Drug Approval Process

Question 1

T or F. movement of drugs from prescription to over-the-counter status leads to reduced costs

Answer 1

T, but the cost burden often shifts from the HMO to the consumer.

Question 2

How does prescription use in the South compare to the rest of the nation?

Answer 2

the mid-south (TN-AR- MS) experiences a higher prescription drug use than does the population in general. As a general rule, the more drugs a patient is taking concurrently, the greater the risk for adverse drug-drug interactions.

Question 3

The Food and Drug Administration (FDA) falls under the aegis of the ____.

Answer 3

Department of Health and Human Services (DHHS)

Question 4

Drugs are the responsibility of the ______.

Answer 4

Center for Drug Evaluation and Research (CDER)

Question 5

What did the Pure Food and Drug Act of 1906 do?

Answer 5

prohibited mislabeling and adulteration of drugs

Question 6

What did the Opium Exclusion Act of 1909 do?

Answer 6

prohibited importation of opium

Question 7

What did the Amendment to the Pure Food and Drug Act in 1912 do?

Answer 7

prohibited false or fraudulent advertising claims

Question 8

What did the Harrison Narcotic Act of 1914 do?

Answer 8

Established regulations for use of opium, opiates, and cocaine (marijuana added in 1937)

Question 9

What did the Food, Drug, and Cometic act of 1938 do?

Answer 9

required that new drugs be safe as well as pure (no proof of efficacy). Enforcement by FDA

Question 10

What did the Durham-Humphrey Act of 1952 do?

Answer 10

Vested in the FDA the power to determine which products could be sold without prescription

Question 11

What did the Kefauver-Harris Amendments of 1962 to the Food, Drug, and Cosmetic Act do?

Answer 11

Required proof of efficacy as well as safety for new drugs and for drugs released since 1938; established guidelines for reporting of information about adverse reactions, clinical testing, and advertising of new drugs

Question 12

What did the Comprehensive Drug Abuse Prevention and Control Act of 1970 do?

Answer 12

Outlined strict controls for habit-forming drugs; established drug schedules and programs to prevent and treat drug addiction

Question 13

What did the Orphan Drug Amendments do?

Answer 13

Provided incentives for development of drugs that treat rare diseases (less than 200,000 in USA)

Question 14

What did the Drug Price Competition and Patent Restoration Act of 1984 do?

Answer 14

Abbreviated NDAs for generic drugs (bioequivalence data). Patent life extended to account for FDA review process (max less than 5 extra years of 14 years post-NDA approval)

Question 15

What did the Prescription Drug User Free Act of 1992 (and 2007) do?

Answer 15

Manufacturers pay use fees for certain NDAs

Question 16

What did the Dietary Supplement Health and Education Act of 1994 do?

Answer 16

Established standards for dietary supplements prohibited full FDA review as drugs. Required specific ingredient and nutrient information labeling that defines dietary supplements and classifies them as part of the food supply but allows unregulated advertising

Question 17

What did the Bioterrorism Act of 2002 do?

Answer 17

Enhanced controls on dangerous biologic agents and toxins. Seeks to protect safety of food, water, and drug supply

Question 18

What did the FDA Amendments Act of 2007 do?

Answer 18

Grants FDA greater authority over drug marketing, labeling, and direct-to-consumer advertising; requires post-approval studies; established active surveillance systems, makes clinical trial operations and results more visible to the public governs Phase IV studies and labeling issues and reporting adverse events

Question 19

T or F. Drugs developed as antidotes to potential terrorism select agents are the one group of drugs that receive approval based solely upon animal tests.

Answer 19

T. Clearly it would be unethical to conduct trials of these lethal toxins in humans.

Question 20

What is a risk/benefit profile?

Answer 20

whether or not the potential benefits of a potential drug choice outweigh the risks in that patient.

Question 21

Are dosing recommendations typically personalized today?

Answer 21

Most drug dosing is still based upon the “one size fits all” concept. So dose recommendations try to balance risks/benefits across the patient spectrum. This is increasingly recognized as the wrong approach and a more individualized dosing profile will ultimately be adopted for many drug classes.

Question 22

The first step in drug development is formulation of a correct, therapeutic compound. How does this work?

Answer 22

Developers begin with a standard compound and alter molecule characteristics including pks, metabolism, solubility, route of administration, etc.- to look at effects on activity. This is driven by modeling studies now and is becoming efficient

Question 23

Preliminary techniques keep things simple and cheap, involving ___ systems.

Answer 23

in vitro. Animal systems are no longer the first choice for ethical reasons and because they involve the use of larger quantities of the test agent. Synthesis is expensive; you don’t want the time and cost of producing large quantities of a “candidate” only to immediately find it is useless in your assay systems.

Question 24

How did pharm products used to be made? How is that different today?

Answer 24

Once upon time, you began with compounds that produced an effect, then tried (sometime in an incomplete manner) to establish how they worked.These days, with molecular modeling and molecular biology, one can synthesize “candidates” to specifically interact with a known receptor motif.

Question 25

What are “first in class” drugs?

Answer 25

First the treat a specific thing.Most often the result of phenotypic analysis, i.e. treating a recognized clinical condition. However, once the new ‘target” is recognized and the drug comes to market, competitors hone in on the already defined receptor to develop their “me too” drugs.

Question 26

What are some issues that still need to be figured out even once a drug candidate has been successful in in vitro testing?

Answer 26

Just because a “candidate” works in a cell assay or indeed in a cell- free system, it doesn’t mean that, from a physico-chemical perspective, the compound could be administered to patients. There are many considerations, such as solubility, metabolism, and potential drug-drug interactions

Question 27

What is “high throughput screening” (HTS)?

Answer 27

many in vivo issues of a drug (solubility, drug-drug interactions, etc.) are highly automated and are therefore easily reproducible

Question 28

Why must assays determine in vivo characteristics of a drug candidate such as solubility, etc. still be cheap and easy?

Answer 28

most of these “candidates” will fall by the wayside before the process is over!

Question 29

What are Herg channels?

Answer 29

potassium channels in polarized membranes (potassium is an important regulator of membrane polarity-especially in the heart)

Question 30

What happens if Herg channels are upset by a drug?

Answer 30

the membrane can become hyper-responsive, leading to cardiac arrhythmias (QT prolongation)The most famous example in recent history was the antihistamine drug called terfenadine.

Question 31

Is Herg channel interaction testing common?

Answer 31

In order to spare the financial burden, peer embarrassment and shareholder anger, drug copmanies now test for potential Herg channel interactions before the drug ever moves into clinical trials. This is often done on a contract basis by specialist companies.

Question 32

If no Herg channel disruption occurs during experimentation, does that mean it won’t during clinical use?

Answer 32

Absence of a reaction in an experimental system in no way guarantees the absence of such interactions in clinical use. This MUST be confirmed by clinical experience

Question 33

T or F. Toxicity testing is time-consuming and expensive.

Answer 33

T. Two to 6 years may be required to collect and analyze data on toxicity and estimates of therapeutic index on at least 2 animal species

Question 34

Toxicity testing is typically done via ____.

Answer 34

Animals. Large numbers of animals may be needed to obtain valid preclinical data

Question 35

What are some alternatives being tried instead of the use of animals?

Answer 35

Cell and tissue culture in vitro methods and computer modeling are increasingly being used, but their predictive value is still limited. Nevertheless, some segments of the public attempt to halt all animal testing in the unfounded belief that it has become unnecessary.

Question 36

T or F. Extrapolations of therapeutic index and toxicity data from animals to humans are reasonably predictive for all toxicities.

Answer 36

F. Many, but not all. Seeking an improved process, a Predictive Safety Testing Consortium of five of America’s largest pharmaceutical companies with an advisory role by the Food and Drug Administration (FDA) has been formed to share internally developed laboratory methods to predict the safety of new treatments before they are tested in humans.

Question 37

What must first happen for a drug candidate to enter clinical trials?

Answer 37

One vital aspect is the review and acceptance by the Institutional Review Board (IRB)also need informed consent

Question 38

How long does the FDA have to review a clinical trial application?

Answer 38

30 days

Question 39

What are some things needed on a clinical trial application for review by the IRB?

Answer 39

protocol overview, clear objectives, study design, patient inclusion/exclusion info, etc.

Question 40

The Phase I clinical trial is essentially a ____.

Answer 40

dose-finding exercise in humans.T he developer has discovered the Maximum Tolerated Dose (MTD) in animal model systems, but what is it in humans.

Question 41

How is MTD in humans performed during a phase I trial?

Answer 41

A dose escalating study

Question 42

How is a drug-escalating study done?

Answer 42

only conducted on 10-15 healthy adult volunteers (or terminal cancer patients in development of cancer drugs)starting from a lower dose than the animal trials (except if cancer patient) and work way up to see when/if adverse events occur to find the MTD

Question 43

What occurs in Phase II trials?

Answer 43

The Phase II trial involves more patients (typically 100-300), is more expensive and explores or refines the optimal dosing regimen and dose- pharmacokinetic relationship.Begin with MTD from Phase I and vary dosing regimen to extend toxicity profile

Question 44

T or F. Phase II trials involve patients with the intended disease for which the drug is being developed

Answer 44

T.

Question 45

What happens if a drug gets a positive response from a phase II trial?

Answer 45

the trial is extended to 30-40 more patients and further if the activity is again evident in that group Active, non-toxic groups then proceed to phase III trials

Question 46

What is the major criterion for acceptance of a drug?

Answer 46

Will the benefits of the drug outweigh the risks?

Question 47

What occurs in Phase III trials?

Answer 47

patient base is extended to close to 1000. This is often conducted in a blinded fashion to eliminate bias. Multi-center trial is common

Question 48

What is a blinded trial? Double blinded?

Answer 48

In the former, the patient doesn’t know whether or not they are receiving the candidate drug, in the latter, neither the doctor nor the patient is aware of what is being given to the patient. To avoid bias the comparator is formulated in an identical fashion.

Question 49

Are Phase III trials typically long or short? When can they be stopped short?

Answer 49

Long, but can be stopped because of superior efficacy of trial agent or increased risk to users compared to normal practice

Question 50

What is the placebo effect?

Answer 50

giving a patient anything can often times improve their outcome regard of what it is. Typically, 30-50% of the placebo group in trials will improve

Question 51

What is the impact of the placebo effect?

Answer 51

It can be very hard to prove efficacy in some drug classes like psychiatric therapy often newly approved drugs fail to be placebos in later studies

Question 52

What happens if all clinical trials are successful?

Answer 52

the developer files an NDA with the FDA, sends them the several truckloads of files and, as noted earlier, pays the fee for review. If the risk-benefit ratio fall in favor of benefit, then the FDA can issue an approval notice, the license to market this new patent medicine.

Question 53

What kinds of documentation are required for FDA review following successful clinical trial?

Answer 53

drug safety in animal and human trials, evaluation of carcinogenic and teratogenic status, drug stability

Question 54

What three responses can a drug get from FDA review?

Answer 54

Approved, Disapproved, and Approvable but more info is needed (i.e. for labeling, effect, etc.)

Question 55

What is Pharmacometrics?

Answer 55

simultaneous quantitative understanding of drug dose or exposure and response (pharmacodynamics)These days the discipline of pharmacometrics (computer modeling) is used to extrapolate data from clinical trials to other scenarios without the need for more or redesigned trials. It’s a relatively recent development in clinical studies, but it will become increasingly important in the future.

Question 56

Pharmacometrics is used for what 3 broad areas?

Answer 56

evidence of effectiveness, dose optimization, and improvement in future trial design by gaining insight into causes of clinical trial failure

Question 57

What kinds of situations would warrant accelerated review by the FDA?

Answer 57

In order to bring to market drugs that could have an immediate impact upon the lives of patients with serious or life-threatening illness, like cancer, the FDA may grant approval for clinical availability contingent upon confirmation of limited clinical trials.

Question 58

What are generic drugs?

Answer 58

Those appearing in the marketplace after the patent on the original drug has expired.

Question 59

Do generic drugs undergo Phase I-III trials? What do they require?

Answer 59

No. All they need is abbreviated bioequivalence studies. These are inexpensive, being conducted in a limited number of volunteers.Essentially the developer is trying to show that the generic drug produces the same plasma concentration vs. time profile as the patent product.

Question 60

How is bioequivalence measured in generic drugs?

Answer 60

measure AUC plasma drug levels in 24-36 healthy volunteers and compare with brand name drug. These types of studies must be repeated whenever the manufacturer changes a component of the drug product.

Question 61

Upon approval can anyone buy the drug? Why or why not?

Answer 61

Upon approval the new drug may only have been given to a few thousand people. Genetic diversity being what it is, there is a distinct possibility that safety has NOT been established in all genotypes.Hence, post-marketing review is essential to gain “confidence” that all is well in the “real world.”this is called Phase IV

Question 62

Physicians should be very wary of rushing to employ a new drug as soon as it comes on the market, especially if other agents are available to treat the given medical condition. One could argue that it is safer for them to wait for the collective experience to develop and the position of the new drug in the marketplace to be established.

Answer 62

Physicians should be very wary of rushing to employ a new drug as soon as it comes on the market, especially if other agents are available to treat the given medical condition. One could argue that it is safer for them to wait for the collective experience to develop and the position of the new drug in the marketplace to be established.

Question 63

Is adverse event reporting mandatory by law?

Answer 63

no but it is a vital, voluntary process in maintaining safety.MedWatch is a system employed for logging such events

Question 64

What is a black box warning?

Answer 64

Where a risk is identified, the FDA may require the issuance of a BLACK BOX WARNING. As the name implies this is essential information for the prescriber relating to the risk of serious or life- threatening adverse effects. It denotes restriction in use, increase risks for adverse events or prohibition of use with concurrent drugs.A black box warning is the STRONGEST WARNING that the FDA can require.

Question 65

What must a physician do to permit possession of and perscription of ‘controlled substances’?

Answer 65

To permit possession of and prescription of these agents a physician or pharmacist must apply for and be granted a DEA license. Both individuals have to comply with paperwork requirements.

Question 66

The highest schedule drug that can be legally prescribed is a Schedule __ agent.

Answer 66

II. Schedule I drugs have no legitimate clinical use of nationwide approval (heroin, LSD, marijuana, mescaline).

Question 67

Does the FDA monitor drug name?

Answer 67

Yes, it also tracks reports of errors in getting similarly named drugs and can require a name change

Question 68

Does the FDA currently require pharmacogenomic labeling?

Answer 68

Yes, the FDA requires pertinent pharmacogenomic information to be included in drug labeling to aid in physicians selecting appropriate drugs and doses.

Question 69

What kinds of pharmcogenomic information is typically included on labels?

Answer 69

description of polymorphic enzymesprevalence of alleles, genotypes, etc. and their effect on PK parameters, such as clearance, half life, and AUC

Question 70

How does the FDA monitor Direct To Consumer Advertising (DTCA)?

Answer 70

The FDA monitors print and electronic (TV) advertising and is now wrestling with the new media, like tweeting and text messaging.

Question 71

What is off-label use?

Answer 71

Drugs are approved by the FDA for specific indications, e.g. migraine, muscle spasm, etc. These are the only indications for which adverts can be produced. However, physicians can prescribe the drug for a legitimate medical use that has not been formally approved by the FDA and this is legitimate and legal.

Question 72

Can a drug company advertise off label uses?

Answer 72

No, this is illegal.

Question 73

Off label prescribing is usually done with what kind of medicine?

Answer 73

“Off-label” prescribing is most commonly done with older, generic medications that have found new uses but have not had the formal (and often costly) applications and studies required by the FDA to formally approve the drug for these new indications. However, there is usually extensive medical literature to support the off-label use.

Question 74

What are some types of permitted advertising?

Answer 74

1) product claim2) Reminder advertisements3) Help-seeking advertisements

Question 75

What are the requirements of product claim advertisements?

Answer 75

can give name, at least one FDA-approved use for the drug, most significant risks of the drug, and must present balanced description of the benefits and risks

Question 76

What are the requirements of reminder advertisements?

Answer 76

can give name, but not drug use, doesn’t contain risk information because the ad does not say what they drug does or how well it workscannot suggest, in words or pictures, anything about benefits or risksHowever, black box drugs must have risks addressed

Question 77

What are the requirements of help-seeking advertisements?

Answer 77

describe a disease or condition and does not recommend or suggest a specific drug treatment. Encouraging dialogue with a health care professional and gives telephone number.

Question 78

What are some reasons for drug recall?

Answer 78

lack of assurance of sterility, sub-potency, contamination of any kind (microbial, chemical), etc.

Question 79

What is an orphan drug?

Answer 79

a drug that doesn’t really have a market of patients because they target rare diseases so they are not produced often