বুধবার, ১৯ জুন, ২০১৩

Lytro finally enables camera's WiFi chip, introduces iOS companion app as well

Lytro finally enables camera's WiFi chip, introduces iOS companion app as well

Though Lytro early adopters might not know it, every one of those little light field cameras actually has a WiFi chip embedded inside, lying dormant until the company decides to flip the switch. Well, that time has finally come in the form of a firmware update, and wouldn't you know it, it coincides nicely with the release of a new iOS app as well. Dubbed Lytro Mobile, the app connects with the device over WiFi (naturally), letting you view its contents on your favorite iOS device. Simply select the Camera feature in the app, and it'll prompt you to swipe the Lytro's menu drawer until you see the WiFi logo as shown in the picture above. Tap it, follow the on-screen instructions, and voilà, you're now able to upload your images directly to Lytro.com either over a cellular or WiFi connection, no USB plug required.

Like the Lytro desktop app, the mobile version lets you refocus a picture and change its center of perspective via Perspective Shift. You can also add captions and geotagging data, and share your living pictures via Facebook, Twitter, email or SMS. Along with letting you see what's on your camera itself, the app also gives you access to a mobile version of the Lytro website. You can check your profile, view the most popular and most recently uploaded pictures and "like" any photo that strikes your fancy. Interestingly, the app also lets you create an animated GIF out of a living picture -- simply select either "refocus" or "perspective shift" on any of your Lytro shots to have one of those two animations added to your camera roll (we've included an example GIF after the break). Last but not least, the Lytro Mobile app has a series of tips for Lytro owners to learn more about their camera. To learn more about the app, check out the screenshots, video and release after the break. Or you can just head to the App Store link to download it right now.

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Source: Lytro Mobile (App Store)

Source: http://feeds.engadget.com/~r/weblogsinc/engadget/~3/okaZk_Anhq4/

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Microsoft reportedly neared deal for Nokia's device business, but talks broke down

Microsoft was reportedly near deal for Nokia's device business, but talks broke down

It's often been rumored that Microsoft had an eye on Nokia's handset business. It made perfect sense for both companies -- one a struggling pioneer of the mobile industry and the other a struggling stalwart from the first wave of smartphones. According to the Wall Street Journal's sources, the two were actually quite close to striking a deal and were having "advanced talks" in London as recently as this month. But, according to the all-too-familiar "people familiar with the matter," those talks have broken down. Those same sources say it was Microsoft that walked away from the table over concerns about Nokia's asking price, especially in light of its continued failure to put a significant dent in Apple and Samsung's market share. Though it seems like dreams of a Microsoft-Nokia merger are dead for the moment, don't expect the disagreement to severely affect the duo's partnership. Nokia is still reliant on Microsoft's help to stand out in the market and Microsoft needs the Finnish manufacturer to keep pumping out flagship handsets with Windows Phone on them.

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Source: Wall Street Journal

Source: http://feeds.engadget.com/~r/weblogsinc/engadget/~3/OoR8AYIbYDY/

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Report: Slowdown in health care costs to continue

WASHINGTON (AP) ? There's good news for most companies that provide health benefits for their employees: America's slowdown in medical costs may be turning into a trend, rather than a mere pause.

A report Tuesday from accounting and consulting giant PwC projects lower overall growth in medical costs for next year, even as the economy gains strength and millions of uninsured people receive coverage under President Barack Obama's health care law.

If the calculations are correct, cost spikes because of the new health care law should be contained within a relatively narrow market segment. That would come as a relief for Democrats in an election year during which Republicans plan to use criticism of "Obamacare" as one of their main political weapons.

"There are some underlying changes to the system that are having an impact, and we can expect lower increases as we come out of the recession," said Mike Thompson of PwC's Health Research Institute, which produced the study. Cost "is still going up, but not as much as it used to."

The report comes with a caveat that sounds counterintuitive at first: Self-employed people and others who buy coverage individually could well see an increase in premiums in 2014.

The reasons have to do with requirements in the health care law. For example, starting next year insurers must accept patients with pre-existing medical problems, who cost more to cover. Also, new policies have to provide a basic level of benefits more generous in some cases than what's currently offered to individual consumers.

About 160 million workers and family members now have job-based coverage and are less likely to be affected. The individual market is much smaller, fewer than 20 million people. Still, it's expected to grow significantly over the next few years as a result of the health care law, which will also provide tax credits to help many people afford their premiums.

The U.S. spends more than $2.7 trillion a year on health care, well above any other developed country. But quality is uneven, there's widespread waste and fraud, and the system still leaves about 45 million people uninsured.

For years U.S. health care spending has grown much faster than the overall economy and workers' wages, but since the recession those annual increases have slowed dramatically. The debate now is whether that's a continuing trend. The answer will be vitally important, not only for companies and their employees, but for taxpayers who foot the bill for government programs such as Medicare, Medicaid and Obama's coverage expansion.

PwC's report forecasts that direct medical care costs will increase by 6.5 percent next year, one percentage point lower than its previous projection. The cost of care is the biggest component of premiums, followed by administrative expenses and overhead.

Cost-shifting to workers and efficiency measures from employers got most of the credit for slowing growth. PwC also said the health care law's push for hospitals and doctors to be more accountable may be starting to have an impact.

Four big factors were seen as pushing costs down next year:

?Patients seeking more affordable routine services in settings like clinics springing up in retail stores, as opposed to a doctor's office or the emergency room.

?Major employers contracting directly with hospital systems that have a proven record for complicated procedures such as heart surgery and certain back operations.

?The government ramping up penalties on hospitals that have too many patients coming back with problems soon after being discharged.

?Employers' ongoing effort to shift more costs to workers through higher annual deductibles, the amount people must pay each year before insurance picks up.

By using such shifting, PwC estimates that employers may be able to drive their share of next year's cost increase even lower than 6.5 percent.

On the other hand, two big factors will push costs upward:

?The high price of new "specialty" drugs to treat serious chronic illnesses such as autoimmune diseases and some types of cancer.

?Industry consolidation, with big hospitals buying up smaller ones, as well as medical practices and rehab centers. The downside of the demand for greater efficiency by employers and government is that it may be fostering new health care monopolies.

Associated Press

Source: http://hosted2.ap.org/APDEFAULT/bbd825583c8542898e6fa7d440b9febc/Article_2013-06-18-Health%20Care%20Costs/id-0f648f132b384932b48b0ef61a714013

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Supreme Court says states may not add citizenship proof for voting (Washington Post)

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NNPC to tackle environmental degradation - Vanguard News

By KUNLE KALEJAYE

Nigerian National Petroleum Corporation, NNPC has tasked its staff to imbibe the consciousness and spirit of preservation and friendliness toward the environment as part of measure to prevent the environment from total degradation.

Speaking to newsmen in Lagos, Manager, NNPC Lagos Zonal office, Mr. James Adebola said the corporation on a yearly basis observes the World Environment Day in order to educate its members to be aware on the need to protect and save the environment.

?As you are aware, every June 5 is World Environmental Day and NNPC year in year out has always been observing it in order to sensitize our members on the need for them to be aware to protect, save the environment and ensure that it is not abused.

It is part of NNPC?s contribution towards saving the environment that is why we are observing it here in Lagos office. The public need to be sensitized, but we are using our staff as a means to spread the message to the larger society so that the larger society will see their sterling example in protecting the environment and follow suit. We are also hoping that some of us that are NNPC staff, who are involve in policies formation should be able to interact with political leaders and to influence decision on what NNPC is doing.

We should be cautious of environment and ensure that it is not abuse, it is our responsibility to keep a very safe environment for our future generation.?

Comments are moderated. Please keep them clean and brief.

Source: http://www.vanguardngr.com/2013/06/nnpc-to-tackle-environmental-degradation/

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মঙ্গলবার, ১৮ জুন, ২০১৩

'Kick-Ass 2' Exclusive: Meet Your Heroes And Villains

MTV News has exclusive behind-the-scenes footage from the superhero sequel, complete with action-packed shots from the film's new faces.
By Brett White

Source: http://www.mtv.com/news/articles/1709224/kick-ass-2-heroes-villians-exclusive.jhtml

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Mapping translation sites in the human genome

June 16, 2013 ? Because of their central importance to biology, proteins have been the focus of intense research, particularly the manner in which they are produced from genetically coded templates -- a process commonly known as translation. While the general mechanism of translation has been understood for some time, protein synthesis can initiate by more than one mechanism. One of the least well understood mechanisms is known as cap-independent translation.

Now, John Chaput and his colleagues at Arizona State University's Biodesign Institute have produced the first genome-wide investigation of cap-independent translation, identifying thousands of mRNA sequences that act as Translation Enhancing Elements (TEEs), which are RNA sequences upstream of the coding region that help recruit the ribosome to the translation start site.

The new study outlines a technique for mining whole genomes for sequences that initiate cap-independent translation within the vastness of the genome.

The research has important implications for the fundamental understanding of translation in living systems, as well as intriguing potential in the biomedical arena. (Many viral pathogens are known to use cap-independent translation to hijack and redirect cellular mechanisms to translate viral proteins.)

The lead author of the study is Brian P. Wellensiek, a senior scientist in Biodesign's Center for Evolutionary Medicine and Informatics. The group's results appear in the current issue of the journal Nature Methods.

During most protein synthesis in eukaryotic cells, cap-dependent translation dominates. The process begins after DNA is first transcribed into mRNA, with the aid of an enzyme polymerase. mRNA now forms the coded template from which the translated proteins will be generated. The mRNA code consists of sequences made from 4 nucleic acids, A, C, G & U, with each 3-letter grouping (known as a codon), corresponding to one amino acid in the protein being synthesized.

A key component in the translation process is the ribosome, which migrates along the single stranded mRNA, reading the codons as it goes. Before it can do this however, it must locate a special structure at the 5' end of the mRNA strand known as the cap. In normal cap-dependent translation, the ribosome is recruited to the 5' end of mRNA via a specialized cap-binding complex.

Cap-independent translation allows the ribosome to begin reading the mRNA message without having to first locate the 5' cap structure. Cap-independent translation occurs in eukaryotic cells during normal processes including mitosis and apoptosis (or programmed cell death). It is also a feature in many forms of viral translation, where the viral transcript is able to recruit the ribosome and co-opt its function to preferentially translate viral RNA.

In the current study, Chaput designed an in vitro selection strategy to identify human genome sequences that initiate cap-independent translation. The technique is able to select candidates from a pool of trillions of genomic fragments. Once a set of sequences was identified as translation enhancing elements, they were shown to function effectively in both cell-free and cellular translation systems.

As Chaput explains, most research on cap-independent translation has been conducted using RNA fragments derived from viruses. "These RNA molecules will fold into shapes that appear to mimic some of the initiation factors that that you would find in eukaryotic translation," he says. More recently, similar RNA molecules have been identified in cellular systems, though the sequences tend to be much shorter and function in a different manner.

Chaput's method of studying such sequences on a genome-wide scale involves first generating a DNA library of the entire human genome. Using enzymes, the genome is cut into random fragments of around 200 base pairs each. These sequences are then transcribed into mRNA.

Applying a technique known as mRNA display, the fragments are tagged in specific way, such that amino acid sequences resulting from successful translation events remain bound to the mRNA fragments that generated them. "Essentially, what we're doing is taking a library of human mRNA and tagging those sequences that act as translation enhancing elements," Chaput says. Those sequences bearing an attached peptide affinity tag can then be separated out from the remaining untranslated sequences, reverse transcribed, amplified using PCR technology and subjected to subsequent rounds of selection.

The sequences were later mapped onto the human genome. As expected, the complete library of sequences used at the start of the experiments mapped fairly evenly across the genome. But the sequences selected via mRNA display as translation enhancing elements tended to cluster in non-coding regions of the genome. The authors speculate that such sequences may have been evolutionarily selected against, as they have the potential to disrupt normal cap-dependent translation.

Roughly 20 percent of the translation enhancing elements functioned as internal ribosomal initiation sites, again turning up primarily in non-coding genomic regions. The origin of these sequences remains mysterious. It is conceivable that they were surreptitiously brought on board as a result of human interaction with different types of viruses.

Once Chaput's group had acquired a library of 250 distinct translation enhancing elements through selection using mRNA display, the sequences were screened for translation enhancing activity, which was quantified using a light based assay employing a luciferase reporter molecule.

By measuring levels of luciferase, the enhancement of each sequence could be assessed relative to background noise, with the better translation enhancing elements displaying 50-100 fold enhancement (and some as much as 1000-fold enhancement). The next step was to determine which of these sequences could function as internal ribosomal initiation sites.

To do this, the same 250 sequences were inserted into a vector bearing a hairpin structure. As Chaput explains: "If the ribosome latched onto the 5' end, it would hit that hairpin and would fall off. However if the ribosome skipped the hairpin and recognized the sequence on the other side of the hairpin independently and translated it, that's an indication that the sequence is functioning as an internal ribosomal initiation site." Both assays (for translation enhancement and internal ribosomal initiation) were validated under cell-free conditions and in human cells, using a vaccinia virus vector.

A study of this scope is possible thanks to innovative techniques for in vitro selection (such as mRNA display), as well as a revolutionary technology permitting massively parallel RNA sequencing (known as deep sequencing), which provides unprecedented speed and read accuracy.

Much remains to be learned about atypical translation processes. The mechanism of action for translation enhancing elements is still obscure, particularly in the case of internal ribosomal initiation sites. Similarly, the particular gene products that may result from cap-independent translation have yet to be identified and characterized.

Source: http://feeds.sciencedaily.com/~r/sciencedaily/health_medicine/genes/~3/giXLkqwIWhM/130616155211.htm

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