https://go.pub2srv.com/afu.php?id=1479657

Tuesday, 4 January 2022

Best Nursing Shoes for Male Nurse

 NEW BALANCE 608V5 AND YOU:

When you have new balance 608 v5,its easy and comfortable to move around all day.The new model 608 v5 includes and improved heelpad for premium cushioning and the best ABZORB outsole flakes for superior flexibility.

For Athletes: The New Balance 608v5 provides players with a high level of support in achieving their goals. That is why the New Balance 608 v5 is not designed to fit any image but to fit in every way  Which is why athletes like 608 v5 based on their performance.

The fifth version of the 608 v5 is designed to accommodate everyday men's and women's athletes. It is a verstyle shoe used for walking, gym, fitness and jogging.

Product Review: This product has a total score of 9.45 out of 10 based on 608 v5 reviews.

 Key Features of Product 608 v5:

 Ease of Binding: Its Closure Type is Strong and Seamless. The strap can be tightened or loosened at will.  Very easy to wear.

Quality of material: Strong quality soft and standard material is used.

 People's opinion: 608 v5 has full customer support based on its merits. 

Reasonable price: It is possible to get high quality shoes at reasonable price by purchasing. 

Color Variety: 608pv5 is available in almost every color. 

Overall Satisfaction: 608 v5 Overall satisfactory performance in terms of purchases.

Maintaining Physical Fitness: 608 v5 is perfect for maintaining your fitness in any area of ​​life. 

Comfortable to wear:  The sole of the shoe helps the foot absorb external pressure and increases your speed. It is very comfortable to wear. 

Outsole: The shoe rubber outsole has deep flakes that help your feet move in the shoe.

+3 K Analytics Review for New Balance 608: The 608 v5 Cross Trainer for Men is a very easy and comfortable shoe.

Upper sole: The fifth version of the New Balance 608 v5 uses standard leather for its upper unit. It gives the wearer comfort and strength of the foot. Extra soft leather straps around the heel and on the toes to strengthen the shoe structure.  In this version, the upper edges are extended upwards to provide extra support on both sides of the foot around the heel.

The inside of the shoe: The leather inside the shoe is kept fresh and airy with the help of holes so that the feet feel pleasant  freshness. 

608 v5 Shoe Outsole: The auxiliary outsole is fitted with an auxiliary standard leather strap that is stable during movement. Extends the unit to the front to cover the toes and protect them from collision.  The 608's outsole is lined with rubber at the bottom. Due to the non-marking of the rubber, it does not leave unwanted marks on the floor and the outsole design has been completely improvesid

Midsole: The midsole is placed inside a full length foam unit in the midsole to support the feet like a pillow. It helps to withstand the repetitive effects of regular exercise.  Keeps feet comfortable and light.

Pros:

Texture: Most users appreciate the texture and flexibility of the comfortable shoes offered by the 608. 

Size Fitness: New Balance 608v5's width and overall size of fitness fit consumers very much enjoyed. 

Color Scheme: The color scheme of 608 v5 is very elegant and attractive and similar to the colors of clothes. Especially the black color was very much liked by the consumers. Durability of the product: -  Appreciated the passage of time.

Physical Fitness: Most of the users were amazed that their arch felt physically fit while using this model.

 Disadvantages:

Excessive price: According to some people, the price of the shoe is little high.

Ankle Collar:Some customers desire that the ankle collar should have more support - the collar is a little higher to reach.

Monday, 29 November 2021

Jen Shah Net Worth: How Rich is RHOSLC Star Actually?

 Jen Shah Net Worth: How Rich is RHOSLC Star Actually?

 

Jen Shan, the face of popular reality tv show The Real Housewives of Salt Lake City. Jen who is the finest actor as well as an entrepreneur and a marketing expert has a net worth estimated to be $3 million. The companies on her name are JXA Fashion, The Shah Beauty and The Real Shah Lashes.

 

                                    Jen Shah Considered Her Job To Be A "Wizard of Oz" Before She Was Arrested

 

Early Life and Family

 

Jen Shah was born to Sione Kaisa Lui and Charlene Bonnie Vincent Lui on 4th oct, 1983 in Utah US. Her father, a rugby player passed away in 2008. She was brought up with five siblings Judd, Jessica, Jerrit, Jacob and Jehohn in a mixed ethnical background.

 

Jen Shah Net Worth and Career

Jen shah career started well with the reality tv show “The Real Housewives of Salt Lakes City”. Fortunately, she was selected for the first season telecasted on BRAVOTV in Nov 2020.  The story line was around six women in Sale Lake City.

 

Her dedication and hard work of 20 years was finally paid as she founded big marketing companies. After that she started off her acting career. Jen is associated with direct marketing making infomercials, direct mailing and print campaigns.

 Her expertise has made her leading businesswomen with exceptional business skills and commands. As the demand of her business, she has to travel a lot owning four different homes in NYC.

Her team consist of assistants to manage her looks, manage her work during covid. This all helped her to maintain her top position in her show.

 

Jen Shah Husband- Sharrieff Shah

Sharrieff shah, happily partner to Jen shah is ha NFL’s Utah cornerback coach for over 9 years now. Jen Shah is living happy life with her two sons Sharrieff Jr. 26 and Omar 16 years age now. She feels delightful after cooking healthy brunch for them.

 

Jen Shah Net Worth

 

Jen is acting as a full-time housewife on a reality tv show for a handsome amount. Jen shah personal wealth is estimated around $3 Million getting pai around $50,000 to $100,000 for her popular show. 

 

Source: https://exactnetworth.com/jen-shah-net-worth/

 

Monday, 30 March 2020

Coronavirus vaccine: when will it be ready?

Human trials will begin imminently – but even if they go well and a cure is found, there are many barriers before global immunisation is feasible
When will a coronavirus vaccine be ready? Illustration by James Melaugh.
 When will a coronavirus vaccine be ready? Illustration by James Melaugh. Illustration: James Melaugh/The Observer
Even at their most effective – and draconian – containment strategies have only slowed the spread of the respiratory disease Covid-19. With the World Health Organization finally declaring a pandemic, all eyes have turned to the prospect of a vaccine, because only a vaccine can prevent people from getting sick.
About 35 companies and academic institutions are racing to create such a vaccine, at least four of which already have candidates they have been testing in animals. The first of these – produced by Boston-based biotech firm Moderna – will enter human trials imminently.
This unprecedented speed is thanks in large part to early Chinese efforts to sequence the genetic material of Sars-CoV-2, the virus that causes Covid-19. China shared that sequence in early January, allowing research groups around the world to grow the live virus and study how it invades human cells and makes people sick.
But there is another reason for the head start. Though nobody could have predicted that the next infectious disease to threaten the globe would be caused by a coronavirus – flu is generally considered to pose the greatest pandemic risk – vaccinologists had hedged their bets by working on “prototype” pathogens. “The speed with which we have [produced these candidates] builds very much on the investment in understanding how to develop vaccines for other coronaviruses,” says Richard Hatchett, CEO of the Oslo-based nonprofit the Coalition for Epidemic Preparedness Innovations (Cepi), which is leading efforts to finance and coordinate Covid-19 vaccine development.
Coronaviruses have caused two other recent epidemics – severe acute respiratory syndrome (Sars) in China in 2002-04, and Middle East respiratory syndrome (Mers), which started in Saudi Arabia in 2012. In both cases, work began on vaccines that were later shelved when the outbreaks were contained. One company, Maryland-based Novavax, has now repurposed those vaccines for Sars-CoV-2, and says it has several candidates ready to enter human trials this spring. Moderna, meanwhile, built on earlier work on the Mers virus conducted at the US National Institute of Allergy and Infectious Diseases in Bethesda, Maryland.
Sars-CoV-2 shares between 80% and 90% of its genetic material with the virus that caused Sars – hence its name. Both consist of a strip of ribonucleic acid (RNA) inside a spherical protein capsule that is covered in spikes. The spikes lock on to receptors on the surface of cells lining the human lung – the same type of receptor in both cases – allowing the virus to break into the cell. Once inside, it hijacks the cell’s reproductive machinery to produce more copies of itself, before breaking out of the cell again and killing it in the process.
All vaccines work according to the same basic principle. They present part or all of the pathogen to the human immune system, usually in the form of an injection and at a low dose, to prompt the system to produce antibodies to the pathogen. Antibodies are a kind of immune memory which, having been elicited once, can be quickly mobilised again if the person is exposed to the virus in its natural form.
Traditionally, immunisation has been achieved using live, weakened forms of the virus, or part or whole of the virus once it has been inactivated by heat or chemicals. These methods have drawbacks. The live form can continue to evolve in the host, for example, potentially recapturing some of its virulence and making the recipient sick, while higher or repeat doses of the inactivated virus are required to achieve the necessary degree of protection. Some of the Covid-19 vaccine projects are using these tried-and-tested approaches, but others are using newer technology. One more recent strategy – the one that Novavax is using, for example – constructs a “recombinant” vaccine. This involves extracting the genetic code for the protein spike on the surface of Sars-CoV-2, which is the part of the virus most likely to provoke an immune reaction in humans, and pasting it into the genome of a bacterium or yeast – forcing these microorganisms to churn out large quantities of the protein. Other approaches, even newer, bypass the protein and build vaccines from the genetic instruction itself. This is the case for Moderna and another company, CureVac, both of which are building Covid-19 vaccines out of messenger RNA.
Cepi’s original portfolio of four funded Covid-19 vaccine projects was heavily skewed towards these more innovative technologies, and last week it announced $4.4m (£3.4m) of partnership funding with Novavax and with a University of Oxford vectored vaccine project. “Our experience with vaccine development is that you can’t anticipate where you’re going to stumble,” says Hatchett, meaning that diversity is key. And the stage where any approach is most likely to stumble is clinical or human trials, which, for some of the candidates, are about to get under way.
Clinical trials, an essential precursor to regulatory approval, usually take place in three phases. The first, involving a few dozen healthy volunteers, tests the vaccine for safety, monitoring for adverse effects. The second, involving several hundred people, usually in a part of the world affected by the disease, looks at how effective the vaccine is, and the third does the same in several thousand people. But there’s a high level of attrition as experimental vaccines pass through these phases. “Not all horses that leave the starting gate will finish the race,” says Bruce Gellin, who runs the global immunisation programme for the Washington DC-based nonprofit, the Sabin Vaccine Institute.
There are good reasons for that. Either the candidates are unsafe, or they’re ineffective, or both. Screening out duds is essential, which is why clinical trials can’t be skipped or hurried. Approval can be accelerated if regulators have approved similar products before. The annual flu vaccine, for example, is the product of a well-honed assembly line in which only one or a few modules have to be updated each year. In contrast, Sars-CoV-2 is a novel pathogen in humans, and many of the technologies being used to build vaccines are relatively untested too. No vaccine made from genetic material – RNA or DNA – has been approved to date, for example. So the Covid-19 vaccine candidates have to be treated as brand new vaccines, and as Gellin says: “While there is a push to do things as fast as possible, it’s really important not to take shortcuts.”
An illustration of that is a vaccine that was produced in the 1960s against respiratory syncytial virus, a common virus that causes cold-like symptoms in children. In clinical trials, this vaccine was found to aggravate those symptoms in infants who went on to catch the virus. A similar effect was observed in animals given an early experimental Sars vaccine. It was later modified to eliminate that problem but, now that it has been repurposed for Sars-CoV-2, it will need to be put through especially stringent safety testing to rule out the risk of enhanced disease.
It’s for these reasons that taking a vaccine candidate all the way to regulatory approval typically takes a decade or more, and why President Trump sowed confusion when, at a meeting at the White House on 2 March, he pressed for a vaccine to be ready by the US elections in November – an impossible deadline. “Like most vaccinologists, I don’t think this vaccine will be ready before 18 months,” says Annelies Wilder-Smith, professor of emerging infectious diseases at the London School of Hygiene and Tropical Medicine. That’s already extremely fast, and it assumes there will be no hitches.
In the meantime, there is another potential problem. As soon as a vaccine is approved, it’s going to be needed in vast quantities – and many of the organisations in the Covid-19 vaccine race simply don’t have the necessary production capacity. Vaccine development is already a risky affair, in business terms, because so few candidates get anywhere near the clinic. Production facilities tend to be tailored to specific vaccines, and scaling these up when you don’t yet know if your product will succeed is not commercially feasible. Cepi and similar organisations exist to shoulder some of the risk, keeping companies incentivised to develop much-needed vaccines. Cepi plans to invest in developing a Covid-19 vaccine and boosting manufacturing capacity in parallel, and earlier this month it put out a call for $2bn to allow it to do so.
Once a Covid-19 vaccine has been approved, a further set of challenges will present itself. “Getting a vaccine that’s proven to be safe and effective in humans takes one at best about a third of the way to what’s needed for a global immunisation programme,” says global health expert Jonathan Quick of Duke University in North Carolina, author of The End of Epidemics (2018). “Virus biology and vaccines technology could be the limiting factors, but politics and economics are far more likely to be the barrier to immunisation.”
The problem is making sure the vaccine gets to all those who need it. This is a challenge even within countries, and some have worked out guidelines. In the scenario of a flu pandemic, for example, the UK would prioritise vaccinating healthcare and social care workers, along with those considered at highest medical risk – including children and pregnant women – with the overall goal of keeping sickness and death ra tes as low as possible. But in a pandemic, countries also have to compete with each other for medicines.
Because pandemics tend to hit hardest those countries that have the most fragile and underfunded healthcare systems, there is an inherent imbalance between need and purchasing power when it comes to vaccines. During the 2009 H1N1 flu pandemic, for example, vaccine supplies were snapped up by nations that could afford them, leaving poorer ones short. But you could also imagine a scenario where, say, India – a major supplier of vaccines to the developing world – not unreasonably decides to use its vaccine production to protect its own 1.3 billion-strong population first, before exporting any.
Outside of pandemics, the WHO brings governments, charitable foundations and vaccine-makers together to agree an equitable global distribution strategy, and organisations like Gavi, the vaccine alliance, have come up with innovative funding mechanisms to raise money on the markets for ensuring supply to poorer countries. But each pandemic is different, and no country is bound by any arrangement the WHO proposes – leaving many unknowns. As Seth Berkley, CEO of Gavi, points out: “The question is, what will happen in a situation where you’ve got national emergencies going on?”
This is being debated, but it will be a while before we see how it plays out. The pandemic, says Wilder-Smith, “will probably have peaked and declined before a vaccine is available”. A vaccine could still save many lives, especially if the virus becomes endemic or perennially circulating – like flu – and there are further, possibly seasonal, outbreaks. But until then, our best hope is to contain the disease as far as possible. To repeat the sage advice: wash your hands.
 This article was amended on 19 March 2020. An earlier version incorrectly stated that the Sabin Vaccine Institute was collaborating with the Coalition for Epidemic Preparedness Innovations (Cepi) on a Covid-19 vaccine. It was further amended on 30 March to remove an incorrect reference to CureVac being a “Boston company”; its world headquarters are in Tübingen, Germany.

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Monday, 24 April 2017

Fun with cop

Funny Bout

Sunday, 23 April 2017

Charlie Chaplin in Plane

Charlie Chaplin in a War funny video

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