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The Viral Talk
The Viral Talk
Author: Federico De Angelis, Bobbie-Anne Turner
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What is a virus? What does spillover mean? How can viruses infect humans? If these are things that you would like to know but lack the time or energy to research them, then welcome to The Viral Talk, the show which gives brief, direct and easy-to-understand answers to the big questions in virology. I am your host Federico De Angelis, a PhD student studying SARS-CoV-2 and other coronaviruses at the Roslin Institute, University of Edinburgh. Join me every other week to discover all the aspects of these obscure but fascinating organisms. Join in and Let's Go Viral.
29 Episodes
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What do scientists mean when they talk about the innate immune system? What are the differences between innate and adaptive immunity? What is the immune system composed of? This and much more in this episode of The Viral Talk. Key takeaways:- Our immune system can be divided in 'innate' and 'adaptive'. - The innate immune system is quick and acts broadly. The adaptive immune system takes longer to kick in, but it is much more effective. - The innate immune system is composed of multiple layers. Physical barriers like the skin, mucosal barriers like mucus and saliva, and chemical barriers like our stomach pH protect us from the vast majority of pathogens. - Sometimes these are not enough, so most cells in our body have sentinels on their outside and inside that look for signs of infection and activate a general, quick immune response, leading to activation of some of our white blood cells, as well inflammation, swelling and increase in temperature. -The masterminds for the activation of our innate antiviral response are the interferon genes. There are multiple types of interferons, and they act as signaling molecules that induce an antiviral state inside the cell. For the sciency people:Book chapter on innate immunity - https://www.ncbi.nlm.nih.gov/books/NBK459455/ Explanation on interferon - https://www.dummies.com/article/academics-the-arts/science/biology/innate-immunity-built-in-defenses-169110/ Timestamps: Core episode start - 1.24Viral News of the day -13.50Ask a virologist section - 36.30Calls to ActionFollow the Viral Talk on IG - https://www.instagram.com/the_viral_talk_/ On X - https://x.com/the_viral_talk
This is 'Ask a professional', the format of the Viral Talk where the focus is on the science but most importantly on the PERSON behind the science. From insect-borne viruses to SARS-CoV-2 and vaccines, we're going to interview experts from the UK and the world on their research, career, future prospects and tips for the younger generations of scientists. In this episode Federico interviews Dr Valerie Odon, newly appointed group leader at the University of Strathclyde in virology. In this episode we're gonna talk about cells investigating intruders (viruses), the wisdom of mothers and the challenges that come with becoming your own boss. For the sciency people: How a cellular protein recognises viral RNA and stops virus replication - DOI: 10.1093/nar/gkz581How that same protein differs in humans and birds and this leads to differences in immunity - doi: 10.1261/rna.079102.122Who is Valerie Odon? - https://www.strath.ac.uk/staff/odonvaleriedr/ Follow The Viral Talk on IG - https://www.instagram.com/the_viral_talk_/ Follow us on X - @The_Viral_Talk
Welcome to the 2nd season of ‘Ask a professional’, the format of the Viral Talk where the focus is on the science but most importantly the PERSON behind the science. From insect-borne viruses to SARS-CoV-2, we’re going to interview experts from the UK and the world on their research and then we’re
going to talk about their career, future prospects and tips for younger generations of future scientists.
In this episode Federico interviews Dr Ben Brennan, group leader at the Centre for Virology Research at the University of Glasgow. They're gonna talk about ticks living up to 4 years, reverse engineering viruses to make vaccines and headbutting walls until they fall down.
For the sciency people:
What are bunyaviruses - https://www.sciencedirect.com/science/article/abs/pii/S1879625715001261
Bunyaviruses and climate change - doi: 10.1111/j.1469-0691.2009.02849.x
Oropouche virus in Brazil - doi: 10.1016/S1473-3099(24)00672-8
Who is Ben Brennan- https://www.brennanlab.co.uk/
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What are coronaviruses? How
are they structured and what is being done to be more prepared next time another one emerges? This and much more in this new episode of The Viral Talk.
Join your usual host Federico and an old friend of the show Bobbie-Anne Turner from the University of Liverpool to hear about the dreaded coronaviruses!
Key points:
The scientific community has known
about coronaviruses for a long time. The first coronavirus ever discovered was a poultry coronavirus named Infectious bronchitis virus and was discovered in the 1940s.
The first human coronaviruses were
discovered together in the 60s by the common cold unit in the UK, and were human coronaviruses OC43 and 229E;
Coronaviruses are very diverse but have roughly the same genome structure. They all possess a set of 14 non-structural genes necessary to make the proteins that allow the virus to make more copies of itself. And they all possess four structural proteins, which make the building blocks of the viral particle (or virion).
These four proteins, called Spike, Envelope, Membrane and Nucleocapsid all have important functions during infection. Spike is found on the surface of the virus and is the protein that
allows it to infect cells. Envelope is thought to have a general role in coordinating the assembly process of the virus inside the cell. The Membrane protein is the physical outer layer of the viral particle, which contains its genome and on which the Spike protein is found, and the Nucleocapsid wraps around the newly made copies of viral genome and packages it
inside the virus.
Different viruses can have a variable number of 'accessory' genes, which help the virus during infection by fighting the host immune response or facilitating spread between cells.
Coronaviruses are very diverse,
there are four different groups called Alpha-, Beta-, Delta- and Gamma-coronaviruses. Alpha and Beta coronaviruses usually infect mammals, Delta
and Gamma coronaviruses more often than not infect birds, but this is not an absolute.
Some coronaviruses are specialists,
meaning that they only infect a specific type of host, while others, like
SARS-CoV-2, can be quite generalists, and infect a series of animals.
This characteristic is important for emergence and re-emergence, and it tells us that it is important to be constantly surrounding the environment and both wild animals and human-adjacent animals. The biggest example of this is deer in America and now in Europe, as it seems that SARS-CoV-2 has taken a home in white-tailed deer that might act as a wild reservoir for the virus.
Apart from the pandemic, the scientific community is very interested in coronaviruses because in the last 20 years there have been three different instances of emergence of highly pathogenic coronaviruses, with SARS-CoV in 2003, MERS-CoV in 2012 and SARS-CoV-2 in 2019.
There is a lot going on in the scientific community to be prepared for when the next one comes forward. Environmental surveillance is going strong. There are strong efforts to develop a
pancoronavirus vaccine to make sure we’d be protected against any coronavirus. There are many international consortia, such as the UK-ICN,
the SARS-CoV-2 G2P consortia, and many more, that foster international collaboration, inform governments and integrate lab and social sciences to better tackle the
practical problems emerging from pandemics and governance.
For the sciency people
Intro to Coronaviruses: 10.1038/220650b0
History of coronaviruses: 10.33493/scivis.20.01.04
Coronavirus diversity: https://doi.org/10.3389/fpubh.2022.926677
What are the human coronaviruses: 10.1038/220650b0
Relevant links
What’s the UK-ICN? https://uk-icn.co.uk/
What’s the G2P consortium? https://gtr.ukri.org/projects?ref=MR%2FW005611%2F1
Call to actions
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What are the differences between acute and persistent viral infections? How can certain viruses stay with us forever and never be cleared? This and much more in this episode of The Viral Talk.
Key takeaways:
An acute infection is characterized by a sudden or rapid development of disease, that can either be resolved quickly or lead to death;
In a persistent infection, the virus is not cleared by our body, and it either becomes latent (e.g Herpes Simplex Virus) or it keeps replicating at low levels for very long periods of time (e.g. Hepatitis B Virus, HIV);
For a latent infection to become a persistent infection,
it needs two characteristics: persistence and reversibility.
Reversibility is the ability of a virus to resume
active viral replication after undergoing latency, persistence is the ability
to stay in our body without being eliminated/cleared for a long period of time.
A latent virus that lacks a way to be ‘re-activated’
only causes dead-end infections.
Herpesviruses and Retroviruses are the only known
viral families able to undergo latency.
Latency is a successful survival strategy that allows
viruses to avoid being cleared by the host’s defences.
In addition to latent viral infections, there is
another type of infection which is chronic viral infections.
In chronic infections, the virus keeps replicating
inside the host for long periods of time without being cleared, causing low levels of pathology. The best example for this is HIV, followed by Hepatitis B virus.
Constant rounds of infection by these viruses lead to
the onset of the diseases they’re known for, AIDS and hepatitis, respectively.
Articles for the most interested:
General definition of persistent viral infections - https://www.ncbi.nlm.nih.gov/books/NBK8538/
Common threads in persistent viral infections - https://journals.asm.org/doi/10.1128/jvi.01905-09
Retroviruses in the human genome - https://www.frontiersin.org/articles/10.3389/fimmu.2018.02039/full
How do viruses go latent? - https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2914632/#:~:text=In%20latent%20infection%2C%20the%20full,additional%20properties%3A%20persistence%20and%20reversibility.
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How can tiny viruses hijack a cell and make it do their bidding? How can they survive a whole organism trying to get rid of them? This and much more in this episode of The Viral Talk.
Key takeaways:
Viruses make three types of proteins. One type to replicate, one type to protect their genome once they're outside of the host, and one to modify the cell they infect at their 'whim'.
The proteins they use to change the structure of the cell often work through 'mimicry'. They have motifs/domains that resemble cellular proteins, which interact with our proteins to either stop their function or re-direct it.
Common to most viral infection is a phenomenon called host translation shut off, in which cellular protein production goes down and viral protein production goes up.
Translation shut off can be achieved by either destroying cellular mRNA or tricking the cellular translation machinery into believing that viral mRNA is in fact cellular mRNA.
Viruses have also evolved multiple ways to shut down the immune response of cells, through accessory proteins that are not incorporated into the final viral particles but without which they don't fare very well.
They have also evolved multiple ways to mimic cellular 'messenger molecules', by doing so causing distruptions in the way cells can respond to infection.
These viral proteins are also very important targets for the development of antiviral drugs.
Articles for the most interested:
DOI:10.1038/nri980 - Viral mimicry of messenger molecules
DOI: 10.1038/ncomms4952 - Influenza mimicry of histone 3
DOI: 10.1006/viro.2000.0816 - HIV Nef protein and MHC
DOI: 10.1038/nrmicro267 - Viral Cap snatchin
https://viralzone.expasy.org/1579#:~:text=Viruses%20have%20evolved%20ways%20of,to%20evade%20host%20immune%20response%20 - Nice resource that lists way in which viruses cause translation shut off.
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How do viruses cause disease? What are the processes that make us sick and what can we do about it? This and much more in this episode of The Viral Talk.
Takeaways:
When viruses infect our cells they hijack them and sequester all the resources that the cell might need to stay alive, causing it to malfunction and die.
Infected cells also recognize that they're infected and 'self-destruct' to stop the infection.
When cells recognize a virus they release signals that call in the immune system, which leads to inflammation and cell death.
The virulence of a virus is dependent both on its genomic content and its 'tropism' aka the tissues and cells that it infects.
Influenza has a preference for cells of the respiratory tract and causes respiratory infections. HIV infects immune cells and therefore causes AIDS.
Some viruses like Ebolaviruses do not have a preferred cell and are able to infect most of them, causing very severe, generalised infections.
The type of disease is also due to mutations in our genome, which can make us more or less prone to severe immune responses called 'cytokine storms'.
Links and scientific papers:
What are mRNA vaccines? How do they work and why are they considered revolutionary? This and much more in this episode of the Viral Talk.
Key Takeaways:
Vaccines work by introducing an element that resembles a pathogen into our body, so that our immune system can learn to counter it without the need to get infected first.
Vaccination induces our body to produce antibodies, which are tiny proteins that recognise and attach themselves to the pathogen.
mRNA vaccines are a relatively new technology that inject into our body the instructions (messenger RNA) to produce one or more proteins of the pathogen they target.
COVID-19 mRNA vaccines give the cell the instructions to produce the SARS-CoV-2 Spike protein, which is 'used' by the virus to enter inside the cells. In this way, when the virus infects a vaccinated person, antibodies will attach onto the Spike protein of the virus and prevent it from getting inside our cells.
The mRNA vaccine technology has been in development for more than a decade and was initially thought to vaccinate against cancer.
mRNA vaccines are faster to produce, more flexible and easier to update compared to other traditional vaccines.
COVID-19 vaccines do not give people COVID-19, as they do not contain virus particles.
COVID-19 vaccines were produced so quickly because vast amounts of resources and money were put in their development from the get-go. No corners were cut in the experimental phase and many studies suggest that they provide very high protection against severe COVID-19 disease.
COVID-19 vaccines do not contain fetal elements, microchips, trackers or other dangerous elements.
The biggest components of COVID-19 vaccines are water, sugar, lipids and mRNA, in this order.
For your interest:
How do vaccines work?- https://www.youtube.com/watch?v=4SKmAlQtAj8&ab_channel=naturevideo
mRNA vaccines review - https://www.nature.com/articles/s41573-021-00283-5
Efficacy of SARS-CoV-2 mRNA vaccine - DOI: 10.1056/NEJMoa2035389
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How many types of viruses are there? How do scientist classify them and why is it important to know? This and much more in this episode of the Viral Talk.
Key takeaways:
Scientists predict hundreds of millions of different viral species on our planet, but they can all be grouped in 'only' seven different groups.
These seven groups have been theorized by virologist David Baltimore based on the different types of genomes they can have, and how this affects the way in which they replicate.
In nature, almost all organisms follow the central dogma of biology: DNA->RNA->Proteins. But not all viruses follow it.
The seven groups are:
double stranded DNA viruses (e.g. herpesviruses)
single stranded DNA viruses (e.g. many bacterial viruses)
double stranded RNA viruses (e.g. rotaviruses)
positive sense single stranded RNA viruses (e.g. coronaviruses)
negative sense single stranded RNA viruses (e.g. Influenza virus)
double stranded RNA viruses with DNA intermediate (e.g. HIV)
double stranded DNA viruses with RNA intermediates (e.g. Hepatitis B virus)
Knowing how viruses replicate beforehand can give us a heads-up on potential targets for antiviral drug development.
Examples include antivirals against HIV and other retroviruses.
For people who'd like to know more:
Original paper on Baltimore classification - DOI: 10.1128/br.35.3.235-241.1971
Success story on antivirals against HIV: DOI: 10.1016/S0166-3542(98)00025-4
Visual explanation of Baltimore classification scheme: https://www.youtube.com/watch?v=W2YOZnvgcuk&ab_channel=Shomu%27sBiology
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What are bacteriophages? Are they important for our ecology and what do we know about them? Join the host Federico De Angelis in understanding what these viruses are, what they do and how we can harness their potential.
Takeaways:
- Bacteriophages are bacterial viruses. They only infect bacteria.
- They are the most abundant biological entity on the planet.
- Phages are very specific, with one phage species infecting a single bacterial species.
- Phages have two distinct infectious cycles. The lytic cycle during which they infect bacteria and kill them by bursting out, and the lysogenic cycle, where their genome is integrated in the genome of their host, turning them into prophages.
- Sometimes lysogenic phages establish symbiotic relationships with their host, for example Vibrio cholera, the bug responsible for Cholera, has a prophage in its genome that encodes for the toxin responsible for the watery diarrhea it causes.
- Phages can be engineered to target specific virulent bacteria and treat antibiotic resistant infections.
Additional info for the most interested:
Review on sea phages - https://www.nature.com/articles/nature04160
In-depth article about Vibrio cholera - https://www.nature.com/articles/nrmicro2204
Resource on bacteriophages biology - https://www.khanacademy.org/science/biology/biology-of-viruses/virus-biology/a/bacteriophages
TedX Talk on Phage therapy - https://www.youtube.com/watch?v=kPqbcvCTE80&ab_channel=TEDxTalks
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What is an emerging virus? How do new viral pathogens emerge, which viruses are the ones on our watchlist and what is being done to prevent a new pandemic from happening? Join the host Federico De Angelis in understanding what are the threats that virologists from all over the world are trying to tame.
Takeaways:
Emerging viruses are agents responsible for a new or previously non-recognized infection.
For a new viral pathogen to emerge, it needs the ability to infect a different host from its reservoir, and to diffuse in the new host population. The chances of both these things happening are very slim.
The WHO has made a list of the viruses to watch in 2015 encompassing: 1) severe emerging coronaviruses SARS and MERS, 2) Filoviruses like Ebola and Marburg virus, 3) Nipah virus, 4) Rift valley virus, 5) Crimean congo haemorragic fever virus and 6) Lassa fever virus. All these viruses are RNA viruses. These viruses have been put on the list based on a series of characteristics. They are all able to infect humans, but not to spread very well human-to-human.
Ever since the COVID-19 pandemic, a great deal of effort has gone into: surveillance, basic lab research for development of antivirals and vaccines, and a lot more effort in the development of infrastructure for better international collaborations, from PPE manufacturing to data sharing.
Additional info for the most interested:
Youtube lecture from Prof. Vincent Racaniello at Columbia University on emerging viral diseases:
https://www.youtube.com/watch?v=5ZQFy-d7ISk&ab_channel=VincentRacaniello
Review on cross-species transmission of emerging viruses: https://doi.org/10.1016/j.celrep.2022.110969
Pan-coronavirus vaccine development pipeline:
https://www.nature.com/articles/d41573-022-00074-6
What is the Pandemic Preparedness Treaty?
https://commonslibrary.parliament.uk/research-briefings/cbp-9550/
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What needs to happen for a virus to successfully infect a host? What is the infectious cycle? Join the host Federico De Angelis in finding out what are all the obstacles that must be overcome by viruses in order to establish an infection, and what happens once viruses manage to get inside a cell.
Takeaways:
Viruses can only infect us through our openings, such as the mouth, nose, eyes, genitals and scratches or bruises on our skin.
Once they get inside the host they have to survive a multiple of physical and chemical defenses at each site of entry.
Viruses have proteins on their surfaces which act as keys to cells. In order to infect us they need to stumble upon the correct cell with the correct 'door lock' (molecule/receptor) on the cell surface.
When viruses find the right cell and get inside, they have to release their genetic content either in the cytoplasm (if RNA viruses) or in the nucleus (if DNA viruses), but there are exceptions. This allows their genome to be copied in high numbers, and their proteins to be produced.
Produced viral proteins then hijack the cell in many different ways to transform it in a 'virus factory'.
When the viral genome has been copied and the viral proteins produced, these then are transported to the surface of the cell, where they can assemble into a mature viral particle and exit the cell to find other cells and re-start the cycle.
Additional sources:
Review on viral entry inside the cell - https://www.nature.com/articles/nrmicro817
Review on the viral life cycle - https://bio.libretexts.org/Bookshelves/Microbiology/Microbiology_(OpenStax)/06%3A_Acellular_Pathogens/6.02%3A_The_Viral_Life_Cycle
BBC bitesized guide to non specific body defenses - https://www.bbc.co.uk/bitesize/guides/znpxwty/revision/2
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What does the term 'spillover' mean? How do zoonoses apply to our everyday life? What can we do to reduce the chances of new pandemics happening? Join the host Federico De Angelis to find out.
Takeaways:
A zoonosis (or zoonotic event) takes place when a pathogen that is adapted at infecting one species (e.g. humans), manages to 'jump' and infect a different one.
Between 60 and 75% of all human pathogens come from our exposure to animals.
There are human factors which can increase the chances of zoonosis happening - climate change, deforestation, 'bushmeat' trade.
It is well within our power to adopt behaviors that decrease the probability of a new pandemic to happen.
David Quammen book 'Spillover' - https://davidquammen.com/spillover
Estimates on human pathogens emergence - https://europepmc.org/article/PMC/3367654
https://royalsocietypublishing.org/doi/10.1098/rstb.2001.0888
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Coming soon - Join the host Federico De Angelis in discovering the basic biological principles of coronaviruses, their host type, how many they are and the type of infection they cause.
How are viruses transmitted to stay in the population? What can we do to stop them? Join the host Federico De Angelis in finding out about the different types of viral transmission and learn about the behaviors that can stop them.
Takeaways:
· Viruses can be transmitted person-to-person
· Through food and water
· On objects
· Via insects(!)
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Coming Soon...
What does zoonosis mean? What happens when a virus enters in a new host? Listen to the next episode of The Viral Talk to find out!
What are viruses? Are they alive? Should we care? Listen to this episode to discover these tiny organisms and learn more about their biology.
Takeaways:
- 1) Viruses are organisms that can spread between individuals; 2) That take the resources to spread and reproduce from other organisms; 3) that must get inside the cells of the organisms they infect to reproduce; 4) That are made of DNA or RNA contained within a coat of proteins.
- Viruses are fundamentally dead (except when they are intracellular).
- We should not humanize them. Viruses are passive agents.
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What does the term co-infection mean? What happens when two viruses infect us at the same time and why is it important for our health? This and much more in this episode of The Viral Talk.But also, a new host joins the show, episodes take on a new structure, and we answer questions from the audience. Key takeaways:- A co-infection occurs when two or more pathogens infect the same host at the same time- There are multiple types of co-infections, as we can be infected by bacteria, parasites and viruses, and different types of co-infections have different effects on our bodies- There are multiple types of viral co-infections as well - we can be infected by different strains of the same virus (e.g. Flu), different viruses that infect the same type of cells (e.g. SARS-CoV-2 and RSV) or different viruses that infect different parts of our body (e.g. HIV and HepC) - For a long time it was assumed that co-infections would worsen the outcome of the individual infections, but researchers have found that this is not necessarily the case- Vaccines against commonly co-occurring pathogens are being tested. For the sciency people: Why won't different strains of flu be friends? - https://doi.org/10.1371/journal.pbio.3001941Hep C and HIV co-infection review - 10.3748/wjg.v8.i4.577RSV and SARS-CoV-2 in mice - 10.1101/2023.05.24.542043 Follow the viral talk on IG - https://www.instagram.com/the_viral_talk_/ On X (Twitter) - https://twitter.com/The_Viral_TalkAnd linkedin - https://www.linkedin.com/company/the-viral-talk/
Welcome to the 2nd Special Episode of The Viral Talk. In this episode our host Federico interviews Faye Watson, Churchill Fellow and Public Engagement Officer for the School of Medicine and Veterinary medicine at the University of Edinburgh (although not for long!!).
Faye is going to talk to us about her project on improving prevention and outreach for the communities affected by blood-borne viral infections (e.g. HIV and HepC) in Scotland, and how to use Botswana and South Africa as model countries to tackle the inherent challenges of doing this type of work. Join us for a most informative conversation on what needs to be done to tackle these type of infections and also (but not less importantly) on the importance of forming human connections in our fight against infectious diseases.
Link to the youtube interview
https://www.youtube.com/watch?v=WjSc_Icp7Ww
Bits of info
Who is Faye Watson?
https://www.fayewatson.co.uk/
What is the Churchill Fellowship?
https://www.churchillfellowship.org/
What is Unseen Hands?
https://cvr-engagement.co.uk/unseen-hands
https://foshostudios.com/project/cvr-unseen-hands/
FoSho Studios
https://foshostudios.com/
This is ‘Ask a professional’, the format of the
Viral Talk where the focus is on the science but most importantly the PERSON behind the science. From insect-borne viruses to SARS-CoV-2, we’re going to interview experts from the UK and the world on their research and then we’re
going to talk about their career, future prospects and tips for younger generations of future scientists. In this episode Federico interviews Dr Chris Hill, group leader at the Department of Biology of the University of York. In this episode we're gonna talk about discovering that the tooth fairy is not real, looking at single molecules down the microscope and the pervasiveness of Imposter Syndrome among young researchers.
For the sciency people:
How do some viruses manage to pack more information than physically possible - 10.1146/annurev-virology-111821-120646
How viruses hijack our protein production machinery - doi: 10.1083/jcb.200205044
The wonderful bioimaging facilities at the University of York https://www.york.ac.uk/research/themes/technologies-for-the-future/bioimaging/#:~:text=Researchers%20at%20York%20have%20developed,more%20about%20Resonant%20Hyperspectral%20Imaging.
Imposter syndrome and how big of a problem it is - https://www.bps.org.uk/research-digest/women-and-early-career-academics-experience-imposter-syndrome-fields-emphasise
Who is Chris Hill- https://www.hill-lab.co.uk/pi
Follow Chris on X - https://twitter.com/chillzaa
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This is the first SPECIAL episode of The Viral Talk. It was recorded in Liverpool at the UK-International Coronavirus Network Early Career Researchers symposium.
The Viral Talk team was invited to take part to a fantastic initiative organized by the UK-ICN to encourage young scientists to share knowledge, hopes, dreams and to network in Liverpool on the 1st of March 2024.
Three early career researchers were chosen to come on the show and talk about their experience, their projects, and their hopes for the future. The guests were:
-Bobbie-Anne Turner, a third year PhD student at the University of Liverpool in Prof. Julian Hiscox lab, trying to identify which cellular proteins bind and interact with a specific structural protein of many human coronaviruses.
-Carla Ruiz, a first year PhD student from IRTA CReSA (Barcelona) trying to establish a model organism for 'Long' COVID-19
-Nuno Santos, a postdoc at the Francis Crick Insitute in Dr David Bauer lab studying the evolution of coronaviruses and the way their genetic code (RNA) changes.
What is the UK-ICN?
https://uk-icn.co.uk/
Who are the speakers?
Bobbie-Anne Turner - https://uk.linkedin.com/in/bobbie-anne-turner
Carla Ruiz - https://es.linkedin.com/in/carla-ruiz-casas-92a0971a1?trk=people-guest_people_search-card
Nuno Santos - https://www.crick.ac.uk/research/find-a-researcher/nuno-santos
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This is ‘Ask a professional’, the format of the
Viral Talk where the focus is on the science but most importantly the PERSON behind the science. From insect-borne viruses to SARS-CoV-2, we’re going to interview experts from the UK and the world on their research and then we’re
going to talk about their career, future prospects and tips for younger generations of future scientists. In this episode Federico interviews Dr Ed Emmot, group leader at the Centre for Proteomics Research at the Universty of Liverpool. In this episode we're gonna talk about proteins that cut other proteins, how viruses can benefit from that and the importance of finding your niche.
For the sciency people:
The role of proteolysis in SARS-CoV-2 infection - http://dx.doi.org/10.1038/s41467-021-25796-w
Book chapter on the proteomics of viruses - https://www.sciencedirect.com/science/article/pii/B9780444519801500173#:~:text=sensitivity%20and%20fidelity.-,Proteomics%20is%20a%20promising%20approach%20for%20the%20study%20of%20viruses,disease%2C%20and%20accelerates%20drug%20development
A simple overview on the concept of proteolysis - https://www.news-medical.net/life-sciences/An-Overview-of-Proteolysis.aspx
Who is Ed Emmot - https://www.liverpool.ac.uk/systems-molecular-and-integrative-biology/staff/edward-emmott/publications/
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