US RAC Review Questions RAPS Modules
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questions with answers |\ |\
In which situation is an IND not required?
|\ |\ |\ |\ |\ |\ |\
A) You intend to conduct a clinical trial with an investigational
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\
new drug|\
B) You intend to conduct a clinical trial with an approved drug to
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\
support a marketing application for a new indication
|\ |\ |\ |\ |\ |\ |\
C) You intend to collect blood samples from subjects to look for
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\
biomarkers or pharmacogenetic information |\ |\ |\
D) You intend to conduct a clinical trial using 2 of your approved
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\
drugs in a new combination - CORRECT ANSWERS ✔✔C) You
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\
intend to collect blood samples from subjects to look for
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\
biomarkers or pharmacogenetic information |\ |\ |\
In the clinical development plan for an investigational
|\ |\ |\ |\ |\ |\ |\ |\
antihypertensive drug, which of the following studies would |\ |\ |\ |\ |\ |\ |\ |\
typically be conducted first:
|\ |\ |\
A) 1 month repeat dose toxicology study
|\ |\ |\ |\ |\ |\
B) Single dose escalation PK study in healthy volunteers
|\ |\ |\ |\ |\ |\ |\ |\
C) Multiple dose PK study in healthy volunteers
|\ |\ |\ |\ |\ |\ |\
D) Single dose escalation study in hypertensive patients -
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CORRECT ANSWERS ✔✔B) Single dose escalation PK study in
|\ |\ |\ |\ |\ |\ |\ |\ |\
healthy volunteers |\
,A sponsor must report an unexpected, fatal or life-threatening
|\ |\ |\ |\ |\ |\ |\ |\ |\
experience believed to be associated with an unapproved |\ |\ |\ |\ |\ |\ |\
drug/biologic:
|\
A) to FDA, investigators and IRBs within 7 calendar days
|\ |\ |\ |\ |\ |\ |\ |\ |\
B) to FDA and investigators within 7 calendar days
|\ |\ |\ |\ |\ |\ |\ |\
C) to FDA within 14 calendar days
|\ |\ |\ |\ |\ |\
D) to FDA and investigators within 7 working days - CORRECT
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\
ANSWERS ✔✔B) to FDA and investigators within 7 calendar days
|\ |\ |\ |\ |\ |\ |\ |\ |\
Which of the following is a covered study as defined under
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\
Financial Disclosure regulations: |\ |\
A) Phase I dose escalation study
|\ |\ |\ |\ |\
B) Phase I/II Pharmacokinetic Study
|\ |\ |\ |\
C) A large open label safety study conducted at a large number
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\
of study sites
|\ |\
D) Phase III pivotal study - CORRECT ANSWERS ✔✔D) Phase III
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\
pivotal study |\
Your company is developing a product to treat a serious and life
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\
threatening disease. A clinically meaningful, well established |\ |\ |\ |\ |\ |\ |\
primary endpoint will be used in the pivotal studies. Which
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\
regulatory strategy might you select prior to commencing Phase
|\ |\ |\ |\ |\ |\ |\ |\ |\
3 studies?
|\
,A) Request Special Protocol Assessment
|\ |\ |\ |\
B) Request Fast Track Designation
|\ |\ |\ |\
C) Request Priority Review
|\ |\ |\
D) Approval under Subpart H, Accelerated Approval of New Drugs
|\ |\ |\ |\ |\ |\ |\ |\ |\
for Serious or Life Threatening Illnesses - CORRECT ANSWERS
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\
✔✔A) Request Special Protocol Assessment
|\ |\ |\ |\
As a regulatory affairs professional, you are responsible for
|\ |\ |\ |\ |\ |\ |\ |\ |\
developing the content of an information package for a Type B |\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\
meeting with FDA. Your primary objective is to:|\ |\ |\ |\ |\ |\ |\
A) Reach consensus on content from contributing team members
|\ |\ |\ |\ |\ |\ |\ |\
B) Ensure content is sufficient to support meeting objective(s)
|\ |\ |\ |\ |\ |\ |\ |\ |\
and questions to FDA
|\ |\ |\
C) Provide appropriate preclinical summary
|\ |\ |\ |\
D) Provide appropriate clinical summary - CORRECT ANSWERS
|\ |\ |\ |\ |\ |\ |\ |\
✔✔B) Ensure content is sufficient to support meeting objective(s)
|\ |\ |\ |\ |\ |\ |\ |\
and questions to FDA
|\ |\ |\ |\
You, a regulatory affairs professional, are assessing the
|\ |\ |\ |\ |\ |\ |\ |\
information to be submitted in support of a marketing application |\ |\ |\ |\ |\ |\ |\ |\ |\
for a new dosage form for a listed drug. You lack right of
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\
reference to one key preclinical report. Which type of application
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\
will you prepare for submission?
|\ |\ |\ |\
A) 505 (b) (1)
|\ |\ |\
B) 505 (b) (2)
|\ |\ |\
, C) 505 (j)
|\ |\
D) PMA - CORRECT ANSWERS ✔✔B) 505 (b) (2)
|\ |\ |\ |\ |\ |\ |\ |\
8) If FDA were to invoke the Application Integrity Policy, which of
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\
the following is a possible outcome?
|\ |\ |\ |\ |\
A) Defer review of pending application(s)
|\ |\ |\ |\ |\
B) "File" a marketing application at the 60 day review
|\ |\ |\ |\ |\ |\ |\ |\ |\
C) Grant a waiver or deferral for pediatric clinical study
|\ |\ |\ |\ |\ |\ |\ |\ |\
D) Approve a marketing application - CORRECT ANSWERS ✔✔A)
|\ |\ |\ |\ |\ |\ |\ |\ |\
Defer review of pending application(s)
|\ |\ |\ |\
9) Which of the following supplements to an approved NDA/BLA
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\
must be approved by FDA prior to distributing product made
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\
using the change? |\ |\
A) Make change(s) to comply with USP
|\ |\ |\ |\ |\ |\
B) Change in the technical grade of an excipient, same
|\ |\ |\ |\ |\ |\ |\ |\ |\
specifications and use |\ |\
C) Add a warning statement to prescribing information
|\ |\ |\ |\ |\ |\ |\
D) Process change outside the validated range - CORRECT
|\ |\ |\ |\ |\ |\ |\ |\ |\
ANSWERS ✔✔D) Process change outside the validated range
|\ |\ |\ |\ |\ |\ |\
10) Which of the following products would not be regulated by
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\
CDER?
|\ |\ |\ |\ |\ |\
questions with answers |\ |\
In which situation is an IND not required?
|\ |\ |\ |\ |\ |\ |\
A) You intend to conduct a clinical trial with an investigational
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\
new drug|\
B) You intend to conduct a clinical trial with an approved drug to
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\
support a marketing application for a new indication
|\ |\ |\ |\ |\ |\ |\
C) You intend to collect blood samples from subjects to look for
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\
biomarkers or pharmacogenetic information |\ |\ |\
D) You intend to conduct a clinical trial using 2 of your approved
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\
drugs in a new combination - CORRECT ANSWERS ✔✔C) You
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\
intend to collect blood samples from subjects to look for
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\
biomarkers or pharmacogenetic information |\ |\ |\
In the clinical development plan for an investigational
|\ |\ |\ |\ |\ |\ |\ |\
antihypertensive drug, which of the following studies would |\ |\ |\ |\ |\ |\ |\ |\
typically be conducted first:
|\ |\ |\
A) 1 month repeat dose toxicology study
|\ |\ |\ |\ |\ |\
B) Single dose escalation PK study in healthy volunteers
|\ |\ |\ |\ |\ |\ |\ |\
C) Multiple dose PK study in healthy volunteers
|\ |\ |\ |\ |\ |\ |\
D) Single dose escalation study in hypertensive patients -
|\ |\ |\ |\ |\ |\ |\ |\ |\
CORRECT ANSWERS ✔✔B) Single dose escalation PK study in
|\ |\ |\ |\ |\ |\ |\ |\ |\
healthy volunteers |\
,A sponsor must report an unexpected, fatal or life-threatening
|\ |\ |\ |\ |\ |\ |\ |\ |\
experience believed to be associated with an unapproved |\ |\ |\ |\ |\ |\ |\
drug/biologic:
|\
A) to FDA, investigators and IRBs within 7 calendar days
|\ |\ |\ |\ |\ |\ |\ |\ |\
B) to FDA and investigators within 7 calendar days
|\ |\ |\ |\ |\ |\ |\ |\
C) to FDA within 14 calendar days
|\ |\ |\ |\ |\ |\
D) to FDA and investigators within 7 working days - CORRECT
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\
ANSWERS ✔✔B) to FDA and investigators within 7 calendar days
|\ |\ |\ |\ |\ |\ |\ |\ |\
Which of the following is a covered study as defined under
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\
Financial Disclosure regulations: |\ |\
A) Phase I dose escalation study
|\ |\ |\ |\ |\
B) Phase I/II Pharmacokinetic Study
|\ |\ |\ |\
C) A large open label safety study conducted at a large number
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\
of study sites
|\ |\
D) Phase III pivotal study - CORRECT ANSWERS ✔✔D) Phase III
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\
pivotal study |\
Your company is developing a product to treat a serious and life
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\
threatening disease. A clinically meaningful, well established |\ |\ |\ |\ |\ |\ |\
primary endpoint will be used in the pivotal studies. Which
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\
regulatory strategy might you select prior to commencing Phase
|\ |\ |\ |\ |\ |\ |\ |\ |\
3 studies?
|\
,A) Request Special Protocol Assessment
|\ |\ |\ |\
B) Request Fast Track Designation
|\ |\ |\ |\
C) Request Priority Review
|\ |\ |\
D) Approval under Subpart H, Accelerated Approval of New Drugs
|\ |\ |\ |\ |\ |\ |\ |\ |\
for Serious or Life Threatening Illnesses - CORRECT ANSWERS
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\
✔✔A) Request Special Protocol Assessment
|\ |\ |\ |\
As a regulatory affairs professional, you are responsible for
|\ |\ |\ |\ |\ |\ |\ |\ |\
developing the content of an information package for a Type B |\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\
meeting with FDA. Your primary objective is to:|\ |\ |\ |\ |\ |\ |\
A) Reach consensus on content from contributing team members
|\ |\ |\ |\ |\ |\ |\ |\
B) Ensure content is sufficient to support meeting objective(s)
|\ |\ |\ |\ |\ |\ |\ |\ |\
and questions to FDA
|\ |\ |\
C) Provide appropriate preclinical summary
|\ |\ |\ |\
D) Provide appropriate clinical summary - CORRECT ANSWERS
|\ |\ |\ |\ |\ |\ |\ |\
✔✔B) Ensure content is sufficient to support meeting objective(s)
|\ |\ |\ |\ |\ |\ |\ |\
and questions to FDA
|\ |\ |\ |\
You, a regulatory affairs professional, are assessing the
|\ |\ |\ |\ |\ |\ |\ |\
information to be submitted in support of a marketing application |\ |\ |\ |\ |\ |\ |\ |\ |\
for a new dosage form for a listed drug. You lack right of
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\
reference to one key preclinical report. Which type of application
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\
will you prepare for submission?
|\ |\ |\ |\
A) 505 (b) (1)
|\ |\ |\
B) 505 (b) (2)
|\ |\ |\
, C) 505 (j)
|\ |\
D) PMA - CORRECT ANSWERS ✔✔B) 505 (b) (2)
|\ |\ |\ |\ |\ |\ |\ |\
8) If FDA were to invoke the Application Integrity Policy, which of
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\
the following is a possible outcome?
|\ |\ |\ |\ |\
A) Defer review of pending application(s)
|\ |\ |\ |\ |\
B) "File" a marketing application at the 60 day review
|\ |\ |\ |\ |\ |\ |\ |\ |\
C) Grant a waiver or deferral for pediatric clinical study
|\ |\ |\ |\ |\ |\ |\ |\ |\
D) Approve a marketing application - CORRECT ANSWERS ✔✔A)
|\ |\ |\ |\ |\ |\ |\ |\ |\
Defer review of pending application(s)
|\ |\ |\ |\
9) Which of the following supplements to an approved NDA/BLA
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\
must be approved by FDA prior to distributing product made
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\
using the change? |\ |\
A) Make change(s) to comply with USP
|\ |\ |\ |\ |\ |\
B) Change in the technical grade of an excipient, same
|\ |\ |\ |\ |\ |\ |\ |\ |\
specifications and use |\ |\
C) Add a warning statement to prescribing information
|\ |\ |\ |\ |\ |\ |\
D) Process change outside the validated range - CORRECT
|\ |\ |\ |\ |\ |\ |\ |\ |\
ANSWERS ✔✔D) Process change outside the validated range
|\ |\ |\ |\ |\ |\ |\
10) Which of the following products would not be regulated by
|\ |\ |\ |\ |\ |\ |\ |\ |\ |\ |\
CDER?
