally. It runs in families, suggesting a strong genetic cause, and is marked by mood swings from depression to feelings of euphoria and creativity thats considered the manic phase.

Read the original:
Stem Cells Shed Light On Bipolar Disease

Harvesting samples for producing stem cells can be rather painful. Techniques can involve collecting large amounts of blood, bone marrow or skin scrapes. The reality is intrusive measures such as these can be very off-putting. But what if it was as simple as a finger-prick? Such a DIY approach, which is so easy it can be done at home or in the field without medical staff, has been developed by researchers at Singapore's A*STAR Institute of Molecular and Cell Biology (IMCB).

Unlike previous techniques that require comparatively large cell samples, the ICMB team has managed to successfully reprogram mature human cells into hiPSCs with high efficiency using less than a single drop of blood. Pluripotent stem cells are important in many forms of medical research and treatment as they have the potential to become any other cell type in the body.

"It all began when we wondered if we could reduce the volume of blood used for reprogramming," says Dr Loh Yuin Han Jonathan, Principal Investigator at IMCB. "We then tested if donors could collect their own blood sample in a normal room environment and store it. Our finger-prick technique, in fact, utilized less than a drop of finger-pricked blood."

It is hoped that this much less invasive method of sample collection will help attract more donors to increase the samples available to researchers. Blood samples have been found to remain viable for 48 hours after collection and in culture this can be extended to 12 days, opening up remote areas for potential cell harvesting. This could benefit research and treatment with the recruitment of donors with varied ethnicities, genotypes and diseases now possible. It is hoped the technique will also lead to the establishment of large-scale hiPSC banks.

"We were able to differentiate the hiPSCs reprogrammed from Jonathans finger-prick technique, into functional heart cells," says Dr Stuart Alexander Cook, Senior Consultant at the National Heart Centre Singapore and co-author of the paper. "This is a well-designed, applicable technique that can unlock unrealized potential of biobanks around the world for hiPSC studies at a scale that was previously not possible."

The team has filed a patent for their innovation and their paper has been published online at Stem Cell Translational Medicine.

Source: A*STAR

Original post:
Finger-prick technique opens door for DIY stem cell donors

When it comes to understanding bipolar disorder, many questions remain unanswered such as what truly causes the condition and why finding proper treatments is so difficult.

But now, researchers have taken a huge step towards solving some of the disorders complex mysteries.

Through groundbreaking stem cell research, scientists from the University of Michigan Medical School and the Heinz C. Prechter Bipolar Researcher Fund transformed skin cells from people with bipolar disorder into neurons that mimicked those found in their brains. They were then able to compare these nerve stem cells with cells derived from people without bipolar disorder and study how the neurons responded to medications for the condition.

Detailed in the journal Translational Psychiatry, this study marks the first time researchers have derived a stem cell line specific to bipolar disorder.

Once we have derived nerve cells, were able to study those cells and determine how they behave compared to other cells and how they behave in response to medications, principal investigator Dr. Melvin McInnis, of the Prechter Bipolar Research Fund, told FoxNews.com. So if we can understand the basic biological problems with these cells, we can potentially identify interventions that further how we understand the illness and how we treat it.

Also known as manic-depressive illness, bipolar disorder is a brain condition characterized by intense shifts in mood alternating between periods of high energy and mania to periods of severe anxiety and depression. While the condition is known to run in families, scientists still arent fully certain what causes its development, believing it to be a combination of genetics and other factors.

Additionally, the most common form of treatment for the disorder, lithium, is also somewhat of a mystery.

We really do not know and understand what drives these fluctuations in moods; we dont understand how the medications truly work that help individuals with variability in their moods, McInnis said. We dont know why an individual will become ill at a particular time. All we know is really at an observational level.

In order to better understand what is happening in the bipolar mind, McInnis and his team took small samples of skin from individuals who had been diagnosed with bipolar disorder. These samples were then exposed to specific growth factors, which coaxed the cells into becoming induced pluripotent stem cells (iPSCs) meaning they had the ability to turn into any type of cell. Subsequently, the cells were exposed to an additional set of growth factors, which coaxed them into becoming neurons.

This process has also been used to better understand other complex brain disorders, such as schizophrenia and conditions that cause seizures. According to McInnis, the technique allows researchers to examine how cells behave as they develop into a whole new type of cell, as well as how they function when they finally become neurons.

See the original post here:
Bipolar disorder breakthrough

Contact Information

Available for logged-in reporters only

Newswise MADISON, Wis. Desperate patients are easy prey for unscrupulous clinics offering untested and risky stem cell treatments, says law and bioethics Professor Alta Charo of the University of Wisconsin-Madison, who is studying stem cell tourism.

Stem cells are cells that can form many types of cells in the body, and that makes them inherently promising and dangerous. Stem cell tourism refers to people traveling, both within the U.S. and abroad, in pursuit of advertised stem cell therapies to purportedly treat a variety of medical conditions.

The evidence for therapeutic use of stem cells is very limited, except for bone marrow stem cells, but patients all over the world are convinced stem cells will cure their disease, says Charo. While there are some very promising results in the early clinical trials for stem cell therapies using embryonic and other kinds of stem cells, the treatments being advertised by these clinics are dubious, mostly ineffective, and sometimes positively harmful.

Patients are being hoodwinked, but there are dilemmas about tackling (the treatments) at regulatory or political levels.

The outrage over failures in stem cell tourism is limited, Charo says. Patients may pay tens of thousands of dollars for procedures that may carry no promise of success or carry grievous risks of failure. Most people have no reason to pay attention, and those who are paying attention are sick, so they are focused on trying anything, Charo says. If it does not work, they are already in a bad position with plenty to think about.

During a search for stem cell therapies on the web, Charo found products that supposedly enhance the natural formation of stem cells in the skin alongside approved and unapproved treatments in the United States, and stem cell clinics outside the United States, like a stem cell treatment for spinal conditions that might be innocuous, but is probably useless.

Some American operators are trying to slip through Food and Drug Administration regulation, says Charo, who served as senior policy advisor in the Office of the Commissioner of the FDA between 2009 and 2011. The FDA regulates medical devices, tissue transplants and drugs, but not organ transplants or the way medicine is practiced.

To sell a product that can heal without claiming it is a drug, some clinics remove stem cells from a patient, grow them with minimal manipulation, and then reinsert the resulting cells back to the same patient. There has been a long-running battle over whether that is a tissue transplant akin to organ transplantation and thus the practice of medicine, or a tissue transplant that is acting like drug, Charo says. If the latter, then what you do is subject to FDA [regulation], so you have to prove that your product is safe and effective, which almost always requires expensive clinical trials.

More here:
'Stem Cell Tourism' Takes Advantage of Patients, Says Law Professor

For the first time, scientists have succeeded in coaxing laboratory cultures of human stem cells to develop into the specialized, unique cells needed to repair a patient's defective or diseased bladder.

The breakthrough, developed at the UC Davis Institute for Regenerative Cures and published today in the scientific journal Stem Cells Translational Medicine, is significant because it provides a pathway to regenerate replacement bladder tissue for patients whose bladders are too small or do not function properly, such as children with spina bifida and adults with spinal cord injuries or bladder cancer.

"Our goal is to use human stem cells to regenerate tissue in the lab that can be transplanted into patients to augment or replace their malfunctioning bladders," said Eric Kurzrock, professor and chief of the division of pediatric urologic surgery at UC Davis Children's Hospital and lead scientist of the study, which is titled "Induction of Human Embryonic and Induced Pluripotent Stem Cells into Urothelium."

To develop the bladder cells, Kurzrock and his UC Davis colleagues investigated two categories of human stem cells. In their key experiments, they used induced pluripotent stem cells (iPS cells), which were derived from lab cultures of human skin cells and umbilical blood cells that had been genetically reprogrammed to convert to an embryonic stem cell-like state.

If additional research demonstrates that grafts of bladder tissue grown from human stem cells will be safe and effective for patient care, Kurzrock said that the source of the grafts would be iPS cells derived from a patient's own skin or umbilical cord blood cells. This type of tissue would be optimal, he said, because it lowers the risk of immunological rejection that typifies most transplants.

In their investigation, Kurzrock and his colleagues developed a protocol to prod the pluripotent cells into becoming bladder cells. Their procedure was efficient and, most importantly, the cells proliferated over a long period of time -- a critical element in any tissue engineering application.

"What's exciting about this discovery is that it also opens up an array of opportunities using pluripotent cells," said Jan Nolta, professor and director of the UC Davis Stem Cell program and a co-author on the new study. "When we can reliably direct and differentiate pluripotent stem cells, we have more options to develop new and effective regenerative medicine therapies. The protocols we used to create bladder tissue also provide insight into other types of tissue regeneration."

UC Davis researchers first used human embryonic stem cells obtained from the National Institutes of Health's repository of human stem cells. Embryonic stem cells can become any cell type in the body (i.e., they are pluripotent), and the team successfully coaxed these embryonic stem cells into bladder cells. They then used the same protocol to coax iPS cells made from skin and umbilical cord blood into bladder cells, called urothelium, that line the inside of the bladder. The cells expressed a very unique protein and marker of bladder cells called uroplakin, which makes the bladder impermeable to toxins in the urine.

The UC Davis researchers adjusted the culture system in which the stem cells were developing to encourage the cells to proliferate, differentiate and express the bladder protein without depending upon signals from other human cells, said Kurzrock. In future research, Kurzrock and his colleagues plan to modify the laboratory cultures so that they will not need animal and human products, which will allow use of the cells in patients.

Kurzrock's primary focus as a physician is with children suffering from spina bifida and other pediatric congenital disorders. Currently, when he surgically reconstructs a child's defective bladder, he must use a segment of their own intestine. Because the function of intestine, which absorbs food, is almost the opposite of bladder, bladder reconstruction with intestinal tissue may lead to serious complications, including urinary stone formation, electrolyte abnormalities and cancer. Developing a stem cell alternative not only will be less invasive, but should prove to be more effective, too, he said.

More:
Stem cell findings may offer answers for some bladder defects, disease

PUBLIC RELEASE DATE:

21-Mar-2014

Contact: Charles Casey charles.casey@ucdmc.ucdavis.edu 916-734-9048 University of California - Davis Health System

(SACRAMENTO, Calif.) For the first time, scientists have succeeded in coaxing laboratory cultures of human stem cells to develop into the specialized, unique cells needed to repair a patient's defective or diseased bladder.

The breakthrough, developed at the UC Davis Institute for Regenerative Cures and published today in the scientific journal Stem Cells Translational Medicine, is significant because it provides a pathway to regenerate replacement bladder tissue for patients whose bladders are too small or do not function properly, such as children with spina bifida and adults with spinal cord injuries or bladder cancer.

"Our goal is to use human stem cells to regenerate tissue in the lab that can be transplanted into patients to augment or replace their malfunctioning bladders," said Eric Kurzrock, professor and chief of the division of pediatric urologic surgery at UC Davis Children's Hospital and lead scientist of the study, which is titled "Induction of Human Embryonic and Induced Pluripotent Stem Cells into Urothelium."

To develop the bladder cells, Kurzrock and his UC Davis colleagues investigated two categories of human stem cells. In their key experiments, they used induced pluripotent stem cells (iPS cells), which were derived from lab cultures of human skin cells and umbilical blood cells that had been genetically reprogrammed to convert to an embryonic stem cell-like state.

If additional research demonstrates that grafts of bladder tissue grown from human stem cells will be safe and effective for patient care, Kurzrock said that the source of the grafts would be iPS cells derived from a patient's own skin or umbilical cord blood cells. This type of tissue would be optimal, he said, because it lowers the risk of immunological rejection that typifies most transplants.

In their investigation, Kurzrock and his colleagues developed a protocol to prod the pluripotent cells into becoming bladder cells. Their procedure was efficient and, most importantly, the cells proliferated over a long period of time a critical element in any tissue engineering application.

"What's exciting about this discovery is that it also opens up an array of opportunities using pluripotent cells," said Jan Nolta, professor and director of the UC Davis Stem Cell program and a co-author on the new study. "When we can reliably direct and differentiate pluripotent stem cells, we have more options to develop new and effective regenerative medicine therapies. The protocols we used to create bladder tissue also provide insight into other types of tissue regeneration."

Continue reading here:
Stem cell findings may offer answers for some bladder defects and disease

SINGAPORE: Scientists at A*STAR's Institute of Molecular and Cell Biology (IMCB) have developed a method to generate human induced pluripotent stem cells (hiPSCs) from a single drop of finger-pricked blood.

The new technique could potentially boost the number and diversity of donors, and facilitate the setting up of large-scale hiPSC banks, said the Agency for Science, Technology and Research (A*STAR) in a news release on Thursday.

Current sample collection for reprogramming into human induced pluripotent stem cells include invasive methods, such as collecting cells from the bone marrow or skin, which may put off potential donors.

Although the stem cells may also be generated from blood cells, a large amount of blood is usually required.

But scientists at IMCB showed for the first time that single-drop volumes of blood are sufficient for reprogramming into human induced pluripotent stem cells.

As those cells show properties remarkably similar to human embryonic stem cells, they are invaluable for basic research, drug discovery and cell therapy.

The finger-prick technique is the world's first to use only a drop of finger-pricked blood to yield hiPSCs with high efficiency.

The work is published online in the Stem Cell Translational Medicine journal.

Lead scientist for the finger-prick hiPSC technique Dr Jonathan Loh Yuin Han said, "Our finger-prick technique, in fact, utilised less than a drop of finger-pricked blood. The remaining blood could even be used for DNA sequencing and other blood tests."

Senior consultant at the National Heart Centre Singapore and co-author of the paper, Dr Stuart Alexander Cook, said, "We were able to differentiate the hiPSCs reprogrammed from Jonathan's finger-prick technique, into functional heart cells."

The rest is here:
A*STAR scientists create stem cells from drop of blood

Scientists at A*STAR's Institute of Molecular and Cell Biology (IMCB) have developed a method to generate human induced pluripotent stem cells (hiPSCs) from a single drop of finger-pricked blood. The method also enables donors to collect their own blood samples, which they can then send to a laboratory for further processing. The easy access to blood samples using the new technique could potentially boost the recruitment of greater numbers and diversities of donors, and could lead to the establishment of large-scale hiPSC banks.

By genetic reprogramming, matured human cells, usually blood cells, can be transformed into hiPSCs. As hiPSCs exhibit properties remarkably similar to human embryonic stem cells, they are invaluable resources for basic research, drug discovery and cell therapy. In countries like Japan, USA and UK, a number of hiPSC bank initiatives have sprung up to make hiPSCs available for stem cell research and medical studies.

Current sample collection for reprogramming into hiPSCs include invasive measures such as collecting cells from the bone marrow or skin, which may put off many potential donors. Although hiPSCs may also be generated from blood cells, large quantities of blood are usually required. In the paper published online on the Stem Cell Translational Medicine journal, scientists at IMCB showed for the first time that single-drop volumes of blood are sufficient for reprogramming into hiPSCs. The finger-prick technique is the world's first to use only a drop of finger-pricked blood to yield hiPSCs with high efficiency. A patent has been filed for the innovation.

The accessibility of the new technique is further enhanced with a DIY sample collection approach. Donors may collect their own finger-pricked blood, which they can then store and send it to a laboratory for reprogramming. The blood sample remains stable for 48 hours and can be expanded for 12 days in culture, which therefore extends the finger-prick technique to a wide range of geographical regions for recruitment of donors with varied ethnicities, genotypes and diseases.

By integrating it with the hiPSC bank initiatives, the finger-prick technique paves the way for establishing diverse and fully characterised hiPSC banking for stem cell research. The potential access to a wide range of hiPSCs could also replace the use of embryonic stem cells, which are less accessible. It could also facilitate the set-up of a small hiPSC bank in Singapore to study targeted local diseases.

Dr Loh Yuin Han Jonathan, Principal Investigator at IMCB and lead scientist for the finger-prick hiPSC technique, said, "It all began when we wondered if we could reduce the volume of blood used for reprogramming. We then tested if donors could collect their own blood sample in a normal room environment and store it. Our finger-prick technique, in fact, utilised less than a drop of finger-pricked blood. The remaining blood could even be used for DNA sequencing and other blood tests."

Dr Stuart Alexander Cook, Senior Consultant at the National Heart Centre Singapore and co-author of the paper, said "We were able to differentiate the hiPSCs reprogrammed from Jonathan's finger-prick technique, into functional heart cells. This is a well-designed, applicable technique that can unlock unrealized potential of biobanks around the world for hiPSC studies at a scale that was previously not possible."

Prof Hong Wanjin, Executive Director at IMCB, said "Research on hiPSCs is now highly sought-after, given its potential to be used as a model for studying human diseases and for regenerative medicine. Translational research and technology innovations are constantly encouraged at IMCB and this new technique is very timely. We hope to eventually help the scientific community gain greater accessibility to hiPSCs for stem cell research through this innovation."

Story Source:

The above story is based on materials provided by A*STAR. Note: Materials may be edited for content and length.

Read this article:
Stem cells created from a drop of blood: DIY finger-prick technique opens door for extensive stem cell banking