I strong-downvoted this post. I had hoped the reasons why would be obvious. Alas not.

Scientific (in)credibility

The comments so far have mainly focused on the cost-effectiveness calculation. Yet it is the science itself that is replete with red flags: from grandiose free-wheeling, to misreporting cited results, to gross medical and scientific misunderstanding. [As background: I am a doctor who has published on the genetics of inflammatory bowel disease]

Several examples before I succumbed:

• Samuel et al. 2010 is a retrospective database review of 6 patients treated with itraconazole for histoplasmosis in Crohn's Disease (CD) (N.B. Observational, not controlled, and as a letter, editor- rather than peer-reviewed). It did not "report it cured patients with CD by clearing fungus from the gut": the authors' own (appropriately tentative - unlike the OP) conjecture was any therapeutic effect was mediated by immunomodulatory effects of azole drugs downstream of TNF-a. It emphatically didn't "suggest oral itraconazole may be effective against Malassezia in the gut" (as claimed in the linked website's FAQ) as the presence or subsequent elimination of Malassezia was never assessed - nor was Malassezia mentioned.
• Crohn's disease is not a spondyloarthritis! (and neither is psoriasis, ulcerative colitis, or acute anterior uveitis). As the name suggests, spondyloarthritides are arthritides (i.e. diseases principally of joints - the 'spondylo' prefix points to joints between vertebrae); Crohn's a disease of the GI tract. Crohn's can be associated with a spondyloarthritis (enteropathic spondyloarthritis). As the word 'associated' suggests, these are not one and the same: only a minority of those with Crohn's develop joint sequelae. (cf. Standard lists of spondyloarthrides - note Crohn's simpliciter isn't on them).
• Chronic inflammation isn't a symptom ('spondoyloarthritide' or otherwise), and symptoms (rather than diseases) are only cured in the colloquial use of the term.
• However one parses "[P]roving beyond all doubt that Crohn's disease is caused by this fungus will very likely lead to a cure for all spondyloarthritide symptoms using antifungal drugs." ('Merely' relieving all back pain from spondyloarthritides? Relieving all symptoms that arise from the set of (correctly defined) spondyloarthritides? Curing all spondyloarthritides? Curing (and/or relieving all symptoms) from the author's grab bag of symptoms/diseases which include CD, Ulcerative Collitis, Ankylosing spondylitis, Psoriasis and chronic back pain?) The antecedent (one n=40 therapeutic study won't prove Malassezia causes Crohn's, especially with a competing immunomodulatory mechanism already proposed); the consequent (anti-fungal drugs as some autoimmune disease panacea of uncertain scope); and the implication (even if Malasezzia is proven to cause Crohn's, the likelihood of this result (and therapy) generalising is basically nil) are all absurd.
• The 'I love details!' page notes at then end "These findings satisfy Koch’s postulates for disease causation, albeit scattered across several related diseases." Which demonstrate the author doesn't understand Koch's postulates: you can't 'mix and match' across diseases, and the postulates need to be satisfied in sequence (i.e. you find the microorganism only present in cases of the disease (1), culture it (2), induce the disease in a healthy individual with such a culture (3), and extract the organism again from such individuals (4)).
• The work reported in that page, here, and elsewhere also directly contradict Koch's first postulate. Malasezzia is not found in abundance in cases of disease (pick any of them) and not in healthy individuals (postulate 1): the author himself states Malasezzia is ubiquitous across individuals, diseased or not (and this ubiquity is cited as why this genus is being proposed in the first place).

Intermezzo

I'd also rather not know how much has been spent on this so far. Whatever it is, investing another half a million dollars is profoundly ill-advised (putting the money in a pile and burning it is mildly preferable, even when one factors in climate change impacts). At least an order of magnitude cheaper is buying the time of someone who works in Crohn's to offer their assessment. I doubt it would be less scathing than mine.

Meta moaning

Most EAs had the good judgement to avoid the terrible mistake of a medical degree. One of the few downsides of so doing is (usually) not possessing the background knowledge to appraise something like this. As a community, we might worry about our collective understanding being led astray without the happy accident of someone with specialised knowledge (yet atrocious time-management and prioritisation skills among manifold other relevant personal failings) happening onto the right threads.

Have no fear: I have some handy advice/despairing pleas:

• Medical science isn't completely civilizationally inadequate, and thus projects that resort to being pitched directly to inexpert funders have a pretty poor base rate (cf. DRACO)
• Although these are imperfect, if the person behind the project doesn't have credentials in a relevant field (bioinformatics rather than gastroenterology, say), and/or a fairly slender relevant publication record, and scant/no interest from recognised experts, these are also adverse indicators. (Remember the nobel-prize winner endorsed Vit C megadosing?)
• It can be hard to set the right incredulity prior: we all want take advantage of our risk neutrality to chase hits, but not all upsides that vindicate a low likelihood are credible. A rule-of-thumb I commend is 10^-(3+n(miracles)). So when someone suggests they have discovered the key mechanism of action (and consequent fix) for Crohn's disease, and ulcerative colitis, and ankylosing spondylitis, and reactive arthritis, and psoriasis, and psoriatic arthritis, and acute anterior uveitis, and oligoarthritis, and multiple sclerosis, and rheumatoid arthritis, and systemic lupus erythematosus, and prostate cancer, and benign prostatic hyperplasia, and chronic back pain (n~14), there may be some cause for concern.
• Spot-checking bits of the write-up can be a great 'sniff test', especially in key areas where one isn't sure of one's ground ("Well, the fermi seems reasonable, but I wonder what this extra-sensory perception thing is all about").
• Post value tends to be multiplicative (e.g. the antecedent of "If we have a cure for Crohn's, how good would it be?" may be the crucial consideration), and so its key to have an to develop an understanding across the key topics. Otherwise one risks conversational bikeshedding. Worse, there could be Sokal-hoax-esque effects where nonsense can end up well-received (say, moderately upvoted) provided it sends the right signals on non-substantive metrics like style, approach, sentiment, etc.

I see these aspects of epistemic culture as an important team sport, with 'amateur' participation encouraged (for my part, implored). I had hoped when I clicked the 'downvote' arrow for a few seconds I could leave this to fade in obscurity thereafter. When instead I find it being both upvoted and discussed like it has been, I become worried that it might actually attract resources from other EAs who might mistakenly take conversation thus-far to represent the balance of reason, and detract from EA's reputation with those who recognise it does not (cf. "The scientific revolution for altruism" aspiration). So I feel I have to am to write something more comprehensive. This took a lot longer than a few seconds, although fortunately my time is essentially worthless. Next time we may not be so lucky.

Interesting post, thanks for sharing. Although I am skeptical for some reasons I note below, the potential upside to such a cheap treatment for a very unpleasant disease seems highly worth pursuing. For context, I'm viewing this post as an academic biologist who develops methods for microbiome data analysis and collaborates with some clinicians, though my background is ecology and evolution rather than medicine.

While reading the post, I struck by how the referenced evidence for the author's (Martin Laurence) hypothesis is entirely from citations to his own papers and a short reply to a journal article (I don't think peer reviewed) about anecdotal observations from six IBD patients. The author's papers referenced take the form of reviews and argued hypotheses from research done by others, rather than original experiments, and seem to be about spondyloarthritis, prostate cancer and MS rather than Crohn's directly. Given that IBD and Crohns disease are popular research topics in biomedical research and specifically in microbiome research, I found this lack of reference to others in support of the main hypothesis suspicious, and it made me think the hypothesis is controversial or not well subscribed to in the field. That is not to say it is unfounded, but I would have expected some acknowledgement if this is an "out there" view and discussion of why that included some references to the mainstream view and coverage of the controversy. I would also expect that building further evidence that would convince other researchers and mainstream funders in the field would be the next step, rather than crowd funding a clinical trial, and so would have liked to see an explanation for why this strategy isn't being taken.

I also felt that the reasons under Neglectedness and Funding Gap didn't explain why other biomedical researchers aren't pursuing this, or why the author isn't soliciting funds through standard biomedical funding agencies. The lack of incentive for private drug companies mentioned does not explain why standard agencies and organizations aren't funding it. It is true that fungi are often neglected over bacteria in microbiome studies, but if there is good evidence that fungi are playing a role in Crohn's and they've been historically neglected, they I would expect researchers to be jumping on this hypothesis, and for standard biomedical funders to be glad to fund it, unless for reasons mentioned above.

After reading the FAQ on the author's website, I suspect the author is forgoing the mainstream route and soliciting small private donations because he is operating outside academia and lacks academic or hospital collaborators who can apply for the needed grants. But without these collaborators, I don't see how the proposed clinical trial could be orchestrated. This is not to say that I think the author is wrong in pursuing this work or not credible, but I feel that ignoring these issues makes the post seem less credible than it might otherwise be.

Hmmm.. this post seems overconfident. Also it's a seriously way out there hypothesis. But between RA+AS+IBD+prostate Ca we're probably talking about a few percent of first-world morbidity, or at least health expenditures. The authors' include some folks with great credentials, and the written argument in Laurence 2018 is seemingly reasonable (on a skim). Very plausible that I've missed glaring mistakes in their analysis, but if not this seems like a high EV experiment.

This is an interesting project! I hope you're able to show it to people who are in a good position to evaluate whether it's really such a promising idea (Open Phil has certainly made some grants for research on health issues not specific to the developing world), and that you'll post about further updates on the Forum.

I think that this post gets off slightly on the wrong foot with this analysis:

There are ~2 million Crohn’s disease sufferers worldwide, and many use immunomodulatory injections (such as adalimumab which costs ~50K$ USD/year) to reduce inflammation and symptoms. A back of the envelope calculation suggests this would have a direct economic impact of 50K$ x 2M = ~100B$ USD/year.

The back-of-the-envelope calculation assumes that the drugs reach every person with the disease, that all of those people were already using the expensive injections (I assume the drug wouldn't be as useful to people who've already had stomach surgery, but maybe it would be?), and that the drugs will replace the expensive injections entirely. The analysis also ignores the cost of getting the drug to patients worldwide (including getting past each country's equivalent of the FDA) and the chance that it might not be approved in some countries.

Of course, if a cure can really be developed and marketed for a cost in, say, the tens-of-millions-of-dollars range, this would still be a very good opportunity for impact. But the oversimplified impact calculation looks a bit like "gilding the lily" (trying to exaggerate the benefits of something that, even with a more realistic calculation, still looks good).

On the other hand, a true "cure" would also bring benefits to all future sufferers of Crohn's, so in another sense, the impact calculation may be somewhat understated. I'd love to see a more comprehensive analysis at some point, as Zeke suggested.

Hi Zeke, I would have liked to do a more detailed analysis of impact, but QALY/WALYs are not my expertise, and I would have made many mistakes. This analysis would be very valuable, both for the narrow scope (Crohn's disease), and the full potential scope of the project (the other diseases shown in bold). Crohn's affects young adults for life. Total worldwide prevalence is not know precisely due to poor monitoring in many countries. Many studies report Crohn's and ulcerative colitis prevalence combined.