Monday 29 October 2012

Mechanism found for destruction of key allergy-inducing complexes, Stanford researchers say

Mechanism found for destruction of key allergy-inducing complexes, Stanford researchers say [ Back to EurekAlert! ] Public release date: 28-Oct-2012
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Contact: Rosanne Spector
manishma@stanford.edu
650-725-5374
Stanford University Medical Center

STANFORD, Calif. Researchers have learned how a man-made molecule destroys complexes that induce allergic responses a discovery that could lead to the development of highly potent, rapidly acting interventions for a host of acute allergic reactions.

The study, which will be published online Oct. 28 in Nature, was led by scientists at the Stanford University School of Medicine and the University of Bern, Switzerland.

The new inhibitor disarms IgE antibodies, pivotal players in acute allergies, by detaching the antibody from its partner in crime, a molecule called FcR. (Other mechanisms lead to slower-developing allergic reactions.)

"It would be an incredible intervention if you could rapidly disconnect IgE antibodies in the midst of an acute allergic response," said Ted Jardetzky, PhD, professor of structural biology and senior investigator for the study. It turns out the inhibitor used by the team does just that.

A myriad of allergens, ranging from ragweed pollen to bee venom to peanuts, can set off IgE antibodies, resulting in allergic reactions within seconds. The new inhibitor destroys the complex that tethers IgE to the cells responsible for the reaction, called mast cells. Severing this connection would be the holy grail of IgE-targeted allergy treatment.

The first time a potential allergen enters the body, some people respond by making allergen-specific IgE antibodies. These antibodies stick around long after the initial allergen is cleared from the body. Most of the antibodies get snagged by IgE-specific receptors called FcRs, which are exposed on the surface of mast cells. The mast cells are then primed to react the next time a person encounters the allergen.

Dissociation of this IgE-FcR interaction is a sought-after goal of allergy treatment for a good reason: IgE-coated mast cells are grenades of histamine, and re-encountering the allergen is equivalent to pulling out the clip. When an allergen makes a return visit, it binds to the pre-loaded IgE on the mast cell surface, triggering the release of inflammatory mediators including histamine that promote the allergic response. As allergy sufferers are well aware, these nasty reactions can occur within a matter of seconds. In a severe allergic response, sudden anaphylactic shock and death can be the result.

The key to actively disabling the allergic response lies in the separation of IgE from the FcRs on the surface of mast cells. But separating these dangerous couples is a tall order because their interaction is extremely stable sensitizing the mast cells for weeks. Currently available treatment using omalizumab (an anti-IgE antibody sold under the trade name Xolair) can block new interactions between IgE and FcR, but it is not designed to pry the molecules apart once they've formed a bond on the surface of a mast cell. So Xolair can dampen the allergic response, but as stated on the product's website: "Xolair is not a rescue medicine and should not be used to treat sudden asthma attacks."

While simply blocking IgE binding is helpful for some allergy sufferers, when it comes to the rapid quenching of an acute allergic response, "what you'd really like to do is get rid of it," said Jardetzky. Along with scientists at the University of Bern, his team discovered that an engineered protein inhibitor called DARPin E2-79 stripped IgE from the mast cell receptor. Using this inhibitor, "an interaction that normally lasts for hours or days in terms of its stability is stripped off in a matter of seconds," said Jardetzky.

DARPin E2-79 is one of a family of engineered inhibitors containing protein-binding regions called ankryin repeats. While Jardetzky's group was using structural biology and biophysical approaches to probe the weak spots in the IgE-FcR interaction, scientists at the University of Bern were tinkering with DARPins that dampened IgE's disastrous effects. The collaboration of the two groups resulted in the characterization of DARPin E2-79, an inhibitor that goes beyond mere blockade to actively disassemble the IgE-FcR power couple.

Jardetzky's group solved E2-79'S structure and used this information to model its interaction with the IgE-FcR pair. Then, using sensitive biochemical techniques that detect step-by-step binding interactions between molecules, the teams were able to tease out the mechanism that the inhibitor uses to break the IgE-FcR bond.

The researchers found that E2-79 hastens the separation of the two molecules by taking advantage of a moment of weakness in the relationship between IgE and FcR. IgE maintains its interaction with FcR using two contact points, and occasionally one of these points releases while the other one keeps the pair together. Normally this brief looseness isn't enough to separate the couple, but E2-79 can swoop into the small space between them, effectively driving the couple apart.

While E2-79 is the first molecule to display these IgE stripping characteristics, Jardetzky hopes that this work will stimulate the discovery of smaller compounds capable of working even more efficiently. Drug developers generally expect large macromolecules like E2-79 to be less potent than small molecule inhibitors and unlikely to be able to disrupt complexes, so the fact that E2-79 worked so well was a surprise. Small molecules are more amenable to oral administration, and are easier and cheaper to manufacture than large macromolecules. "Now we're in the hunt for a small molecule that could have this kind of activity. That would be the real hit," said Jardetzky.

The discovery of E2-79's mechanism of IgE inhibition could lead to rapid discoveries from other labs as well. Now that scientists know what mechanism to look for, they may be inspired to dig back through freezers full of IgE inhibitors that were identified years ago, said Jardetzky. In the light of techniques described in this study, perhaps once-neglected inhibitors will show new promise in the treatment of allergic disease.

###

The study's primary authorship was shared between Beomkyu Kim, PhD, a Stanford graduate student, and Alexander Eggel, PhD, at the University of Bern. The other Stanford co-author is research assistant Svetlana Tarchevskaya.

The study was funded by the National Institutes of Health, the American Asthma Foundation and the Swiss National Science Foundation. Information about Stanford's Department of Structural Biology, which also supported the work, is available at http://structuralbio.stanford.edu/.

The Stanford University School of Medicine consistently ranks among the nation's top medical schools, integrating research, medical education, patient care and community service. For more news about the school, please visit http://mednews.stanford.edu. The medical school is part of Stanford Medicine, which includes Stanford Hospital & Clinics and Lucile Packard Children's Hospital. For information about all three, please visit http://stanfordmedicine.org/about/news.html.



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Mechanism found for destruction of key allergy-inducing complexes, Stanford researchers say [ Back to EurekAlert! ] Public release date: 28-Oct-2012
[ | E-mail | Share Share ]

Contact: Rosanne Spector
manishma@stanford.edu
650-725-5374
Stanford University Medical Center

STANFORD, Calif. Researchers have learned how a man-made molecule destroys complexes that induce allergic responses a discovery that could lead to the development of highly potent, rapidly acting interventions for a host of acute allergic reactions.

The study, which will be published online Oct. 28 in Nature, was led by scientists at the Stanford University School of Medicine and the University of Bern, Switzerland.

The new inhibitor disarms IgE antibodies, pivotal players in acute allergies, by detaching the antibody from its partner in crime, a molecule called FcR. (Other mechanisms lead to slower-developing allergic reactions.)

"It would be an incredible intervention if you could rapidly disconnect IgE antibodies in the midst of an acute allergic response," said Ted Jardetzky, PhD, professor of structural biology and senior investigator for the study. It turns out the inhibitor used by the team does just that.

A myriad of allergens, ranging from ragweed pollen to bee venom to peanuts, can set off IgE antibodies, resulting in allergic reactions within seconds. The new inhibitor destroys the complex that tethers IgE to the cells responsible for the reaction, called mast cells. Severing this connection would be the holy grail of IgE-targeted allergy treatment.

The first time a potential allergen enters the body, some people respond by making allergen-specific IgE antibodies. These antibodies stick around long after the initial allergen is cleared from the body. Most of the antibodies get snagged by IgE-specific receptors called FcRs, which are exposed on the surface of mast cells. The mast cells are then primed to react the next time a person encounters the allergen.

Dissociation of this IgE-FcR interaction is a sought-after goal of allergy treatment for a good reason: IgE-coated mast cells are grenades of histamine, and re-encountering the allergen is equivalent to pulling out the clip. When an allergen makes a return visit, it binds to the pre-loaded IgE on the mast cell surface, triggering the release of inflammatory mediators including histamine that promote the allergic response. As allergy sufferers are well aware, these nasty reactions can occur within a matter of seconds. In a severe allergic response, sudden anaphylactic shock and death can be the result.

The key to actively disabling the allergic response lies in the separation of IgE from the FcRs on the surface of mast cells. But separating these dangerous couples is a tall order because their interaction is extremely stable sensitizing the mast cells for weeks. Currently available treatment using omalizumab (an anti-IgE antibody sold under the trade name Xolair) can block new interactions between IgE and FcR, but it is not designed to pry the molecules apart once they've formed a bond on the surface of a mast cell. So Xolair can dampen the allergic response, but as stated on the product's website: "Xolair is not a rescue medicine and should not be used to treat sudden asthma attacks."

While simply blocking IgE binding is helpful for some allergy sufferers, when it comes to the rapid quenching of an acute allergic response, "what you'd really like to do is get rid of it," said Jardetzky. Along with scientists at the University of Bern, his team discovered that an engineered protein inhibitor called DARPin E2-79 stripped IgE from the mast cell receptor. Using this inhibitor, "an interaction that normally lasts for hours or days in terms of its stability is stripped off in a matter of seconds," said Jardetzky.

DARPin E2-79 is one of a family of engineered inhibitors containing protein-binding regions called ankryin repeats. While Jardetzky's group was using structural biology and biophysical approaches to probe the weak spots in the IgE-FcR interaction, scientists at the University of Bern were tinkering with DARPins that dampened IgE's disastrous effects. The collaboration of the two groups resulted in the characterization of DARPin E2-79, an inhibitor that goes beyond mere blockade to actively disassemble the IgE-FcR power couple.

Jardetzky's group solved E2-79'S structure and used this information to model its interaction with the IgE-FcR pair. Then, using sensitive biochemical techniques that detect step-by-step binding interactions between molecules, the teams were able to tease out the mechanism that the inhibitor uses to break the IgE-FcR bond.

The researchers found that E2-79 hastens the separation of the two molecules by taking advantage of a moment of weakness in the relationship between IgE and FcR. IgE maintains its interaction with FcR using two contact points, and occasionally one of these points releases while the other one keeps the pair together. Normally this brief looseness isn't enough to separate the couple, but E2-79 can swoop into the small space between them, effectively driving the couple apart.

While E2-79 is the first molecule to display these IgE stripping characteristics, Jardetzky hopes that this work will stimulate the discovery of smaller compounds capable of working even more efficiently. Drug developers generally expect large macromolecules like E2-79 to be less potent than small molecule inhibitors and unlikely to be able to disrupt complexes, so the fact that E2-79 worked so well was a surprise. Small molecules are more amenable to oral administration, and are easier and cheaper to manufacture than large macromolecules. "Now we're in the hunt for a small molecule that could have this kind of activity. That would be the real hit," said Jardetzky.

The discovery of E2-79's mechanism of IgE inhibition could lead to rapid discoveries from other labs as well. Now that scientists know what mechanism to look for, they may be inspired to dig back through freezers full of IgE inhibitors that were identified years ago, said Jardetzky. In the light of techniques described in this study, perhaps once-neglected inhibitors will show new promise in the treatment of allergic disease.

###

The study's primary authorship was shared between Beomkyu Kim, PhD, a Stanford graduate student, and Alexander Eggel, PhD, at the University of Bern. The other Stanford co-author is research assistant Svetlana Tarchevskaya.

The study was funded by the National Institutes of Health, the American Asthma Foundation and the Swiss National Science Foundation. Information about Stanford's Department of Structural Biology, which also supported the work, is available at http://structuralbio.stanford.edu/.

The Stanford University School of Medicine consistently ranks among the nation's top medical schools, integrating research, medical education, patient care and community service. For more news about the school, please visit http://mednews.stanford.edu. The medical school is part of Stanford Medicine, which includes Stanford Hospital & Clinics and Lucile Packard Children's Hospital. For information about all three, please visit http://stanfordmedicine.org/about/news.html.



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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/2012-10/sumc-mf102612.php

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Friday 26 October 2012

Real Estate Agent Oren Alexander Is 25 - Business Insider

Oren Alexander celebrated his 25th birthday by breaking the record for the most expensive home sold in Miami, according to The Wall Street Journal.

The Indian Creek mansion sold for a cool $47 million.?

Alexander's accolades don't stop there. He's been named to Forbes' 30-under-30 most successful real estate agents list, was ranked No. 1 company wide for GCI Month of August, and was the top selling agent for Prudential Douglas Elliman in August 2009.

Alexander is apart of a growing trend of younger agents trying to break into the real estate scene. While Alexander might be a star of the younger generation, the median age of a real estate agents is still 56 years old, according to The WSJ.

Coming from a real estate family, Alexander learned the ropes of the luxury market from his parents at the age of 18, before heading off to the University of Colorado.

Alexander told The WSJ:

"Quite frankly, I'm addicted to my job?the hours, the lifestyle. I love that I get to hang out with wealthiest people in the world and it's considered work. Plus, being a broker is entrepreneurial?and entrepreneurship is dominating right now."

Currently, Alexander is marketing more than $175 million in property ? including a $95 million mansion in Alpine, N.J.

To help market his luxury properties, Alexander takes to Twitter, tweeting photos of new properties going up around the city, or when news breaks in the industry. He has more than 4,800 followers.

The Real Deal dubbed Alexander "The Party Boy," spotting him at hot-spots such as Mister H or the Mulberry Project. He and his twin brother, Alon, were also named two of NYC?s hottest bachelors by Gotham Magazine in 2011.

DON'T MISS: Tour The $47 Million Mansion Oren Alexander Just Sold

Source: http://www.businessinsider.com/real-estate-agent-oren-alexander-is-25-2012-10

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    Brian Tracy's 21 Success Secrets of Self Made Millionaires

    Brian Tracy's 21 Success Secrets of Self Made Millionaires

    http://www.21MillionaireSecrets.com 21 Success Secrets of Self Made Millionaires by Brian Tracy
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    Categories: People & Stories

    Cradle of Filth - Cradle of Fear (self Made Trailer) (16+)

    Cradle of Filth - Cradle of Fear (self Made Trailer) (16+)

    hope you like it...i worked for hours to choose scienes to be fit with music...pretty good scienes from full video that i have never seen on trailers...and the music is different then others...worth to try check it out guys...16+ yes there will be blood!!!
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    Self Improvements and Self Help Made Easy

    Self Improvements and Self Help Made Easy

    http://www.selfimprovementsguide.com SELF Everything you always wanted to know about self improvement, self help, and personal development Feel free to browse all 15 of our self improvement guides on self growth, inspirational, self hypnosis, stress, happiness, motivational, and positve thinking. Also get your FREE report on "Creativity Development". This is the Ultimate self improvement, self-help, self growth, self-hypnosis, and personal development site.
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    A Self-made Hovercraft Is Born

    A Self-made Hovercraft Is Born

    This video is about two guys (A. Huisman and S.Cusack) who built a remote control hovercraft for a school project. We tested it on land, and after that on water. Watch the video to see the results.. :-)
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Obama and Bill Clinton to campaign together

President Barack Obama walks the corridors of Bellagio Hotel and Casino before speaking to employees during an unscheduled visit after a campaign event nearby on Wednesday, Oct. 24, 2012, in Las Vegas. (AP Photo/Pablo Martinez Monsivais)

President Barack Obama walks the corridors of Bellagio Hotel and Casino before speaking to employees during an unscheduled visit after a campaign event nearby on Wednesday, Oct. 24, 2012, in Las Vegas. (AP Photo/Pablo Martinez Monsivais)

WASHINGTON (AP) ? President Barack Obama and Bill Clinton will campaign together Monday, opening the final full week before Election Day with a three-state battleground blitz.

The joint rallies underscore Clinton's role as perhaps Obama's most important surrogate in the tightly contested White House race with Republican Mitt Romney. In campaign events, television advertisements and a well-regarded speech at the Democratic convention, the former president has been a chief defender of Obama's economic record, winning praise for sometimes explaining that record better than Obama himself.

The two will headline rallies Monday in Orlando, Fla., Youngstown, Ohio, and Prince William County, Va. It's the first time Obama and Clinton will campaign together during this election, though they have shared the stage at fundraisers and appeared together briefly at the party convention.

The three states are among the biggest electoral prizes up for grabs in the Nov. 6 election. Polls show Obama has an edge in Ohio, but Romney has whittled away the president's earlier leads in Florida and Virginia.

For Obama and Clinton, the rallies serve as another benchmark in a year that has solidified their transition from political rivals to allies.

Following his convention speech, Clinton has made a series of solo appearances on Obama's behalf. A high-profile event in Ohio last week also featured Bruce Springsteen.

Clinton has also appeared in campaign ads, including one out this week where the former president argues that Obama "got it right" with his economic agenda. And he's helped both Obama's campaign and the main super political action committee supporting him raise money.

Obama advisers are banking that Clinton's presence on the campaign trail will shore up the Democratic base. And they hope undecided voters will draw a connection between Obama's policies and the ones Clinton pushed when he presided over a thriving economy.

___

Follow Julie Pace at http://twitter.com/jpaceDC

Associated Press

Source: http://hosted2.ap.org/APDEFAULT/89ae8247abe8493fae24405546e9a1aa/Article_2012-10-25-Obama-Bill%20Clinton/id-e1d1c3046ff94524af8c0b306b8502e0

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Thursday 25 October 2012

Candy and kids: What's the connection? - The Orange County Register

Study after study says there's no evidence that sugar makes kids more hyperactive and generally run around like little demons.

Parents and teachers who are around children more often than researchers in lab coats might beg to differ.

A trick-or-treater on Main Street in Seal Beach selects his treat on Halloween in 2010.

JOSHUA SUDOCK, THE ORANGE COUNTY REGISTER

ADVERTISEMENT

The week of Halloween is a blast for kids and their parents, but it's also a challenge, especially since Oct. 31 falls on a Wednesday this year, smack in the middle of the school week. Costumes, decorations, parties, staying up late and, of course, mountains of candy can create enough distractions to drive adults batty.

Some schools are using this week to take a couple days off for staff development time. The Newport-Mesa Unified district is closed for kindergarten through 12th grade on Nov. 1, when kids might otherwise show up bleary-eyed from trick-or-treating, or amped up from those Tootsie Rolls that scientifically don't cause rowdiness. The Huntington Beach City district (kindergarten through eighth grade) has staff development days Nov. 1-2.

Huntington Beach City Superintendent Gregg Haulk said concerns about the holiday account for about 50 percent of the decision behind scheduling staff development for this week, "to avoid some of the issues with having students in school the day of or day after Halloween. It just throws them out of their schedules and makes it difficult to focus."

Last year all seven elementary schools and two middle schools in the district took Monday and Tuesday off ? Halloween and that dreaded day after. Even though schools are open this Halloween, costumes, parties and parades are discouraged, with revelry largely confined to fall festivals and carnivals put on by school PTAs on late afternoons or weekends.

"We're trying to stay focused," said Julie Jennings, principal at Dr. Ralph E. Hawes Elementary School in Huntington Beach, an institution named for a physician whose primary focus was the health of young children. It's a school that on Monday started a program called the 100 Mile Club, led by a parent, marathoner Linda Williams, in which kids run a little bit from 8 to 8:20 each day to work toward 100 miles for the school year.

"The health of a person is vital to how well they do in school, and how well they can think and process information," Jennings said.

ADVICE FOR PARENTS

Even the most health-conscious parents shouldn't get too strict about sweets during Halloween "season."

"To make a kid feel bad about wanting to have candy on Halloween is just ridiculous," says Dr. Patricia Riba, a pediatrician who specializes in childhood obesity and nutrition. She likes coconut herself, and on Halloween night, she says: "I will have my Almond Joy."

But families can mitigate the effects by serving healthy meals and snacks leading up to Halloween. It's also OK to be the parents who give out Play-Doh and stickers. "My house hasn't gotten egged yet," Riba says.

Also, parents can explore the other fun aspects of Halloween ? pumpkin patches, haunted houses and the outing itself on the big night. "You don't need to go to a million houses," she said.

And don't nag once the sounds of the drop-drop-drop in the bag or bucket signal the accumulation of piles of Snickers and Skittles. "I hear parents the whole night saying, 'Don't have too much,'" Riba said. "The kids feel restricted, and they start hoarding and hiding the food. Then you're in the position of policing it, and it's a forbidden food, and it gets into all these unhealthy food dynamics. ... You don't want Halloween candies lasting for a month."

THE BIG SELL-OFF

Unless you want to pull a Jimmy Kimmel and lie to your kids by telling them you've scarfed all their Halloween candy (videotaping their reactions is optional), you could participate in what's become a trend the past few years: selling excess inventory to a local dentist. Several practitioners are offering candy buybacks. One of them is Dr. Jeffrey T. Jones of Villa Park, who offers $1 a pound.

Jones also emphasized the importance of not letting candy sit around for weeks, transforming from "sometimes food," as Cookie Monster would call it, to a part of the everyday diet. Here's a tip: Chocolate is easier brushed and rinsed off the teeth than hard, tacky candy like a Jolly Rancher.

It's a good idea to brush and floss (or floss and brush) 20-25 minutes after consuming any food, candy or otherwise, Jones said.

"If you're gonna eat candy, go brush and floss. Don't allow the acid buildup to linger," he said.

Contact the writer: lhall@ocregister.com or 714-796-2221


Source: http://www.ocregister.com/articles/halloween-375466-candy-kids.html

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On Deck ? Sports ? Bangor Daily News ? BDN Maine

BASEBALL

Hitting League Membership

At UMaine, Orono, at Paul J. Mitchell Batting Pavilion, Hitting League Membership, all levels, session 2 Jan. 1-March 31, Mondays and Tuesdays (6:30-9:30 p.m.), Saturdays (8 a.m. to 1 p.m.), $400 for each session or $750 for both, for info, contact UMaine assistant baseball coach Ryan Forest 581-1096 or ryan.forrest@umit.maine.edu

BASKETBALL

CM Travel Basketball

At Waterville, Alfond Youth Center, coaches informational meeting for Central Maine 7-8 Girls and Boys Travel league, Sunday, Nov. 11, 4 p.m., for info, contact league commissioner Cleveland Brown, 314-1876 or cebsports@hotmail.com

Bangor basketball

The Bangor Parks and Recreation Department is now accepting registrations for its 2012-2013 Youth Basketball Program, for all children in grades 2-3 and 4-5 with separate boys and girls leagues, $35 for residents and $45 for nonresidents, to register go to www.BangorParksandRec.com or stop by the Bangor Parks and Rec. Center at 647 Main St., for info call 992-4490

Open gym

The Bangor Parks and Recreation Department is offering open gym for adults to come and play basketball on Tuesday nights from 8-9:30 p.m. starting Nov. 6 at the Parks and Recreation Center at 647 Main St., $2 fee per person each night, for info contact the Parks and Recreation at 992-4490 or go to www.BangorParksandRec.com.

Fort Kent girls program

At Fort Kent Elementary School, Fort Kent Rec?s basketball all program for girls in grades 4-6, practices and games on Mondays, Tuesdays, Wednesdays or Thursdays 6-8 p.m., starting in late October, $20 for residents, $25 for nonresidents, registration deadline Oct. 15, register at Parks and Rec office, 416 West Main St., to volunteer or for more info contact director Ann Beaulieu 834-3730.

Skill Development

At Old Town, Fall Basketball Skill Development, weekly sessions in October, offensive/defensive skill development, shooting improvement, physical conditioning and strength development; for info, contact Brian McDormand 290-7641 bmac195554@msn.com

Saturday, Nov. 3

At Gorham, University of Southern Maine men?s basketball team?s Huskies? Shooting Clinic, 9 a.m. to 3 p.m., open to boys grades 3-10, $45 preregistration, $50 on clinic day, for info, contact Karl Henrikson at karlh@usm.maine.edu.

Sunday, Nov. 4

At Waterville, Colby College, 15th Maine Elite Girls Basketball Showcase, girls grades 9-12, $35 per player, college coaches will be in attendance, players must preregister, for info, contact Bill Libby, bill.libby33@yahoo.com or 207-866-4124

CANOE RACING

Saturday, Nov. 10

At Orrington, first Muskrat Scramble, canoes and kayaks, 4.5 miles flat water on Sedgeunkedunk Stream, no entry fee, prizes, 1 p.m. registration, 2 p.m. race, for info, call 825-4577 or email lawmerr@midmaine.com

CROSS COUNTRY

Sunday, Oct. 28

At Bangor (Saxl Park) and Westbrook (Smiling Hill Farm), 2 p.m. race start, first in a series of Maine USATF cross country meets, 12:30 p.m. registration, 1 p.m. course walk, $4 registration, $15 USATF membership, runners 8 and under run 2K, 9-10, 11-12 run 3K, 13-14 run 4K, and 15 and older run 5K, for info contact Allan Geiser 949-3317 or mhawk916@yahoo.com.

FIELD HOCKEY

Majestix tryouts

At Waterville, Alfond Youth Center, tryout dates for Majestix indoor field hockey teams: Nov. 3, U12 (8-10 a.m.), U14 (10 a.m.-noon); Nov. 4 and 7, U16 (7-9 p.m., 6-7:45 p.m.), Nov. 5 and 7, U19 (8-10 p.m., 8-9:45 p.m.); for info or to register, go to www.mainemajestixfh.com

HOCKEY

Interval training

At Bangor, Bangor Parks and Recreation Center, 647 Main St., high-intensity interval training, Mondays and Wednesdays, 6-7 p.m., through Nov. 28; $45 for Bangor residents, $50 for nonresidents or $5 per class; contact www.BangorParksandRec.com or 992-4490.

Try Hockey for Free

At Brewer, Penobscot Ice Arena, Saturday, Nov. 3, 3-4 p.m., an opportunity for area youth to try hockey for free to see if they are interested in playing or just for something fun and different to do, preregister at USAhockey.com or at the door, for info contact George Bishop 944-5965 or vpinstructional@breweryouthhockey.org.

Learn to Skate

At Brewer, Penobscot Ice Arena, Learn to Skate and Learn to Play hockey programs, on Saturdays, 16 weeks, $99 per skater, to register log onto www.brewerhockey.org and click on the registration link and follow the online instructions, all skaters also need to register with USA Hockey prior to registering with Brewer Youth Hockey, major credit card is needed register, birth certificates are required, for info, contact George Bishop 944-5965 or vpinstructal@brewerhockey.org.

At Bangor, the Bangor Parks and Recreation Department is accepting registrations for its Learn to Skate Lessons for ages 4 and up, session I is Nov. 4-Dec. 16, session II is Jan. 6-Feb. 10, at Sawyer Arena on Sundays, go to www.BangorParksandRec.com or stop by the Bangor Parks and Rec. Center at 647 Main St. to see times and descriptions, for info, call 992-4490

ROAD RACING

Friday, Oct. 26

At Orono, first Black Bear 5K Night Run, 7 p.m., all entries must be received in the Campus Recreation Office, no later than 6:45 p.m. on Oct. 26, accepting only the first 100 runners; entry fee of $5 per person or donate can/item of food, run will take place in the University Forest, start and finish will be at the New Balance Rec Center, for info, contact Charles Bloedon, race director, Maine Bound Center, the University of Maine, Orono, ME, 04469-5747 207.581.1752. www.umaine.edu/campusrecreation

Sunday, Oct. 28

At Orland, Wildlands Trail Run, noon, 7 miles, registration 10:30-11:30 a.m., at the Great Pond Mountain Wildlands as accessed through the South Gate entrance on Route 1 near the intersection of Route 176 in East Orland, for info contact Peter John Keeney, 207-288-3909 or to pre-entry pktrldrt@myfairpoint.net

At Foxcroft Academy, Pumpkin Waddle 5K Road Race/Walk, 1-1:45 p.m. registration, 2 p.m. start, $6 students, $12 adults, proceeds benefit Foxcroft Academy Key Club Children?s Charities.

Saturday, Nov. 3

At Bangor, Make a Footprint 5K and fun run/walk, fun run at 9 a.m., 5K at 9:45 a.m., course winds through residential neighborhoods and starts in front of First Baptist Church on Center Street, benefits Kenya Mission team for ?Kupenda for the Children.?

Sunday, Nov. 4

At Penobscot Nation, Community Building, Indian Island, 4th Annual Ralph K. Thomas 8K Run, race-day registration 8-9:15 a.m., race starts 10 a.m., preregistration $12, $15 on race day, $10 and $12 for children up to age 10, proceeds to benefit Diabetes Prevention & Awareness, for info contact Robert.Bryant@penobscotnation.org or 817-7358; or Dee.Love@penobscotnation.org or 817-7301

Saturday, Nov. 10

At Orono, 2nd annual Veterans Day 5K, presented by University of Maine Army ROTC, late registration and number pickup 6-7:45 a.m., race start 8 a.m., shower and restroom facilities available, $10/person, make checks payable to Twentieth Maine Honor Society, proceeds go to The Wounded Warrior Project and The 20th Maine Society, mail entries to Army ROTC University of Maine, Room 114 Armory, Orono, ME 04469, for info phone MS Ferland at 270-581-1121, entries must be received in Army ROTC office no later than 4 p.m., Nov. 9

ROLLER DERBY

Rock Coast tryouts

At Northport, Rock Coast Rollers tryouts, Nov. 3-4 at gym in fitness center at Point Lookout, for women ages 18 and over, for info contact Quincy McCarthy 443-907-3307 or rockcoastrollers.training@gmail.com or visit www.rockcoastrollers.weebley.com

SOCCER

Grassroots registration

At Bangor, Seacoast United Blackbear accepting registrations for winter session of Grassroots

Soccer Program, ages 4-9, introductory program teaches soccer in fun and friendly environment, for more info visit www.seacoastunitedblackbear.com or contact Ryan Pelletier at 922-1014 or by email at rpelletier@seacoastunited.com.

Jr. Academy registration

At Bangor, Seacoast United Blackbear accepting registrations for winter and winter/spring Jr. Academy Program, also known as Jr. Blackbear, ages 7-12, development program in a training environment which emphasizes skill development through individual and small group activities and small-sided play, for more info visit www.seacoastunitedblackbear.com or contact Billy Shannon at 922-1016 or by email at wshannon@seacoastunited.com.

VOLLEYBALL

Maine Juniors tryouts

At Portland, Maine Juniors tryouts on Nov. 9 for U15-U18 gold-level players and Nov. 11 for all other teams, registration is now open online at the Maine Juniors website: mainejuniors.org, the complete tryout schedule for all players is also available on the Maine Juniors website, high school girls volleyball players as well as those who attend schools without an official varsity volleyball program are invited to these tryouts.

Source: http://bangordailynews.com/2012/10/24/sports/on-deck-23/

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Social media tricks every entrepreneur should know - Modern Dignity

The Rules are Changing

Just as the Internet and ecommerce changed the way that we did business back in the nineties, social media is changing the way we do ecommerce business on the web today.? From YouTube videos to twitter to real time instant messaging to LinkedIn profiles pages, customers are relying more and more on social media to shape their experience on the web.? They are also expecting companies to connect with them through these tools.? In many ways this is a time of unprecedented opportunity for companies to understand their customer?s needs immediately and experience what their customer is experiencing in order to understand them more fully and provide the best possible customer service at the same time.? Here are some tips that are vital for correctly using social media outlets to their fullest potential to the benefit of your business.

Rehumanize Yourself

Customers are tired of canned ads.? It is becoming more apparent every day that Internet users are not interested in clicking on random banner ads, and they do not respond to advertisements on the web the same way they would in traditional broadcast media forums such as television and radio.? In order to connect with customers on the social networks, you must connect with customers on a human level.? Instead of plugging links for your newest sale or ad campaign via Twitter, perhaps you could send relevant links to customer testimonials or helpful how to videos that relate to your product. ?Keep it professional, but you do not have to spend all of your time directly plugging your brand.? Showing yourself to be a human with individual interests, especially if they are relevant to your company?s brand, is vital showing the human face to your business.

Cost Efficient Research

Social media sites are excellent low cost tools for customer research.? Whether it?s researching trends on Twitter, groups in LinkedIn, or your follower demographics in Facebook, social media provides one of the lowest cost and most accurate ways to track customer interest, the latest hot trends, and customer demographics.? The interesting thing about social media is the amount of personal information that people display about themselves on their profiles.? And remember to not be stingy about your own information ? if you are going to use social media sites, it is important that you are seen as an invested community member.? Remember, others can see your profile just as you can see theirs.

Opportunities for Great Customer Service

Customer service opportunities through text chat or video chat can be a great boon to your company?s ability to service your customers.? On top of this, many customers will openly express concerns or complaints via sites like Twitter.? The great thing for you as a company is that you can address these problems directly with the customer as the problems come up.? The challenge, however, is that you do not have much of a choice about this, because if you do not address your customer?s issues right away, they tend to escalate and get passed around to the rest of the social media community with break neck speed.

Relationships with Reporters

Just as your company has a highly public face that must be managed, reporters also have a public image that they manage.? In the past there were unfortunate occurrences that happened from time to time when a reporter or other member of the media misunderstood a company?s product or intent.? With social media, while it does not stop these occurrences, it gives companies and members of the media direct access to one another, in the public arena, where they can ask questions and clear up misunderstandings better than ever before.

?

?

Author Bio: This article is posted by Jason Phillips, a freelance blogger and an entrepreneur. He is very passionate about video chatting and often enjoys free webcam chat.

Source: http://www.moderndignity.com/social-media-tricks-every-entrepreneur-should-know/

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Squaremouth Answers Question about Travel Insurance for an ...

From Lonely Planet?s Travel Forum (the full discussion can be found here):

I am starting my 6 month round the world trip (US,?Central America,?Cuba,?Europe, trans siberian train) and would like to buy travel insurance. As my residency is in?Hong Kong?and I start the journey from?Australia, I am?having trouble finding a travel insurance policy that suits me ? I don?t have residency in Australia, so couldn?t find one from an Australian company, and for Hong Kong travel insurance, I am required to depart from Hong Kong? or it wouldn?t cover me if Cuba is part of my trip?

Could someone please help me as I am leaving on 20th Oct, ?and I really hope to get the travel insurance before departure.

Squaremouth?s Response:

There are travel insurance policies that will provide international medical coverage based on your residency situation. The effective date is usually the date of departure, so you could just select your departure from Hong Kong as your date of departure. However, if you would rather to postpone coverage until you arrive in Australia, an international medical policy will also allow this, without your residency being an issue.

Trawick International?s ?Safe Travels International? policy is a low-cost option that will provide $50,000 in emergency medical, unlimited evacuation and repatriation, and $7500 in return air trip interruption coverage. This plan also includes life insurance, non-medical evacuation, and baggage & personal items loss benefits. As long as you are not looking for a policy that includes cancellation coverage, this might be a good option for you.

?

?

Related articles:

Source: http://blogs.squaremouth.com/travel-advice/squaremouth-answers-question-about-travel-insurance-for-an-around-the-world-trip/

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Wednesday 24 October 2012

New target for cancer research uncovered

ScienceDaily (Oct. 24, 2012) ? In a new paper released October 24 in Nature, BioFrontiers Institute scientists at the University of Colorado Boulder, Tom Cech and Leslie Leinwand, detailed a new target for anti-cancer drug development that is sitting at the ends of our DNA.

Researchers in the two scientists' laboratories collaborated to find a patch of amino acids that, if blocked by a drug docked onto the chromosome end at this location, may prevent cancerous cells from reproducing. The amino acids at this site are called the "TEL patch" and once modified, the end of the chromosome is unable to recruit the telomerase enzyme, which is necessary for growth of many cancerous cells.

"This is an exciting scientific discovery that gives us a new way of looking at the problem of cancer," Cech said. "What is amazing is that changing a single amino acid in the TEL patch stops the growth of telomeres. We are a long way from a drug solution for cancer, but this discovery gives us a different, and hopefully more effective, target."

Cech is the director of the BioFrontiers Institute, a Howard Hughes Medical Investigator and winner of the 1989 Nobel Prize in chemistry.

Co-authors on the study include postdoctoral fellows Jayakrishnan Nandakumar and Ina Weidenfeld; University of Colorado undergraduate student Caitlin Bell; and Howard Hughes Medical Institute Senior Scientist Arthur Zaug.

Telomeres have been studied since the 1970s for their role in cancer. They are constructed of repetitive nucleotide sequences that sit at the ends of our chromosomes like the ribbon tails on a bow. This extra material protects the ends of the chromosomes from deteriorating, or fusing with neighboring chromosome ends. Telomeres are consumed during cell division and, over time, will become shorter and provide less cover for the chromosomes they are protecting. An enzyme called telomerase replenishes telomeres throughout their lifecycles.

Telomerase is the enzyme that keeps cells young. From stem cells to germ cells, telomerase helps cells continue to live and multiply. Too little telomerase produces diseases of bone marrow, lungs and skin. Too much telomerase results in cells that over proliferate and may become "immortal." As these immortal cells continue to divide and replenish, they build cancerous tumors. Scientists estimate that telomerase activation is a contributor in up to 90 percent of human cancers.

To date, development of cancer therapies has focused on limiting the enzymatic action of telomerase to slow the growth of cancerous cells. With their latest discovery, Cech and Leinwand envision a cancer drug that would lock into the TEL patch at chromosome ends to keep telomerase from binding there. This approach of inhibiting the docking of telomerase may be the elegant solution to the complex problem of cancerous cells. Cech, a biochemist, and Leinwand, a biologist, joined forces to work on their latest solution.

"This work was really made possible by the fact that our labs are so close," Leinwand said. "My lab was able to provide the cell biology and understanding of genetics, and Tom's lab allowed us to explore the biochemistry. We have a unique situation at BioFrontiers where labs and people comingle to make discoveries just like this."

Leinwand is the chief scientific officer of the BioFrontiers Institute and a professor of molecular, cellular and developmental biology.

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Story Source:

The above story is reprinted from materials provided by University of Colorado at Boulder.

Note: Materials may be edited for content and length. For further information, please contact the source cited above.


Journal Reference:

  1. Jayakrishnan Nandakumar, Caitlin F. Bell, Ina Weidenfeld, Arthur J. Zaug, Leslie A. Leinwand, Thomas R. Cech. The TEL patch of telomere protein TPP1 mediates telomerase recruitment and processivity. Nature, 2012; DOI: 10.1038/nature11648

Note: If no author is given, the source is cited instead.

Disclaimer: This article is not intended to provide medical advice, diagnosis or treatment. Views expressed here do not necessarily reflect those of ScienceDaily or its staff.

Source: http://feeds.sciencedaily.com/~r/sciencedaily/top_news/top_health/~3/ucIfvAbodo8/121024164721.htm

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Dry Skin Care Tips

women with good skinSome people have an oily skin while others have dry skin, which is also known as xerosis in medical terms. Dry skin is most common in dry environments and cooler months. The skin can shrivel and result in scaling, wrinkling, acne breakouts and itching when the skin cells don?t contain enough moisture. However, there is nothing to worry about. Taking proper skin care to introduce moisture to your skin can alleviate the unsightly appearance and discomfort of dry skin. Avoid exposing to known irritants and allergens can also help. Here are some simple yet effective dry skin care tips. Take a look!!!

Adjust Bathing Habits:

Often people think and believe that taking a long bath or shower can help dry skin. However, MayoClinic.com. notes that soaking your body in a hot shower or taking bath for a long time with hot water can actually make your skin even drier. The high temperature of hot water or water can dry up the natural protective oil that lubricates and moisturizes your skin, making your skin over dry. Limit your bathing or showering time to 15-20 minutes to prevent further skin drying. Make sure that you pat your skin dry right after shower with a clean towel.

Boost Moisture:

Boosting moisture in the environment, on the surface of your skin or in the body is another great skin care tip for dry skin. Dehydration of your skin cells can also contribute to dry skin, so drinking a lot of water daily is a good way to keep your skin smooth. Use of humidifier in your room may also help you fight against dry skin, since the apparatus produces moisture or humidity to the surrounding air.

Dry SkinDry skin care tips include using a good moisturizer on a daily basis. Moisturizing your skin by applying a topical moisturizer on a regular basis will also help you keep your skin soft and smooth. According to the NIH (National Institute of Health), greasy skin care products may not feel good to touch, but such products work best for dry skin to introduce moisture to your skin. Applying lotions or creams right after shower can keep more water and moisture than applying after at other times.

Choose Appropriate Products:

According to the MayoClinic, cleansers and soaps that are astringent and abrasive in nature can increase the risk of dry skin. Some people may develop rashes and dry skin in response to certain bath products and cosmetics, so get to know what is your skin type and what compounds or chemicals do not suit your skin. Mild products made up of natural ingredients or moisturizers and which contain no artificial fragrance are a good choice for dry skin. Also, it?s better to avoid using soap bars and consider using liquid cleanser if you have dry skin.

Avoid Irritants:

Laundry detergents, cosmetic products or rough fabrics such as canvas or wool can be irritants for people with sensitive skin, and they can intensify dry skin. Each skin type may react to clothing; products or toiletries in different ways so make note of the products that cause allergy or make your skin drier, and avoid such products. Using the right kind of skin care products is also one of the most important skin care tips for dry skin.

Gentle Cleansing:

Understand that dry skin demands a lot of skin cells stimulation and cleansing. Apply generous amount of skin moisturizer all over your body after a shower to avoid dry skin. This will help you saturate the outer layers of the skin and gives you that moist and soft look.

Daily Cleanser for Dry Skin:

Combine 1-teaspoon of olive oil, orange juice and one egg yolk, and then add a few drops of lime-juice and rose water into it. Stir them together properly and apply this paste over your face regularly before you go to bath. Leave it on for a few minutes to dry and then rinse it off with cool water. This remedy helps to rejuvenate your dull skin and also gives glow to your face.

In spite of following these dry skin care tips, if you don?t find any improvement in your skin, always consult a skin specialist and ask for the right skin care products and other tips to help you keep your skin smooth and soft.

Source: http://acne.ygoy.com/2012/10/23/dry-skin-care-tips/

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Tuesday 23 October 2012

Military-academic divide must be closed

Relations between academia and the military services are not known for their cordiality. The flash point was the Vietnam War. Campuses across the country were incubators of the anti-war movement and arenas for major protests. Many units of the Reserve Officers' Training Corps were shut down, especially at the Ivies. More recently, the government's ?Don't-Ask-Don't Tell? policy for gays was a source of friction at some universities.

The repeal of that policy and the fading of history have helped clear the way for better relations, most pointedly symbolized by the return of the ROTC to Harvard after a 40-year absence. Still, a walk across the average U.S. college campus offers few clues, if any, that our country is at war, and university curriculum and programs seldom touch on military families or military culture.

This divide between civilian and military culture on universities and colleges needs to close further, and there's a pressing need to move now.

With the end of the Iraq war and the winding down of the Afghanistan conflict, tens of thousands of military service members will be returning home to civilian life as the Pentagon recalibrates its force levels around the world. They face gloomy prospects. The job market is weak with the unemployment rate of veterans already higher than the national average.

Some universities and colleges have formed partnerships with non-academic organizations to help veterans train for jobs, as well as to do research on the challenges they confront readjusting to civilian life. More could be done, such as creating scholarship funds for veterans and giving course credit for time and experience in the military, depending on the major. But there's another area where colleges and universities could make a big difference: training teachers, principals, social workers, psychologists, counselors and other education professionals to understand the academic and social-emotional challenges faced by military children.

It is not uncommon for these kids ? 1.3 million mostly enrolled in public schools ? to attend nine schools before graduating from high school and to end and restart friendships every year. Many are barred from participating in a favorite sport because they lack residency requirements. And too many fall behind academically because of varying course-credit policies among the schools they attend.

The American Association of Colleges of Teacher Education, the Military Child Educational Coalition and Joining Forces, a campaign to help veterans and their families started by first lady Michelle Obama and Jill Biden, have partnered to create Operation Educate the Educators. The group has signed up more than 100 university schools of education to include materials about military families in their teacher training and internship programs.

These materials are contained in four guidebooks, the product of a consortium partnership involving the University of Southern California and eight Southern California military-connected school districts. They give teachers, principals, school social workers and other staff members background knowledge on military children, as well as practical, easy-to-implement programs that have a proven track record. For example, future teachers, administrators and student support staff serving military families should be trained in military-connected schools as part of their degree program.

Other universities are tapping graduate and undergraduate students to tutor and mentor military children, among them the University of California-San Diego, Old Dominion University, John Hopkins University, University of North Carolina-Chapel Hill and the University of Arizona. This year at UCSD, up to 500 undergraduate interns with training in military culture will be tutoring military students in San Diego public schools, as well as participating in after-school and arts programs; others will mentor military youth in college. This program alone could provide about 20,000 hours a year of extra help and support for students.

This, of course, represents just a small step toward what's needed. Veterans deserve sensitive, well-prepared teachers, administrators and support staff who know how to make their children feel welcome, supported and part of school. Colleges and universities can help make this happen by offering in their education, social work, arts and letters, and psychology graduate-degree programs training in military family culture and in the special needs of military families. No extra funding required.

By training a generation of professionals to understand military family culture, colleges and universities can make the academic-military divide a part of history.

Ron Avi Astor, Ph.D., is the Richard M. and Ann L. Thor Professor in Urban Social Development at the University of Southern California School of Social Work and Rossier School of Education.

Source: http://www.mysanantonio.com/opinion/commentary/article/Military-academic-divide-must-be-closed-3972073.php

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