MCQ Quiz: Surrogate Endpoints

In clinical trials, endpoints are used to measure the effects of a therapy. While a true clinical endpoint directly measures how a patient feels, functions, or survives, researchers often use surrogate endpoints as a substitute. For PharmD students, the ability to critically evaluate clinical literature requires a deep understanding of the validity, application, and limitations of surrogate endpoints, especially in fields like oncology where they are commonly used.

1. A surrogate endpoint in a clinical trial is best defined as:

• A direct measure of how a patient feels, functions, or survives
• A laboratory measure or physical sign used as a substitute for a clinically meaningful endpoint
• An endpoint that is only used in Phase 1 trials
• A measure of the cost-effectiveness of the therapy

Answer: A laboratory measure or physical sign used as a substitute for a clinically meaningful endpoint

2. Which of the following is considered the “gold standard” clinical endpoint in most oncology clinical trials?

• Tumor response rate
• Progression-Free Survival (PFS)
• Overall Survival (OS)
• Biomarker normalization

Answer: Overall Survival (OS)

3. A primary advantage of using a surrogate endpoint in a clinical trial is that it can:

• Always perfectly predict the effect on the true clinical endpoint
• Allow for a trial to be completed more quickly and with fewer patients
• Eliminate the placebo effect
• Provide a direct measure of patient quality of life

Answer: Allow for a trial to be completed more quickly and with fewer patients

4. In a hypertension trial, a change in blood pressure is often used as a surrogate endpoint for the true clinical endpoint of:

• Stroke or myocardial infarction
• Serum creatinine
• Patient-reported dizziness
• The cost of the medication

Answer: Stroke or myocardial infarction

5. Progression-Free Survival (PFS) in an oncology trial is defined as the length of time that a patient:

• Lives after starting treatment, regardless of disease status
• Lives with the disease without it getting worse
• Experiences a complete disappearance of the tumor
• Remains on the study drug without any side effects

Answer: Lives with the disease without it getting worse

6. A major limitation or “divorce” discussed in oncology literature is when a drug improves a surrogate like PFS but fails to improve:

• The tumor response rate
• The drug’s palatability
• Overall Survival (OS)
• The patient’s white blood cell count

Answer: Overall Survival (OS)

7. For a surrogate endpoint to be considered valid, it must:

• Be easy and inexpensive to measure
• Be on the causal pathway of the disease
• Accurately predict the effect on the clinical endpoint
• Be a novel biomarker

Answer: Accurately predict the effect on the clinical endpoint

8. Which of the following is a direct measure of clinical benefit, and therefore NOT a surrogate endpoint?

• Lowering LDL cholesterol
• Reducing viral load in HIV
• Preventing death from cardiovascular disease
• Shrinking a tumor

Answer: Preventing death from cardiovascular disease

9. The use of surrogate endpoints can lead to what potential regulatory outcome?

• A delay in the drug approval process
• Accelerated approval of a drug by the FDA
• A requirement for longer and larger clinical trials
• The immediate generic availability of the drug

Answer: Accelerated approval of a drug by the FDA

10. “Response Rate” in an oncology trial, a common surrogate endpoint, typically measures the proportion of patients whose:

• Tumors shrink by a certain amount
• Quality of life improves
• Survival is extended by five years
• White blood cell count returns to normal

Answer: Tumors shrink by a certain amount

11. A key challenge when interpreting a trial that uses only a surrogate endpoint is the:

• Certainty that the results translate to meaningful patient benefit
• Uncertainty about whether the observed effect on the surrogate will lead to a real clinical benefit
• Simplicity of the statistical analysis
• Fact that these trials are always double-blind

Answer: Uncertainty about whether the observed effect on the surrogate will lead to a real clinical benefit

12. In diabetes trials, a reduction in HbA1c is a surrogate endpoint for:

• The prevention of long-term microvascular complications
• The immediate cure of diabetes
• The cost of insulin
• Patient satisfaction with treatment

Answer: The prevention of long-term microvascular complications

13. Why might a drug improve Progression-Free Survival (PFS) but not Overall Survival (OS)?

• The drug has significant toxicity that counteracts the benefit of delaying progression
• Patients receive effective subsequent therapies after progressing on the study drug
• The delay in progression is not long enough to impact survival
• All of the above

Answer: All of the above

14. When critically appraising a clinical trial, a pharmacist should always question the ________ of the surrogate endpoint used.

• color
• name
• validity
• cost

Answer: validity

15. The “applicability to clinical practice” of a trial that relies on a surrogate endpoint depends heavily on:

• The strength of the association between the surrogate and the true clinical endpoint
• The number of patients enrolled in the trial
• The reputation of the journal in which it was published
• The cost of the study drug

Answer: The strength of the association between the surrogate and the true clinical endpoint

16. A drug could lower a patient’s cholesterol (surrogate endpoint) but fail to reduce heart attacks (clinical endpoint) if the drug:

• Has an off-target effect that increases cardiovascular risk, like raising blood pressure
• Is too inexpensive
• Is too effective at lowering cholesterol
• Has no side effects

Answer: Has an off-target effect that increases cardiovascular risk, like raising blood pressure

17. The evaluation of surrogate endpoints is a key topic in courses on:

• Clinical trial evaluation and evidence-based practice
• Sterile compounding
• Pharmacy law
• The history of pharmacy

Answer: Clinical trial evaluation and evidence-based practice

18. In HIV/AIDS treatment, a reduction in viral load is a well-accepted surrogate endpoint for:

• Curing the HIV infection
• Delaying the progression to AIDS and improving survival
• The cost of antiretroviral therapy
• The patient’s adherence to the medication

Answer: Delaying the progression to AIDS and improving survival

19. What is a primary reason for the “divorce” between response rate and overall survival in oncology?

• Tumor shrinkage does not always translate into a longer life, especially if it is not durable or if the tumor becomes resistant
• Response rate is a direct measure of survival
• All tumors that shrink will eventually be cured
• Response rate is more difficult to measure than survival

Answer: Tumor shrinkage does not always translate into a longer life, especially if it is not durable or if the tumor becomes resistant

20. A pharmacist explaining trial results to a physician should be careful to:

• Equate a change in a surrogate endpoint with a proven clinical benefit
• Differentiate between a statistically significant change in a surrogate endpoint and a proven clinical benefit
• Ignore the endpoint that was used in the trial
• Focus only on the p-value of the primary endpoint

Answer: Differentiate between a statistically significant change in a surrogate endpoint and a proven clinical benefit

21. Which of the following is a true clinical endpoint?

• Bone mineral density
• Prevention of a hip fracture
• Serum lipid levels
• Blood glucose levels

Answer: Prevention of a hip fracture

22. The main appeal of using PFS as a primary endpoint in an oncology trial is that:

• It occurs earlier than death, allowing for faster trial results
• It is a direct measure of patient quality of life
• It is less expensive to measure than overall survival
• It is not affected by subsequent lines of therapy

Answer: It occurs earlier than death, allowing for faster trial results

23. The concept of “clinical outcomes” is a fundamental part of:

• Evidence-based medicine
• Pharmaceutical calculations
• Drug compounding
• Pharmacy informatics

Answer: Evidence-based medicine

24. A drug receives accelerated approval based on a surrogate endpoint. What is typically required by the FDA post-approval?

• A confirmatory trial to verify the drug’s effect on a true clinical endpoint
• No further studies are needed
• A trial comparing the drug to placebo in healthy volunteers
• A price reduction for the medication

Answer: A confirmatory trial to verify the drug’s effect on a true clinical endpoint

25. A key question a pharmacist should ask when evaluating a trial based on a surrogate is:

• How well-established is the link between this surrogate and a meaningful patient outcome?
• Is the surrogate endpoint easy to pronounce?
• Was the trial sponsored by a large pharmaceutical company?
• How many authors are on the paper?

Answer: How well-established is the link between this surrogate and a meaningful patient outcome?

26. A patient-reported outcome (PRO) that measures symptoms or quality of life is considered a:

• Surrogate endpoint
• Clinical endpoint
• Biomarker
• Pharmacokinetic parameter

Answer: Clinical endpoint

27. In some cases, a significant improvement in PFS can be considered:

• A clinically meaningful benefit on its own, even if OS is not improved
• An irrelevant finding in all circumstances
• A sign that the drug is not effective
• A reason to stop the clinical trial early for futility

Answer: A clinically meaningful benefit on its own, even if OS is not improved

28. The use of surrogate endpoints is most common in trials for:

• Chronic diseases where the true clinical endpoint may take years to occur
• Acute conditions that resolve quickly
• Healthy volunteers
• Non-pharmacological interventions

Answer: Chronic diseases where the true clinical endpoint may take years to occur

29. The main focus of the reading “Irreconcilable Differences” is the frequent disconnect between:

• Response rates, PFS, and Overall Survival
• Phase 1 and Phase 2 clinical trials
• The cost of a drug and its efficacy
• Pharmacists and physicians

Answer: Response rates, PFS, and Overall Survival

30. When a new drug is approved based on a surrogate endpoint, pharmacists play a crucial role in:

• Monitoring for the drug’s real-world effect on clinical outcomes
• Recommending the drug for all patients regardless of indication
• Ignoring the post-marketing surveillance data
• Assuming the drug is curative for the disease

Answer: Monitoring for the drug’s real-world effect on clinical outcomes

31. Which of these is a surrogate endpoint?

• Stroke
• Heart attack
• CD4 cell count in HIV
• Death

Answer: CD4 cell count in HIV

32. A potential bias when measuring Progression-Free Survival is that:

• It is an objective measure with no room for interpretation
• The timing and frequency of tumor assessments can influence the results
• It can only be measured at the end of a patient’s life
• It is not affected by imaging technology

Answer: The timing and frequency of tumor assessments can influence the results

33. An ideal surrogate endpoint should capture the ________ effect of a treatment on the clinical endpoint.

• opposite
• net
• partial
• unrelated

Answer: net

34. The FDA’s acceptance of a surrogate endpoint for a specific disease is based on:

• The biological plausibility of the relationship
• Epidemiological evidence
• Evidence from clinical trials
• All of the above

Answer: All of the above

35. A pharmacist reading a clinical trial abstract should first identify:

• The primary endpoint of the study and whether it is a clinical or surrogate endpoint
• The names of all the study investigators
• The statistical software that was used for the analysis
• The location where the study was conducted

Answer: The primary endpoint of the study and whether it is a clinical or surrogate endpoint

36. Overall Survival (OS) is considered a robust clinical endpoint because it is:

• Easy to measure and not subject to interpretation bias
• A subjective measure reported by the patient
• The earliest endpoint to occur in a trial
• The best measure of tumor shrinkage

Answer: Easy to measure and not subject to interpretation bias

37. When counseling a patient about a new drug approved based on a surrogate endpoint, it is important to convey:

• That the drug is guaranteed to make them live longer
• That the drug has been shown to improve a marker related to their disease, and studies on long-term benefit are ongoing
• That the drug has no known side effects
• That the drug is still considered experimental and should not be taken

Answer: That the drug has been shown to improve a marker related to their disease, and studies on long-term benefit are ongoing

38. The “Prentice criteria” are a set of statistical conditions used for what purpose?

• To validate a surrogate endpoint
• To calculate a p-value
• To randomize patients in a clinical trial
• To determine the cost of a drug

Answer: To validate a surrogate endpoint

39. A focus on surrogate endpoints is a key component of understanding:

• Drug literature evaluation
• Non-sterile compounding
• Pharmacy calculations
• Health informatics

Answer: Drug literature evaluation

40. If a trial shows a drug improves a surrogate endpoint but worsens quality of life, the drug’s overall value is:

• Clearly established
• Questionable
• Not relevant to the pharmacist
• Guaranteed to be high

Answer: Questionable

41. The use of surrogate endpoints is driven by a need for more ________ drug development and approval.

• expensive
• lengthy
• efficient
• complicated

Answer: efficient

42. Which of the following best describes the relationship between a surrogate endpoint and a clinical outcome?

• The surrogate is intended to be a predictor of the clinical outcome
• The clinical outcome is a predictor of the surrogate endpoint
• The two are completely independent of each other
• The surrogate endpoint is always a more reliable measure

Answer: The surrogate is intended to be a predictor of the clinical outcome

43. A pharmacist must be cautious when a new drug’s marketing focuses exclusively on its effect on a(n):

• Validated clinical endpoint
• Unvalidated surrogate endpoint
• Overall survival
• Quality of life measure

Answer: Unvalidated surrogate endpoint

44. In a trial for osteoporosis, bone mineral density (BMD) is a common surrogate endpoint for what?

• The clinical endpoint of fractures
• The cost of calcium supplements
• Patient-reported pain
• The patient’s height

Answer: The clinical endpoint of fractures

45. The “divorce” between surrogate and clinical endpoints highlights the importance of:

• Relying solely on surrogate endpoints for all clinical decisions
• Critical appraisal of the evidence and not over-interpreting surrogate data
• Disregarding all clinical trials that use surrogate endpoints
• Trusting all conclusions presented in a research paper

Answer: Critical appraisal of the evidence and not over-interpreting surrogate data

46. A lecture on surrogate endpoints in oncology would likely emphasize the difference between:

• PFS and OS
• Phase 1 and Phase 4 trials
• Intravenous and oral chemotherapy
• Benign and malignant tumors

Answer: PFS and OS

47. The primary reason a trial might choose PFS over OS as its primary endpoint is:

• OS is a less important outcome to patients
• PFS events (progression or death) occur more frequently and earlier than death alone
• PFS is a more objective measure than OS
• The FDA no longer accepts OS as a valid endpoint

Answer: PFS events (progression or death) occur more frequently and earlier than death alone

48. Evaluating the “applicability to clinical practice” requires a pharmacist to consider if the trial’s endpoints are:

• Statistically significant
• Relevant and meaningful to their own patient population
• Easy to measure in the lab
• Novel and previously unpublished

Answer: Relevant and meaningful to their own patient population

49. An understanding of surrogate endpoints is most critical when evaluating trials for what type of drugs?

• Drugs with a long history of established clinical benefit
• Drugs seeking accelerated approval based on early data
• Over-the-counter medications
• Generic drugs seeking approval based on bioequivalence

Answer: Drugs seeking accelerated approval based on early data

50. The ultimate goal when using a surrogate endpoint is that an improvement in the surrogate will:

• Lead to a tangible, beneficial effect on how a patient feels, functions, or survives
• Increase the cost of the drug
• Make the drug more difficult to administer
• Have no correlation with the patient’s actual health status

Answer: Lead to a tangible, beneficial effect on how a patient feels, functions, or survives

G S Sachin

I am a Registered Pharmacist under the Pharmacy Act, 1948, and the founder of PharmacyFreak.com. I hold a Bachelor of Pharmacy degree from Rungta College of Pharmaceutical Science and Research. With a strong academic foundation and practical knowledge, I am committed to providing accurate, easy-to-understand content to support pharmacy students and professionals. My aim is to make complex pharmaceutical concepts accessible and useful for real-world application.

Mail- Sachin@pharmacyfreak.com