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mRNA Cancer Vaccine Reprograms Immune System to Tackle Glioblastoma in 48 Hours (insideprecisionmedicine.com)
406 points by birriel 6 months ago | hide | past | favorite | 230 comments



Richard Scolyer, first patient for a Glioblastoma vaccine, is 10 months in and counting. (I'm not sure if it's mRNA based.) The treatment was vaccine, followed by surgery to remove the tumour, followed by more vaccine to prevent recurrence. The vaccine course is up to 8 out of 10 planned doses. So far it hasn't come back.

https://www.facebook.com/ProfRScolyer

https://en.wikipedia.org/wiki/Richard_Scolyer#Cancer_diagnos...


My father went under surgery to get this removed. It was 6cm and completely grew back within 3 months. He died 7 months later.


I'm sorry for your loss


Is this the same as glioblastoma multiforme (GBM)? I'm not a doctor, but I thought GBM was a death sentence? Progress on that front would be amazing.


Yes, it’s that cancer. Median survival is a little over a year iirc.

Often treatment focus is on quality of life issues, because they are often found due to physical deficits.


ThTs pretty good because glioblastomas are real real bad


A friend of mine 23 years died of glioblastoma. Completely undetected, he went to bed with a mild headache and died during his sleep.

If we find a cure for glioblastoma the challenge would be detection before it's too late.


And they tell me my health anxiety is "irrational".


To be honest that's not a bad way to go out. Better than years and years of treatment for something and a slow death. But yeah, the detection aspect would be interesting assuming these mRna viruses could cure cancer.


Yes, I wholeheartedly agreed.

This stance came shortly after I just buried my mother-in-law. Had been doing home-based hospice care for 3 (now deceased) parents of mine. Took 19-years solidly out of my life.

So, yes. Quicker the better, at least for me.


Super traumatic for his girlfriend though...


How can it be a vaccine if he already had Glioblastoma? Surely it's a treatment not a vaccine?


> A vaccine is a biological preparation that provides active acquired immunity to a particular infectious or malignant disease.

With viruses and bacteria the immune system eventually catches up and vaccinating tends to be done before the host is infected (rabies vaccination is an outlier since it still works even after infection during the latent period). With cancer the immune system usually doesn’t recognize the threat which is why vaccinating after the fact is still effective.


Yep, the goal of these vaccines are to program the body to have a strong immune reaction to the cancer/tumor.


The definition is broader than that. Think of a vaccine as something which teaches your immune system to fight some particular thing.

The most common application is as a preventative measure to protect you from an infectious disease. But it can be used for other diseases (like cancer, which is not infectious) and it can be used after you're sick.

Fun fact: if an unvaccinated person is exposed to measles, they can get the MMR within 72 hours of exposure, and it will still reduce the severity of the disease. (Source: https://www.cdc.gov/vaccines/vpd/mmr/public/index.html )


Not all vaccines are (purely) prophylactic. This is what we would call a therapeutic vaccine.


Because the definition of vaccine has been muddled with what used to be called gene therapy. In this case, they are tricking the body's immune system to attack specific cancer cells like it would learn to attack a flu virus or any other antigen.


they couple it with surgery despite how the vaccines are supposed to remove the tumors themselves?

it seems odd but i guess its meant to aid the process?


With tumors the mass matters. Each remaining cancer cell gives it another chance to stumble on a mutation that can allow it to escape your treatment.

BTW, that's also why so many tumor drugs work well in mice.


I guess a die-off of so many cancer cells as is in tumor, would cause a lot of stress to the body. So they cut as much as they can and only leave small groups of cells to be targeted with other methods.


So now we only need to detect the cancer in an earlier stage, and surgery might not even be necessary (?)


Even if the immune system completely destroys the tumor, I'd be worried about tumor detritus (is that the right word?) floating around in the brain? It might be better than the alternative, but I'd think that's one spot you really don't want cobwebs gathering in.


If the immune system actually works properly, no, not really a huge concern. Leukocytes and macrophages fully consume foreign matter, enclosing it in a phagosome. This then merges with a lysosome, where the matter is broken down into harmless components, although some stays on the surface of the cell to activate other immune cells against that particular brand of gunk.


MRNA and personalized cancer vaccines are showing tremendous potential in a lot of cancers: https://jakeseliger.com/2024/04/12/moderna-mrna-4157-v90-new.... GBM is particularly gnarly; one of the few other treatments in trials I'm aware of is DCVax: https://www.uclahealth.org/news/article/fda-approval-brain-c....

One big problem is the FDA's slowness regarding treatments for otherwise fatal diseases like GBM.


>One big problem is the FDA's slowness regarding treatments for otherwise fatal diseases like GBM.

What do you mean by slowness? They can't skip all the safety stuff!


Not just safety, but also effectiveness. FDA checks whether the trial(s) to prove the drugs effectiveness were run correctly (eg. the randomization, the control group, etc.), if the statistical analysis was done right, if the endpoints are appropriate (response to treatment is not always objective) etc. etc.

The FDA (and EMA in Europe) are the only thing that protects desperate patients from fraudsters, charlatans and pharma-companies just looking for a return on their investment.


Ideally this is what would happen. In practice there have been very public failures in being overly cautious and aggressive.

While Aduhelm reduces Aβ it has no clinically significant effect. Still, the FDA approved it. Mercifully it'll be discontinued in November.

The covid vaccine represented a huge policy failure by the FDA. While people in nursing homes died in droves we got small clinical trials. When you've got 90 year olds in a congregate setting facing a 50% chance of death, maybe it's time to stop pretending thalidomide may be lurking around every corner. The pediatric trials were just as bad. Due to their sizing it was statistically impossible to detect rare adverse effects. Yet, vaccination was delayed for children while these fruitless trials ran.

In my own experience I had a low cost, high throughput covid testing protocol ready to go in early April 2020. It took the FDA until August 2020 to provide templates and another month to grant emergency use authorization. We could've drastically ramped up testing when it was needed most of the FDA has treated an emergency like an emergency.


Is it your opinion that trials for the Covid vaccine should have been skipped to vaccinate people earlier, or that proper trials should have actually been done to know the efficacy and safety before testing it on the public?


Either would've been preferable to what was done. Waiting on a provably fruitless trial in the midst of pandemic is regulatory homicide.

Throughout 2020, more than 9% of all people in nursing homes died of covid. Depending on age case fatality rates were upwards of 50%. The vaccine should've been offered to these people on a compassionate use basis. Even at the time it was obvious that actual harm posed by the virus vastly outweighed any hypothetical risk of adverse vaccine reaction. Drastically expanding the vaccinated population through compassionate use would have rapidly provided efficacy and safety data.


> Throughout 2020, more than 9% of all people in nursing homes died of covid. Depending on age case fatality rates were upwards of 50%.

That's just about most difficult population to determine primary cause of death for. Most people in nursing homes have multiple comorbidities and a long list of medications. Its easy enough to know when someone died with Covid, its much more difficult (if not impossible) to know after the fact whether that's what caused their death or if the infection began after an existing condition worsened and weakened their immune system further.

> Drastically expanding the vaccinated population through compassionate use would have rapidly provided efficacy and safety data.

That wouldn't have helped get efficacy or safety data for the general public though. Vaccinating that population could absolutely have helped determine efficacy for that population and I agree it feels like a reasonable action given the potential risks for that population, but the data wouldn't be useful for the general public that are younger and/or in better health prior to infection.


> That's just about most difficult population to determine primary cause of death for.

Nursing home quality, COVID-19 deaths, and excess mortality https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8776351/

At the peak, excess nursing home mortality was nearly 6000 per week. Quibbling about "died with covid" versus "died of covid" isn't a useful exercise. Dead is dead and the excess mortality came from somewhere.


> Quibbling about "died with covid" versus "died of covid" isn't a useful exercise.

It isn't quibbling when the specific topic is whether or not to treat a population with an untested vaccine (assuming the trials were skipped for at risk populations as proposed above).

In a general sense, I totally agree the "with" versus "of" debate isn't useful. But when considering giving an at risk population an untested vaccine, how is that not important? Any intervention could have downsides, and more importantly an preventative intervention for a secondary infection may not be worth the risk depending on the risk profiles.

One tricky question that would have to be answered is whether the excess deaths were related to changes in nursing home treatment and general conditions. Nursing homes were effectively locked down in many areas, reducing human contact and potentially negatively impacting care. Vaccines would have no impact there, and if the untested vaccine has negative side effects we would have only made things worse.


Vaccine risks tend to be very quickly detectable. The phase three trial timing was driven by needing enough infections and there weren't enough.


Totally fair, by far the most common vaccine issues show up soon after injection. There is still the population challenge though. Dealing specifically with patients with multiple comorbidities and prescriptions would make it pretty tricky to recognize and then isolate the risk factors of anything that does show up.

Strokes, heart attacks, circulatory issues, etc are likely pretty common in that population and any increase there after treatment may go unnoticed as a change. If you do recognize it they'd have to stop treatments entirely as you wouldn't know whether its a risk to everyone or specific to some combination of age, comorbidities, and/or other medications.


The nursing homes were charnal houses. You would need one hell of a stroke risk to make the vaccine not worth it. The andrenovirus vector clotting was fast appearing and rare enough continuing was worth it in elderly populations.


People in nursing homes died from untreated illness. They were completely locked down, and isolated from friends and family. They weren't allowed to be transported to actual hospitals. Anyone with simple bacterial pneumonia was left to die.

In the UK, nursing homes were discovered to be sedating patients and not administering water and nutrition. I wouldn't be surprised to learn the same happened in the US.


If something would've gone wrong with rushing the vaccine like that it would've given the anti-vax people a massive boost and the vaccine refusal rates would've skyrocketed.

The refusal rates were already too high with anti-vax people making up lies/distorting data. If they actually had real data things would've been much worse.


> If something would've gone wrong

Anti-vaxxers simply don't care about truth vs. falsehoods. They don't care about the actual 3-phase clinical trial with tens of thousands of participants.


How about telling the public the truth? Say something like, "This particular vaccine has not been tested up to normal FDA standards. It may not be as safe as other vaccines. But we are convinced that it will do more good than harm, given the danger of Covid for the unvaccinated."

You could let the public make an actual decision based on actual information, rather than telling them little, projecting false certainty, and then trying to force them to do what you think is the best course. I mean, look, not everyone can be treated like adults. But I think the majority of people can. Tell them the truth, and let them decide.


You're not thinking it through. Lets say that vaccine ends up killing thousands of people.

That event will then be used in a way that is wildly out of context as fodder by all the anti-vaxxers out there to scare people into not getting vaccinated later when the vaccine is safer.

For the next 50 years anti-vaxxers and scammers will be using that event to scare people about vaccines.

It is not worth the risk because of the potential outcomes.


It sure sounds like you're coming at this with your mind already set that (a) there is some meaningful number of people that are entirely anti-vaccines and (b) that they are absolutely wrong.

If a vaccine is rolled out and kills thousands, the example you gave, why shouldn't some people take notice of that and be concerned? Is there no level of risk that would also make you consider not taking a new and untested, or under tested, vaccine?


That is why we should never allow a procedure that will roll out a vaccine that will kill thousands. Which we didn't do with Covid because the backlash that would create against ALL vaccines would be terrible and result in massive loss of life long term.


How do we define an acceptable refusal rate? The vaccines were largely untested and given under emergency use authorization. Shouldn't it be reasonable for people to choose for themselves whether to take part in the vaccine campaign or not, especially when we can't provide solid data to support safety or efficacy?

At the end of the day, in my opinion, there is no magic number for vaccine acceptance that is a metric to define beforehand. Refusal rates are a backward looking metric only and simply reflect the willingness to participate and trust in the general public.


How many doses would we need to give out to not call them "largely untested"?

Far more covid vaccines were given out to more people then almost all prescription medications have been. They were FDA approved officially in 2021, and at the end of the day all of the covid vaccines given an EUA were much safer than even mundane things like driving a car.

High vaccine uptake rates save lives. Pretending otherwise requires you to misrepresent the data.


Are you member of the Pharma Mafia, or just pested with religious idiocy?


It's not religious to recognize that medical advances, especially in pharmaceuticals, have done more to extend lifespans and save lives in the last 100+ years than anything else.

The pharma industry has been consistently producing what would easily be called life saving miracles in any other context. Anyone unable to see that is the biased one.


Ignoring the VAERS data is not religious?


That isn't real data. Anyone can write anything on VAERS. There is no verification. People write crazy stuff like the vaccine turned them into the hulk.

But lets be real, you almost certainly already know that. So you very likely fall into the category of people who intentionally misrepresent the data so you can pretend that vaccines are a bad thing.


That is the same blabla I read from many of your brothers in faith. Up to 2019, there are some studies that clearly show that the VAERS data underestimates the bad side effects of (some) vaccines, up to a factor of 100.

Of course it is possible that the highly political, near-religious atmosphere during the Covid-Circus biased the reporting for the mRNA vaccines in the other direction. But this has to be objectively studied. That never happened. One of the many things that make me deeply distrust the mRNA vaccines.

Your very general statement "so you can pretend that vaccines are a bad thing" shows your propaganda. I am vaccinated against several pathogens. But the topic "immune system" is really complicated, the knowledge up to date is not sufficient to force people. Especially vaccination of children has to be thoroughly justified. Search on Google Scholar for "Peter Aabye".


>Up to 2019, there are some studies that clearly show that the VAERS data underestimates the bad side effects of (some) vaccines, up to a factor of 100.

You mean before vaccines became extremely politicized? I think we can safely assume those numbers aren't useful anymore now that the well has been poisoned.

>But this has to be objectively studied.

There were plenty of double blind studies on the covid vaccines. Those are the gold standard. I'm not even sure what you are asking for here.


What? The numbers from before the poisening are not useful, because of the poisoning?

I asked for studies on the reliability of VAERS data about the Covid vaccines.

RCTs are just one brick of the science building. And of the plenty you think exist, I have encountered only a few good ones, yet. The Cleveland Clincs study is one of them, but they justctested for infection and didn't include the outcome all-cause mortality or hospitalization for some unknown reasons. The US veterans study seems to prove a lower mortality for vaccinated, but the cohort is for sure not representative. Btw, those two showed a clearly monotonic increasing probability of acquiring a Covid19 infection with number of vaccinations.

RCT fanatism is not helpful.


Something did go wrong; of the 3 vaccines the FDA approved, 1 of them had to be recalled due to causing fatal blood clots.


Which effected almost no one, yet here you are talking about it. Imagine if an early covid vaccine had killed thousands. That would have had a massive chilling effect on vaccine uptake.


> Which effected almost no one, yet here you are talking about it. So you think the FDA was wrong to recall it? And yes, I'm talking about it because plenty of people were skeptical of the vaccines because they thought they were undertested. And given the recall, they were absolutely right.

> Imagine if an early covid vaccine had killed thousands. That would have had a massive chilling effect on vaccine uptake. You're making it sound like the chilling effect would be a bad thing, when it would actually be the correct response. There are plenty of examples in the history of medicine of the cure being worse than the disease.


Over 18 million doses of the J&J vaccine were given out. 6 women died. I don't think you could ever have testing to catch such a low rejection rate, and that rate is less dangerous than actual covid was, so those people weren't "right". Also that rate is less dangerous than driving a car, so this whole thing is silly.

We had safer vaccines available though so switching to them is even better, which we did.

> You're making it sound like the chilling effect would be a bad thing, when it would actually be the correct response.

That chilling effect would still exist when the vaccine was safe, making it the incorrect response. Conversations like this make it very clear why we need to be very careful about vaccine safety and we should never release a vaccine that will kill thousands EVEN if that vaccine would save lives overall.


> Still, the FDA approved it.

The FDA approved it via accelerated approval. The intent being "allow access to promising medicine while additional data is collected".


Remember the pandemic? The FDA had safety and effectiveness data by end of August for the vaccine and were unprepared to do an analysis in less than a few months. Nor did they consider drafting the party boys of the Ozarks to get the efficiency data faster. As a result the winter of 2020-2021 saw thousands of preventable deaths.

There's also the part where distribution was done in a way that deliberately killed people so that racial equality goals could be met. Perhaps the worst example of this kind of thinking were teachers in SF getting vaccinated but school not starting again.


"The FDA (and EMA in Europe) are the only thing that protects desperate patients from fraudsters, charlatans and pharma-companies just looking for a return on their investment."

EMA has some people that were recruited from Big Pharma.


Yes, the system works, and we have very little poison being sold as medicine.

The issue is that with some illnesses/stages, we do not have a good treatment, and a lot of people would like the calculus to be different. We do have compassionate drug rules, but they're a pain for many people.

I'm not in that situation, and not sure how I'd react; but I can see how, having an incurable illness, with tons of suffering or a few months left to live, I might want to try everything. Hydroxychloroquine, Chinese acupuncture, herbal remedies, and experimental treatments.


True for _all_ 'safety stuff.' However, safety requirements for late-stage patients with very few other options ought to differ from safety requirements for mass adoption.


>However, safety requirements for late-stage patients with very few other options ought to differ from safety requirements for mass adoption.

Do they not already?


They already do.


Why is it that so many people need to die in the name of safety?


Because nobody's counting deaths from "not doing stuff". Everybody counts deaths from actions done (things built, products sold, meds taken) but nobody's counting losses from things (like meds) simply missing.

In effect we regulated doing stuff so much in the name of safety that we ended up in an infinite "analysis paralysis" mode where the you have to absolutely prove zero harm from new products/services while completely ignoring the harm the current status quo does.

See current debates over AI, self-driving cars, and of course, meds.


What do you mean "nobody's counting"? Excess mortality from delayed or denied treatments are measured all the time in medical research. How do you think these drugs get made in the first place? We just had a pandemic where a calculated decision was made that the small risk of myocarditis was massively outweighed by the benefits of mass vaccination. When was the last time you saw a drug ad that didn't list potentially fatal or debilitating side effects? "We need something to solve problem X even if it carries risk Y" is absolutely par for the course.


Because you can't honestly presume to know the outcome of a clinical trial of an untested product.


You've proposed a nonsensical epistemic framework. Knowing isn't binary.

You should have a probability distribution over possibilities, based on your experience with similar drugs, expert hunches and animal trials. You then use that to estimate risks and benefits. Then compare this risk-reward profile with the risks of doing nothing -- in this case, near certain death from brain cancer.

This "can't presume to know" framework is just sophistry. And I think deep down you know that, if you had a death sentence from brain cancer you'd be begging them to let you in the trial even if they "couldn't presume to know".


Maybe the person calling the FDA "nonsensical" should be someone who has actually researched, manufactured, and sold a pharmaceutical product, not some rando on HN. People who dismiss patient safety cannot be taken seriously in my worldview - which thankfully every developed country's regulatory body shares.


You’re missing that we have treatments with known risk/benefits vs research treatment X with undefined risk and reward.

It’s extremely challenging if not impossible to obtain informed consent in this situation.

We’ve been through this before where a fancy new treatment with promising early/lab results usurped conventional therapy only to later be found inferior.

Earlier TKIs and NSCLC are a recent example that comes to mind.


It's not undefined, though. That's the point I'm getting at. There is no binary of known and unknown. A tentative picture exists based on animal trials and expert judgment. That tentative picture informs an estimation of the risk to reward profile which is then the basis for an informed decision.

This is decision making under uncertainty. It's bad practice to say that uncertainty always means "don't do it".


Its absolutely ridiculous the level of arrogance to presume you can apply some debate-bro logic and talk your way out of NOT HAVING ANY DATA. NOT HAVING ANY DATA means your product fails. End of story, thanks for playing, nice try, go back to level one and try again. NOT HAVING ANY DATA means we deny you authorization to inject our babies with untested vaccines.


So run the clinical trial, advertise the product as untested and dangerous-to-lethal in the meantime, and let people make their own choices?


Smoking is already advertised as dangerous-to-lethal and look how effective it is in preventing people from smoking.

In huge oversimplification some crazy or fraudulent people will claim it cures blindness or cold sores, some other people will believe them and will have to deal with the real danger-to-lethal consequences, with the rest of society paying for their medical care afterwards.


> Smoking is already advertised as dangerous-to-lethal and look how effective it is in preventing people from smoking.

Pretty effective.

In Australia throwing a few diseased lungs on the packs and increasing public awareness has seen usage drop from 35% of the population in 1980 to 11% today.

Not all the drop is purely related to advertising, price increases and restricting sale to out of sight locked access in shops have also helped.

https://www.tobaccoinaustralia.org.au/chapter-1-prevalence/1...


Sure it's effective if you're looking at the reduction rate of existing number alone. But reverse the problem and the very big effort of warning about dangerous-to-lethal stuff still doesn't stop 11% of people from doing so. That's quite bad, when you think about going from zero (you can't willy-nilly use untested medicine) to 11% of the society.


> Sure it's effective if you're looking at the reduction rate of existing number alone.

That's exactly correct bart, it reduced smoking by over two thirds and kept it that way.

> still doesn't stop 11% of people from doing so.

Like seatbelts, vaccines, and all other health and safety procedures that also don't have a 100% total absolute success rate .. nor never claimed to.

Who wants to wrap people in bubble wrap and lock them away from the world? Are you advocating for that?


From another perspective it took massive change in generations and over 40 years of campaigning and it is still a problem for the 11 percent.


Knocking back smoking by two thirds has saved billions for the national health system.

On the books, totally worth it.


And cost billions in state pensions. I'm not suggesting that's any sort of counterargument but the costs should possibly be offset against other types of end-of-life care.


It's been discussed. The balance has so far fallen on the side of anti smoking policy.

Australia is a democracy with many small parties and several quasi independant larger party (three main large parties) members, there's been scope for almost anyone to campaign to repeal anti-smoking policy by either running directly or by lobbying their local of federal rep.

People have campaigned for hunting, for cannabis, for many things .. so far no one, to my knowledge, has campaigned to repeal the anti smoking policies.


Sure, but imagine doing the same effort that likely requires critical mass for actual adaption on small obscure medicines and illnesses.


Are they addictive? Then regulate them as addictive drugs.

Are they not addictive? Then it seems a stretch to compare them to cigarettes.


I have a new drug. It's called aceite deserpiente.

It's a cure for lyme disease, impotence, ALS, chronic fatigue, cancer and aging. Trials are pending but what are you waiting for, do you want to die for lack of trying? 10k/dose.


> aceite deserpiente

Nice name choice for your example; I was thinking of paracetamoxyfrusebendroneomycin myself, yours is better.


See, the thing is, I can just choose not to buy it.


Would you know not to?

My mum bought into a lot of homeopathy and Bach flower remedies. Thought she was doing me and dad a favour by getting both, and even "secretly" gave dad doses of the latter (and I was a kid so didn't have much say), so I was fortunate both categories were basically nothing.

But her and dad?

One of the Bach flower remedies was "for memory"… she got Alzheimer's about 20 years younger than her mother.

When my dad was dying of cancer, there was some mineral he thought he was short of (magnesium?), and he didn't realise the homeopathic pills labelled "magnesium" didn't actually contain any magnesium.


Sure, but look at homeopathy. It's like a virus - you don't optimize for killing the user, because a dead user can't buy more meds, and also you might get sued. Instead you optimize for having as purely placebo an effect as you can. (It's also cheaper.) For that reason, I suspect the scam market is already saturated. Will some people get scammed into taking dangerous chemicals? Sure, but that's already the case cause those aren't regulated as medications.

IMO, prevent use of addictive ingredients, but beyond that inform, don't forbid.


I see where you're going with that, but history has demonstrated widespread use of substances where the risks were long-term and/or mild and so the selection pressure you describe wasn't sufficiently fast-acting, some of which are now regulated or banned, and others are still widely available — off the top of my head: Radium paint; Victorian-era cosmetics containing lead, mercury, arsenic, etc.; alcohol and nicotine in general; atomic explosion testing as tourist attractions; indoor wood fires to make places seem more cozy; electrolytic foot spas; ionic bracelets; asbestos.


Several of these involve housing. IMO it makes sense to regulate safety in the housing market because the housing market is broken - I would not be surprised if at least in some cities, complete knowledge of the consequences of asbestos in the walls wasn't a deterrent even if the renter was fully rational. With those that don't, I think full information and personal responsibility is still the best approach. Do you want the cancer creme or the non-cancer creme?

That said, I think we would get most of the benefit of regulation if we just required an advisory consultation with your GP before you could buy a product whose safety wasn't established. A lot of the danger of overregulation rests on trivial inconvenience vs outlawing experimentation, and I think something like that could split both groups. "Yes, I want to enable experimental mode on my body."


This already happens, it's called 'compassionate use'

https://www.ema.europa.eu/en/human-regulatory-overview/resea...


I mean, if you have an aggressively terminal disease with no known cure, I think the risk-reward calculus is somewhat different from the average drug

The issue, as comes up incessantly in all manner of situations, is the way we regulate drugs as a whole. A lack of safety testing should mean a higher standard of informed consent should be used, not that it should be illegal for someone to get ahold of it

I see lots of benefit to regulatory agencies controlling what claims can be made about medications and holding people selling them to account for quality control failures. Agencies preventing consenting adults from making their own risk-reward calculations does badly on both principle and outcomes


While I agree that my calculation on safety would be different for a terminal illness for which no cure exists, we still need to be careful. The very nature of this situation creates desperate people who are willing to ignore a simple warning label in favour of hope.

Any system / regulator still needs to force companies to prove their treatment has the claimed effect, and block any that simply don't. On safety, I think there's more wiggle room, however. Treatment here can be based on likely ill effects vs the known effects of the illness of the patient.


Nah, I actually think the effectiveness standard is far worse than the safety standard due to what a "block" means and how "effectiveness" is tested.

An RCT, the gold standard by which medicines are often tested, can easily show a negligible effect size because of the vast confound space of individual differences. A medicine that works perfectly for many of a study's participants will be considered "ineffective" routinely

And hey, in cases like that I think the regulators should absolutely have the power to say "selling this without explaining these caveats is criminal fraud", but not that people can't try the drug anyway if informed of the risks and low likelihood of success as determined by the agency's analysis

In an effort to standardize process and appease large incumbent industry players (often, as here, by erecting enormous entry barriers in front of lucrative markets), we frequently create metrics that are too blunt and remedies that favor governments flexing disproportionate power over the lives and choices of individuals


I think this risks creating a perverse incentive where actually creating a cure is hard but looking like you maybe, sometimes, if you squint just right, cure the illness is easy. So companies start to ignore those hard cures in favour of sugar pills with warning labels on.


You can already do that though. There's a massive essentially unregulated market full of "supplements" and "alternative medicine" and "faith healing" you can play in if you're dedicated to the business of scamming people who don't look at claims skeptically, including but not limited to people who have terminal diseases. This regulatory process does absolutely nothing to prevent that. However, due to the broad authority of agencies like the FDA and DEA to outlaw drugs that demonstrably do something, we are left with a situation where most of what gets shut down is actual useful medicine


There’s a big difference between a black market existing and the government throwing its hands up and saying “let’s just legalise it!”

Weak regulation that allows non-medical products to masquerade as medicine is not the same as “nothing can be done.” Things absolutely can be done.


These aren't black markets, and they're frankly not regulation failures either. Regulatory bodies serve an important role in creating a standard people can rely on for claims that things work as medicine. They should not serve the role of making it so that people can't get their hands on things at all if the regulatory body doesn't deem them effective. If a person can see that a treatment is not FDA-approved and decides to try it anyway, the FDA's hands are clean. The failure is that if someone tries and fails to get their treatment approved, it's often more illegal to sell it than if they just claimed it worked without trying to go through the proper channels

This situation is made even worse by the Controlled Substances Act and the Analogue Act, which not only artificially restrict both supply and access to a ton of effective medications, but also create this onerous donuthole where a substance can be shown to be effective enough to warrant criminalization, but not pass the rigorous standards to be approved as medicine. It would be a lot better for everyone but enormous pharmaceutical monopolies and police states if we kept regulatory bodies' role to quality control, an official standard by which medical claims could be judged as a guide for laypeople, and fraud prevention.


> If a person can see that a treatment is not FDA-approved and decides to try it anyway, the FDA's hands are clean. The failure is that if someone tries and fails to get their treatment approved, it's often more illegal to sell it than if they just claimed it worked without trying to go through the proper channels.

This is a regulation failure because a good regulatory framework shouldn’t allow this at all. It’s not about whether “the FDA’s hands are clean,” it’s about what system should be in place that gets us to the outcome we want. In my mind, this would be a place where ineffective treatments aren’t allowed (because why should they be?), but safety/efficacy is then traded off against what the patient needs.

Coming from outside the USA, it sounds to me like the regulatory system isn’t achieving any of that? I think I agree with the broad thrust of what you’re putting forward, my issue only comes with the “guide” part. Medical experts need to be the ones leading the treatment because… well… they’re the experts.

Don’t get me wrong, I can see how Americans distrust government after having a president suggest drinking bleach during Covid might work live on TV.


I'm not even sure how you want this to work. Like in your ideal model, does this mean you can't go buy bleach?


No because bleach is a cleaning product and it works. But I don’t want a pharmacy advertising sugar pills as being able to cure anything outside of your sweet tooth. Obviously this is an extreme example (I’m sure even the USA doesn’t allow sugar pills to be sold as actual medicine) but I’m taking from this thread that there are ineffective medicines being sold but potentially useful medicines being blocked. Maybe I’m wrong, I don’t live in the US.


Right, regulatory agencies should absolutely resolve false advertising disputes, and the FDA is well-positioned to assess claims about medicinal efficacy. I don't think it should be able to prevent people from voluntarily accessing experimental treatments they can't verify, knowing the risks of doing that, which they currently do


> What do you mean by slowness? They can't skip all the safety stuff!

One can be fast and safe, it's just that requires spending a lot of money.

It's analogous to cache prefetching and branch prediction in CPUs, except the cost of bad predictions is measured in millions of dollars rather than tens of CPU cycles, and also that the predictions are much harder.


You seem to imply that the only possible source of slowness if safety, which might not be the case (I've no idea).


Not that it should matter, but they are also VERY expensive. There is a new standard for NCPDP (how pharmacies and payers send transactions for payment) coming out in the next few years called F6. One of the big changes over the current standard is drugs that cost more than $1M can be processed in a single transaction. https://www.cms.gov/files/document/fact-sheet-11-2022.pdf


Sounds effective, I've always had a hunch the real path to controlling cancer is not a singular approach. Cancer mutates too much.

>> “Instead of us injecting single particles, we’re injecting clusters of particles that are wrapping around each other like onions, like a bag full of onions,” said Elias Sayour, MD, PhD, a UF Health pediatric oncologist who pioneered the new vaccine. “And the reason we’ve done that in the context of cancer is these clusters alert the immune system in a much more profound way than single particles would.” Results from the canine trial showed how the vaccine reprogrammed the tumor microenvironment (TME) within days, allowing the activated immune system cells to fight the tumor.

https://www.cell.com/cell/abstract/S0092-8674(24)00398-2


When COVID hit one of the few positives was that a lot of people joined in cross-discipline research to address it. This type of treatment sounds amazing, and I know mRNA vaccines were in development for a long time before COVID, but I have to wonder if this research would have taken a lot longer to happen had COVID not happened. What other secondary impacts has the research into COVID had?


That reminds me of a piece about the "source code" of one of the mRNA vaccines [0], which had an amusing bit showcasing how one kind of pre-pandemic research was hugely important in preparing the necessary tools for when they were needed:

> It turns out that, unmodified, freestanding Spike proteins collapse into a different structure. If injected as a vaccine, this would indeed cause our bodies to develop immunity... but only against the collapsed spike protein.

> And the real SARS-CoV-2 shows up with the spiky Spike. The vaccine would not work very well in that case.

> So what to do? In 2017 it was described how putting a double Proline substitution in just the right place would make the SARS-CoV-1 and MERS S proteins take up their ‘pre-fusion’ configuration, even without being part of the whole virus. This works because Proline is a very rigid amino acid. It acts as a kind of splint, stabilising the protein in the state we need to show to the immune system.

> The people that discovered this should be walking around high-fiving themselves incessantly. Unbearable amounts of smugness should be emanating from them. And it would all be well deserved.

[0] https://berthub.eu/articles/posts/reverse-engineering-source...


MRNA's for aggressive cancers are going to do some amazing things. This is one example of "death sentence" cancer being stopped cold. To that end, the trade offs for MRNA's make complete sense. It's a great place to do long terms studies and see what happens down stream.

What covid did prove out is that there IS risk. https://www.health.gov.au/our-work/covid-19-vaccines/advice-...

Biologics (what vaccines are) are weird. The FDA should be stepping back from restricting the use of these on INFORMED patients who have limited other choices and mandating the long term study that we need for this class of treatments. IF were extending peoples lives and finding those secondary a tertiary risks in patents who would have otherwise died we will all benefit in the long run.

Between Pro and Anti vax camps it is dam near impossible to have a rational conversation about the topic. One more thing that has been polarized into the abyss... sigh!


The AstraZeneca vaccine mentioned in your link is not mRNA based.


> What covid did prove out is that there IS risk.

Not an mRNA vaccine and vaccine risk regardless of vaccine type was known and acknowledged for many decades before COVID.


We had a nice discussion here, you had your arguments, got the few mistakes pointed out, all factual, civilized and nice. Nobody called you sheep, antiamerican, or puppet of the global government. So let's not bring the anti-vax "polarization" into this, because the two camps are simply not the same. Edit: I have yet to see such a rational discussion with an anti-vax. Won't say it cannot happen, but to me it's like bigfoot.


If the were able to have that kind of discussion with you on the pros and cons of vaccines, would you still perceive them as antivax?


Interesting point! Anti vaccines yes obviously, but I wouldn't call them "antivax" (anymore) as it seems I reserved in my mind that name for the wild mob - for better or for worse. Because there's no good thing without downsides and discussing downsides is just as important, regardless how one prioritizes them. We are all different organisms and what works for one won't necessarily work the same for the other, and we need solutions for all.


Thing is that people used to label you as anti vax during that time period even when you thought vaccines as a whole were a good thing, but in certain situations they did more damage and in other situations it was possible that risks vs benefits calculation wasn't clear.


That's because the anti-vax people are sometimes an actual threat to other people's lives.

Especially during the pandemic every argument was had ad nauseam and a (similarity to) certain narrative wasn't perceived as coming from good faith anymore. People were tired of explaining the difference between DNA and RNA, between relative risks of the vaccines and infection, herd immunity, ... . At some point you never knew, if the person you are debating will go full conspiracy nut. Even genuinely skeptical people were often worried because of opportunistic clout chasers were spreading misinformation.

See the comment above where the AstraZeneca vaccine got conflated with mRNA vaccines. Bad start...

There were no vaccination mandates. However, "anti-vaxxers" were offended people decided to keep them out of their groups, shops, communities, ... by vaccination status. They want to have the cake and eat it too. Their idea of discrimination is overreaching and entitled.


> There were no vaccination mandates.

"Get the vaccine or lose your job" absolutely is a mandate. This really was a thing.


A private de facto "mandate", not a governmental one.

Well, yes, that's what I was getting at: Freedom cuts both ways here. If you choose to not get vaccinated, others should be allowed to, at the very least, choose not to have you around. Immunity is not a private belief, but has severe, sometimes existential implications for other people.

I assume, it's pretty much the same with guns in the US. You are allowed to own them, carry them, but not allowed to bring them everywhere, if someone's ruling within private jurisdiction forbids it.


> not a governmental one.

Only because it was struck down by courts. The US government did attempt it, and even told employers to abide by it while they appealed (before it was struck down again).


Can you link me a source?



I didn't know that. Thanks. This does in fact invalidate my point above.


> This type of treatment sounds amazing, and I know mRNA vaccines were in development for a long time before COVID, but I have to wonder if this research would have taken a lot longer to happen had COVID not happened.

At least BioNTech was able to take the billions they made from pivoting into COVID vaccines and use the money to speed up their cancer-related pipelines. Running clinical studies is expensive and difficult to do if you have to beg for money for an unproven platform.


My SO's PI died of Glioblastoma a few years ago, completely derailing their career path, halting all research, and leaving behind a grieving and struggling family. It's difficult to picture how my life would be different had this treatment been available.


My dad died from that also, luckily for me, I was still in middle school and it had almost no impact on my career path. It's difficult to picture how my life would be different had this treatment been available.


What's "PI"?



> completely derailing their career path, halting all research

That's a real odd way to characterize a person's death.


I don't think they meant it in a negative way. The last line makes me think they mean it in a sort of self-reflective butterfly effect way.

Similar to how anyone might reflect on how the death of a relative or friend ultimately led them to being the person they are now in some way.


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My point is that text doesn't necessarily convey how they meant it. Their experience of the advisor's passing was indirect, so it isn't all that crazy that what stands out to them is how it affected their SO and the obvious effect it'd have had on the advisor's family.


That's because I'm me and not anyone else. It was pretty traumatic for my SO and everyone else around the PI. The PI insisted on going into work and continuing on like nothing changed even as they were mentally deteriorating. If I don't include details about the tragedy it might be because I don't want to bring that energy to my comment and not because I somehow was oblivious to their significance.


There was nothing at all wrong with your comment.


Detailing the impact a death has on the surrounding family and person's work as a personal account is fine. Your criticism is what's weird here.


Why are you being so dramatic? Life is short, let it go


Read the sentence again, more slowly this time.


It’s still odd to characterize a person’s death in terms of someone else’s career progression. Probably because it’s uncommon to see a death characterized by it’s second order effects. Usually it’s the family or friends and it’s more personal. OP didn’t say anything wrong though.


> It’s still odd to characterize a person’s death in terms of someone else’s career progression.

OP even went another level, since it was their SO's career progression that was affected, thus affecting OP. Agreed, they're not wrong, but it was odd.


They’re not wrong in the sense they’re factually correct: OP’s life would have been different had a cure been available. But if OP’s SO approached her PI on their deathbed and said “Dear PI, what about my SO?” They’d probably be met with incredulity.


Well it is a good thing that nothing like that happened then, isn’t it?


PI = ?


Principal investigator. It’s what phd students call their academic advisor/boss during graduate school


Probably Principal Investigator. I'd guess the "SO" is a PhD student and now his/her program is up in the air.


Significant Other.


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Which is OK when talking about oneself and your experience.


Not really, we humans put death of others generally way above career of others, even if closer.

There is this thing called emotional intelligence which branches into many things and situations, and can't be learned even though I've seen a lot of folks performing imitation very well, till something novel comes around and it all falls apart.


I simply disagree and don't think it is reasonable to try to police everyone's speech.

I think using death as an opportunity to lecture others is far worse than providing an insightful common about it's impacts.


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One can grieve for the loss of a persons life while grieve for the impact of that loss on your own. The person who died is literally dead and as such entirely insensate to such things. However the people who depended on them - their family, as they also noted, as well as people whose livelihood depended on them, are all also affected by their death in a profound way. The impact on their life cascades on indefinitely, perhaps even generationally. The person who died is surely missed - but when someone upon whom many people depend dies that dependency can cause grief well beyond the loss of a loved one or friend.


> leaving behind a grieving and struggling family

For these words, I assume they were talking about the PI's family. The rest I assume they were illustrating how these deaths affect far more people than just the families of the ones lost to cancer.


Deaths CAN be a great inconvenience, and nobody implied choice but you. It sucks when people die, and impacts can vary with connection.

It is more honest to the dead to honor and state your real loss. A dead human can be both a loved one and teacher to different people, depending on the connection. This person didn't lose a lover, they lost a teacher, and that matters too.

You don't even need to have liked someone to have lost something when they die


As we see more and more promising therapies like this, that are essentially custom fit to the patient, it makes me all the more worried about the US health care systems. A treatment like this will be expensive, which in the long run means that we'll have a society where people with money won't have cancer (or at least will have a less deadly version), while the people without money will not. We'll be converting cancer to a problem of poverty. None of this is to say that we shouldn't pursue these advancements, but rather we should start thinking about how we can change our system to ensure that every member of our society has equal access to medicine.


> We'll be converting cancer to a problem of poverty.

Outcomes are already disparate.

” People in low- and middle-income counties in the United States are more likely to die of cancer than those who live in high-income counties. Eight factors, including lack of access to high-quality clinical care, food insecurity, smoking, and obesity may explain more than 80% of the relationship between poverty and disparities in cancer death rates at the county level, according to a new study.”

And

” In low-income counties, the average cancer death rate in 2014 was 230 per 100,000 people, compared with 205 per 100,000 in middle-income counties and 186 per 100,000 in high-income counties.”

—- https://www.cancer.gov/news-events/cancer-currents-blog/2018...


In Canada, despite free healthcare, some of this comes down to how much personal research you do and how hard you advocate in order to be treated at a high-skill facility.

It is still an SES game, because higher levels of education (correlated with income) allows individuals to see beyond “well the doctor told me, so that’s what I’ll do”. Higher SES also comes with the ability for a more flexible work schedule, and the ability to travel to larger city centres where the high-skill care is more likely to be.


>we should start thinking about how we can change our system to ensure that every member of our society has equal access to medicine.

I dont think that is a healthy or reasonable goal, in the US or anywhere. Some care is labor intensive and costly, and simply not scalable to everyone. It is possible that time helps reduce the burden.

The only way to have equal care is to eliminate high end care.


> The only way to have equal care is to eliminate high end care.

That's one way to think of it. But you also can just say: the only way to have equal care is to raise the standard of all care to the quality of high end care. That's worth trying to achieve even if it's not logically perfect. Most things in life aren't but trying to get there is still a "reasonable goal". It's just about priorities.

The elephant in the room is also access to preventative care. Many people wait until the last possible moment to seek medical care because they can't afford otherwise, or do not have access to local medical facilities. Improving access to preventative medicine and care, which is often cheaper and more simple than cutting-edge procedures, would lower the overall demand on last-minute medical infrastructure, like an ER or hospital, which is often what people think of when someone says "access to medicine". An excellent example of this is Costa Rica, where much more effort is spent on access to preventative medicine and all of the infrastructure required for that. As a result, Costa Rica's health care system rates higher than the US while also spending 1/10th per capita on healthcare.

A lot of the healthcare system in America is just what we've ended up with, often as a result of greed and a relatively recent extreme distrust of public options, rather than some sort of clear eyed logical end point of healthcare rationalization. Improving access to medicine and raising the over standard of universal care is still a goal worth trying to achieve.


I agree it makes financial sense to provide universal access to preventative care and basic (read cheap) healthcare.

I think it is counter-productive in addition to being logically irrational to focus on equal access to high end care. It isn't possible and it poisons the well for meaningful change. Not everyone should have access to 10 million dollar care on the social dime. There is no upper limit on possible costs, so actively seeking equality just means banning higher care for those who can afford it.

I dont think that the US outcome is the result of greed. companies are just as greedy in costa rica or eurpoe. Rather, US healthcare costs are the result of illogical and schizophrenic policy choices, with incompatible choices that dont work together. I could rant for hours about what those are, if you are interested. At the end, it is like a crowdsourced car that doesnt work. Someone picked a porche engine, and someone else picked bicycle tires, and someone else picked a tractor frame, so it doesnt work at all.


> That's one way to think of it. But you also can just say: the only way to have equal care is to raise the standard of all care to the quality of high end care. That's worth trying to achieve even if it's not logically perfect. Most things in life aren't but trying to get there is still a "reasonable goal". It's just about priorities.

This is a good example of the common liberal fallacy of Utopianism.


Im not familiar with the concept. Is Utopianism the phenomenon of focusing on an a goal, without considering the cost of achieving it, and critically considering what it would realistically look like when they are achieved.


Ya that’s about right.

Utopianism is the quest to attain or implement an ideal society.


Capitalism and technology will make it cheaper over time, if we just let it. Africans without reliable electricity has magic pocket devices straight out of Star Trek. We can find a way to make personalized medicine dirt cheap too, but you can't force it through legislation.


Cancer being mostly a problem of poverty is still a substantial upgrade from being a problem that just kills all people with little to no mercy.


GBM is horrible.

At my first company, our VP of Sales, Luke Little, was one of my favorite people to hang with; I was still barely 20 and he was in his 40's but he had quite the mischievous twinkle in his eye and was willing to join us kids in tomfoolery and tell us about the world. We were acquired and got a great exit in July; he had a seizure driving the Cobra he bought to celebrate a few months later; he went downhill quickly and died within a couple of years. He had a young son, too.


> but the canine patients lived a median of 139 days, compared with a median survival of 30–60 days typical for dogs with the condition

so you might get an improvement in overall survival but not a cure for GBM


GBM median survival for humans (according to the article) is 15 months.

If the effect is linear, the boost to survival time in humans would be an additional 19 months. With the death sentence of GBM hanging over your future, an additional year-and-a-half is huge.


It is and it isn't. A year and a half would go by so quickly. But if it were a high-quality year and a half and not spent in a hospital ward, I guess it's better than the alternative.


It's highly non-linear, as you allude to.

For a mother with a young child, getting another 1.5 years can be the difference between the child not knowing their mother and having some memory of her.

For someone with no or adult children, it can be a lot less significant. My dad passed away from cancer when I was 30 and while I certainly would have taken an extra year with him, it wouldn't have changed much.


Nothing like a deadline to make the most of 18 months. I have a 4 and 6 year old and if I were in this situation I'd cherish the hell out of that time. And hope for further improvements in treatment (and a stroke of luck) in the meantime.


It is and it is. My dad died of a GBM in 2022, 17 months after his diagnosis. If he had had another 19 months, I'd have made him breakfast this morning.

I find it much easier to sympathize with people's desire for additional time with terminally-ill loved ones now.


How about we could let people make that decision for themselves?


I said nothing about making the decision for anyone else.


I'm in the camp of having 18months of non painful survival being a massive change, because it buys you time to wait for another therapy later.


You could say the same for 20 years, in the grand scheme of things.


I'm a bit more optimistic. The article specifically mentions that it is too soon to look at efficacy. There could have been a lot going on with these dogs that shortened their lives that was unrelated to the GBM. Optimizing the treatment for dosing, timing, etc and applying it sooner are likely to greatly improve its efficacy.


Very unlikely to be a cure for GBM, but there's often the hope that therapies can stack very well-- both from combined effect against disease and sometimes sensitizing the disease to other therapy. The dogs were not receiving the human standard of care treatment-- who knows what surgery, radiotherapy, immunotherapy, and chemotherapy can do combined.


The dogs were not humans with human cancer, so we shouldn't expect a clean translation of the results


Of course not, and the relevant xkcd, etc. Not our first rodeo here. It's going to take a long time to get gold standard proof that survival is augmented.

It's still exciting news. They're ramping up through phase 1 to phase 2 in humans, and already have evidence of similar immune response in human patients.


this requires individualized treatment based on the description which will make the implementation costly and impractical. They need to extract a piece of the tumor from the brain.


Surgical resection of glioblastoma is usually (not always) one of the first steps in treatment, so you get that "for free".

But yes, I would expect it to be quite costly.


yes but thats only the first step in this case. then they need to prepare the individualized mRNA shot from there. How long it takes and how complex it is is another question.


Yes, most of the promise of mRNA with cancer is the prospect for individualized therapy. But individualized therapy intrinsically means you're going to be a doing a patient-specific manufacturing step.

Sequencing and RNA synthesizing are widely available commercial services at this point, though not cheap.

There's a lot of magic to take mRNA and formulate it to last in the human body and go and do what you want, but it isn't likely to be the costly part of all of this if there's some small volume of people being treated this way.


If any treatment can extend the life of a patient up to 3 times (as was in the canines), that's significant. Some treatments only have a response efficacy of a few months, but you add a few of these together in sequence, and you build a year.


still does not change my conclusion. its a treatment, not a cure.


Yet


Indeed, you have ascertained the the article's topic— big progress in GBM research— and correctly distinguished it from a topic the article wasn't about.


Is there a good book about cancer for a layman? That can help them understand what exactly the disease is, it's variants and a list of potential strategies to beat the disease.


https://en.wikipedia.org/wiki/The_Emperor_of_All_Maladies

is a good overview of the history of radical surgery and chemotherapy, and the emergence of modern treatment to 2010


I found this book, which traces the surprisingly long and fascinating history of using immunotherapy to treat cancer up to the present day, well, fascinating:

The Breakthrough: Immunotherapy and the Race to Cure Cancer - Wikipedia https://en.wikipedia.org/wiki/The_Breakthrough:_Immunotherap...

My uncle died of a glioblastoma, and shortly after I read this book, I was myself diagnosed with cancer (treated conventionally, hopefully cured). Immunotherapies like mRNA vaccines seem to be our best hope for finding reliable, permanent cures for a lot of different cancers. I am sorry that for many of our loved ones, a cure will have come too late.


> the surprisingly long and fascinating history of using immunotherapy to treat cancer

Well yeah, it has been known for a long time that cancer can do what it does because of the immune system's failure to eliminate the "defective" cells. Also, there are the rare "spontaneous remissions" where, for some reason, the immune system eventually catches up and manages to destroy the cancer. So there have been many attempts to harness the immune system in cancer treatment. Glad to see that all that work is finally bearing fruit (fingers crossed)...


Not a book, but the Kurzgesagt series on cancer are a great start.

https://www.youtube.com/watch?v=zFhYJRqz_xk and https://www.youtube.com/watch?v=uoJwt9l-XhQ

Also while not about cancer specifically, the book Immune by the kurzgesagt founder Philipp Dettmer has a chapter on it and the relation to the immune system. Which is very relevant for these new immunotherapies.


”The Emperor of all Maladies” by Siddhartha Mukherjee is fantastic


Wikipedia is usually a pretty good starting point. In addition to summarized content, reference links should be available.


Wikipedia is a rabbit hole. It seems too wide.

I want someone that has already done comprehensive research to guide me on what I should be paying attention to.


The Emperor of all Maladies


This seems to be a much better application of a gene therapy shot of this kind that has such a small targeted scope. A virus that mutates would clearly be an exercise in playing constant catch-up, but this seems a lot more realistic.

Is there anything that works to replace the delivery system that's more reliable/predictable than the lipid-based carriers?


I'm glad they're testing this. A vaccine approach always has the risk of hitting healthy tissue as well with the immune response. And when that tissue is brain tissue...

Testing is necessary anyway to get insurance companies to pay for something. They like to deny coverage, and if the treatment is not proved to work that's an easy excuse.


This is an area where mRNA immunization can be very effective. I hope that this can be widely deployed in the next years, it can make a real difference. Something that also has great potential is the use of phages, that should definitely receive at least equal parallel research attention.


“To generate each vaccine RNA was first extracted from each patient’s own surgically removed tumor…”

Wait!? It can be any tumor right or do they have to open my skull and take a sample of the actual tumor they want to get rid of.


It has to be the same tumor


I guess you can wait for metastasis instead for easier access. /s


mRNA research is going to change medicine for the better.


It has that potential for sure, but I hope the people researching and developing these tools aren't that optimistic. We need to be skeptical until treatments are proven, going in optimistic for a field-changing breakthrough is a great way to misread the data or fail to design proper studies.


I'm confused and the term vaccine. My understanding was that a vaccine contains a deactivated virus. Is mRNA not a form of gene therapy? I understand not wanting to spook people away getting the shot during an actual pandemic and altering terminology, but isn't this something other than a "vaccine"?


"A vaccine is a biological preparation that provides active acquired immunity to a particular infectious or malignant disease.[1][2] The safety and effectiveness of vaccines has been widely studied and verified.[3][4] A vaccine typically contains an agent that resembles a disease-causing microorganism and is often made from weakened or killed forms of the microbe, its toxins, or one of its surface proteins. The agent stimulates the body's immune system to recognize the agent as a threat, destroy it, and recognize further and destroy any of the microorganisms associated with that agent that it may encounter in the future."

https://en.m.wikipedia.org/wiki/Vaccine

Sounds like this is a vaccine given that criteria.


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Sure. My analysis is that they have yet to complete a human efficacy trial or provided any statistics.


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> does the global medical establishment even have a chance at salvaging the reputation of mRNA?

AstraZeneca's Covishield is not an mRNA vaccine; it is a viral vector vaccine, using Adenovirus. The small possibility of blood clots was acknowledged by medical authorities after a few months of use, with some jurisdictions going so far as to suspend its use, citing the mRNA vaccines as a safer alternative.

https://en.wikipedia.org/wiki/Oxford%E2%80%93AstraZeneca_COV...


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> but these blood clot deaths with negative COVID tests were not unique to the AstraZeneca vaccine

I think Johnson and Johnson's covid vaccine (also an adenovirus vaccine) was also associated with blood clots, but do you have any evidence of clots with the mRNA vaccines? I recall reports of Myocarditis in younger men that got little value from the mRNA vaccines, but this is the first I've heard of blood clots.


To whatever extent a cancer vaccine turns out to be effective, those people will be free to continue dying of cancer at a higher rate than the rest of the population. It's not contagious like covid. If they want to hold a grudge about chaotic messaging and policy in the early fog of war of a novel global public health crisis forever, then cool for them.


https://www.europarl.europa.eu/doceo/document/E-9-2023-00120...

Deaths: 1 579 for the AstraZeneca vaccine;.

The EMA notes that no causal link has been confirmed: ‘The fact that someone has had a medical issue or died after vaccination does not necessarily mean that this was caused by the vaccine.

Even though this is the EU, your 'hundreds of thousands died' is not true in any way and is a lie.

You were told it is not an mRNA vaccine which you are ignoring.

"okay, you might get it, but you won't spread it"

This ignores the evolution of the virus itself into variants which changed the efficacy of the vaccines based off of previous variants.

What you're saying here is classic anti-vax stuff. "I'm just skeptical, I don't trust medicine now" while offering up totally false information.

Never mind that vaccines rapidly stopped covid from flooding hospitals killing people and giving them long term problems. Now it's not a problem and the only thing that slowed down progress was people spreading misinformation and lies.


> "okay, you might get it, but you won't spread it"

> This ignores the evolution of the virus itself into variants which changed the efficacy of the vaccines based off of previous variants.

The trials that gave us the very high efficacy numbers didn't test infection/transmission at all. More than likely nothing changed here, and the messaging was just a lie by people who didn't understand the press releases, which only said it prevents sickness.


I'm not sure who you're talking about, I've noted above that I still find the medical establishment trustworthy, and that my kids are fully vaccinated. I'm fully vaccinated and boosted, but there were studies done that showed excess fatalities NOT attributable to COVID were correlated with the vaccination rate of the country. This also doesn't mean individual vaccines are unsafe, as that is still a very rare occurrence.

Consider that if 4 billion people get a vaccine with a 1/10,000 (0.01%) chance of causing myocarditis / blood clots / other side effects resulting in sudden death, that would still mean 400,000 dead, and those deaths aren't meaningless to the families they affect. It's very insensitive to accuse those who've lost loved ones and then continued to get boosters anyway because it's the right thing to do of pushing a "classic anti-vax agenda"


Consider that the actual chance of TTS (clots) is about 2 per 100,000 (ten times less than your "guess") and that when these issues occur they are NOT always fatal - in a country of 20 million that all get the Astra-Z vaccine 400 people will have a TTS side affect and perhaps 2 of those might die.

Consider, also, the real world where such things were noticed early on, where Astra-Z use was downgraded, and community health centes were advised to stay alert for issues.

ie. 4 billion people did not get a vaccine with TTS issues.

See, for example: https://www.health.gov.au/our-work/covid-19-vaccines/advice-...

and note well AstraZeneca is no longer available in Australia


> AstraZeneca's Covishield is not an mRNA vaccine

I wouldn't expect this distinction to matter much


When I got my AstraZeneca vaccine (in 2021?) I remember it was common knowledge that fatal blood clots were a side effect, and from the evidence at the time I estimated that the chances of it killing me were 1 in 500,000. Have those odds changed with new information?


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Wow. This side effect was pretty much common knowledge in Australia due to a notable early incident and the press coverage it received. It was even factored into the early vaccination process here with the AstraZeneca vaccine not being made available to everyone due to the risks, and that was somewhat of a political hot potato due to that particular vaccine being the one the government had put their money behind, signed deals, and if I recall correctly, even begun manufacturing doses before the final clinical trials were completed.


That’s just not true. Several countries stopped using the vaccine until more data was available. For example in Germany. And then when the vaccine was used again it was only used on a subset of the population (older people because this risk was minimal in those cases). It was discussed at the highest level and all throughout the country.


Exactly, there was and is no mystery. It’s right there in the EU’s insert.

https://www.ema.europa.eu/en/medicines/human/EPAR/vaxzevria-...


It depended your your location and circle.

I'm my experience, in California/USA there was strong political denial of anything possibly negative about the vaccines.

Public health authorities were proclaiming that there were no possible side effects, even as other countries were restricting demographics and discontinuing use.


> Public health authorities were proclaiming that there were no possible side effects, even as other countries were restricting demographics and discontinuing use.

If we're talking about the Astrazeneca vaccine in particular in this subthread, with its clotting side effects-- it's worth noting that it never received a US EUA. It's not surprising that US agencies never restricted its use, having never authorized its use in the first place.


Nah - it was a real thing (and I like vaccines and science) with a risk running at about 2 issues in every 100,000 Asta-Z innoculations with symptoms cropping up within 42 days or so.

(With the bulk of issues being non fatal)

"hundreds of thousands" didn't die though, in all of Australia there was just one person that "probably maybe" died due to TTS (IIRC).

It was first spotted in the European adverse side affect database and written about early on.

More (on TTS and A-Z in AU): https://www.health.gov.au/our-work/covid-19-vaccines/advice-...


That's definitely not true. I remember clearly health authorities and the media were completely open that 1 in N people will die from blood clots. From the beginning.


This is blatant historical revisionism. It was always "save and effective" and that's all people know. Furthermore if you refused to take it you were forced out of the company.


It was always "effective enough relative to the safety risk of rare blood clots". There was never any attempt to suppress knowledge of blood clots, it was international news and widely acknowledged by everyone as a risk associated with the AZ vaccine.


You could both be right, especially depending on where you live and work.


Maybe employers wanted to weed out employees who are subject to emotion and ideology that keeps them from correctly assessing the relative risk levels between two options.


My body, my choice.


True.

But the tricky thing is at what level of supermajority should companies be allowed to discriminate against you based on your choices with your body?


Cancer tends to have an interesting relationship with cellular protein transport. And as a consequence has problems dealing with heat. The protein transport mechanism by which immune surveillance is conducted is shared with cells surviving heat increases via ejection of heat shock proteins.

I once tried to find if there were any studies about incidence of cancer plotted against incidence of high fever in the same individuals but wasn't able to find anything. It may also point to the incidence of cancer actually rising due to suppression of other diseases.

This is plausible due the fact that diseases are a constant in nature and therefore evolution would take their presence as a given as much as the seasons or the sun. It would be very unfortunate if numerous anti-cancer adaptions simply haven't evolved because regular fevers took care of those cancer precursors.


After my COVID shot, I got 2 or 3 days of Transient Global Amnesia. It has scarred my son, who worries about amnesia every single time he's a little delirious from an illness or some such.

By my estimation, the people who threatened and socially pressured others to get an unfinished, experimental gene therapy injection that was always socially enforced to be referred to in polite company as a "vaccine" are the ones liable for any damages that might occur. My son may be scared of random amnesia for the rest of his life. What does he get? What do I get?

What do the people get who believed themselves to be above moral reproach specifically because they were afraid? How do we make sure such people never get to make a decision on my or my sons' behalf ever again?

To say nothing of my cousin, a death of despair due to overblown lockdowns that did more damage than COVID.

What do we do to make sure this doesn't happen again? The answer cannot be "nothing."


Wow that sounds pretty scary. I'm sorry you and your family had to endure that. I'm also very sorry about your cousin.

I share some of your concerns about using mRNA technology as an annual preventative solution against COVID and flu. Even though I'm triple Pfizer mRNA vaccinated I'd probably go for a non-mRNA solution going forward (my employer finally dropped their COVID vaccine requirement but maintain an annual flu vaccine requirement).

But it seems to me that mRNA is a fantastic tool for fighting deadly cancers. Without treatment, the patient is absolutely going to die.

I know. My mom died of glioblastoma back in September 2019. The tumor was wrapped around her thalamus so we had very limited treatment options -- at the time the most advanced treatments needed access to the tumor which is hard to do when it's in the center of your brain.

Hang in there MisterDizzy and, since we are on Hacker News here, remember one of the principles of software development -- use the right tool for the right job. For me, right now, that looks like tried and true protein-based vaccines for those annual vaccinations and fancy mRNA platforms for those specialized treatments.


Thank you for the reply. It seems like this particular application of mRNA is a lot more promising than attempting to use it against a virus, which would mean constantly playing catch-up with the mutations. I hope mRNA has an application for something like this.


The article isn't about that vaccine.


Your son probably needs therapy if he's this terrified of a non-life-threatening incident that is quite rare more than the incidence of death from covid-19.

it was never about being afraid, it was about taking part in society and helping so that your son, young people, the elderly and immune compromised don't die.

as for "experimental gene therapy injection", mRNA vaccines are vaccines and the mRNA in the vaccine does not alter genes, that's actual misinformation about how mRNA vaccines work.




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