Category: Corona Virus Vaccine

Representative Bill Foster (DIL) is leading an effort to encourage U.S. regulators to allow volunteers to be infected with the pandemic coronavirus to speed vaccine testing.

By Jon CohenApr. 21, 2020 , 11:55 AM

Sciences COVID-19 reporting is supported by the Pulitzer Center.

Political support is building for regulators in the United States to embrace the controversial strategy of intentionally infecting volunteers with the virus that causes COVID-19 in order to test experimental vaccines. Such human challenge trials could greatly accelerate the development of an effective vaccine, 35 members of the House of Representatives argue in a letter sent yesterday to the heads of the U.S. Food and Drug Administration (FDA) and its parent agency, the Department of Health and Human Services (HHS).

[A] more risk-tolerant development process is likely appropriate in the case of a COVID-19 vaccine, write the group of lawmakers, which includes both Democrats and Republicans. The enormous human cost of the COVID-19 epidemic alters the optimization of the risk/benefit analysis.

The lawmakers also back the idea of parallel, simultaneous testing of different doses of a vaccineas opposed to the traditional practice of sequential testing that, for safety reasons, begins by giving trial participants the lowest dose first and then ratchets up. Parallel testing could more quickly move a candidate vaccine from small studies that look only at safety and immune responses to larger ones that actually assess efficacy, the letter notes.

The letter was spearheaded by Representatives Bill Foster (DIL), a physicist, and Donna Shalala (DFL), former HHS secretary. This is designed as much as anything to give the FDA political cover needed to approve challenge trials, Foster tells ScienceInsider. The FDA must be worried that theyre going to have these trials, something bad is going to happen, therell be a bad story in the newspaper about a sympathetic person who got unlucky in one of these trials and didnt survive. And then Congress is going to go and say: Lets have a hearing on this, and start dragging them in. One of my goals in here was to let them know that Congress understands that there are no risk-free paths here.

According to the latest tally by the World Health Organization (WHO), 76 vaccine candidates are already under development around the world. Five have moved into clinical trials. But public health officials have cautioned that, from start to finish, it takes at least 1 yearand more likely 18 monthsto prove whether a candidate is safe and effective. And thats if no problems surface.

Stanley Plotkin, a leading vaccine researcher at the University of Pennsylvania who has advocated human challenge studies for COVID-19 vaccines, welcomes the congressional show of support. It is urgent that authorities like FDA and WHO give challenge studies immediate consideration, as they could speed up the use of vaccines even before formal licensure that would depend on additional data, Plotkin says.

In theory, challenge trials could enroll volunteers who are at low risk of harm from the virus that causes COVID-19dubbed SARS-CoV-2such as young adults who rarely develop serious symptoms after becoming infected naturally. Our situation in this pandemic is analogous to war, in which there is a long tradition of volunteers risking their health and lives on dangerous missions for which they understand the risks and are willing to do so in order to help save the lives of others, the letter states. Every week of delay in the deployment of a vaccine to the seven billion humans on Earth will cost thousands of lives.

Critics of human challenge studies note that many unknowns remain about SARS-CoV-2. Conducting proper studies would require time to grow the viruses to be used in the challenges under sterile conditions and to determine the optimal challenge dose. Whats more, Sinovac, a Chinese company that began clinical trials of its COVID-19 vaccine last week, says it may complete the first two phases of testing by the end of June and seek regulatory approval for emergency use of their candidate in high-risk people like health care workers, which is another way to shortcut answers to whether a produce is safe and effective.

Foster counters that testing a vaccine in health care workers who are needed in a hot spot also has risks, as it might take them out of work for a time. He hopes the letter just makes the FDA a little less scared, stressing that its pretty clear that the only way were really finally going to get out of this [pandemic] is when we have an effective vaccine.

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United States should allow volunteers to be infected with coronavirus to test vaccines, lawmakers argue - Science Magazine

A coronavirus vaccine being developed by Oxford University will enter human trials as early as this Thursday, according to the U.K.s health secretary.

The U.K. government will provide 20 million ($24 million) to the universitys team and a further 22.5 million to Imperial College, where scientists are also working on a vaccine. Scientists at Oxford have previously said the aim is to produce a million doses of the vaccine by September.

Secretary of State for Health and Social Care Matt Hancock praised both teams for making rapid progress and said the U.K. will throw everything weve got at developing a vaccine.

He also said the government would invest in manufacturing capabilities so that if either vaccine was successful it could be available for British people as soon as humanly possible.

We are going to back them to the hilt and give them every resource that they need to get the best possible chance of success as soon as possible. The upside of being the first country in the world to develop a successful vaccine is so huge that I am throwing everything at it.

Read:These 21 companies are working on coronavirus treatments or vaccines

However, he insisted vaccine development was a process of trial and error and trial again.

The Oxford University project, a collaboration between the universitys Jenner Institute and Oxford Vaccine Group, opened recruitment for the clinical trial for healthy adults between 18 and 55 at the end of March, having begun research on a vaccine against the coronavirus-borne disease COVID-19 in February. Trials will now begin as soon as this Thursday, the health secretary revealed in the governments daily briefing on Tuesday.

Praising the team, Hancock said reaching this stage in normal times would take years.

Also:GSK, Sanofi to team up on COVID-19 vaccine

Speaking at the end of March, Adrian Hill, director of Oxford Universitys Jenner Institute, said: The Oxford team had exceptional experience of a rapid vaccine response, such as to the Ebola outbreak in West Africa in 2014. This is an even greater challenge.

Vaccines are being designed from scratch and progressed at an unprecedented rate. The upcoming trial will be critical for assessing the feasibility of vaccination against COVID-19 and could lead to early deployment.

Read on:Hydroxychloroquine as treatment for COVID-19 shows no benefit and more deaths in VA study

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Oxford University coronavirus vaccine to begin human trials on Thursday as U.K. throws everything at vital breakthrough - MarketWatch

Here are five things you need to know about the coronavirus outbreak this Tuesday evening. We'll have another update on Wednesday morning.

Health Secretary Matt Hancock, giving the daily briefing at Downing Street, has revealed that a potential coronavirus vaccine being developed by Oxford University will be trialled in people from Thursday. "The upside of being the first country in the world to develop a successful vaccine is so huge that I am throwing everything at it," he said. It comes as the number of hospital deaths from coronavirus in the UK has risen by 823 to 17,337 people.

New figures from the Office for National Statistics show deaths in England and Wales have hit a 20-year high, but experts also believe virus deaths could well have peaked. There were about 8,000 more deaths in the week up to 10 April than is normal at this time of year. But separate analysis by NHS England is being highlighted by experts which showed the number of deaths in hospitals has been falling since 8 April.

Capt Tom Moore, the 99-year-old war veteran who has raised more than 27m for the NHS, has appeared via video link to open a new Nightingale hospital in Harrogate. Social distancing rules meant a virtual ceremony had to be held for the opening of the 500-bed facility at Harrogate Convention Centre, which was converted into a hospital in less than three weeks.

Born eight weeks early and weighing just 3lbs 5oz (1.5kg), Peyton Maguire was diagnosed with Covid-19 at just three weeks old. "I think the doctor was trying to keep me calm but I was sobbing," her mum Tracy, from Lanarkshire, says. Peyton was given steroids to help strengthen her lungs and received "amazing" care from neonatal nurses in hospital. Fortunately she has now recovered, with mum and baby leaving hospital on Monday.

Imagine you've been sailing around the world, blissfully unaware of the global pandemic changing our lives. That's what happened to Elena Manighetti and Ryan Osborne, who asked their loved ones to keep in touch - but not to share bad news. So after 25 days at sea, they attempted to dock on a small Caribbean island in mid-March. There, they found all the island's borders were closed and discovered the world had been suffering from a pandemic they'd heard nothing about.

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Coronavirus: Evening update as human vaccine trials to start this week - BBC News

For indispensable reporting on the coronavirus crisis and more, subscribe to Mother Jones' newsletters.

You have perhaps seen on news programs that there are already several dozen potential coronavirus vaccines in development already. Some of them have even been given to people! So whats the deal with the 12-18 month timeline to get them ready for widespread deployment? Heres a quick primer:

Most vaccines work by using a weakened or dead version of the virus, which stimulates your immune system into creating antibodies without actually making you sick. However, it generally takes 3-6 months just to develop these attenuated viruses, and we dont have the time for that.

This adds up to 15-27 months. Since new techniques are being used and we have never developed a coronavirus vaccine before, the low end of this estimate is unlikely. Even with lots of different groups pursuing lots of different avenues, 18-24 months is a lot more likely. Maybe a little less for emergency use on a smallish number of people. (And who would pick these lucky folks?) Maybe more if were being too optimistic about how well these trials will go.

The rest is here:

Why Will It Take So Long to Develop a Coronavirus Vaccine? - Mother Jones

Saphora Smith

1h ago / 6:18 PM UTC

A potential coronavirus vaccine being developed at the University of Oxford in Britain will be trialed on people starting Thursday, Britains Health Secretary Matt Hancock said.

Hancock said Tuesday two leading vaccine developments were taking place in Britain one at the University of Oxford and another at Imperial College London as he announced more than $50 million in fresh funding for the trials.

He added that the project at Imperial would receive more than $27 million to support its phase two clinical trials and beyond, while Oxford University would be granted more than $24 million to fund its clinical trials.

We have put more money than any other country into the global search for a vaccine, he said. Both of these promising projects are making rapid progress and Ive told the scientists leading them that we will do everything in our power to support.

Hancock added that at the same time the U.K. will invest in manufacturing capabilities so that if either of these vaccines safely works then they can make it available for the British people as soon as humanly possible.

But he warned that nothing about the process was certain.

Ali Vitali

2h ago / 5:28 PM UTC

Their numbers were small, but their message was powerful.

Nearly two dozen nurses from National Nurses United stood in protest outside the White House Tuesday, demanding more Personal Protective Equipment and a codification of protective standards as healthcare workers across the country find themselvesunderprepared on the frontlines of the coronavirus crisis.

Were here because our colleagues are dying, Erica Jones, a nurse at Washington Hospital Center in D.C., told NBC News. Jones stood silently Tuesday as the names of 50 nurses who died from COVID-19 were read aloud in the shadow of the White House.

Read the full story here.

Rev. Dr. William J. Barber and Jonathan Wilson-Hartgrove

2h ago / 5:24 PM UTC

Though President Donald Trump insists on calling it an invisible enemy, COVID-19 is ever before us and the data increasingly make clear that the South will soon become ground zero for coronavirus deaths.

COVID-19, then, is a contrast dye, highlighting the South as the native home of poverty in America.

Read the full opinion piece here.

David K. Li

2h ago / 5:15 PM UTC

New York Gov. Andrew Cuomo said Tuesday he faced sharp questions - from his own adult daughters - on why he had not looked overseas to buy coronavirus test kits.

Cuomo said his family was watching TV news on Monday night when a story aired on Maryland Gov. Larry Hogan, who with help from his wife, just scored 500 test kits from her native South Korea,

"My daughter turns to me and looks at me and says, 'Wow that was really smart,' " said Cuomo, father of three adult daughters. "One of my other daughters, who's a little more pointed in life ... said, 'Why didn't you think of that, Dad? Why didn't you think of buying test kits from South Korea?'"

The New York governor was hammering home his belief that the federal government should take the lead in securing equipment to contain the pandemic, though he heaped praise on his Maryland counterpart: "God bless Larry Hogan; he really thought outside the box."

Ben Kesslen

3h ago / 4:47 PM UTC

Germany's famous Oktoberfest, the world's largest beer festival, has been cancelled, Bavarian officials announced Tuesday.

"It hurts, it's such a pity," Minister PresidentMarkus Sder of Bavaria, in southern Germany, said in a news conference. "We have agreed that the risk is simply too high."

The festival, planned to begin in late September and last through early October, usually draws around six million visitors from around the world. But Soder said "as long as there is no vaccine, as long as there is no medicine, special care must be taken," adding that the festival could have been a potential "virus hub."

Dan Good

3h ago / 4:39 PM UTC

Georgia reported nearly 20,000 confirmed coronavirus cases and 800 deaths Tuesday days ahead of Gov. Brian Kemp's planned reopening of many of the state's businesses.

The latest numbers, announced at noon Tuesday, reflect an increase of 482 cases and 24 deaths since the previous update at 7 p.m. Monday. The counties with the most coronavirus cases are Fulton (2,208 cases and 82 deaths), Dekalb (1,534 cases and 29 deaths), and Dougherty (1,446 cases and 103 deaths).

An additional 3,779 remained hospitalized withCOVID-19 on Tuesday.

Despite the state's coronavirus death toll continuing to rise, Kemp on Monday announced plans to reopen businesses such as gyms, barber shops, and bowling alleys. Kemp'sdecision was criticized by many state and local leaders.

There's nothing about this that makes sense," Stacey Abrams said in an interview on MSNBCs Morning Joe. "The mayors of Atlanta, Albany and Savannah have all questioned the wisdom of doing this. And the fact is the governor didn't consult with mayors before making this decision.

Pete Williams

3h ago / 4:50 PM UTC

President Donald Trump cited both public health concerns and the economy as reasons for suspending immigration into the U.S. in his tweet Monday night announcing the move.

"In light of the attack from the Invisible Enemy, as well as the need to protect the jobs of our GREAT American Citizens, I will be signing an Executive Order to temporarily suspend immigration into the United States!" he wrote.

Can the president do that? The answer appears to be yes. Any such sweeping action is bound to produce court challenges, but it's not at all clear that they would succeed.

The president would probably cite the same legal authority that he used to justify his March 11 executive orderrestricting entry by travelersfrom countries coping with the pandemic; it's a provision of federal law the Immigration and Nationality Act that gives a president very broad power.

Read the full story here.

David K. Li

3h ago / 4:18 PM UTC

A Louisiana pastor who has defied state orders against large gatheringswas arrestedTuesday for allegedly backing his church bus dangerously close to a protester.

Pastor Tony Spell of Life Tabernacle Church in the city of Central, near Baton Rouge, was charged with aggravated assault in connection to the incident Sunday that was caught on tape, police said.

Central police chief Roger Corcoran said local authorities are trying to enforce the law and insisted that Spell isn't being denied his freedom to practice religion.

"They're trying to make a mockery of this, like he's some kind of victim," Corcoran told NBC News on Monday night. "No one, not one person, is trying to stop him from preaching the word."

Read the full story here.

David K. Li and Tom Winter

4h ago / 3:48 PM UTC

At least another 481 New York state residents died from complications related to COVID-19 in the past 24 hours, officials said Tuesday.

The state's coronavirus death toll has now reached 14,828 since the outbreak, Gov. Andrew Cuomo said.

There were 1,308 new patients hospitalized with COVID-10 on Monday, down from rates of 2,000 a day late last week.Cuomo called it good news while noting, "Our definition of good has changed here.

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Coronavirus live updates: Trump says he is suspending immigration over coronavirus - NBC News

Vaccines can help end the coronavirus pandemic, but its impossible to put a clear timeline on their development. We will have to deal with the virus for the foreseeable future, and theres no guarantee that we will have widespread vaccinations in 2021 or even 2022.

There is always a sense of optimism when we start writing about coronavirus vaccines. The unprecedented impetus, the huge sums invested, the numerous talented research teams it all gives a sense of the world coming together and working towards a common goal.

We shouldnt get carried away by a sense of exuberance, however. There are few guarantees when it comes to vaccines, and putting all our long-term eggs in the vaccine basket can end up backfiring if we dont take other mitigation measures.

It typically takes a decade or so to develop a new vaccine. Of course, this is not your typical situation. More than 80 vaccine projects have kicked off around the world an effort the likes of which has never been seen before. In this scenario, some immunologists have said that if everything goes right, we may have a vaccine in 12-18 months. As humans are inherently optimistic, we tend to interpret that as well have a vaccine in a year but thats not what researchers are saying.

For starters, a vaccine needs to produce an immune response. This is the crux of any vaccine, but its far from being the only requirement. A vaccine also needs to be safe and not cause any significant side effects. Even when an immune response has been produced, and it is efficient in a large enough percentage of the population, it takes months and months of clinical treatments to ensure that the vaccine is indeed safe and effective and there are no guarantees.

Theres no guarantee an immune response will be produced. Theres no guarantee that it will be safe. Theres essentially nothing to promise us that we will have a vaccine in a year, or two years, or any given time.

Then, even assuming we have a vaccine, scaling production for millions or billions of doses is not exactly a trivial task, especially in a struggling economy. It will take months if not years before a sufficient part of the population is immunized.

Considering all these factors, its easy to see a future where most of us dont get a coronavirus vaccine in 2021 or even 2022. David Nabarro, Professor of Global Health at Imperial College, London, and an envoy for the World Health Organisation on COVID-19 recently said that we will have to live without the vaccine for the foreseeable future and our best chance is to adapt to it.

In an interview with The Observer,Nabarro said the public should not assume that a vaccine will definitely be developed soon.

You dont necessarily develop a vaccine that is safe and effective against every virus. Some viruses are very, very difficult when it comes to vaccine development so for the foreseeable future, we are going to have to find ways to go about our lives with this virus as a constant threat.

That means isolating those who show signs of the disease and also their contacts. Older people will have to be protected. In addition hospital capacity for dealing with cases will have to be ensured. That is going to be the new normal for us all.

This doesnt mean that we shouldnt try to develop a vaccine; quite the contrary. The more vaccine projects there are, the greater the odds of actually developing one in a 12-18 month timeframe. But its just not certain. In a recent opinion article for The Guardian, Patrick Vallance, the UK government chief scientific adviser, said there are reasons to be optimistic about vaccines but it will take time. How much time? Again, its hard to say.

The most optimistic version weve heard comes from Oxford scientists, who say that we may have a vaccine by September. The most pessimistic is that well never have a vaccine. The reality is probably somewhere in between, but exactly where it lies on the axis between September and never, its hard to say. This its hard to say is a key element of our fight with COVID-19 uncertainty is a key problem posed by the virus, and whether we like it or not, uncertainty is part of this challenge.

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Vaccines in shining armor Can vaccines really save us from the coronavirus? - ZME Science

Hanneke Schuitmaker: Well, with working from home and social distancing, it's sort of a blurry timeline for me. I try to get up early in the mornings. The alarm is set for 6:30 a.m., I start work at 7:45 and finish in the evening at 9 or 10 p.m. I do stop occasionally to eat dinner with my family and walk my dog. I cannot say that the hours I spend working on this vaccine are normal. They add up to be a lot because there's so many things happening in parallel. While Im working from home, I do a lot of virtual meetings with my team, with sub teams, and with management to coordinate, to discuss our lab results, and to make decisions.

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Im Working 14-Hour Days To Develop The Coronavirus Vaccine - Refinery29

Paul McKay, a molecular immunologist at the Imperial College School of Medicine in London, checks a dish of bacteria containing genetic material from the new coronavirus. He and his team are testing a candidate vaccine. Tolga Akmen/AFP via Getty Images hide caption

Paul McKay, a molecular immunologist at the Imperial College School of Medicine in London, checks a dish of bacteria containing genetic material from the new coronavirus. He and his team are testing a candidate vaccine.

Right now scientists are trying to accomplish something that was inconceivable a decade ago: create a vaccine against a previously unknown virus rapidly enough to help end an outbreak of that virus. In this case, they're trying to stop the spread of the new coronavirus that has already infected tens of thousands of people, mainly in China, and given rise to a respiratory condition now known as COVID-19.

Typically, making a new vaccine takes a decade or longer. But new genetic technologies and new strategies make researchers optimistic that they can shorten that timetable to months, and possibly weeks and have a tool by the fall that can slow the spread of infection.

What's the urgency?

"Vaccines are really our most successful tool to prevent an infectious disease," says David Weiner, executive vice president and director of the Vaccine & Immunotherapy Center at the Wistar Institute in Philadelphia.

It used to take a long time to make vaccines, because scientists had to isolate and grow the virus in the lab. But now, it's possible to skip that step altogether and build a vaccine based on a virus' genetic sequence.

Chinese scientists made that genetic sequence from the new coronavirus public in early January, just weeks after the first infections with the virus were reported. That prompted several labs to start work on building a vaccine.

Vaccines work by teaching an individual's immune system to recognize an invading virus and neutralize it. The vaccine that Weiner and his colleagues are developing is what's called a DNA vaccine.

They'll first turn pieces of the new coronavirus' genetic code (which is RNA) into complementary snippets of DNA. These snippets will then be injected into someone's skin, where they will be taken up by skin cells. The skin cells will then turn those DNA sequences into proteins identical to the ones a virus would produce, and those will be what "teaches" the immune system to recognize the new virus.

Weiner and his colleagues are in the process of determining which viral sequences produce the best "teachers."

This isn't Wistar's first stab at rapid vaccine development. Weiner and his team worked on a vaccine for Ebola after an outbreak of that virus in 2014.

Including the initial time needed for animal testing and human safety testing, "We were able to go from no vaccine to a vaccine tested in the clinic in about 18 months 15 to 18 months," he says. They also made a vaccine against the coronavirus that causes Middle East respiratory syndrome, after an outbreak in South Korea. "And we were able to design and develop and move into the clinic in 11 months."

Weiner says he's hoping to halve that time with the vaccine they are making against the new coronavirus.

Keith Chappell at the University of Queensland in Brisbane, Australia, thinks he can do even better. He, too, has a vaccine that's based on the virus' genetic sequence. The Queensland team has come up with an approach it calls the molecular clamp. It works by improving the body's immune response to certain viral proteins.

"Our goal was to be able to hit 16 weeks from sequence information to having a product that is shown to be safe and effective [in lab tests] and is ready for administration to the first humans," Chappell says.

Right now, Chappell and his colleagues are also trying to figure out which genetic sequences will be most effective at helping the immune system recognize the coronavirus.

"Next steps will be moving into animal models for testing and also working out how to scale up to get to the levels that would be required in humans and beyond," he says.

Both Chappell's team in Australia and Weiner's team in Philadelphia, in collaboration with the pharmaceutical company Inovio, are getting financial support from a fairly new organization called CEPI, the Coalition for Epidemic Preparedness Innovations. CEPI is a global partnership of public, private and philanthropic organizations; it's also supporting efforts at the biotech companies Moderna and CureVac.

Ami Patel, a research assistant professor at the Wistar Institute, is working with David Weiner and others on a DNA vaccine against the new coronavirus. The team is in the process of determining which viral sequences produce the best "teachers" to help the human immune system defeat the virus. Darien Sutton hide caption

Among other vaccine efforts worldwide, the pharmaceutical giant Johnson & Johnson is working on a vaccine, and GSK has also offered to help new vaccine efforts. Researchers at Imperial College London have developed a vaccine that's already being tested in animals, and vaccine efforts are also reportedly underway in China.

CEPI CEO Richard Hatchett says the organization was created when people realized that an Ebola vaccine had been under development for a decade and it still took more than a year to get it to people when the 2014 Ebola outbreak occurred in western Africa.

"There were a number of enlightened global public health leaders who said, 'You know, that shouldn't happen. We should have some kind of an organization to develop vaccines against epidemic diseases,'" he says.

Even in the rosiest of scenarios, Hatchett says, once the vaccine is in hand, it still needs to get to the people who need it, and that takes time at least weeks to months, depending on the urgency.

Naturally, public health officials would like to have a vaccine as soon as possible. If the coronavirus outbreak pattern is anything like those of flu outbreaks, it will tend to taper off when the weather gets warmer and pick up as winter approaches and people spend more time indoors.

"We are making very aggressive efforts in the hopes of having a vaccine available some form of vaccine available, potentially, as early as this fall," Hatchett says.

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Is A Coronavirus Vaccine Coming Soon? Maybe By Fall ...

SARS-CoV-2, the virus that leads to coronavirus disease 19 (COVID-19), has spread rapidly from the first known cases in China in December 2019 to countries around the world.

On March 10, 2020, the World Health Organization (WHO) reported that there were 113,702 confirmed cases of COVID-19 around the world, plus 4,012 deaths.

In response to this global health crisis, researchers are working on developing a coronavirus vaccine as soon as possible.

Learn more about vaccine development and the possible timeline in this article.

Researchers striving to develop a coronavirus vaccine are working with different approaches, including:

The sections below will discuss these approaches in more detail.

Whole virus vaccines use weakened or dead forms of the virus that causes the disease.

They can be effective at providing immunity in the long run, but there is a risk that some people could develop symptoms of the illness due to the vaccination.

Reports state that Johnson & Johnson, Codagenix, and researchers at the University of Hong Kong are working on this kind of vaccine.

Recombinant protein subunit vaccines do not carry the risk of causing an infection in people who receive them, because they do not contain any live pathogens.

Researchers are investigating whether or not they can make a recombinant protein subunit vaccine that targets a protein called spike (S-) protein. The new coronavirus uses the S-protein to attach to and infect cells.

Novavax, Clover Biopharmaceuticals, the University of Queensland, and a consortium led by Texas Childrens Hospital for Vaccine Development are using this approach to develop a coronavirus vaccine.

Other researchers are investigating whether or not they can create a vaccine using antibodies from the SARS outbreak that began in 2002.

SARS has many similarities to COVID-19, as they are caused by related coronaviruses.

So far, scientists have shown that the antibodies that neutralize the SARS-causing virus can also limit how well the new coronavirus infects cells in laboratory studies.

Read more about the development of an antibody vaccine here.

Nucleic acid vaccines inject genetic material, such as DNA or RNA, into a live host. The cells that contain the new nucleic acid then make the proteins that were encoded in the DNA or RNA, which they present to the immune system.

Although the process is complex, nucleic acid vaccines enable the immune system to fight off particular pathogens.

Using nucleic acids such as DNA or RNA to deliver immunity is a promising approach, but to date, it is a technique only available in veterinary medicine.

However, researchers say that three companies are looking to develop a coronavirus vaccine using this approach: Inovio Pharmaceuticals, Moderna Therapeutics, and Curevac.

The CDC recommend that all people wear cloth face masks in public places where it is difficult to maintain a 6-foot distance from others. This will help slow the spread of the virus from asymptomatic people or people who do not know they have contracted the virus. Cloth face masks should be worn while continuing to practice physical distancing. Instructions for making masks at home can be found here. Note: It is critical that surgical masks and N95 respirators are reserved for healthcare workers.

Projections for how long it will take to develop a coronavirus vaccine vary widely, depending on whether the person making the projection is a scientist, politician, or businessperson.

Politicians and manufacturers alike have implied that a coronavirus vaccine could be available within months.

However, based on their knowledge and experience, scientists say that developing a coronavirus vaccine:

If the timeline for the production and distribution of a coronavirus vaccine seems long, that is because there are many steps in place to ensure that it is safe and effective.

Specifically, once researchers create a potential vaccine, prospective producers must submit an Investigational New Drug Application to the Food and Drug Administration (FDA) that describes the product, the manufacturing process, and its effectiveness in animal testing.

In the next phase, a vaccine must successfully complete the following series of clinical trials:

Specific medications to treat COVID-19 do not yet exist. Treatment will focus on alleviating symptoms while a person recovers.

Antibiotics cannot treat COVID-19, as they are meant for bacterial infections and have no affect on viruses such as coronavirus.

However, some researchers are looking at repurposing existing drugs, including antibiotics, as COVID-19 treatments. Learn more here.

Public health experts and medical professionals also recommend that people with the illness try to stay away from others during recovery.

Public health measures that limit the spread of infection include:

Different governments and organizations have taken varying approaches to limiting the spread of coronavirus.

People who think they have been exposed to someone with COVID-19 and develop symptoms such as a fever, cough, or trouble breathing should call their doctor, according to the CDC.

The most important thing that people with mild forms of the disease can do is make sure that they limit contact with others, especially older adults and those with compromised immune systems.

Some people with COVID-19 will require medical treatment, and some may need to stay in the hospital.

Before seeing a doctor or going to the hospital, however, a person should call the facility to alert them to the fact that someone is coming in who may have COVID-19. Also, wear a face mask on the way.

Hospitals are equipped with the medicine and personnel necessary to provide support for the most serious complications, including pneumonia and sepsis.

Vaccines work by prompting the immune system to make antibodies to defend the body against a specific disease, as if they had it.

The key is to do so without actually making the person sick.

After a person receives a vaccination, they develop immunity to the disease, which means that their bodies would be able to fight it off if they ever had exposure to it.

An effective vaccine must stimulate the immune system but not kick it into overdrive. Finding the right balance between an effective vaccine and one that does not cause unwanted side effects is a challenge for all vaccines under development.

During a health emergency, when speed is vital, this part may be the most significant factor to slow down the development of a safe new vaccine.

Vaccines also need to be safe for different groups of people to use, including young children, older adults, healthcare workers, and people with underlying health conditions.

To protect themselves and others from coronavirus, people can try:

COVID-19 is currently a major health challenge as doctors and researchers work to develop effective preventive measures, such as vaccines.

Until a vaccine becomes available, people can protect themselves and others by following guidance from public health and medical experts.

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Coronavirus vaccine: Development, timeline, and more

This week, my father and siblings had an Easter like no other. We held an online "HouseParty" with the whole family, which was a chaotic but fun thing to do, and my sister's children went Easter egg hunting in my parents garden. We were hoping that with the return of warm weather, we could see each other all again in person by summer. But my father threw some cold water on that hope though he did give us a good explanation why.

Dear Nele, Johan, and Peter,

We just had a beautiful Easter weekend, with great weather and a longing to go outside and meet family and friends. In our case, we found again a creative solution for the grandchildren to come by: on Sunday morning, we hid Easter eggs in the garden, and in the afternoon, the children came to look for them, while we looked from a safe distance. It's not the same as before, but for both the children and for us, it was a nice experience.

I think we'll have to get creative like this for another few months, and certainly through thesummer. As you know, we will only have a lasting solution when we get to herd immunity, and the safest way to achieve it is by developing acoronavirusvaccine. We would all want this vaccine to be there sooner rather than later, but my assessment is that a vaccine will likely not be widely available until2021, and possibly later. In the meanwhile, we have to hope for an effective drug byfall. To help you understand this, I thoughtI'd explain the various phases and techniques to get to a vaccine.

Courtesy of Peter Vanham

I'll try to make this as straightforward as possible, but it does require you to sit down and read attentively. In return, I'll summarize some basic insights of decades of virology research and development into an understandable text. If after reading this letter you still want to read more about the specific case of a SARS-CoV2 vaccine (the novel coronavirus' scientific name), I recommend this excellent paper by Fatima Amanat and Florian Krammer SARS-CoV-2 Vaccines: Status Report. Now, let's start!

The main distinction you need to understand is between the initialdevelopment of vaccine candidates and their pre-clinical (non-human) testing, and the subsequentvariousphases of human testing,followed byproduction, distribution, and administration. Forall but three vaccine candidatesfor SARS-CoV-2, we are still in the non-human phase, and many candidates may be 'stuck' in there for weeks, months, or even years, possibly not getting through at all. It's only when they get through the initial phasethat candidates really get to the start of the 'race to the vaccine'.

Compare it, if you will, to the audition rounds ofAmerica's Got Talent, versus the live shows. To extend that analogy a bit, consider that 'Vaccine's Got Talent' welcomes candidates using different methods. But instead of singing, dancing, stand-up, and magic tricks, vaccine candidates can come fromsixdifferent categories: 'live attenuated' or 'inactivated' virus vaccines, 'recombinant protein' vaccines, or 'DNA', 'RNA' or 'vectored' vaccines. Let's look at those a bit more in detail.

Source:Amanat and Krammer,SARS-CoV-2 Vaccines: Status Report, Immunity (2020)

Live attenuated and inactivated vaccinesare easy to make. They are the 'classic vaccines' that we know from the measles and the flu. You isolate a little bit of virus, weaken or 'inactivate' it, and then inject itintoa humanbeingin a portion that is small enough to trigger a reaction from your body. Production capacity for such vaccines exists since the 1950s. If such a vaccine would work, you can go to market relatively quickly.

We also have experience withrecombinant protein vaccines: this method is used, for example, for the human papillomavirus that causes cervical cancer, or for the hepatitis B vaccine. The latter vaccine exists since the 1980s I was vaccinated against Hepatitis B in the 1980s in Belgium and that makes them 'second generation' vaccines. This type ofvaccinedoesn't use the virus itself, but the proteins on the outside of it. In the case of the coronavirus, these vaccines would use the 'spikes of the crown' of the virus, to give you a visual image. It is this 'spike' or 'crown' that the virus uses to attach itself to our cells. If you inject a vaccine that will make us produce antibodies to block the protein from attaching itself, then, the virus might not be able to enter our cells.

Source:Amanat and Krammer,SARS-CoV-2 Vaccines: Status Report, Immunity (2020)

There is a trick with them: it's notcertainwhether human antibodies, elicited against those 'spike', 'surface' or 'envelope' proteins,will protect you from the virus. With HIV,for example, my specialization, we've tried a similar technique for more than 30 years, and we still haven't found one that works. But for the novel coronavirus, there are good signs it could work: for SARS and MERS, notably, two other coronaviruses, the technique did work in some animal models (though the vaccines weren't used widely; the virus died before the vaccine was produced for humans). Still, if this technique works, it might take a little longer to set up the industrial production and administration, but it is certainly possible sinceit'salready in use for papilloma and hepatitis B.

Finally, if one of the above three principlesdoesn'twork, there are also theDNA,RNAorVectored vaccines. The principle for all of them is that you take a piece of the genetic coding of the virus, namely one that would trigger your immune system to get alerted, and inject it intothe human body, where it is taken up by your cells and they produce the 'spike protein' of the virus, against which your immune system will make the antibodies. The technique is new and complicated, and it is part of the 'third generation' of vaccines. Only very recently[starting 2015 in trials, and resulting in anapproved vaccinein late 2019]'viral vector-based' vaccines were used for the first time in humansto control the Ebola outbreak in the east of the Democratic Republic of the Congo with apparent success. Clearly, thistechnique could work, but we have less experience with it, especially to produce and use it at scale. It would, therefore, take more time, but, reportedly, a Chinese company CanSinoBiologicsis moving such avaccinealready into a preliminary human trial.

Over all,these techniques combined, there are currentlymore than 70 vaccine candidatesfor SARS-CoV-2being worked on. That may sound like a lot, but bear in mind that the analogy withAmerica's Got Talentstops here. In the talent show, you'd end up with a winner no matter how many candidates initially signed up. For a new vaccine, however, you can't be sure if there will be a 'winner' at all. You typically need up to 100 vaccine candidates, to get to one winner: one vaccine that works, isn't toxic, and is easy to produce and administer. The 'attrition rate',as we call it, would in such case be 99per cent.

With all but a few of the candidates we currently have, we would normally first need to run 'pre-clinical tests' before wegoto the human test phases. In these pre-clinical tests,the vaccine candidate is given to animals that are sensitive to the virus, and that would get sick if they had the virus and developed the disease. That way, you can test not only if the vaccine candidates create antibodies, but whether they protect against the disease infection. For many SARS-CoV-2 vaccine candidates, this pre-clinical trial is the first real hurdle.

An ethical commission, such asthe National Institutes of Health in the US, or theCoalition for Epidemics Preparedness Innovationin Switzerland, would have to decide whether the various vaccine candidates have to do testing with animals for safety. If the technique is deemed safe, it will go quickly. If you are more experimental, you'll need to do a toxicity test with bunnies (which arethetypical 'guinea pigs') and two other animals, possibly ferrets and hamsters. Such tests can take at least six months in a traditional programme. The vaccine candidate that can't pass this hurdle, will likely lose the race. It will be a first separation between the more than 70candidates, though most will pass this test. As I said, three candidate vaccines already cleared this hurdle. They are currently the 'front-runners'.

After this phase, the real race to a vaccine starts, with clinical tests on humans. It starts withPhase I, with a few dozen patients, in which you look for the best dose of the vaccine in humans, while observing minimal side effects. It is asafety phase. This Phase I takes various weeks, probably at least two months,becauseyou first need to inject the vaccine to a small number of patients, and wait a week or longer to get results. Then you do the same with another few people, and with a higher dose, and again you wait, and so on, until you get to a target dose you will use for the Phase II and Phase III trials.

ThencomesPhase II, with hundreds of patients, to prove the vaccine candidate createsanti-bodiesand createsimmunity response. This phase uses healthy people who are not necessarily faced with the virus, and it will also take a few months. You probably need to give multiple doses, particularly for the RNA, DNA, vector and recombinant vaccines,becausethey break down typically before creating strong immunity. You need a 3-4 week interval in between each 'boost', and see how the body reacts (that can take a week or two). So for thisphase again you need at least two months, and more probably,three months.

Then comesPhase III, where you do a real test foreffectiveness, andprotective immunity: can the vaccine immunity protect against the infection for the disease?This is the 'make or break' phase that will determine whether we have an initial 'winner'. But the phase will take even longer, as you'll need to include a lot of people in your trial to know effectiveness: some will get the real vaccine, and others the placebo, and you need to follow them over time to know if there's a difference in infection between the two groups. That, of course, is a problem: many societies have either strict lockdown measures in place (in much of Europe, the Americas, and the Middle East). Or they have very few infections anymore (in China, Korea, Singapore, and other parts of East Asia).

Either way, this phase willeasily last six months, and again, possibly (much) longer, and for the front-runners, will likely start in thefall of 2020. When it takes place, you can see two logical candidates for trial groups: people who live in homes for the elderly, where there are a lot of infections, and people who work in the health sector. Thethe second group isthe most logical,becausethey are healthy and likely to get exposed to the virus. But you will have to make sure to choose those healthcare workers who haven't gotten the virus before.

So where are we with the vaccine candidatesfor the novel coronavirustoday? There are 78 candidates. That means there are 78 products, for which an analogue exists for other infectious diseases, that create an immune response there. They are all variants of thesixmethods I described above, where you can copy-paste what existed for the previous candidate, by taking the DNA code of the new virus, and apply one of the techniques I mentioned. Almost all of the candidates are based on the 'spike protein' or 'crown', as that protein would fix to the cell, and if you have an anti-body against that, it cannot fix to the cell.

Most of the candidates are still in the non-human development and testingphase.But there is one RNA vaccine currently in Phase I with humans, namely the vaccine of Moderna in Seattle.Another DNA vaccine focusing on the protein isabout to start its Phase I, namely that of Inovio in Pennsylvania. One caveatis that these vaccines by themselves may not be strong enough to reach immunity in humans, and may need to be combined with another, recombinant protein vaccine.Hong Kong'sCanSinoBiologicssays it is about to start a Phase II trial, using the viral vector technique, though no details are known about its Phase I results.

Imagine that any of these frontrunners, or any of the 75 other candidates, successfully make it through Phase III. If they manage to do that, they go to theApproval phase. That is when an institution like the Food and Drug Administration (FDA) in the US, the European Medicines Agency (EMA) in Europe, or the National Medical Products Administration (NMPA) in China, give their'blessing'to the vaccine. Sometimes this phase can take half a year, but in this case, we can assume it will be treated with utmost speed, and then it can be done in a few short weeks.

Then you go tomanufacturing, distribution and administration. Those are the economic and logistical aspects. How long this phase lasts, depends on the category that comes through. Here, the frontrunners may lose time, and the laggards may win time: the vaccines using live and attenuated virus, as well as those using the dead virus, have been produced and administrated at large scale before, whereas the others haven't, at least not at the same scale and speed. For the first-generation vaccines, large pharma companies have the capacity to ramp up their production quickly. But if it is a smaller company, maybe it will take longer.You can look at a few to many months. A good example is the influenza virus. That is being made every year in a couple of months.

In the end, SARS-CoV2 vaccines will not be realistically available for another 12-18 months. And even then, we must be lucky every step of the way.

Take the example of H1N1or the 'Swine flu' virusin 2009. It is the only example in recent history where we managed to make a new vaccine insixmonths (because the winning candidate was very quickly identified, and Phase I, II and III were not necessary), and even then, the vaccine came too late to affect the second wave of infections. To end on a note of optimism, though, the more I read about this virus, the more I also think we may find a vaccine on a rather quick timelinebecausethere are enough vaccines that have worked for similar viruses.

In the meanwhile, we must hope for the development of an efficient drug, and until then, manage very well the existing spread, with varying degrees of lockdown, testingand tracing, and social distancing measures. One drug that could help us a lot, as it looks promising, isRemdesivir. It has worked for SARS and MERS, and similar drugs are being used against hepatitis and HIV. It stops the multiplication of the virus. So,there's a good chance that this one, or a variant, will work against thecoronavirus. If you can give this at the first point of infection, it will work very well. It could be that this drug will be on the market by the fall.

Until then, we better get ready for a summer like no other. We may not see each other again for another couple of months, and when we do, it will have to be more like the Easter egg hunt, than sitting together at a table, close to each other. But on the bright side, we're learning to use Zoom, WhatsApp and HouseParty, so we can all come together anyway.

Dad, Guido Vanham

Guido Vanham is Professor of Virology at the University of Antwerp, and former Head of Virology at the Institute of Tropical Medicine in Antwerp, Belgium. His son, Peter Vanham, is Head of the International Media Council at the World Economic Forum, and a member of its COVID Taskforce.

This article is part of the COVID Action Platform for Media, a coalition of over 20 media from around the world. The Platform aims to create meaningful and constructive content on the COVID pandemic, and syndicates it through its media partners.

Link:

Why a vaccine for the coronavirus takes so long to develop - Business Insider - Business Insider