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507-Year-Old Clam May Be the World’s Oldest Living Being – History of Yesterday
Posted: October 2, 2022 at 4:18 pm
umanity is forgetting what the most important resource in this world is. Time for many may not be as valuable, especially when you are surrounded by a cruel world. The average lifespan of a human is around72 yearsand for some, that is more than enough, but deep down despite how difficult life gets we all want to live forever.
During recent research, we have seen a hand full of creatures that are able tolive more than 200 years, almost triple that of the average human. However, knowing that there has been a creature that had lived for 5 centuries after humanitys destruction of this planet is truly a mind-blowing fact.
Ming the clam was discovered off the coast ofIceland at a depth of 262 feet(80 meters) by a team of researchers from Bangor University. The team was looking to study the growth lines in clamshells as part of a project that would show how the climate has changed over the last millennium. If you ever looked at the shell of a clam you would be able to see lines that would give an indication of how old that clam is. Professor Chris Richardson from Bangor University has an interesting description for them:
They are like tiny tape-recorders sitting on the sea-bed and integrating signals about water temperature and food over time. (Quote by Professor Chris Richardson)
The team started to count the rings and initially reached the conclusion that the clam they have discovered was405 years old. Its scientific name isArctica Islandica, but it is more commonly known as Quahog. This species is actually known to live for very long periods of time, many of which had been found before wereover 200 years old.
Whilst analyzing the age of the clam,it had died the same year in 2006. It had not been very well-specified exactly what caused the death of the clam, but it was most probably triggered by having the clam taken away from its original habitat. The rough shells tell an intriguing story, but they had even more to unfold.
In 2013, a team of researchers from around the world picked up the shells to conduct a more thorough study. During this study, the researchers have concluded that the clam was actually100 years olderthan what the previous research team has analyzed in 2006, making it 507 years old and the oldest living being known to mankind.
This means that the clam was born in 1499, thesame year Pope Pius IV, leader of the Catholic Church was born. The reason why researchers named the clam the mollusk Ming is because during the period of time it was born theMing Dynastywas ruling China (1368 to 1644).
Can you believe that Ming actually lived during the same timeLeonardo da Vinci painted Mona Lisa? Alive during the timeShakespeare was writing his incredible novelsand alive during five centuries of constant wars? This clam was so lucky for not intercepted humans for 500 years, yet the moment it did it died. What does this tell you about our kind?
Experts from the University of Bangor speculate that this species could actually surpass600 years of ageand that there are probably even older specimens waiting to be discovered. During morecurrent researchit had been discovered that the secret to the longevity of Quahog clams is a slowed-cell replacement process. There is a big possibility that our planet hosts even older beings that are still alive. As much as human curiosity is pushing me and the rest of humanity to find these creatures, I wish humanity will never find them, so they wont end up like Ming.
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I should look forward to early retirement, but I think I’m dreading it – CBC.ca
Posted: at 4:18 pm
This First Person column is the experience of Roxane Anderson, a 62-year-old social worker in Selkirk, Man.
For more information about CBC's First Person stories, please see theFAQ.
I turn a page in my day-timer to the next work week. At the top of "Monday,"I write "62" in red ink, to represent the remaining days I must work in orderto qualify for early retirement. The same number of years I have been on this Earth.
My banker says I should work until age 65. According to my iPhone countdown app, that's 1,172 days away! The 62 countdown sounds better.
Am I burnt out or just getting too old? Can I find my "reset"button to get me through to age 65?
I am a registered social worker working in disability services for the province of Manitoba, counting the days to retirement.
In recent years, my work has changed. Before, I was in the field on home visits, returning to the office at the day's end to chart my case notes. Today, I spend most of my time in the office on email and paperwork. The social disconnect is not a good fit.
It's hard to fit the workload inside a seven-and-a-half-hour day. There's always unfinished paperwork and unanswered emails. The back and forth on email is dizzying. Why doesn't anyone still use the phone? I'm told, "You work with millennials, that's how they function."
When I emailed a government service to get help finding a resource and phone number for a client, this was the reply: "Google is your friend."
What? My client doesn't have internet. That's why I reached out to get a working phone number. (I choose not to email back. There's no time.)
On the cusp of retirement, I am struggling to continue in social work. At 3a.m., I find myself waking up in a sweat, thinking about what is not doneand who is still waiting for services. Did I mitigate risk? Did I ensure that clients were safe and protected? What did I miss?
Driving to work, inside the privacy of my car, I can let go of the flood of tears. This helps to get through the day.
Maybe I don't fit in anymore. Since the pandemic, my work world has changed. There are fewer workers to meet the needs of more clients. My older colleagues retired.
Normally, I'm quite good at helping my clients stay positive and strong in meeting their personal goals. Social work is about building strong relationships. I used to do lots of home visits, working with clients and their families. But, today, not so much. Is that what I'm missing? The human contact? In trying to find hope for my clients, I'm struggling to generate hope in myself.
I fear I'm burning out. Is that from workload or from growing old?
When the work computer freezes, it's time for a reboot. I'm now trying to do that for myself, too.
I try to keep a healthy perspective. I trained to stave offcompassion fatigue. Consulted with other registered social workers. Got more exercise. Improved my diet. Worked on better sleep. I spend quality time with family and friends. I've shortened how I write my case notes. I make phone appointments to cut out travel time. I'm working smarter and harder.
In three years, I'll be 65 and in blissful retirement, yet I can't get through the next three workdays. This should be the best of times, not the worst of times, and right now, I feel like I'm failing.
Perhaps I'm dreading my option of early retirement. I'll lose my identity as a social worker. I won't be needed anymore.
Then there are financial worries. Rising inflation. A furnace replacement. New shingles on the house roof. Longevity runs in my family. Will my pension be enough to sustain me in a retirement home, with meals, activitiesand a monthly entertainment nightwhen I'm 80? When I'm 90?
This time next month, I'm scheduled for heart scans due to new pain in my chest. It's either angina-based on family history or work anxiety. I'll know soon if I have one or the other or a combination of both.
It's time for a reset. The countdown has started, and in 62 days, my heart may be in early retirement.
This column is part ofCBC's Opinion section.For more information about this section, please read thiseditor's blogand ourFAQ.
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International Coffee Day 2022: How The Beloved Brew Helps Fight Cancer, Kidney Disease And Depression – ABP Live
Posted: at 4:18 pm
International Coffee Day 2022: Today is International Coffee Day. A steaming cup of joe is something many people consume to give their morning a quick boost. While its charm comes mainly from its smell and taste, coffee also comes with various health benefits. From increasing longevity to reducing risk of cancer, here is what studies have found over the years:
Coffee and Longevity
Drinking one cup of coffee per day, whether caffeinated or decaffeinated, is associated with a three per cent reduced risk of death, according to a review of 21 studies totalling more than 10 million participants. The review, published in the Journal of Human Nutrition and Dietetics, also stated that drinking three cups of coffee per day is associated with a 13 per cent reduced risk of death.
Drinking coffee, caffeinated or decaffeinated, is associated with reduced risk for death from various causes, according to a study from the International Agency for Research on Cancer (IARC). It was a multi-national cohort study conducted in 10 European countries, and analysed more than 500,000 people. The study was published in the journal Annals of Internal Medicine in 2017.
A study conducted on over 400,000 people found that coffee consumption is associated with lower likelihood of death from disease. The study was published in The New England Journal of Medicine in 2012.
Coffee and Cancer
Drinking both caffeinated and decaffeinated coffee is associated with reduced risk of liver cancer, according to a meta analysis of human prospective studies. Coffee was found to be associated with reduced risk of hepatocellular carcinoma, including in those with pre-existing liver disease. The findings were published in the British Medical Journal.
Consumption of four cups of coffee per day is associated with a 10 per cent reduced risk of post-menopausal breast cancer, according to a study published in the journal Nutrients in 2018.
Coffee consumption is associated with a lower risk of colon cancer in women. According to a study published in the International Journal of Cancer in 2018, there is a 20 per cent reduced risk of colon cancer in women who drink more than three cups of coffee per day, compared to those who drink less than one or less.
Coffee and Diabetes
People who drink four or more cups of coffee per day have a 50 per cent lower risk of Type 2 diabetes, according to a study published in the Journal of Agricultural and Food Chemistry in 2011.
Cafestol, a compound found in coffee, has been found to increase insulin secretion, reduce fasting glucose levels and improve insulin sensitivity in mice. Thus, cafestol could help stave off type 2 diabetes, according to a study published in the Journal of Natural Products in 2017.
Coffee and Stroke
Coffee consumption can modestly reduce the risk of stroke among women, according to a survey conducted on more than 83,000 women over many years. The findings were published in the Journal of the American Heart Association in 2009.
Coffee is associated with reduced risk for death from various causes, including stroke, according to a study from the International Agency for Research on Cancer. The study analysed more than 500,000 people, and was published in the Annals of Internal Medicine in 2017.
Tea and coffee consumption are inversely associated with risk of cardiovascular disease and stroke in the general population, according to a large-scale study in Japan, published in the journal Stroke in 2013.
Coffee and Kidney Health
Coffee consumption is associated with a reduced risk of chronic kidney disease, according to a study published in the Journal of Renal Nutrition in 2020.
Coffee and Mental Health
Coffee consumption is linked with a reduced risk of depression, according to an independent meta-analysis conducted by Dr Alan Leviton, Harvard Medical School.
Coffee has antioxidant effects. Since coffee has anti-oxidative properties, it helps reduce the blood levels of oxidative-stress indicators in people who have a major depressive disorder
Coffee also helps reduce the levels of inflammation-related proteins in depressed people.
Coffee also provides the gut microbiome with nutrients to metabolise coffee constituents into beneficial substances, and promotes a healthy microbiome.
ALSO READ | Can Coffee Waste Help Neuroscience? New Study Says Yes, Explains How
History of Coffee
Coffee cultivation and trade began on the Arabian Peninsula, and by the 15th century, coffee was grown in the Yemeni district of Arabia. By the 16th century, coffee was known in Persia, Egypt, Syria and Turkey.
In public coffee houses, which started appearing in cities across the Near East, coffee was called qahveh or khaneh.
By the 17th century, coffee made its way to Europe, and by the mid-17th century, there were more than 300 coffee houses in London.
The Indian Muslim saint Baba Budan, while returning from a pilgrimage to Mecca, brought seven coffee beans from the port of Mocha, Yemen to Mysore, India, by hiding them in his beard. He planted the seven seeds of coffee in the courtyard of his hermitage in Chikmagalur, Karnataka, and that became the birthplace and origin of coffee in India.
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Corey Feldman And Jamison Newlander Talk The Lost Boys And The Birth Of The Two Coreys – Forbes
Posted: at 4:18 pm
Corey Feldman and Jamison Newlander as The Frog Brothers in 'The Lost Boys.'
"Edgar Frog was the first time where I really had to create a character that was completely disconnected, completely separated from me as a human and becoming this other guy," recalled Corey Feldman as we discussed the iconic 80s teen vampire movie, The Lost Boys.
When he made it, the actor already had memorable performances in a string of classic movies under his belt, including The Goonies, Gremlins, and Stand by Me. However, his role as Edgar Frog, one half of The Frog Brothers, opposite Jamison Newlander as his brother Alan, gave him a string of unique experiences.
I caught up with Feldman and Newlander to talk about their shared experience, the influence of 80s action heroes, and the birth of The Two Coreys.
Simon Thompson: You knew The Lost Boys would be a great movie but did you have any clue about its longevity or influence?
Jamison Newlander: It would have been impossible for me at 15 to assess that, but I noticed that little by little, everybody was getting excited about it. Joel Schumacher, the director, was enthusiastic about it; everyone was excited about what Joel was doing, and that built with each scene. That's how I assessed that. Something was going on; we were making something cool.
Thompson: Corey, by then, you'd already worked on a slew of great movies. Did this one feel unique in its own way?
Corey Feldman: By that point in my career, firstly, I was able to assess a script and know that it was great and had all the right chemistry and the right workings of a great movie, but also knowing the directors. When you're working with a great director and a great producer, you know it's going to be great. Although I didn't really know Joe's work as much, I was surprised to find out later that he was the guy who wrote The Wiz. That's pretty cool. He'd also worked with Woody Allen as a costume designer and done all these other things. I was also a bit jaded at the time because, as a kid, you don't know anything other than your own life experience, and for me, every movie I did went to number one at the box office, so I didn't know anything else. Richard Donner was supposed to direct it initially, and I figured we did The Goonies together, and this was kind of a vampire, little bit older version of The Goonies, so it would be another biggie. Then it evolved into something much different. That said, thinking that Richard Donner would be a part of it, I assumed it would be a number one film, and when Joel came in, I watched his work and how he operated, and I knew he really cared. He was very passionate. The director of photography, Michael Chapman, was brilliant and took hours to set up every single shot and the scope was amazing.
Thompson: Did you ever read for each other's roles?
Newlander: I think that Corey had the standing already in the industry with audiences that I think that it was natural that he would be the lead Frog, Edgar.
Feldman: The head Frog, pulling the strings (laughs). We have a rivalry about that. Those are always the right roles for us. When they passed the director's baton to Schumacher, the first time I met with him, he was like, 'Hey, listen, I think you're right for this, but you got to make some adjustments. I need you to grow your hair as long as you can. I need you to go and watch Sylvester Stallone, Chuck Norris, and Arnold Schwarzenegger movies, and I want you to formulate a character.' For me, it was a big departure. Until that point, I was a kid, and playing a kid, it was as natural as it could be. Stand by Me was the first time where I had to dig deep and pull out some really hard emotions that I'd been dealing with. Edgar Frog was the first time where I really had to create a character that was completely disconnected, completely separated from me as a human and becoming this other guy. I really dug getting into that and creating a character and manifesting this human. When they first connected me with Jamison, it was a day where they brought in several different potential Alans, and I was reading with all of them. It was kind of like, 'Where's the chemistry going to be?' As soon as Jamison and I read together, there was just this instant magic where I just knew that he took it very seriously. He's very dedicated.
Newlander: We did both take it very seriously.
(Left to right) Jamison Newlander, Corey Haim, and Corey Feldman in 'The Lost Boys.'
Thompson: Hearing you talk about playing The Frog Brothers, you do seem very earnest. In The Lost Boys, they always reminded me of the interlude characters in Shakespearean plays who can have levity but also a key role in laying the narrative.
Feldman: And that's the fun of it, isn't it? If we weren't taking it seriously, you probably wouldn't go along for the ride. You've got these two 14-year-old boys who are taking themselves so deadly seriously, even though the rest of the world is laughing at them and saying they're just kids, and you don't even know what the hell you're doing. It's that first meeting with the first vampire, that real confrontation where it's like, 'Okay, it's not just comic books and talking about it anymore. This is a real vampire, and we're about to get killed if we don't do what we say we were going to do.' There is that pivot in the movie. I think what makes it so much fun is watching these kids get invested in it.
Newlander: Joel really pushed us in that way to develop these characters. They're quite apart from what we were like in real life, and I thought it was really cool. He did say. 'Watch those movies,' and it made a real difference.
Thompson: I was going to ask if your references were the same.
Newlander: Yeah, but I think ultimately we found our own groove with it. Maybe I was a little more Chuck Norris, and Corey was more Stallone, but that's where it naturally landed. I think that's also because I was naturally very serious, which added to it.
Feldman: A funny anecdote is that I ended up meeting Stallone for the first time years after the film came out. I went to his house, I walked in, and he's got this giant statue of Rocky, and he was like, 'Come in. How are you doing? I was like, 'I'm excited to meet you because I played you. He goes, 'Oh, yeah, that's right. You did a pretty good job.' That's one of those amazing moments when you're meeting the guy you emulated for a role.
Thompson: Talking about amazing moments, The Lost Boys was where we witnessed the creation of The Two Coreys.
Newlander: I got to see that front and center from early on. That was a pivotal summer for the Coreys. It was amazing to watch that develop, and I was a part of that because we were all very close. Aside from being in a major motion picture, we had a very kid summer.
Feldman: We all got along really well and enjoyed each other's company, but Corey Haim and I had this crazy bond. Jamison and I are still like brothers, but our thing went on a whole other level with Corey and me. It started with what was poised to be a rivalry, given that a girl was involved. I was in love with this girl, and she didn't have eyes for me. She was talking about Corey Haim all the time, and I was like, 'Who is this guy?' and she was like, 'Oh, he's in the teen magazines. Don't you recognize him? He's always next to you on the pages.' I didn't know what she was talking about, so I'd go and look. Suddenly, Joel Schumacher is in the wardrobe fitting and on the phone with somebody, and he says, 'Oh, we've got the two Coreys...' and I'm like, 'Two Coreys? I'm just one guy.' I quickly found out Corey Haim was going to be in the movie, and I was like, 'Oh boy, how's this going to go?' We were both young actors, and we're both Jewish, we're both the same height, there's so much that similar. He calls me and leaves a message on my answering machine one day. I come home from school, and there's a message like, 'Hey, man, it's Corey Haim. What's up, buddy? Yo, we're going to be working together, man. It's really cool. I thought maybe we could get together and hit the beach or whatever.' I was amazed at how friendly and open he was, and he had this amazing energy. We instantly connected, we immediately bonded, and then we were pretty much inseparable.
The Lost Boys is available on 4K Ultra HD and Digital.
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Transhumanism: The Final Frontier? – Evening Standard
Posted: at 4:11 pm
I
ts a sunny September afternoon in present day London and Im talking to a woman who thinks Im an ape-brained meatsack. To be fair, Dr Elise Bohan, 32, who is really very nice, believes everyone herself included is an ape-brained meatsack. A senior research scholar at Oxfords vaunted Future of Humanity Institute, she has spent half her life thinking about the promise and perils of artificial intelligence, the limits of human wetware (your brains, bodies and all the mushy bits in between), and how we avoid getting steamrollered by the smarter-than-human machines lurking at the edge of tomorrow. As the author of Future Superhuman: Our Transhuman Lives in a Make-or-break Century, she is trying to do something about it.
Being told that my flabby, pasty body is illequipped to keep pace with a world of robot workers, lethal autonomous machines and smart AI systems that know us better than we know ourselves isnt surprising. Although we rarely recognise it, says Bohan, the 21st century is already a transhuman era: think smartphones, the cloud and our digital second skins, algorithms that know how we want to work out and what we want to google. Our biological bits are struggling to keep up. AI helped Moderna design and manufacture a Covid vaccine in 42 days flat. I, meanwhile, cant remember where I left my iPhone charger 10 minutes ago.
Which is where transhumanism comes in. A transhumanist, Bohan says, is someone who believes in being something better than human. Think of TV shows such as Black Mirror, books like Yuval Noah Huraris Homo Deus and films like Ex Machina and youre in the right ballpark. Its a philosophy. Its a quest. Its a necessity. Its about technological transcendence. Things that make you go hmmm. As Bohan puts it: It strikes transhumanists asobvious that humanity could be better.
If were lucky, humanity gets to be the parents of something magnificent
Whos in the club, I ask? Theres Ray Kurzweil, appointed Googles director of engineering in 2012, who popularised the concept of the technological singularity (the idea that were heading for a rapid intelligence explosion due to exponential improvements in information technology). Elon Musk? Transhumanist. Bill Gates? Transhumanist. Mark Zuckerberg? Big old transhumanist. Musks big play is Neuralink, a secretive company he founded in 2016 to help human and machine intelligence by developing an electronic brain implant, a Fitbit in your skull with tiny wires. Musk told the Joe Rogan podcast in 2020 that it is five to 10 years away. His plans, he says, include giving humans the option of merging with artificial intelligence by exchanging thoughts with a computer augmenting their mental capacity. You might have seen the video of its monkey implanted with the chip playing video game Pong using only its mind. In January it advertised for a clinical trial director to run tests on humans. Small matter that at least eight of the monkeys have died.
I think its a bit grim. This isnt sexy technology, agrees Bohan. Musks SpaceX rockets and Tesla cars are a lot more du jour. Transhumanism has a terrible image problem, she says. Its not fuzzy. Its not what we want to hear. But the idea and Musk is hardly alone here is that we get to piggyback and come along for the ride and be involved in the evolution of that form of digital consciousness. What it means to be human, from our brains and bodies to our values and ways of life, is poised to be transformed as we move from a purely biological species to a techno-human hybrid. Its a very different kind of trans debate. Will I need a subscription fee to buy the best brainwaves? Wont the rich simply get richer, lining their superbodies with, I dont know, literal stardust? Pass. Transhumanism is not merely this life-extension project: lets upload, lets live forever, lets just rack up the billions, says Bohan. So much of it is focused on making the world a better place in a sustainable way. Then why, I ask, does it all feel so undemocratic? A bit bermensch. When people accumulate too much power, it rarely goes well. The thing about history is that the great movers have all been undemocratic, Bohan says. Usually, its tectonic plates or pathogens or the availability of domestic arable crops. Human beings love to think of history in terms of rational actors, kings, emperors, goodies, baddies. I think this is a really interesting moment of history because we so want to believe that were in control.
Plus, she says, democracy hasnt done much to fix climate change in the past 30 years. Sooner or later mankinds trajectory will throw up a doomsday scenario we dont have the tools to deal with, she says: nuclear apocalypse, lab-made virus, rampant AI. Its like were engaged in a complex juggling act. First two balls, then three, then four. As time wears on, the balls are supplanted by live grenades that can detonate on impact. Quick, catch the next one its labelled nukes. And the next pandemics. Dont drop a single one! Good, AI is coming soon.
AI and automation threaten factory jobs, driving jobs heck, any jobs. Wages will tumble. Traditional family models will fall apart. Life scripts will be torn up. Dreams will turn to dust. An eruption of disruption, already underway. Its not panning out for so, so many, she says. And the anger is palpable. Overeducated generations, frankly, dont know what theyre doing. Meanwhile, theres a crude social media landscape of today like Instagram, Snapchat, TikTok its awful, its brain junk, its vapid, I dont know how anyone finds it fulfilling, but its addictive enough for people to be invested in curating their identity and existence in these virtual worlds. Imagine what happens when Mark Zuckerbergs Metaverse finally turns its trillions into something that doesnt look drawn by a toddler with a crayon up its nostril. Well never log off. Which brings us on to another fascinating conundrum: Ive used the Oculus Rift, Ive had virtual sex, quote unquote, and its so immersive, says Bohan. She believes we are 10 years away from enjoying fluent and emotionally enriching conversations with Alexa and her kind. She talks of AI characters conscious? Alive? Who can say? that will evolve from best friend to life partner, sing lullabies, make love. Its wild stuff. But then again, theres already Microsofts Chinese chatbot Xiaoice (pronounced Shao-ice) designed with a focus on high emotional intelligence a simulated 18-year-old with 660 million users, 25 per cent of whom have confessed their love to her. I think a growing subset, particularly of young men, will be opting into this technology, the result being that it skews the sex ratios in the human dating pool, making men ever more scarce. The end of men? Just maybe.
I like my humanity. Im a happy-ish meatsack. I like the sound of rain on the window; I like long, muddy walks and the smell of gorse. I like looking at bell heather and bog asphodels. I like the idea of children I might have one day. I might bore them about flowers, too. I like my friends and my family, I value my weaknesses and my wilfulness, I suffer theirs gladly. I want to think this is all bollocks and billionaires, and that my little life might just be left alone. Its hard to think about transcendence without thinking about endings. I dont like them at all.
Funnily enough, all those impulses I share, says Bohan. Im happiest reading books, talking to my friends, being in the ocean, being outdoors. A quiet simple life Im very big on. Its in my interest to ignore all of this. Maybe I have the means and opportunities to block a lot of this out. [But] I dont think if you have children you can afford to block it out because the ramifications for their development and schooling and so many other things are really important.
She thinks this is bigger than us, as individuals, anyway. That she needs to warn us, that we get busy techno-living or get busy homo-dying. Im talking about future generations for trillions of people yet to be born, more people than have ever lived on this planet. Her hope? That the most beautiful things about humanity do get to survive far into the future and do potentially go on to do amazing things that are beyond the reach of you or I today, that are beyond the reach of the merely human, which doesnt mean its a project of celebrating the demise of humanity. If were lucky, humanity gets to be the parents of something magnificent that can explore the wonders and the mysteries of the universe and consciousness. Her goal is to make us take these ideas seriously, that we dont take it personally, that we dont sulk. I say come friendly bombs, fall upon Silicon Valley. But what do I know? Im obsolete.
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Former GOP candidates push baseless QAnon conspiracy theory that Hurricane Ian was created to punish DeSantis – The Independent
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While Florida residents and emergency crews survey the devastation from Hurricane Ian, which continues to barrel along the East Coast, two former far-right congressional candidates floated a baseless conspiracy theory that the federal government created the storm to punish and target Republicans.
Lauren Witzke, a QAnon-supporting conspiracy theorist who was the GOP candidate for US Senate seat in Delaware in 2020, said she has no doubt that technology exists to manipulate weather that could be used to target Florida Governor Ron DeSantis.
We know the technology does exist, she told former GOP congressional candidate Deanna Lorraine on her far-right conspiracy theory streaming channel, above a caption reading Biden Builds Transhuman Cyborg Army Using Immigrants.
Of course they would be willing to do something like this to target red states. I have no doubt. The technology exists to manipulate weather, Ms Witzke added in a clip captured by watchdog group Right Wing Watch. I know Florida is prone to hurricanes, however this developed to [a category 5 or category 5 storm] overnight, and it does seem to be hitting the conservative areas.
She said she is not putting it past the elites to target something like this towards Florida as punishment for eliminating Covid-19 vaccine requirements and getting rid of child grooming, referencing the states law prohibiting classroom discussion of LGBT+ people and issues by smearing its critics as groomers.
These huge hurricanes always seem to target red states, red districts, and always at a convenient time, typically right before elections or, you know, because possibly Ron DeSantis has been stepping out of line a lot and fighting the deep state, said Ms Lorraine, who received less than 2 per cent of the vote in a race against House Speaker Nancy Pelosi in 2020.
Their claims echo similarly unhinged-from-reality statements central to the QAnon movement in the wake of Hurricane Ida in 2021, which devastated coastal Louisiana with impacts felt throughout the south and East Coast.
QAnons big tent conspiracy theorist movement includes references to deep state-controlled weather manipulation events but fail to address the climate crisis, political figures who deny it, increasingly powerful storms fuelled by climate change, and a lack of critical infrastructure investments to combat them.
Nearly two million people in Florida remain without power after Ian made landfall on Tuesday.
The states death toll also continues to rise as emergency responders survey the damage. Officials have reported at least one confirmed death and 20 unconfirmed deaths in three counties.
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Is the body key to understanding consciousness? – The Guardian
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In 2018, billionaire Silicon Valley entrepreneur Sam Altman paid a startup called Nectome $10,000 to preserve his brain after he dies and, when the technology to do so becomes available, to upload his memories and consciousness to the cloud.
This prospect, which was recently popularised in Amazon Primes sci-fi comedy series Upload, has long been entertained by transhumanists. Although theoretically possible, it is rooted in the flawed idea that the brain is separate from the body, and can function without it.
The idea that the mind and brain are separate from each other is usually attributed to the 17th-century mathematician and philosopher Ren Descartes, who believed that the body is made of matter, and the mind of some other, non-physical substance.
Modern brain research rejects the distinction between the physical and the mental. Most neuroscientists agree that what we call the mind is made of matter. The mind is hard to define, but the consensus now is that it emerges from the complex networks of cells in the brain.
But most people still view the mind and brain as being distinct from the body. In 2016, four prominent brain researchers published an article summarising what we know about consciousness. It begins: Being conscious means that one is having an experience to see an image, hear a sound, think a thought or feel an emotion.
It is, however, becoming increasingly clear that the mind/brain and body are intimately linked, and that the body influences our thoughts and emotions. Being conscious does not just mean having awareness of the outside world. It means being aware of ones self within ones surroundings. The way we experience our body is central to how we perceive our self.
Phantom limbs are a striking demonstration of the importance of the body for self-consciousness. They were described in the mid-16th century by the barber-surgeon Ambroise Par, who reportedly amputated several hundred limbs a day during the Italian war of 1542-46.
Verily it is a thing wondrous, strange and prodigious, he wrote. The patients who have many months after the cutting away of the leg grievously complained that they yet felt exceeding great pain of that leg cut off. At that time, however, few survived the operation, so the phenomenon was seen only rarely, and dismissed as a delusion.
Advances in medicine and military technology changed this. The invention of a bullet called the Mini ball with its greater accuracy, range, and muzzle velocity, increased the number of amputations, while the introduction of anaesthetics and antiseptics improved the survival rates of soldiers who went under the knife.
And so it was that the neurologist Silas Weir Mitchell, who amputated countless arms and legs on the battlefields of the American civil war, came to see that phantom limbs are the rule rather than an exception, experienced by the vast majority of amputees.
The medical community was still sceptical of the phenomenon, however, so Mitchell initially described his observations as a short story, The Case of George Dedlow, published in the Atlantic Monthly in July 1866. The fictional titular character was a composite of the hundreds of thousands of soldiers who were maimed and mutilated during the conflict. He lost all four limbs, one by one, to become a useless torso, more like some strange larval creature than anything of human shape, reduced to [a] fraction of a man.
Mitchells story was so vivid that readers took it as factual, and believed that he was a real patient being treated at Philadelphias South Street Stump hospital. Many wrote him letters of support, some tried to visit him, and some even raised money for his care. But the story played a large part in bringing the phenomenon into the realms of medical science, and Mitchell went on to become the first elected president of the American Neurological Association.
Mitchell recognised phantom limbs as a disturbance of bodily self-consciousness, in which the amputee retains awareness of the missing limb, and feels as if it is still attached to their body. In some amputees, the phantom disappears within weeks or months of amputation. In others, it persists for decades.
Phantoms do not appear only in the form of missing limbs. Women may experience phantom breasts after mastectomy; men can experience phantom erections after amputation of a cancerous penis; and there are reports of phantom eyes, noses, teeth, and even phantom haemorrhoids, bowel movements and gas after surgical removal of the rectum.
Phantom sensations occur because the brain creates a dynamic model of the body by integrating tactile and visual information with limb position signals from the muscles and tendons. This model, variously called the body schema or body image, is crucial for both the perception and control of the body. But when a limb or other body part is removed, the schema is not properly updated, and so it retains an imprint of the missing part. As a result, the individual remains conscious of the missing part often, even more so than of their existing body parts.
Most of us could imagine few things worse than having a limb amputated. But some people want nothing more.
Take Australian Robert Vickers. Before I was 10 years old I knew my left leg somehow didnt belong, Vickers told ABC Radio National in 2009, and that my body would not be as I felt it should be until I had the leg amputated precisely halfway up the thigh.
Vickers harboured this strange desire, and suffered in silence, for more than 30 years. It made him severely depressed, and he received psychotherapy. He was prescribed antidepressants, tranquillisers, and antipsychotics, and received electroconvulsive therapy, but to no avail. He tried, without success, to damage his leg in various ways, in order to force an amputation.
Then, at 41, he submerged the unwanted limb in dry ice until the pain became unbearable. His wife drove him to hospital, where he received the amputation he had wanted for so long. I left hospital two weeks later with my desired stump, and life changed for the better from that day. In the 24 years since, I only regret not doing it sooner.
Vickers is perhaps the best documented case of body integrity identity disorder (BIID), an extremely rare condition, of which fewer than 500 other cases have been reported to date. For most of his life, Vickers believed his experience to be unique, but others suffering from the condition describe it in similar terms.
All report a fascination with amputees, and a desire to amputate, from an early age. The desire usually becomes obsessive, to the extent that they will try self-amputation. Use of dry ice appears to be the most common method, and some have used homemade guillotines or shotguns. In another well-documented case, a 79-year-old New Yorker travelled to Mexico and paid an unqualified doctor $10,000 to amputate his leg. He died of gangrene a week later.
BIID first appeared in medical literature in a 1977 study published in the Journal of Sex Research. The authors of this study including Greg Furth, himself a wannabe amputee described the condition as a paraphilia, or an abnormal sexual behaviour, in which the stump is fetishised because it resembles a phallus, and named it apotemnophilia, meaning amputation love.
Some BIID sufferers do indeed report a sexual aspect to their desire to amputate. But they invariably describe their experience in terms of self-identity. One participant in Melody Gilberts 2003 documentary Whole says that he finally became a person late in life after blowing his own leg off with a shotgun. Another participant told the film-makers that by taking the leg away, Im actually more of a person than I was before Ive corrected the body that was wrong. Vickers has stated that he felt incomplete with his left leg, and that he only became whole after its removal.
The condition was renamed body integrity identity disorder to reflect this. BIID is a disturbance of bodily self-consciousness with a neurological basis, as are phantom limbs. There is evidence to suggest that it occurs because the affected limb is not incorporated into the body schema as it develops in early childhood. Amputation is not offered as a treatment for BIID sufferers, but it could be argued that making it available to them would minimise their risk of self-harm.
Research into bodily awareness is leading us to rethink the nature of consciousness. Our understanding of how the brain works will progress only when we stop observing the brain in isolation, and start thinking of it as one part of a system that includes the body and its environment.
An understanding of how brain and body interact is critical for understanding the phenomena of phantom limbs and BIID. Such interactions also play a key role in mental health conditions such as anxiety and depression, and in eating disorders such as anorexia nervosa. All of these conditions cause symptoms in the body that may be accompanied by disturbances in how the brain interprets those symptoms.
Yet the links between the brain and body are still under-appreciated. Only by taking the body into consideration will we gain a better understanding of these conditions and, it is to be hoped, develop effective treatments for them.
The new understanding of bodily self-consciousness leads us to some surprising conclusions. If bodily awareness is the basis of self-consciousness, then it follows that bumblebees, and even robots, may possess basic consciousness.
A study published in 2020 by researchers in Germany showed that bees can accurately judge gaps between obstacles relative to their wingspan, and reorient their bodies accordingly to avoid inflight collisions. Researchers at Columbia Universitys Creative Machines Lab have developed a starfish-shaped robot with an in-built body schema, which can adjust its gait after having a limb removed. The latest version of this robot creates its own body schema from experience.
If self-consciousness is based in bodily awareness, then it is unlikely that a lab-grown mini-brain could ever become conscious, as some ethicists have claimed. By the same token, transhumanists claim that we will one day gain immortality by uploading our brains to supercomputers will probably always be science fiction.
Body Am I: The New Science of Self-Consciousness by Moheb Costandi is published by MIT Press (22.50). To support the Guardian and Observer order your copy at guardianbookshop.com. Delivery charges may apply
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Cell and Gene Therapy: Rewriting the Future of Medicine – Technology Networks
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Cell and gene therapies seek to correct the root cause of an illness at the molecular level. These game-changing medicines are reshaping how we address previously untreatable illnesses transforming peoples lives.
Cell and gene therapy represent overlapping fields of research with similar therapeutic goals developing a treatment that can correct the underlying cause of a disease, often a rare inherited condition that can be life-threatening or debilitating and has limited treatment options.
While these technologies were initially developed in the context of treating rare diseases caused by a single faulty gene, they have since evolved towards tackling more common diseases, says Professor Rafael J. Yez-Muoz, director of the Centre of Gene and Cell Therapy (CGCT) at Royal Holloway University of London.
A powerful example is the chimeric antigen receptor (CAR) T-cell therapies, which have been approved for treating certain blood cancers. The approach involves genetically modifying a patients T cells in the laboratory before reintroducing them into the body to fight their disease.
For the first time, we had an example of gene therapy to treat a more common disease demonstrating that the technology has wide applicability, enthuses Yez-Muoz.
To date, 24 cellular and gene therapy products have received approval from the US Food and Drug Administration (FDA) including life-changing treatments for patients with rare diseases, such as inherited forms of blindness and neuromuscular conditions. A variety of gene and cell-based therapies for both rare and common diseases are also currently in development across many therapeutic areas, offering hope for many more families in coming years.
This webinar will provide an introduction to the regulatory framework for cell and gene therapies and highlight the importance of chemistry, manufacturing and controls. Watch to learn about regulatory concerns, safety and quality testing throughout the product lifecycle and key acronyms and terminology.
Gene therapies seek to introduce specific DNA sequences into a patients body to treat, prevent or potentially cure a disease. This may involve the delivery of a functional gene into cells to replace a gene that is missing or causing a problem or other strategies using nucleic acid sequences (such as antisense oligonucleotides or short interfering RNAs [siRNAs]) to reduce, restore or modify gene expression. More recently, scientists are also developing genome-editing technologies that aim to change the cells DNA at precise locations to treat a specific disease.
The key step in successful gene therapy relies on the safe and efficient delivery of genetic material into the target cells, which is carried out by packaging it into a suitable delivery vehicle (or vector). Many current gene therapies employ modified viruses based on adenoviruses, adeno-associated viruses (AAV), and lentiviruses as vectors due to their intrinsic ability to enter cells. But non-viral delivery systems such as lipid nanoparticles (LNPs) have also been successfully employed to deliver RNA-based therapeutics into cells.
A big advantage of using viral vectors for gene delivery is they are longer lasting than non-viral systems, states Dr. Rajvinder Karda, lecturer in gene therapy at University College London. Many of the rare diseases were aiming to tackle are severe and we need to achieve long-term gene expression for these treatments to be effective.
While improved technological prowess empowers the development of CRISPR-edited therapies, supply-chain and manufacturing hurdles still pose significant barriers to clinical and commercialization timelines. Watch this webinar to learn more about the state of CRISPR cell and gene therapies, challenges in CRISPR therapy manufacturing and a next-generation manufacturing facility.
Viral-vector gene therapies are either administered directly into the patients body (in vivo), or cells harvested from a patient are instead modified in the laboratory (ex vivo) and then reintroduced back into the body. Major challenges for in vivo gene delivery approaches are with the safe and efficient targeting of the therapeutic to the target cells and overcoming any potential immune responses to the vectors.
As well as getting the genetic material into the affected cells, we also need to try and limit it reaching other cells as expressing a gene in a cell where its not normally active could cause problems, explains Dr. Gerry McLachlan, group leader at the Roslin Institute in Edinburgh.
For example, the liver was identified as a major site of toxicity for an AAV-based gene therapy approved for treating spinal muscular atrophy (SMA), a type of motor neuron disease that affects people from a very young age.
Unfortunately, these viruses are leaky as theyre also going to organs that dont need therapy meaning you can get these off-target effects, says Karda. Theres still work to be done to develop and refine these technologies to make them more cell- and organ-specific.
It is also important to ensure the gene is expressed at the right level in the affected cells too high and it may cause side effects and too little may render the treatment ineffective. In a recent major advancement in the field, scientists developed a dimmer switch system Xon that enables gene expression to be precisely controlled through exposure to an orally delivered small molecule drug. This novel system offers an unprecedented opportunity to refine and tailor the application of gene therapies in humans.
Download this whitepaper to discover an electroporation system that resulted in CAR transfection efficiencies as high as 70% in primary human T cells, can avoid the potential risks associated with viral transduction and is able to produce CAR T cells at a sufficient scale for clinical and therapeutic applications.
In 1989, a team of researchers identified the gene that causes the chronic, life-limiting inherited disease cystic fibrosis (CF) the cystic fibrosis transmembrane conductance regulator (CFTR). This was the first ever disease-causing gene to be discovered marking a major milestone in the field of human genetics. In people with CF, mutations in the CFTR gene can result in no CTFR protein, or the protein being made incorrectly or at insufficient levels all of which lead to a cascade of problems that affect the lungs and other organs.
Our team focuses on developing gene therapies to treat respiratory diseases in particular, were aiming to deliver the CTFR gene into lung cells to treat CF patients, says McLachlan.
The results of the UK Respiratory Gene Therapy Consortiums most recent clinical trial showed that an inhaled non-viral CTFR gene therapy formulation led to improvements in patient lung function.
While this was encouraging, the effects were modest and we need to develop a more potent delivery vehicle, explains McLachlan. Weve also been working on a viral-based gene therapy using a lentiviral vector to introduce a healthy copy of the CTFR gene into cells of the lung.
Kardas team focuses on developing novel gene therapy and gene-editing treatments for incurable genetic diseases affecting the central and peripheral nervous system and Yez-Muoz is aiming to develop new treatments for rare neurodegenerative diseases that affect children, including SMA and ataxia telangiectasia (AT).
But a significant barrier for academic researchers around the world is accessing the dedicated resources, facilities and expertise required to scale up and work towards the clinical development and eventually the commercial production of gene and cell therapies. These challenges will need to be addressed and overcome if these important advancements are to successfully deliver their potentially life-changing benefits to patients.
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After many decades of effort, the future of gene and cell therapies is incredibly promising. A flurry of recent successes has led to the approval of several life-changing treatments for patients and many more products are in development.
Its no longer just about hope, but now its a reality with a growing number of rare diseases that can be effectively treated with these therapies, describes Yez-Muoz. We now need to think about how we can scale up these technologies to address the thousands of rare diseases that exist and even within these diseases, people will have different mutations, which will complicate matters even further.
But as more of these gene and cell-based therapies are approved, there is a growing urgency to address the challenge of equitable access to these innovative treatments around the world.
Gene therapies have the dubious honor of being the most expensive treatments ever and this isnt sustainable in the longer term, says Yez-Muoz. Just imagine being a parent and knowing there is an effective therapy but your child cant access it that would be absolutely devastating.
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Growth in Cell and Gene Therapy Market – BioPharm International
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Biopharma focuses on streamlining biomanufacturing and supply chain issues to drive uptake of cell and gene therapies.
Cell and gene therapies (CGTs) offer significant advances in patient care by helping to treat or potentially cure a range of conditions that have been untouched by small molecule and biologic agents. Over the past two decades, more than 20 CGTs have been approved by FDA in the United States and many of these one-time treatments cost between US$375,00 and US$2 million a shot (1). Given the high financial outlay and patient expectations of these life-saving therapies, it is essential that manufacturers provide integrated services across the whole of the supply chain to ensure efficient biomanufacturing processes and seamless logistics to reduce barriers to uptake.
The following looks at the who, what, when, and why of biomanufacturing and logistics in CGTs in the bio/pharmaceutical industry in more detail.
According to market research, the global gene therapy market will reach US$9.0 billion by 2027 due to favorable reimbursement policies and guidelines, product approvals and fast-track designations, growing demand for chimeric antigen receptor (CAR) T cell-based gene therapies, and improvements in RNA, DNA, and oncolytic viral vectors (1).
In 2020, CGT manufacturers attracted approximately US$2.3 billion in investment funding (1). Key players in the CGT market include Amgen, Bristol-Myers Squibb Company, Dendreon, Gilead Sciences, Novartis, Organogenesis, Roche (Spark Therapeutics), Smith Nephew, and Vericel. In recent years, growth in the CGT market has fueled some high-profile mergers and acquisitions including bluebird bio/BioMarin, Celgene/Juno Therapeutics, Gilead Sciences/Kite, Novartis/AveXis and the CDMO CELLforCURE, Roche/Spark Therapeutics, and Smith & Nephew/Osiris Therapeutics.
Many bio/pharma companies are re-considering their commercialization strategies and have re-invested in R&D to standardize vector productions and purification, implement forward engineering techniques in cell therapies, and improve cryopreservation of cellular samples as well as exploring the development of off-the-shelf allogeneic cell solutions (2).
The successful development of CGTs has highlighted major bottlenecks in the manufacturing facilities, and at times, a shortage of raw materials (3). Pharma companies are now taking a close look at their internal capabilities and either investing in their own manufacturing facilities or outsourcing to contract development and manufacturing organizations (CDMOs) or contract manufacturing organizations (CMOs) to expand their manufacturing abilities (4). Recently, several CDMOsSamsung Biologics, Fujifilm Diosynth, Boehringer Ingelheim, and Lonzahave all expanded their biomanufacturing facilities to meet demand (5).
A major challenge for CGT manufacturers is the seamless delivery of advanced therapies. There is no room for error. If manufacturers cannot deliver the CGT therapy to the patient with ease, the efficacy of the product becomes obsolete. Many of these therapies are not off-the-shelf solutions and therefore require timely delivery and must be maintained at precise temperatures to remain viable. Thus, manufacturers must not only conform to regulations, but they must also put in place logistical processes and contingency plans to optimize tracking, packaging, cold storage, and transportation through the products journey. Time is of the essence, and several manufacturers have failed to meet patient demands, which have significant impacts on the applicability of these agents.
Several CAR T-cell therapies have now been approved; however, research indicates that a fifth of cancer patients who are eligible for CAR-T therapies pass away while waiting for a manufacturing slot (6). Initially, the manufacture of many of these autologous products took around a month, but certain agents can now be produced in fewer than two weeks (7). Companies are exploring new ways to reduce vein-to-vein time (collection and reinfusion) through the development of more advanced gene-transfer tools with CARs (such as transposon, CRISPR (Clustered Regularly Interspaced Short Palindromic Repeats) among others, and the use of centralized organization with standardized apheresis centers (5). Others are exploring the use of the of allogeneic stem cells including Regen Biopharma, Escape Therapeutics, Lonza, Pluristem Therapeutics, and ViaCord (7).
Several gene therapies have also been approved, mainly in the treatment of rare disease (8). Many companies are evaluating novel gene therapy vectors to increase levels of gene expression/protein productions, reduce immunogenicity and improve durability including Astellas Gene Therapies, Bayer, ArrowHead Pharmaceuticals, Bayer, Bluebird Bio, Intellia Therapeutics, Kystal Biotech, MeiraGTx, Regenxbio, Roche, Rocket Pharmaceuticals, Sangamo Therapeutics, Vertex Pharmaceuticals, Verve Therapeutics, and Voyager Therapeutics (8).
While many biopharma companies have established their own in-house CGT good manufacturing practice (GMP) operation capabilities, others are looking to decentralize manufacturing and improve distribution by relying on external contracts with CDMOs and CMOs such as CELLforCURE, CCRM, Cell Therapies Pty Ltd (CTPL), Cellular Therapeutics Ltd (CTL), Eufets GmbH, Gravitas Biomanufacturing, Hitachi Chemical Advances Therapeutic Solutions, Lonza, MasTHerCell, MEDINET Co., Takara Bio, and XuXi PharmaTech (6, 9, 10).
The top 50 gene therapy start-up companies have attracted more than $11.6 billion in funds in recent years, with the top 10 companies generating US$5.3 billion in series A to D funding rounds (10). US-based Sana Biotechnology leads the field garnering US$700 million to develop scalable manufacturing for genetically engineered cells and its pipeline program, which include CAR-T cell-based therapies in oncology and CNS (Central Nervous System) disorders (11). In second place, Editas Medicine attracted $656.6 million to develop CRISPR nuclease gene editing technologies to develop gene therapies for rare disorders (12).
Overall, CGTs have attracted the pharma industrys attention as they provide an alternative route to target diseases that are poorly served by pharmaceutical and/or medical interventions, such as rare and orphan diseases. Private investors continue to pour money into this sector because a single shot has the potential to bring long-lasting clinical benefits to patients (13). In addition, regulators have approved several products and put in place fast track designation to speed up patient access to these life-saving medicines. Furthermore, healthcare providers have established reimbursement policies and manufacturers have negotiated value- and outcome-based contracts to reduce barriers to access to these premium priced products
On the downside, the manufacture of CGTs is labor intensive and expensive with manufacturing accounting for approximately 25% of operating expenses, plus there is still significant variation in the amount of product produced. On the medical side, many patients may not be suitable candidates for CGTs or not produce durable response due to pre-exposure to the viral vector, poor gene expression, and/or the development of immunogenicity due to pre-exposure to viral vectors. Those that can receive these therapies may suffer infusion site reactions, and unique adverse events such as cytokine release syndrome and neurological problems both of which can be fatal if not treated promptly (14).
Despite the considerable advances that have been made in the CGT field to date, there is still much work needed to enhance the durability of responses, increase biomanufacturing efficiencies and consistency and to implement a seamless supply chain that can ensure these agents are accessible, cost-effective, and a sustainable option to those in need.
Cleo Bern Hartley is a pharma consultant, former pharma analyst, and research scientist.
BioPharm InternationalVol. 35, No. 10October 2022Pages: 4951
When referring to this article, please cite it as C.B. Hartley, "Growth in Cell and Gene Therapy Market," BioPharm International 35 (10) 4951 (2022).
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CRISPR Therapeutics Announces FDA Regenerative Medicine Advanced Therapy (RMAT) Designation Granted to CTX130 for the Treatment of Cutaneous T-Cell…
Posted: at 4:07 pm
ZUG, Switzerland and BOSTON, Sept. 28, 2022 (GLOBE NEWSWIRE) -- CRISPR Therapeutics (Nasdaq: CRSP), a biopharmaceutical company focused on creating transformative gene-based medicines for serious diseases, today announced that the U.S. Food and Drug Administration (FDA) granted Regenerative Medicine Advanced Therapy (RMAT) designation to CTX130, the Companys wholly-owned allogeneic CAR T cell therapy targeting CD70, for the treatment of Mycosis Fungoides and Szary Syndrome (MF/SS).
The RMAT designation is an important milestone for the CTX130 program that recognizes the transformative potential of our cell therapy in patients with T-cell lymphomas based upon encouraging clinical data to date, said Phuong Khanh (P.K.) Morrow, M.D., FACP, Chief Medical Officer of CRISPR Therapeutics. "We continue to work with a sense of urgency to bring our broad portfolio of allogeneic cell therapies to patients in need.
Established under the 21st Century Cures Act, RMAT designation is a dedicated program designed to expedite the drug development and review processes for promising pipeline products, including genetic therapies. A regenerative medicine therapy is eligible for RMAT designation if it is intended to treat, modify, reverse or cure a serious or life-threatening disease or condition, and preliminary clinical evidence indicates that the drug or therapy has the potential to address unmet medical needs for such disease or condition. Similar to Breakthrough Therapy designation, RMAT designation provides the benefits of intensive FDA guidance on efficient drug development, including the ability for early interactions with FDA to discuss surrogate or intermediate endpoints, potential ways to support accelerated approval and satisfy post-approval requirements, potential priority review of the biologics license application (BLA) and other opportunities to expedite development and review.
About CTX130 and COBALT TrialsCTX130, a wholly-owned program of CRISPR Therapeutics, is a healthy donor-derived gene-edited allogeneic CAR T investigational therapy targeting Cluster of Differentiation 70, or CD70, an antigen expressed on various solid tumors and hematologic malignancies. CTX130 is being investigated in two ongoing independent Phase 1 single-arm, multi-center, open-label clinical trials that are designed to assess the safety and efficacy of several dose levels of CTX130 in adult patients. The COBALT-LYM trial is evaluating the safety and efficacy of CTX130 for the treatment of relapsed or refractory T or B cell malignancies. The COBALT-RCC trial is evaluating the safety and efficacy of CTX130 for the treatment of relapsed or refractory renal cell carcinoma. CTX130 has received Orphan Drug and Regenerative Medicine Advanced Therapy designations from the FDA.
About CRISPR TherapeuticsCRISPR Therapeutics is a leading gene editing company focused on developing transformative gene-based medicines for serious diseases using its proprietary CRISPR/Cas9 platform. CRISPR/Cas9 is a revolutionary gene editing technology that allows for precise, directed changes to genomic DNA. CRISPR Therapeutics has established a portfolio of therapeutic programs across a broad range of disease areas including hemoglobinopathies, oncology, regenerative medicine and rare diseases. To accelerate and expand its efforts, CRISPR Therapeutics has established strategic partnerships with leading companies including Bayer, Vertex Pharmaceuticals and ViaCyte, Inc. CRISPR Therapeutics AG is headquartered in Zug, Switzerland, with its wholly-owned U.S. subsidiary, CRISPR Therapeutics, Inc., and R&D operations based in Boston, Massachusetts, and business offices in San Francisco, California and London, United Kingdom. For more information, please visit http://www.crisprtx.com.
CRISPR Forward-Looking StatementThis press release may contain a number of forward-looking statements within the meaning of the Private Securities Litigation Reform Act of 1995, as amended, including statements made by Dr. Morrow in this press release, as well as regarding CRISPR Therapeutics expectations about any or all of the following: (i) the status of clinical trials and discussions with regulatory authorities related to product candidates under development by CRISPR Therapeutics including, without limitation, expectations regarding the benefits of RMAT designation; and (ii) the therapeutic value, development, and commercial potential of CRISPR/Cas9 gene editing technologies and therapies. Without limiting the foregoing, the words believes, anticipates, plans, expects and similar expressions are intended to identify forward-looking statements. You are cautioned that forward-looking statements are inherently uncertain. Although CRISPR Therapeutics believes that such statements are based on reasonable assumptions within the bounds of its knowledge of its business and operations, forward-looking statements are neither promises nor guarantees and they are necessarily subject to a high degree of uncertainty and risk. Actual performance and results may differ materially from those projected or suggested in the forward-looking statements due to various risks and uncertainties. These risks and uncertainties include, among others: the potential for initial and preliminary data from any clinical trial and initial data from a limited number of patients not to be indicative of final trial results; the potential that clinical trial results may not be favorable; potential impacts due to the coronavirus pandemic, such as the timing and progress of clinical trials; that future competitive or other market factors may adversely affect the commercial potential for CRISPR Therapeutics product candidates; uncertainties regarding the intellectual property protection for CRISPR Therapeutics technology and intellectual property belonging to third parties, and the outcome of proceedings (such as an interference, an opposition or a similar proceeding) involving all or any portion of such intellectual property; and those risks and uncertainties described under the heading "Risk Factors" in CRISPR Therapeutics most recent annual report on Form 10-K, quarterly report on Form 10-Q and in any other subsequent filings made by CRISPR Therapeutics with the U.S. Securities and Exchange Commission, which are available on the SEC's website at http://www.sec.gov. Existing and prospective investors are cautioned not to place undue reliance on these forward-looking statements, which speak only as of the date they are made. CRISPR Therapeutics disclaims any obligation or undertaking to update or revise any forward-looking statements contained in this press release, other than to the extent required by law.
CRISPR THERAPEUTICS standard character mark and design logo, CTX130 and COBALT are trademarks and registered trademarks of CRISPR Therapeutics AG. All other trademarks and registered trademarks are the property of their respective owners.
Investor Contact:Susan Kim+1-617-307-7503susan.kim@crisprtx.com
Media Contact:Rachel Eides+1-617-315-4493rachel.eides@crisprtx.com
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CRISPR Therapeutics Announces FDA Regenerative Medicine Advanced Therapy (RMAT) Designation Granted to CTX130 for the Treatment of Cutaneous T-Cell...
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