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A Flu Vaccine That s Always in Season

Image: Thomas Fuchs

In the spring of 2013 a strain of influenza virus that had never infected humans before began to make people in China extremely ill. Although the virus, known as H7N9, had evolved among birds, it had mutated in a way that allowed it to spread to men, women and children. Within several months H7N9 sickened 135 individuals, of whom 44 died, before subsiding with the advance of summer weather.

We got lucky with H7N9. Had it triggered a pandemican explosion of infectious disease across a large geographical areawe would have been woefully unprepared, and millions might have died. The trouble is that every new virus requires a new vaccine, and making new vaccines takes time. Even a typical flu season is brimming with slightly mutated versions of familiar viruses. In most cases, manufacturers anticipate these changes and tweak existing formulas so that they will still work against the new strains. When a virus like H7N9 makes a surprise appearance in people, however, manufacturers must scramble to concoct an entirely new vaccine from scratch, which takes too long to prevent a large number of people from becoming sick and dying.

Public health officials have longed for years to turn the tables, envisioning a universal flu vaccine that would be ready and waiting on the shelves to defeat either a marginally mutated strain or a completely unexpected virus. After numerous disappointments, a handful of recent studies indicate that a universal vaccine may at last be close at hand. In an interview last summer National Institutes of Health director Francis Collins suggested that one might be achieved in the laboratory in just five years. Before such a vaccine can reach the general public, however, researchers will have to convince either manufacturers or the government to pay for more studies and demonstrate to the U.S. Food and Drug Administration that the new vaccines are just as safe as those we already use.

Stalking a Killer Flu vaccines have worked on the same principles since investigators first made them in the 1940s. Each vaccine contains flu antigensbits of viral molecules that can trigger an immune response. The antigens used in routine flu vaccines are fragments of a mushroom-shaped protein, called a hemagglutinin, that protrudes from a flu virus's surface and helps the pathogen cling to cells inside an infected individual. Once exposed to those bits of protein, a person's immune system produces sentinel molecules called antibodies that will recognize any flu virus possessing the same hemagglutinin and direct an attack against it.

Flu is a rapidly evolving virus, however, and the structure of hemagglutinin in a given strain changes in small ways every season. Even a minor alteration can make it much more difficult for the immune system to identify and eliminate a flu virus that is nearly identical to its earlier version. This is why we have to get new flu shots every year.

Scientists have searched for decades for a way to outsmart the flu virus rather than always hurrying to outpace it. The first glimpse of more efficient vaccines appeared in 1993, when Japanese researchers discovered that mice sometimes generate a single antibody that blocks infection by two flu strains with different hemagglutinins. Fifteen years later several different teams demonstrated that humans occasionally make these cross-protective, or broadly neutralizing, antibodies as well. Most of these antibodies bind not to a hemagglutinin's mushroom cap but rather to its slender stema region of the molecule where, as it turns out, less structural mutation takes place. Because the stem's makeup is similar across many strains of flu, the researchers reasoned, an antibody that recognizes it could potentially protect against a range of viral strains with distinct caps.

Building on this discovery, several groups have altered the structure of hemagglutinins, creating a cap to which the immune system does not react. Animals exposed to these tweaked proteins produce cross-protective antibodies that bind to the stalk rather than strain-specific antibodies that home in on the cap. Other scientists are trying to get animals and people to make antibodies against a different viral protein, M2, which is embedded in the flu virus's membrane and helps it enter cells. Like the hemagglutinin stalk, M2 changes little.

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A Flu Vaccine That s Always in Season

Syfy’s Thriller ‘Helix’ Ratings Soft In Debut

A killer virus being barely contained in the Arctic was the launch point for Syfys new thriller series Friday. While thats the premise of the series, Helix wasnt exactly bubonic with viewers for its premiere. Despite a strong visual and panel Comic-Con presence last summer plussome hefty promotion, the 90-minute Jeffrey Reiner-directed debut episode garnered just 1.8 million viewers at 10 PM. With a 0.6 rating, Helix pulled in 734,000 viewers in among adults 18-49 and 893,000 in the 25-54 demo. Thats a far cry from the 2.7 million total viewers the channel drew for Defiance when that debuted on April 15, 2013. That two-hour Monday opener had 1.3 million among the 18-49 and 1.4 million among adults 25-54, Syfys top total viewers and 25-54 performances since 2009s Warehouse 13.To give some further context of where Helix stands in the Syfy universe right now,Warehouse 13 had 3.5 million viewers with a 2.5 household rating,1.7 million adults 25-54 and 1.3 million adults 18-49 for the third best viewership debut for any Syfy series behind 2004s Stargate Atlantis (4.2 million) and 2006s Eureka (4.1 million).

Helix, which features ex-The Killing starBilly Campbellas its emotionally troubled CDC pathologist lead, was picked up for a 13-episode straight-to-series order last March.In his return to Syfy,Battlestar Galacticadeveloper/EPRonald D. Mooreis producing Helix withshowrunner Steven Maeda and Lynda Obst. Writer Cameron Porsandeh is co-exec producing the series.

Deadline's Dominic Patten - tip him here.

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Syfy’s Thriller ‘Helix’ Ratings Soft In Debut

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