Clinical Trial Details
— Status: Completed
Administrative data
| NCT number |
NCT05487456 |
| Other study ID # |
P4-REXC-06 |
| Secondary ID |
|
| Status |
Completed |
| Phase |
N/A
|
| First received |
|
| Last updated |
|
| Start date |
July 15, 2022 |
| Est. completion date |
November 7, 2022 |
Study information
| Verified date |
June 2023 |
| Source |
Philip Morris Products S.A. |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
To demonstrate the reduction of Biomarkers of Exposure (BoExp) to selected harmful and
potentially harmful constituents (HPHC) in smokers switching from cigarette (CIG) to P4M3, an
Electronic Nicotine Delivery System (ENDS), compared to continuing cigarette smoking for 5
days.
Description:
Reduced HPHC Exposure in Cigarette Smokers Switching to P4M3 Generation 2.0 Compared to
Continuing Smoking, or Smoking Abstinence
- Who carried out the research? This research was sponsored and funded by Philip Morris
Products S.A.
- What public involvement there was in the study? Sixty-eight healthy, currently smoking,
adults participated in this study.
- Where and when the study took place? The study was conducted at a clinical trial
facility managed by a contract research organization in Belfast, Northern Ireland, from
July 15th to August 31st 2022.
- Why was the research needed? The research was needed to understand the reductions in
exposure to selected harmful and potentially harmful constituents of cigarette smoke in
healthy smokers, who switched exclusively to an electronic nicotine delivery system for
five days.
- What were the main questions studied? The study measured the reductions in exposure to
selected harmful and potentially harmful constituents of cigarette smoke in healthy
smokers switching exclusively to two flavour variants (CA35 and CM35) of P4M3, an
Electronic Nicotine Delivery System, compared to continued smoking of cigarettes or
abstaining from smoking.
- Who participated in the study? Sixty-eight healthy, male or female, adults aged between
21 and 65 years participated in this study. All participants were currently smoking. The
participants did not plan to quit using tobacco and/or nicotine products within the next
3 months and had smoked continuously for at least the last 3 years prior to joining the
study. Each participant was given full and adequate oral and written information about
the nature, purpose, possible risks, and benefits of the study. All participants
received information on the risks of smoking, smoking cessation advice and a briefing on
the P4M3 Electronic Nicotine Delivery System, for example, that its use is not
risk-free. Once each participant had received all the necessary information, and if they
agreed to participate, this was documented in an Informed Consent Form with the date,
time and signature of both the participant and the study doctor. Participants were
informed that they were free to withdraw from the study at any time.
- What treatments or interventions did the participants take/receive? Participants were
randomly assigned to one of four study groups: P4M3 CA35, P4M3 CM35, Cigarette, or
smoking abstinence, for five days in a confinement setting. Participants assigned to one
of the P4M3 arms or the Cigarette arm could use their assigned product at will and as
often as they desired during the five-day confinement period. Participants assigned to
the smoking abstinence arm had to abstain from cigarette smoking. Urine was collected
from each participant for harmful and potentially harmful constituent analysis, for each
24 hours, from Day 1 (i.e., the start of the confinement period) to Day 5 (until
discharge at the morning of Day 6). Participants were also asked to evaluate their
experience of using their assigned products, using the Product Evaluation Scale (PES)
questionnaire. The PES assessed the degree to which subjects experienced the
'reinforcing effects' of the use of P4M3 for both flavour variants in cigarette smokers
switching to P4M3 compared to subjects continuing cigarette smoking. The PES is composed
of five scales which address the degree to which participants experienced different
effects (Product Satisfaction, Psychological Rewards, Aversion, Enjoyment of respiratory
tract sensations, and Craving Reduction) as a result of using the P4M3 or the cigarette,
rated on a 7 point scale from 1 = "not at all" to 7 = "extremely."
- What medical problems (adverse reactions) did the participants have? Overall, during the
product use, 23 adverse reactions occurred in 17 participants, all of them being mild or
moderate in severity. Only one adverse reaction (oropharyngeal pain) was considered
related to an investigational product (P4M3 CM35) and occurred in just one participant.
There were no clinically significant findings in the physical examination, clinical
laboratory, vital signs, or ECG assessments in this study.
- What happened during the study? A presentation of P4M3 (without product use) was made to
the participants during the Screening visit. All participants received information on
the risks of smoking, smoking cessation advice, and a briefing that the use of P4M3 is
not risk-free. Eligible participants, fulfilling all criteria for participation,
returned to the investigational site for confirmation of eligibility at the Admission
visit (Day -2). On Day -2 (Admission), after eligibility criteria had been verified, all
eligible participants were enrolled and performed a product test using both P4M3 flavour
variants for a duration of approximately 10 minutes use per variant. After the product
test, subjects not willing to use P4M3 during the study were to be discontinued and be
replaced. Participants willing to continue their participation in the study started
their confinement period. On Day -1, participants were randomly assigned to one of four
arms: P4M3 CA35 variant; P4M3 CM35 variant; Cigarettes; Smoking Abstinence. Participants
were informed about their randomization arm by the study site staff on Day 1 prior to
the start of product use. The Exposure period in confinement began on Day 1 and
consisted of 5 days of at will use of the assigned product in the P4M3 and Cigarette
arms. Use of any tobacco/nicotine containing product other than the assigned product was
not allowed and, at the discretion of the study doctor, resulted in the participant's
discontinuation from the study. Participants allocated to the Smoking Abstinence arm had
to abstain from Cigarette smoking. Daily 24-hour urine was collected from Day 1 to Day 5
for harmful and potentially harmful constituent analysis. On Day 1, use of P4M3 or
Cigarette smoking in the respective arms was not supposed to start before the end of
24-hour urine collection of Day -1. The 24 hour urine collection period for Day 5 ended
in the morning of Day 6 prior to Discharge. On Day -1 and on Days 1 to 5, participants
completed questionnaires about product evaluation, craving, and liking assessments.
During the confinement period, site staff distributed assigned products to the
participants and recorded all distributed products in the participants' files. Any
participant who wanted to attempt to quit using any tobacco or nicotine-containing
product at any time during the study (that is, to quit P4M3 use or Cigarette smoking)
was encouraged to do so and was to be referred to appropriate medical services. This
decision would not affect the participant's financial compensation, and the participant
was to be considered as remaining in the study. The Exposure period to the assigned
investigational product (P4M3 or Cigarette) ended at 11:00 PM on Day 5, followed by
Discharge on Day 6 after completion of all study procedures. Participants were allowed
to smoke Cigarettes or use other tobacco or nicotine-containing products, at their
discretion, only after discharge from the study. After discharge at Day 6 or from the
day of an early termination, subjects entered a 3-day Safety follow-up period during
which any adverse reactions reported by the participants were collected. The follow-up
of adverse reactions ongoing at discharge was conducted by the investigational site.
- What were the results of the study? The results of this study demonstrated that
switching exclusively from cigarettes to the P4M3 electronic nicotine delivery system
for five days resulted in substantial reductions in exposure to the harmful and
potentially harmful constituents of cigarette smoke, while maintaining comparable levels
of nicotine exposure. The harmful and potentially harmful constituents of cigarette
smoke were examined by measuring their degradation products in participant's urine.
These degradation products are called Biomarkers of Exposure. As another Biomarker of
Exposure, the saturation of hemoglobin in the blood with carbon monoxide was measured.
The magnitude of reduction in the levels of Biomarkers of Exposure were comparable
between both variants of P4M3 (CA35 tobacco flavour and CM35 menthol flavour). The
reductions observed for most of the Biomarker of Exposure levels in the P4M3 arms, in
timing as well as in magnitude, approached those levels observed for smoking abstinence.
Furthermore, no additional safety concerns were associated with P4M3 compared to
cigarette smoking or smoking abstinence.
- How has this study helped patients and researchers? The participants in this study were
healthy, current cigarette smokers. All participants were informed about the health
risks associated with smoking and were given smoking cessation advice. Participants in
this clinical study benefited from repeated and detailed general health check-ups. This
clinical study may help doctors and scientists learn about electronic nicotine delivery
systems. The exposure period in confinement provided information on the exposure
reductions achievable for harmful and potentially harmful constituents in a
well-controlled environment with full control over daily P4M3 and/or Cigarette
consumption, compared to smoking abstinence.
- Details of any further research planned: There is currently no further research planned
with P4M3 Generation 2.0.
