Sunday, January 20, 2013

Researchers turn one form of neuron into another in the brain

Researchers turn one form of neuron into another in the brain [ Back to EurekAlert! ] Public release date: 20-Jan-2013
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Contact: Paola Arlotta
paola_arlotta@harvard.edu
Harvard University

Opening a new avenue in neurobiology

A new finding by Harvard stem cell biologists turns one of the basics of neurobiology on its head demonstrating that it is possible to turn one type of already differentiated neuron into another within the brain.

The discovery by Paola Arlotta and Caroline Rouaux "tells you that maybe the brain is not as immutable as we always thought, because at least during an early window of time one can reprogram the identity of one neuronal class into another," said Arlotta, an Associate Professor in Harvard's Department of Stem Cell and Regenerative Biology (SCRB).

The principle of direct lineage reprogramming of differentiated cells within the body was first proven by SCRB co-chair and Harvard Stem Cell Institute (HSCI) co-director Doug Melton and colleagues five years ago, when they reprogrammed exocrine pancreatic cells directly into insulin producing beta cells.

Arlotta and Rouaux now have proven that neurons too can change their mind. The work is being published on-line today (Jan. 20) by the journal Nature Cell Biology.

In their experiments, Arlotta targeted callosal projection neurons, which connect the two hemispheres of the brain, and turned them into neurons similar to corticospinal motor neurons, one of two populations of neurons destroyed in Amyotrophic Lateral Sclerosis (ALS), also known as Lou Gehrig's disease. To achieve such reprogramming of neuronal identity, the researchers used a transcription factor called Fezf2, which long as been known for playing a central role in the development of corticospinal neurons in the embryo.

What makes the finding even more significant is that the work was done in the brains of living mice, rather than in collections of cells in laboratory dishes. The mice were young, so researchers still do not know if neuronal reprogramming will be possible in older laboratory animals and humans. If it is possible, this has enormous implications for the treatment of neurodegenerative diseases.

"Neurodegenerative diseases typically effect a specific population of neurons, leaving many others untouched. For example, in ALS it is corticospinal motor neurons in the brain and motor neurons in the spinal cord, among the many neurons of the nervous system, that selectively die," Arlotta said. "What if one could take neurons that are spared in a given disease and turn them directly into the neurons that die off? In ALS, if you could generate even a small percentage of corticospinal motor neurons, it would likely be sufficient to recover basic functioning," she said.

The experiments that led to the new finding began five years ago, when "we wondered: in nature you never seen a neuron change identity; are we just not seeing it, or is this the reality? Can we take one type of neuron and turn it into another?" Arlotta and Rouaux asked themselves.

Over the course of the five years, the researchers analyzed "thousands and thousands of neurons, looking for many molecular markers as well as new connectivity that would indicate that reprogramming was occurring," Arlotta said. "We could have had this two years ago, but while this was a conceptually very simple set of experiments, it was technically difficult. The work was meant to test important dogmas on the irreversible nature of neurons in vivo. We had to prove, without a shadow of a doubt, that this was happening."

The work in Arlotta's lab is focused on the cerebral cortex, but "it opens the door to reprogramming in other areas of the central nervous system," she said.

Arlotta, an HSCI principal faculty member, is now working with colleague Takao Hensch, of Harvard's Department of Molecular and Cellular Biology, to explicate the physiology of the reprogrammed neurons, and learn how they communicate within pre-existing neuronal networks.

"My hope is that this will facilitate work in a new field of neurobiology that explores the boundaries and power of neuronal reprogramming to re-engineer circuits relevant to disease," said Paola Arlotta.

###

This work was financed by a seed grant from the Harvard Stem Cell Institute, and by support from the National Institutes of Health, and the Spastic Parapelgia Foundation.



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AAAS and EurekAlert! are not responsible for the accuracy of news releases posted to EurekAlert! by contributing institutions or for the use of any information through the EurekAlert! system.


Researchers turn one form of neuron into another in the brain [ Back to EurekAlert! ] Public release date: 20-Jan-2013
[ | E-mail | Share Share ]

Contact: Paola Arlotta
paola_arlotta@harvard.edu
Harvard University

Opening a new avenue in neurobiology

A new finding by Harvard stem cell biologists turns one of the basics of neurobiology on its head demonstrating that it is possible to turn one type of already differentiated neuron into another within the brain.

The discovery by Paola Arlotta and Caroline Rouaux "tells you that maybe the brain is not as immutable as we always thought, because at least during an early window of time one can reprogram the identity of one neuronal class into another," said Arlotta, an Associate Professor in Harvard's Department of Stem Cell and Regenerative Biology (SCRB).

The principle of direct lineage reprogramming of differentiated cells within the body was first proven by SCRB co-chair and Harvard Stem Cell Institute (HSCI) co-director Doug Melton and colleagues five years ago, when they reprogrammed exocrine pancreatic cells directly into insulin producing beta cells.

Arlotta and Rouaux now have proven that neurons too can change their mind. The work is being published on-line today (Jan. 20) by the journal Nature Cell Biology.

In their experiments, Arlotta targeted callosal projection neurons, which connect the two hemispheres of the brain, and turned them into neurons similar to corticospinal motor neurons, one of two populations of neurons destroyed in Amyotrophic Lateral Sclerosis (ALS), also known as Lou Gehrig's disease. To achieve such reprogramming of neuronal identity, the researchers used a transcription factor called Fezf2, which long as been known for playing a central role in the development of corticospinal neurons in the embryo.

What makes the finding even more significant is that the work was done in the brains of living mice, rather than in collections of cells in laboratory dishes. The mice were young, so researchers still do not know if neuronal reprogramming will be possible in older laboratory animals and humans. If it is possible, this has enormous implications for the treatment of neurodegenerative diseases.

"Neurodegenerative diseases typically effect a specific population of neurons, leaving many others untouched. For example, in ALS it is corticospinal motor neurons in the brain and motor neurons in the spinal cord, among the many neurons of the nervous system, that selectively die," Arlotta said. "What if one could take neurons that are spared in a given disease and turn them directly into the neurons that die off? In ALS, if you could generate even a small percentage of corticospinal motor neurons, it would likely be sufficient to recover basic functioning," she said.

The experiments that led to the new finding began five years ago, when "we wondered: in nature you never seen a neuron change identity; are we just not seeing it, or is this the reality? Can we take one type of neuron and turn it into another?" Arlotta and Rouaux asked themselves.

Over the course of the five years, the researchers analyzed "thousands and thousands of neurons, looking for many molecular markers as well as new connectivity that would indicate that reprogramming was occurring," Arlotta said. "We could have had this two years ago, but while this was a conceptually very simple set of experiments, it was technically difficult. The work was meant to test important dogmas on the irreversible nature of neurons in vivo. We had to prove, without a shadow of a doubt, that this was happening."

The work in Arlotta's lab is focused on the cerebral cortex, but "it opens the door to reprogramming in other areas of the central nervous system," she said.

Arlotta, an HSCI principal faculty member, is now working with colleague Takao Hensch, of Harvard's Department of Molecular and Cellular Biology, to explicate the physiology of the reprogrammed neurons, and learn how they communicate within pre-existing neuronal networks.

"My hope is that this will facilitate work in a new field of neurobiology that explores the boundaries and power of neuronal reprogramming to re-engineer circuits relevant to disease," said Paola Arlotta.

###

This work was financed by a seed grant from the Harvard Stem Cell Institute, and by support from the National Institutes of Health, and the Spastic Parapelgia Foundation.



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?


AAAS and EurekAlert! are not responsible for the accuracy of news releases posted to EurekAlert! by contributing institutions or for the use of any information through the EurekAlert! system.


Source: http://www.eurekalert.org/pub_releases/2013-01/hu-rto011713.php

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Baby Parakeets! - Classified Ad

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Created

January 18, 2013

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Want a beautiful, healthy, and friendly pet bird? Look no further! Not to sound like an infomercial, well to sound like an infomercial, but that's not the point. The point is, we at Keely's Keet's Aviary, a small (or large depending on how you look at it) home breeding hobby, have fantastic pet budgies/parakeets up for adoption!?

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Almost all year long our budgies are doing the budgie and giving us more budgies so we can share the joy these pint sized parrots bring to any person or family. Our birds are hand fed so even the most stubborn natured bird is socialized and used to people, so they are easy to bond with and train! (Which makes the sweet natured birds no effort at all!) Our parakeets are given high quality seeds, vitamins, and fresh fruits and vegetables daily. Sometimes they even eat better then us humans do.?

Blue your favorite color? How about yellow? Can't decide? Get a blue bird with a yellow head! A type of bird we commonly get. From the odd albino to the common green and everything in between (ha, that rhymes) we have most colors and combos in the budgie kingdom. So if your favorite color is red, you're out of luck, parakeets don't come in shades of red! But we have red and orange leg bands! Which bring us to another fact about the best bird a twenty dollar bill can buy! We leg band all our birds so we know how old they are (to the day) and who their parents are. Banding helps in our breeding process but it also helps you identify your bird if you're traveling or your pet is lost or stolen.

To top if off, we have an awesome website with a bunch of information on our operation budgie and how to care for the little balls of feathers. www.keets.me, is the URL. Also we have all the basic starter supplies to get a new or returned bird owner on track! (All at good prices, so don't worry!) For more information or to set up an appointment to see the birds, give us a call at (480) 695-5359. We are around to show the birds most days after 2:00pm, we are in East Mesa, AZ. Pick up only, the birds don't like flying! (That's a joke.)


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Source: http://www.classifiedads.com/birds-ad25273032.htm

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Saturday, January 19, 2013

The holidays were fine once the flu left our house | The Plaincity ...

A whole brand new year lies ahead. What does it have in store for us all? Only God knows so let us put our trust in him. I hope everyone had a great, safe holiday. We had a very nice holiday after the flu bug finally left our house.

Christmas Day was spent here at home. Elizabeth?s friend Timothy and Susan? s friend Mose joined us for the day. It was a memorable day playing games and just being together as a family. Our thoughts and prayers went out to the ones missing family members this holiday season. They are missed even more during the special holiday time.

I put a breakfast casserole in the oven to heat while everyone opened their gifts. Days like that go way too fast.

Sunday we had the annual Christmas potluck dinner after church services. As always there was more than enough food. Daughter Loretta made cupcakes and frosted and decorated them to take along.

Monday evening Jacob, Emma and family came in honor of Joe?s birthday which was Dec. 22. Joe grilled chicken and hot wings while I made scalloped potatoes. We also froze homemade ice cream for our dessert and Emma brought donuts.

Jacob, Emma, and family, Timothy and Mose also spent New Year?s Day here. We had a brunch which was a? breakfast haystack.?

Our breakfast haystack menu was biscuits cut into bite sized pieces, scrambled eggs, fried potatoes, chopped bacon, and diced ham, shredded cheese, green peppers, diced tomatoes, diced onion, cheese sauce, salsa, hot peppers, and sausage gravy. After dishes were washed we exchanged gifts with Emma and Jacob?s family. We had a name exchange which was interesting to see who all had who. Then everyone went sledding in our hay field except for Jacob, Joe, Emma, and I. We stayed in the warm house and played board games.

Timothy had a sled tied behind his pony and gave some pretty fast rides around the hay field. It looked liked it was a challenge to stay on the sled when he took some fast curves.

They also had fun sliding down the hill in the sled. The snow made some nice gliding downhill. When they were all tired from sledding they came back in to warm up. We set snacks out for everyone. Emma brought a lot of snacks too.

I heated up the leftover chicken and wings from the evening before. The rest of the afternoon was spent playing games.

Daughter Elizabeth went back to work at the factory on Wednesday. The children go back to school on Monday. Husband Joe will head back to work at the factory, also on Monday.

Daughter Susan has two more ponies here to train. One is a little miniature pony and the other is a bigger sized pony like our pony Stormy. Her friend Mose?s dad gave Susan the pony to keep for her own. She is excited and eager to train her. Benjamin and Susan have the pony, which is named Roxy, hitched to the pony cart now for the first time. It always makes me a little nervous until she has the ponies going good. Benjamin, 13, enjoys helping her train the ponies. Jacob, Emma, and family went to Berne, Indiana to have Christmas with Jacobs? family. While there they stopped in to say hi to brother Amos, Nancy and family. Amos sent along a roll of his homemade summer sausage he made. It was very good and disappeared quite fast around here. We appreciated it very much.

Looking for an easy cupcake recipe? Try this.

NEVER FAIL

CUPCAKES

1 egg

1/2 cup sour milk

1/2 cup shortening

1 teaspoon soda

1/2 cup hot water

1/2 cup cocoa

1 1/2 cups flour

1 teaspoon vanilla

1 cup sugar

In a large mixing bowl add ingredients in the order listed. Do not mix until the last ingredient has been added. Beat until smooth. Bake at 350 for 15 minutes. Add frosting when cool. Makes 19 cupcakes.

Readers with culinary or cultural questions or to share recipes write Lovina at: Lovina Eicher, c/o Oasis Newsfeatures, P.O. Box 157, Middletown, OH 45042. To learn more about Amish culture and the Amish Cook column and to sign up for the twice weekly newsletter, visit www.amishcookonline.com or ?The Amish Cook Fan Page? on Facebook.

Source: http://plaincity-advocate.com/columnists/lovina-eicher/holidays-fine-flu-left-house/

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Indian court says 2 Italian marines accused of killing fishermen will be tried in India

NEW DELHI - India's Supreme Court ruled Thursday that two Italian marines accused of killing a pair of fishermen off the coast of India last year will be tried in a special court to be set up by the Indian government.

Italy had argued that the shootings took place in international waters and the case should be handled in Italy. New Delhi said the killings happened on an Indian boat within India's territorial waters.

The court ruled that the trial should take place in India in a special court to be set up by the central government in consultation with the chief justice, according to the Press Trust of India. The order removed the case from the jurisdiction of the southern state of Kerala, near where the shooting happened last February.

Italian Consul-General Giampaolo Cutillo said his government was satisfied with at least that small victory.

"The Supreme Court confirmed that Kerala has no jurisdiction in this case, which is basically what we maintained from the very first day," he said.

Marines Massimiliano Latorre and Salvatore Girone were part of a military security team aboard a cargo ship when they opened fire on a fishing boat they said they mistook for a pirate craft and killed two Indian fishermen. The marines were first held in a juvenile reformatory in Kerala before being moved to a guesthouse.

The fatal shooting has been emotionally charged for both India and Italy.

Source: http://www.startribune.com/world/187416351.html

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WARNING! Read THIS Before Vaccinating Your Children

Vaccines are meant to stimulate the body?s immune system to mount an adaptive immunity against a pathogen. In a way, it is a method of pre-empting infections in the body. However, this low-grade infection is easily overcome by the immune system and the body learns to counteract any subsequent invasion by the same pathogen.

At least, in principle, that is how vaccination is supposed to work. However, this may not really be the truth.

Since it was first introduced, vaccination has been met with relentless opposition even as various governments made it compulsory. Today, vaccination is one of the biggest debates in medicine.

Many have asked if vaccination is really needed; whether it works; and what harm it can cause.

This article explains the breadth of the vaccine controversy and why vaccination is bad for your health.

baby vaccine vaccination WARNING! Read THIS Before Vaccinating Your Children

Diseases with Known Links to Vaccination

Over the years, studies have linked vaccination with a number of serious diseases. In fact, it has become a trend for a new disease to appear and an old one to rebound when vaccination is introduced into a population.

Some of the diseases that vaccination has been shown to trigger are:

  • Autism
  • Asthma
  • Arthritis
  • Depression, ADHD (Attention Deficit Hyperactivity Disorder) and other neurological disorders
  • Cancer
  • Allergies
  • Infant and juvenile diabetes
  • Sudden Infant Death Syndrome (SIDS)
  • Kidney diseases
  • Autoimmune diseases

To reduce the widespread criticism of vaccination, most governments and all drug companies do not fund research into this dark side of vaccination.

However, the clinical data is pretty damning. For example, past clinical data paint a clear picture of the emergence of autism. It is no coincidence that the number of diagnosed autism cases skyrocketed just as mass vaccination was made compulsory in 1991.

Medical investigation into this co-occurrence show that autism is most likely the result of hepatitis B and meningitis vaccine.

Even though the FDA (Food and Drug Administration) and CDC (Center for Disease Control) keep insisting that vaccines are safe, they mandate the inclusion of serious warnings of side effects on the labels of vaccines. These health bodies acknowledge that vaccines can cause:

  • Arthritis
  • Kidney failure
  • Epilepsy
  • Heart attacks, bleeding disorders and blood clots
  • Severe allergic reactions
  • Other serious complications require hospital admission

The High Cost of Vaccination

The FDA and the CDC claim that only 5% of the people who get vaccinated report adverse effects. What they actually mean is that only 5% of those vaccinated file a report with VAERS or Vaccine Adverse Injury Report System.

  • The truth is that most people who get vaccinated do not know about this system.

In addition, most vaccinations involve children and when adverse reactions occur immediately, the parents are too troubled looking for solutions to consider reporting these incidents. Furthermore, the process of filing a report is too cumbersome and demands repeated visits to a doctor?s office.

  • Lastly, most adverse vaccine injuries are not reported because they do not occur immediately.

Most of the dangers of vaccines remain silent for years and cause apparently unrelated conditions or simply increase the risk of the serious diseases later in life.

Even in the early days of compulsory and mass vaccination, parents knew that these vaccines were making their children sicker. Most of those who saw direct links between vaccination and adverse reactions that immediately presented, sued the companies making these vaccines.

With increasing threat of successful lawsuits, some of these companies went out of business and the others threatened to stop producing vaccines.

This could have been the natural end of vaccination, except the US government decreed that these companies, although culpable, should be immune from all liability claims related to vaccine injuries.?Once the vaccine producers were vaccinated against liabilities, they thrived, spread and lobbied for the introduction of new vaccines and the enforcement of mandatory vaccinations.

The US government set up VICP (the National Vaccine Injury Compensation Program) in 1998 to compensate those injured by vaccines. Between then and 2011, the VICP has paid more than 2 billion dollars to individuals who reported and have been confirmed to be injured by vaccines.?This huge sum taken out of taxpayers? money to shield vaccine makers from the repercussions of making dangerous vaccines is another solid evidence that vaccination is indeed harmful.

How Vaccines Hurt Us

To understand how vaccines can cause ill-health, the first thing you need to know is how vaccines are made.

Vaccines are made from pathogens. The 3 basic types of vaccines are made from:

  • Living but inactivated microbes
  • Living but attenuated (with reduced infectivity) microbes
  • Components of microbial cells such as the proteins in the cell wall that still contain toxins

In principle, the active agent in a vaccine is used because it can still stimulate the immune system to produce a reaction akin to the one caused by the living and fully active infective agent.?To improve the chances that these weakened microbes will indeed trigger the immune system, adjuvants such as squalene and lipopolysaccharides are added to vaccines to amplify the immune response to vaccines.

A vaccine may produce the desired effect in normal, healthy individuals. However, the definition of normal, healthy individuals does not fit most people.

Vaccines are most likely to cause adverse effect and lasting damage in the young, the elderly, those with nutritional deficiencies and those with compromised immune systems. For such people, vaccines do not protect but rather destroy the body.

In addition, when vaccines are delivered by routes other than direct injection into the blood, the active agents encounter the mucosal membranes of the nose, mouth, gastrointestinal tract and the pulmonary passage to the lungs.

When the active agent end up being virulent, it can cause severe injuries to these precious and fragile sites.

Furthermore, the brain does not play well with vaccines. The body assigns a special immune system to the brain. However, this immune system is still tied to the general immune system. Therefore, when vaccines activate the body?s immune system, it also activates the special one in the brain.?Repeated and prolonged activation of the brain?s immune system can cause autoimmune damage to brain cells. This is believed to be the root cause of most of the neurological damage that cause diseases such as autism, ADHD, major depressive disorder, Parkinson?s disease and Alzheimer?s disease.

Therefore, vaccines can dramatically increase the risk of neurological disorders.

Lastly, there are contaminants to consider. It is quite common to find contaminants in different batches of vaccines. The kind of contaminants that are found in vaccines include:

  • Stray but live and virulent bacteria and viruses
  • Cells from the animals in which they vaccines are made
  • Toxic adjuvants and preservatives added to vaccines

Thiomersal, a mercury-based compound, was a common addition in vaccines before reports of vaccine toxicity forced most health regulatory bodies to ban it from vaccines. However, mercury is still found in flu vaccines.

mercury WARNING! Read THIS Before Vaccinating Your Children

Some of the other toxic additives found in vaccines include:

  • aluminum (a neurotoxic mineral that is also known to cause bone loss),
  • formaldehyde (a known carcinogen),
  • polysorbate 80 (reported to cause infertility in mice), g
  • elatin (a known trigger of anaphylactic reactions in the immune system)
  • and monosodium glutamate (known to cause neurological disorders and seizures).

Vaccinated Vs. Unvaccinated

Does vaccination really provide any sort of protection? This is a question that has been asked endlessly even though available clinical data provide a clear answer.

In one study that compares the incidence of certain childhood diseases between groups of vaccinated children and unvaccinated children, the result conclusively shows that unvaccinated children are less likely to contract common diseases.

Given that we were sold on the promise that vaccines protect us from diseases, these results was rather revealing.

The list below paints a good picture of the dangers of vaccination

  • Asthma ? 18% in vaccinated children (V); 2.5% in unvaccinated children (U)
  • Hay fever ? 10.7% (V); 3% (U)
  • Allergies ? 22.9% (V); 10.6% (U)
  • Neurodermatitis ? 13.2% (V); 7% (U)
  • ADHD ? 7.9% (V); 2% (U)
  • Autism ? 1.1% (V); 0.44% (U)
  • Diabetes ? 0.2% (V); 0.07% (U)
  • Autoimmune disease ? 7% (V); 0.37 (U)
  • Epilepsy ? 3.6% (V); 0.33% (U)
  • Thyroid disease ? 1.7% (V); 0.1% (U)
  • Otitis media ? 11% (V); 1.91% (U)

This list clearly shows that vaccination can increase the risk of disease. It is no wonder then that those who have access to such data do not vaccinate their children.

Similar results were obtained from a Cal-Oregon survey of over 17,000 children. This survey showed that compared to unvaccinated children, vaccinated children had 120% more likely to have asthma, 317% more likely to suffer from ADHD, 185% more likely to have one neurological disorders and 146% more likely to develop autism.

Another revealing survey of doctors and healthcare professionals show that many of them do not get vaccinated and do not vaccinate their own children. Why? Because they know the dangers involved in vaccination including the silent ones that increase the risks of certain serious and expensive diseases later in life.

In addition, these healthcare professionals routinely treat patients with serious vaccine injuries, and they have seen enough such cases to known that vaccines are not as effective or safe as claimed.

Who Benefits from Vaccination?

So who benefits from vaccination? Everyone who has a financial incentive to keep the racket going.

Those who gain from compulsory, mass vaccination include:

  • drug companies,
  • insurance companies
  • and the healthcare systems that deliver these vaccines.

By also making drugs to manage depression, ADHD, diabetes, asthma, allergies, autoimmune disorders and thyroid diseases, these companies get paid to clean after their own vaccines. And they are protected from class-action suits by VICP and the 1986 National Child Vaccine Injury Act.

Healthcare professionals are also not without blame. Doctors get paid to keep these vaccines stocked and to convince their patients to regularly get vaccinated.

In addition, the cost of hospitalization resulting from the long-term effects of vaccine is an endless revenue stream for hospitals.

Just Say No to Vaccination

A growing number of healthcare professionals are challenging the practice of vaccination. More than anything, this is an indication that there is something serious wrong with vaccines.

In a report released by one such group of concerned healthcare professionals, International Medical Council On Vaccination, these doctors, nurses and scientists provide a clear summary of the dangers of vaccination and why it is being blindly sold to everyone.

This report concludes with a simple call for action: say no to vaccination.

Thankfully, the right to refuse vaccination is still alive in every state in the US. Therefore, instead of becoming sold on the fears on treatable diseases such as flu and ear infections only to buy lifelong disorders such as ADHD and autism, educate yourself on the dangers of vaccination and spare your family a future of chronic diseases.

References

Source: http://www.hivehealthmedia.com/warning-read-vaccinating-children/

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Friday, January 18, 2013

NCAA Preview 2013: Harvard

Inside Lacrosse is kicking off the season by previewing the top 40 teams. Here's Five Things to Know About Harvard, ranked No. 36 in the Face-Off Yearbook.

Harvard, sporting a preseason rank of No. 36 in the 2013 Face-Off Yearbook, had a fairly disappointing 2012, going 6-8 overall and going 2-4 in Ivy league play. The Crimson won Ivy League games against Brown (10-9 OT), and Dartmouth (15-10) in 2012 and will look to improve their league form in 2013 despite losing two of their top three scorers to graduation.

1. There Are a Lot of New Faces in Cambridge

The Harvard men?s lacrosse team heads into the 2013 season sporting the No. 4 recruiting class in the nation. Players from established high school programs don?t just dot the roster ? they smother it. Deerfield Academy, Garden City, Manhasset and Gilman are just a few of the places that the Harvard freshman hail from, but coach Chris Wojcik was coy on the identity of any particular player that stood out in fallball, but quick to praise the first-year players as a group: ?I think the whole class has impressed. A number of them will push for playing time right away.?A really talented group. They have great attitudes and have played at top high school programs. I think they have all impressed me, but most of them are looking at playing time right away.? Still, they haven?t proven anything at this level yet.?

2. The Replacements is Just a Movie

The Crimson lose 92 points (65G, 27A) with the departure of Jeff Cohen and Kevin Vaughan to graduation. For a team that finished 22nd in the nation in goals per game (10.36), that?s still a lot of goals to leave unaccounted for, but according to coach Wojcik, there are several players that can slot into their system. ?We don?t look at our current players as replacements. We have a team-oriented system. We assess our current personnel with their strengths and weaknesses in our system.? The Crimson return their second leading scorer in Daniel Eipp (24, 18), who begins his junior campaign as the top option. Said Wojcik of Eipp: ?He?s always been a great dodger, but last year his distribution ability really developed. Last summer he helped Team USA win a gold medal [with the U-19 team], and this year I think the goal for him is to become a complete attackman. Dodge, feed, ride ? do it all. He?s hungry, he?s driven and he?s an emerging leader at attack.?

3. The Midfield Unit is Experienced

Alex White (5 G, 19 GB) has played for four years. He's a very good all-around middie, high lacrosse IQ, he?s big, he?s strong, and he makes plays with his experience. Expect him to be a leader.??

Ryan Stevens (5, 2) is another senior midfielder that will see extended time in 2013. Stevens started two games last season, but he has seen his fair share of the trainers' table. Still, Wojcik believes that his ability as a ?high velocity shooter on the run and up top with both hands? makes him an exciting prospect this spring.

He may not be a senior, but Carl Zimmerman is a converted attackman that notched five goals and dished six assists in 2012. He?s ?very smooth, has good speed, and is an excellent team player who we expect to emerge as a junior,? according to the coach. Zimmerman had his best game in what could have been the Crimson?s best game all year ? an overtime win against Ivy league rival Brown that saw the midfielder score two goals and hand out an assist.

4. Face-offs Will Be Even Stronger in 2013

Sophomore Michel Keegan was Harvard?s top draw man in 2012, finishing with a 59.6% win percentage after taking over primary face-off duties while splitting time with then-freshman Sean Mahon and the aforementioned Alex White. Rick Mole will also take draws for Harvard in 2013. Mole is a converted defenseman, but in addition to Keegan, Mahon and White, Mole took draws, going 15-32 in his seven appearances in 2012. Wojcik was complimentary of Mole in particular, praising his hard work and skillset at the X. The return of all these players from injury is definitely a boon to a face-off unit that was already successful last year.

5. The Overachievers Don?t Want to Underachieve Again

Wojcik was not shy about his team?s record last season. ?Overall last year was disappointing. We underachieved. We started well and dropped three close games. We bounced back against Brown, and we were able to beat Dartmouth, but then we didn?t finish strong. We lost our final four ivy league games. Guys were unhappy. I think we have learned a lot from that season and made a number of adjustments and our guys are very hungry to prove themselves this year.?

The new rule changes are also a point of focus for this team heading into the new season.???I think a lot of us are excited about what this year will being to our teams and the game with all the new rules.??To try and speed up the game, I think for a lot of us this will be a learning year for coaches and players across the country at all levels.??We all know the rules and were practicing new strategies to try and take advantage of the rules, but I think you will see certain philosophies and themes emerge this year and those are yet to be determined.?

Best Bet: Daniel Eipp, junior, attack (24G, 18A)

The Crimson's leading returning scorer is a quick dodger and talented scorer. His athleticism makes him tough to cover one-on-one.

Sleeper Pick: Peter Schwartz, junior attack (4G, 7A in 2011)

The sleeper of the entire offense might be Peter Schwartz. The junior attackman missed all of last year with an injury, but coach Wojcik insists ??he?s back and healthy and he?s very determined to be a big-time contributor on offense. He a great game and can contribute at attack and midfield.? Schwartz?s last season for Harvard saw him contribute four goals and seven assists back in 2011 as a sophomore.

Another player that could be considered a sleeper on the other side of the ball is Gabriel Mendola. Like Schwartz, Mendola missed all of last season. However, Mendola?s freshman year saw him win 75 of 128 face-offs, good for a 58.6% win percentage in addition to scooping 34 groundballs.

Game to Watch: UMass, 1 p.m. Feb. 23

Nothing tests freshmen like a big game right out of the gate. Harvard's season opener in Cambridge will be a great opening atmosphere, with an in-state game against top-tier talent (No. 12 in Face-Off Yearbook). Harvard can get the sting of a disappointing season out of its system quickly with a win.

2012 Record: 6-8
2012 Conference: 2-4
GPG (Rank): 10.36 (22)
GAA (Rank): 9.79 (30)

Related

Source: http://insidelacrosse.com/news/2013/01/17/ncaa-preview-2013-harvard

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FluBlok: FDA Approves New Insect-Based Flu Vaccine That Is Safe For People With Egg Allergy

A new kind of insect-based flu vaccine has been approved for adults by the Food and Drug Administration. It's the first version that is not grown in eggs, meaning people with egg allergies can receive it.

The FDA announced that the vaccine, called FluBlok and produced by Protein Sciences Corp, is different from other vaccines, as it can be made more rapidly in the event of a pandemic "because it is not dependent on an egg supply or on availability of the influenza virus," Dr. Karen Midthun, M.D., director of the Center for Biologics Evaluation and Research at the FDA, said in an agency statement.

Another way it's different? The process of making it involves insect cells.

CNN reports:

Instead, Flublok's production involves programming insect cells grown in steel tanks to produce large amounts of a particular flu virus protein, known as hemagglutinin, according to Protein Sciences, the vaccine's manufacturer.

According to a FluBlok press release, the vaccine also does not contain preservatives, including the mercury-containing thimerosal. It is designed to protect against the H1N1, H3N2, both A strains and one B strain of the influenza virus, and is approved for people between ages 18 and 49.

The safety of FluBlok was tested in a study of 2,300 people; common side effects included muscle aches, headache, fatigue and pain in the area the shot was administered (which the FDA noted are common symptoms for any kind of flu shot). It was found to be 44.6 percent effective against all strains of the flu, the FDA reported.

A relatively small amount of the vaccine is expected to be available by this winter, the New York Times reported, though the FDA noted that the timing of the approval had nothing to do with the current flu outbreak. Protein Sciences Corp said that the vaccine would be largely available for the next 2013-2014 flu season.

Also on HuffPost:

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Source: http://www.huffingtonpost.com/2013/01/17/flublok-insect-based-flu-vaccine-egg_n_2498494.html

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