> ... a Phase II trial, which means it is focused on identifying dosage ranges and side effects in human rather than a large-scale efficacy trial. (It's also the first time you actually give a drug candidate to humans).

FWIW your drug candidate is administered in all phases. Phase I you look for side effects ("safety and tolerability"). Phase II is, as you say, a dose ranging study, but you can't exceed dosages you've already tested for safety. You usually have multiple arms (a placebo and a couple of dosages); when you find an seemingly efficacious dose you then proceed to a Phase III where you test that dosage (or several) on a statistically representative enough sample to hopefully predict results in the population at large.

(former drug designer who has designed some Phase I and II studies).

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Fun fact: when you file your IND with the FDA to test a new drug you aren't actually asking for permission. You're asking them to tell you that if you follow the protocol you have sent them, based on the evidence you've sent them from what you know already, they won't prosecute you for violating the law on administering unapproved drugs. Section 505 for the food and drug law has a bunch of exceptions -- you ask then to tell you you fit in one of the exceptions.

And if they don't tell you "no" in a 30 days...you can go ahead! I wonder if the shutdown extends that 30 days.

Thanks for the correction. I thought Phase I was a pre-human clinical trial for safety, rather than a human clinical trial. I appear to have been mistaken.

No problem. Preclinical work is indeed called preclinical work :-).

Typically you do a bunch of in vitro and in vivo studies when developing your drug candidate. When you're ready to file the IND (asking permission to test on humans) you do a different set of studies specifically to generate the data you need for your submission. Sometimes the agency will even tell you where its concerns may lie so you might use a specific animal or specific test to address them. You also include a lot of in vitro work about how you manufacture (and control the mfg of) your test product.

The difference might be that you take and process a lot of samples in your R&D stage, and then when you prepare your submission you get independent labs to do the work (to show the agency you don't have your "finger on the pan" so to speak). For example on a depot-injectable drug I worked on we did six experiment sites per guinea pig (because we knew tissue diffusion would be only a few millimeters) which saved us time and a lot of money but when preparing for the FDA we did only one per, so we could guarantee to them that any trace of drug found anywhere in the tissue came from a single injection. Likewise we did a lot of pathology ourselves just peering through the microscope (and learned a lot!), but for the FDA we had the animal lab send tissue samples directly to an external pathologist who then sent us a report without any input from us. Etc.