Intro Flashcards by Emily Liu

what is toxicology

study of adverse effects of chemicals on living organisms

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what is a poison

any agent capable of producing a deleterious response in a biological system

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what is “any agent capable of producing a deleterious response in a biological system”

a poison

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what is a toxin

toxic substance produced by biological systems

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what is “toxic substance produced by biological systems”

a toxin

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what is a toxicant

a poison of human origin or as a by-product of human activity

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what is “a poison of human origin or as a by-product of human activity”

a toxicant

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what is a xenobiotic

any compound not normally part of or synthesized by the organism

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what is “any compound not normally part of or synthesized by the organism”

a xenobiotic

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what are 4 kinds of things that a graded response can be used for and why

BP, liver weight, drug clearance and pain

because it can assume a variety of values

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what does quantal mean (basic)

all or none (so there is or isnt a response)

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can you use a dose-response graph for quantal things and why

no because it is all or none

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when are quantal dose response relationships typically used for

describing variability in pharmacodynamic responses in populations

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what do LD50 experiments measure

death

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what do TD50 experiments measure

toxicity

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what units are quantal dose-response relationships used in

probits

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what are probits (2 words)

probability units

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what kind of distribution does quantal responses usually have

normal (Gaussian) distribution

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is the cumulative or non cumulative quantal response curve a normal distribution (explain)

non cumulative (cumulative keeps increasing)

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how does the non cumulative quantal response curve work

at increasing doses, how many animals of the ones left die at that dose

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why does the highest dose have little loses in the non cumulative quantal response curve (shouldn’t it be most death)

not many more animals are still alive at that point

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how does the cumulative quantal response curve work

at each new dose, you add the new deaths to the old ones

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where is the relatively linear portion of the sigmoidal curve (cumulative mortality graph)

between 16 and 84 % death sections

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what does the 16% represent

1 SD from the mean, 50-34

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what does the 84% represent

1 SD from the mean, 50+34

what % encompasses 1 SD from the mean on one side

34%

what % encompasses 1 SD from the mean on both sides

68%

what is a normal equivalent deviation (NED)

units of deviation from the mean

how many NED with a 50% response (and why)

0 (it is the mean)

how many NED with a 84% response (and why)

+1 (1 SD from the mean)

how many NED with a 16% response (and why)

-1 (1 SD from the mean)

how do you convert NED to probit units

you add 5

what is the probit units with a 50% response (and why)

5 (0+5) (it is the mean)

what is the probit units with a 84% response (and why)

6 (1+5) (1 SD from the mean)

what is the probit units with a 16% response (and why)

4 (-1+5) (1 SD from the mean)

what are 3 reasons to convert quantal data to a straight line ?

- more convenient to obtain information | - too difficult and costly to describe full sigmoidal curve

how do you find the line of best fit in probit linear curves

linear regression

where in the straight line probit quantal analysis graph thing is the mean

5! (cause you add 5 to get to probits)

what is therapeutic index

a measure of safety, ratio between TD50 and ED50

what is the criticism of TI calculations

the slope of the lines (which reflect potency of xenobiotic) is not taken into account

what does the slope of the line represent

potency of xenobiotic

what may be a good replacement to therapeutic index

margin of safety

how do you calculate margin of safety

TD1/ED99

what does the ratio in MOS represent

TD1/ED99 represents the dose that gives the first signs of toxicity (TD1) and the dose that produces the wanted effects in nearly everyone (ED99)

what does a MOS<100 mean

it is very dangerous (that there is overlap with the effective dose and toxic dose - no good)

what does it mean if the ED50 and TD50 lines overlap

that there is overlap with the effective dose and toxic dose - no good

what does it mean if the ED50 and TD50 lines DO NOT overlap

it is likely safer, there is no overlap with the effective dose and toxic dose

can you have different TIs for a single drug and why?

yes, because it depends on which toxic endpoint is measured (like the diff effects, such as cancer or liver failure)

are LD50 values absolute numbers and why

not really because of the inherent variability of the testing procedure (like weight, age, etc)

what are 6 reasons that LD50 values vary a lot

because of weight, age, duration of observation, route of admin species, strain of species

what is an acceptable range of LD50 values

it can span an order of magnitude

are classic LD50 experiments done anymore and why (4)

no - no info on chronic - no info on mechanism - waste of animals - more important things than just death

what are some endpoints prior to death that may be more important

non-fatal, like liver kidney and brain damage

what are up-and-down tests used for

approximate lethal dose

how do you do the up and down tests (3 main steps)

- dose one animal - if survives after 1-2 days, test another animal at a higher dose - if it doesnt survive dose another one at a lower dose

what do you do in the up and down tests to the animal you test

observe it for 7 days to check for delayed deaths

how do you determine the approximate lethal dose using the up and down tests

the case with the lowest tested dose at which lethality occurs

how many animals are often tested in up and down tests (ALD)

6-8

what does ALD stand for

approximate lethal dose

how many animals are often tested in traditional LD50 tests

40-50! bad

what is a con with the up and down tests (ALD) compared to the traditional LD50 tests

it takes longer time to complete (sequential testing)

what is sequential testing

practice of making decision during an A/B test by sequentially monitoring the data as it happens

what are the 4 durations for exposure

acute, subacute, subchronic, chronic

what is acute exposure

exposure to a chemical for less than 24 hours (traditional LD50 experiments)

what is subacute exposure

repeated exposure for 1 month or less

what is subchronic exposure

repeated exposure for 1-3 months

what is chronic exposure

repeated exposure for more than 3 months

how can toxic effects from acute and chronic exposure differ

like CNS depression immediately, or chronic long term

why must you carefully choose the dose in chronic testing

to prevent premature mortality

what does MTD stand for

maximum tolerable dose

what is maximum tolerable dose

the dose that suppresses gain in body weight over 90 days

what are the 3 main doses used in chronic testing

1MTD 0. 5 MTD 0. 25 MTD

what will be the maximum dose in animals in chronic testing

a daily dose that results in an area under curve (AUC) that is 25X the AUC for the highest dose in humans that is therapeutically useful (from preliminary pharmacokinetic data from humans)

how long do most carcinogenic potential assays take to do

2 years long

what is the basic reason that it is so hard to know if something causes cancer

because lots of time and animals = $$$$

how many animals are usually used in carcinogenic potential assays

usually like 60, but you may need 1000 to prove a statistical significance

why are rare events difficult to find

because small sample sizes makes it less probable that you will catch the rare event (you need like 600+ to have good odds of catching it

what is an issue with extrapolating what happens with high doses to what may happen with low doses

cause high doses may induce systemic toxicity that is triggering DIFFERENT cellular/systematic events than low doses (those things wouldn't even happen with those low doses)

what is an example of something that happens with high doses that wouldnt happen in low doses

bladder toxicity, cause the high dose would precipitate in urine and affect the tubules

besides dose, what else makes it hard to extrapolate from animal testing

there are sometimes significant intra and interspecies differences in response to xenobiotics

what is an issue with seeing if drugs cause cancer in animal models

cause there is a high baseline tumor incidence in animals anyways, so you dont know if its just caused by the drug

what is a dose issue with animal models

there is a relatively limited number of doses actually tested