In a criminal justice context, an expert toxicologist's opinion is often in the form of whether the concentration in the blood is "consistent with a therapeutic range."

So, for a given medication, there will be studies that say something like (just some random numbers here) "this medication is usually dispensed in doses of 10mg once per day at the low end and 70mg once per day at the high end. People who take a 10mg dose typically have a blood concentration that peaks between X and 2X after approximately an hour, and people who take a 70mg dose typically have a blood concentration that peaks between 7X and 14X after an hour. The substance in the blood has a typical half-life of 8 to 12 hours. On a daily dose, baseline blood levels will stabilize at Y for 10mg daily and Z for 70mg daily."

So, let's say someone has 80X in their blood. A toxicologist will be able to say with confidence "that's not consistent with a therapeutic dose - this person ingested way more of the substance than a doctor would ever prescribe." So, either drug abuse or poisoning.

Now, say someone has 2X in their blood. A toxicologist can say "that's consistent with a therapeutic dose" - but not much more than that. It's quite possible that person took 10mg or 20mg an hour ago, and takes that every day - but they may have taken 70mg 16 to 24 hours ago as a one-off. Or they may have taken 40mg 12 hours ago, and every other day for the last month. Or they may have taken 1,000mg 48 hours ago.

So, that's some of the nuance: it's fairly easy to rule out certain dosage quantities/timelines, but it's much harder to say what actually did happen. A lot of the time, the first one's all that's needed.

A single sample? No. Multiple samples? It depends. When dosed, the concentration in blood rises for a period and then declines as it is metabolized and cleared from the body. Each drug has a sort characteristic curve for the drug and it’s metabolites that you could compare to a series of samples taken over time which you may be able to use to determine the initial dose. It depends a bit on the dynamics of the drug clearance, and at what times you took the samples.

Volume of distribution, time of ingestion, half life of medication, was it taken orally or parenterally, etc, etc, would need to be known.

Also whether this was dose 1 or if there were multiple doses.

But the equations only apply to live people. After death, considerable changes can occur - Some drug concentrations go up, some go down, it’s not exactly predictable.

That being said, I haven’t really used pharmacokinetics and pharmacodynamics for years. Did you ask the person who performed the autopsy?

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I did my PhD on this, but for living patients ;)

As you say, there are many factors at play, most importantly distribution volume and drug elimination rate. For all of these factors, you can estimate the typical value and the between-individual variability in the population. We call this a population pharmacokinetic model.

With just a single concentration, you assume this person is a "typical individual". You can back-calculate (based on time of death and time of taking the drug) what the dosage typically could have been. You need the administration time though, the time of death, and you better hope the drug concentration remained stable between time of death and time of autopsy. In clinical studies, blood samples are often stored in solid co2 (-80C), and for good reason.

Using the known variability in the population, you can also give a confidence range for your initial dose prediction. You can make predictions more precise by adding information. Bodyweight influences likely drug distribution volume. A second drug (with known dosage and administration time) could help you too.

Usually, this technique is done for drugs that need to be in a precise concentration range. Give a dose, measure concentration, estimate blood volume and calculate the optimal dose for that patient. We call this Model Informed Precision Dosing: MIPD. You can apply the same in autopsies, but I doubt it is routinely applied. Cool question!

Adding on to some of the good comments here, many drugs have physical properties that cause them to distribute in body tissues beyond the blood. For instance, when we give patients oral antibiotics for infections of a specific organ (prostatitis, for example), we need to choose an antibiotic that has good penetration to the prostate. Or good bone penetration for osteomyelitis. If a drug is extremely lipophilic and is given to an obese person, the volume of distribution can be effectively limitless and difficult to ascertain, because it distributes beyond the blood and into the fat tissue. The log P value of a drug will give us a clue to how widely the drug distributes, but we would need multiple samples to truly understand the kinetics how the drug is eliminated in a specific patient.

There are also special circumstances that complicate this “2-compartment pharmacokinetics” process. When we give a cancer patient high dose methotrexate infusions, the drug will distribute into any excess body fluid in the patient, like edema. The body will then clear the blood of the drug, but the methotrexate-laden body fluid will effectively re-bolus the patient with the drug and raise their blood levels again, long after we’ve stopped the infusion.

This is a very exact science called pharmacokinetics. But we need some pretty exact info, like time of the last dose and rough dosing history before that. For most marketed drugs we’ll have a population pharmacokinetic model that we could use to give a prediction interval around a likely concentration for a given dose, or to estimate the most likely dose given an observed concentration.

As most of the answers have said, it depends. When monitoring a patient on certain medications, we will test what is called "peak and trough." Peak is when the medication should be at its highest concentration in the bloodstream, which is typically an hour after dose, although this can vary a little with some drugs. Trough is when the concentration should be at its lowest, which is typically just before the next dose. I believe drug half-life has been mentioned previously, so i wont rehash that. Drug interactions, disease, and things like grapefruit can interfere with drug metabolism rates. Most drugs dosing is calculated using amount of drug/weight of patient/time. Blood volume is assumed. Again, not all drugs are the same, and not all humans react the same, but you could roughly guesstimate the initial dose, which was your actual question. This information isn't terribly useful in most clinical settings. I am a clinical laboratory scientist, so this is a bit of what I do.

For many drugs if you knew the route of administration (orally for example) and the time, you could get a pretty good feeling of the dose.

The pharmacokinetics of drugs give you a curve or a line of some kind and it is possible to back calculate.

There are certain caveats. For some things , the original drug is labile and the metabolite in stable, so you would just measure that. But this is a technical thing, like measuring an oxidized version rather than not. Some things are in bound and free forms and it is technically difficult to get both. Some things have endogenous versions that make it hard to tell what you ate vs what you had (erythropoietin , testosterone) because they are indistinguishable. Some things have such a long or short half life that it becomes complicated. Some things that are stored in fat are tricky to figure out doses of. And all sorts of other little quirks. But , a qualified yes is really the answer.

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They do this to make sure the serum is the right level in people who take medications that can change levels based on how long you take it. You need a base number to go off of, so there’s no way to tell exactly how much someone took, but if you’ve tested every month, you’ll know how much that amount will look like in their blood over time. You can tell if someone has overdosed when there’s an amount far greater than a normal dose has entered the system, since it is not longer in the safe therapeutic range and has likely done some damage

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For a process like this you’d need to have data from studies (like clinical trials) to compare against. You couldn’t a priori take an arbitrary drug and back calculate. For instance, some drugs require a biotransformation to become reactive. Some may be bound and metabolized in a certain organ, and still others may have a short half life.

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Yes and no.

I'm finishing up a doctorate in pharmacy and the thing is that there are soooo many factors that go into drug blood concentrations. Genes, the drug in question, diet, underlying conditions, kidney function (hard to tell when they are deceased), etc. All play a factor in drug concentrations.

We do however have basic pharmacokinetics diagrams that can apply to a lot of drugs across large populations. Most of the time they are very basic equations though, usually only considering age, weight, height.

There isn't really a perfect answer here.

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