Clinical Trial Details
— Status: Completed
Administrative data
| NCT number |
NCT05252845 |
| Other study ID # |
MAL22001 |
| Secondary ID |
MR/T006161/1 |
| Status |
Completed |
| Phase |
Phase 2
|
| First received |
|
| Last updated |
|
| Start date |
January 4, 2023 |
| Est. completion date |
September 18, 2023 |
Study information
| Verified date |
October 2023 |
| Source |
University of Oxford |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
Malaria remains one of the leading causes of morbidity and mortality worldwide. Plasmodium
falciparum is a complex pathogen with numerous immune evasion mechanisms which has added
layers of complexity to the development of safe and protective vaccines. There remains an
urgent need to identify and develop more protective and more affordable vaccine candidates
that could achieve the World Health Organization (WHO) goal of 75% efficacy against clinical
malaria.
R21 is a novel pre-erythrocytic candidate malaria vaccine. R21 includes Hepatitis B surface
antigen (HBsAg) fused to the C-terminus and central repeats of the circumsporozoite protein
of P. falciparum (CSP), which self-assemble into virus-like particles in yeast. R21 lacks the
excess HBsAg found and comprises only fusion protein moieties.
R21/MatrixM (MM) had a favourable safety profile and was well tolerated. The majority of
adverse events were mild, with the most common event being fever. None of the serious adverse
events were attributed to the vaccine. At one year, vaccine efficacy remained high, at 77%.
Participants vaccinated with R21/MM showed high titres of malaria-specific anti-
Asn-Ala-Asn-Pro (NANP) antibodies 28 days after the third vaccination, which were almost
doubled with the higher adjuvant dose. Titres waned but were boosted to levels similar to
peak titres after the primary series of vaccinations after a fourth dose administered one
year later.
Currently, there are no safety and immunogenicity data for the use of R21/MatrixM in Asian
populations. This trial will generate the required data for the use of this vaccine in Asia.
For integration with the current targeted malaria elimination (TME) activities, which provide
mass drug administrations at months M0, M1, and M2, it would be most efficient and practical
to provide the vaccine at the same intervals.
In summary: The investigators propose to conduct a safety and immunogenicity trial of
R21/MatrixM in Thai adults. The major aims of this study are to 1) assess the safety and
immunogenicity of R21/MatrixM in Thai adults 2) confirm that the co-administration of
antimalarial drugs with the malaria vaccine R21/MatrixM does not reduce the immunogenicity of
the vaccine and 3) assess the absorption and pharmacokinetics of antimalarial drugs
piperaquine, and a single low dose of primaquine (SLDPQ) when co-administered with
R21/MatrixM.
This is a randomized, open label, single centre, Phase 2 study. 120 healthy non-pregnant Thai
adults, aged 18-55 years, inclusive, will be recruited.
Each participant will be randomized into one of the following study arms in a ratio of 5:5:2,
as follows:
1. R21/MatrixM + Dihydroartimisinin (DHA)-Piperaquine (PIP)+ primaquine (PQ) (Group 1,
n=50) will receive R21/MatrixM + 3 doses DHA-PIP+PQ at Month 0, Month 1 and Month 2
2. R21/MatrixM only (Group 2, n=50) will receive R21/MatrixM standard dose at Month 0,
Month 1 and Month 2
3. DHA-PIP+PQ only (Group 3, n=20) will receive 3 doses DHA-PIP+PQ at Month 0, Month 1 and
Month 2
Description:
This is a randomized, open label, single centre, Phase 2 study.
Screening and eligibility assessment (Screening visit) All potential volunteers will have a
screening visit, which may take place up to 30 days prior to enrolment. Once informed consent
is given, a screening number will be assigned in sequential order. Screening numbers will be
issued consecutively (e.g. R21-001, R21-002, R21-003, …)
Enrolment, baseline assessment, regimen allocation, and first vaccination (Month 0 / Day 0
visit; Baseline visit) All inclusion and exclusion criteria will be checked before enrolment
in the study. Physical examination will be performed. Any new medical issues or symptoms that
have arisen will be assessed. Blood will be collected for baseline P. falciparum testing,
haemoglobin and biochemistry. Participants with parasitaemia or anaemia will be treated
according to national guidelines. Blood will be collected and stored for measurement of
antibodies against P. falciparum circumsporozoite (anti-circumsporozoite antibody) until
shipment to the reference laboratory. Urine will be collected from women of child-bearing age
for immediate pregnancy test.
Enrolment, baseline assessment, regimen allocation, and first vaccination (Month 0 / Day 0
visit; Baseline visit)
All inclusion and exclusion criteria will be checked before enrolment in the study. Physical
examination will be performed. Any new medical issues or symptoms that have arisen will be
assessed. Blood will be collected for baseline P. falciparum testing, haemoglobin and
biochemistry. Blood will be collected and stored for measurement of antibodies against P.
falciparum circumsporozoite (anti-circumsporozoite antibody) until shipment to the reference
laboratory. Urine will be collected from women of child-bearing age for immediate pregnancy
test.
If all inclusion criteria are fulfilled and none of the exclusion criteria apply, the patient
will be enrolled into the study and a case record form (CRF) specific to each participant
completed. Regimen allocation and administration of the vaccine(s) will be on Day 0. The
randomization lists will be prepared by Mahidol-Oxford Tropical Medicine Research Unit
(MORU).
Randomization numbers will be generated in blocks, for the 3 study arms in a ratio of 5:5:2,
as follows:
- R21/MatrixM + DHA-PIP+PQ (Group 1)
- R21/MatrixM alone (Group 2)
- DHA-PIP+PQ alone (Group 3)
Study participants will be assigned the next available randomization number on the list, and
thus will be randomly allocated to Group 1, 2, or 3. This is an open-label study.
Participants and clinical investigators will not be blinded to group allocation.
Subjects will then be vaccinated by intramuscular (IM) needle injection into the deltoid
region of the arm. Subjects in Groups 1 and 3 will also receive anti-malarial medications.
The study participants will be observed closely for at least 30 minutes following the
administration of each study vaccine, with appropriate medical treatment readily available in
case of an anaphylactic reaction.
Subsequent vaccination visits (Month 1 / Day 0 and Month 2 / Day 0 visits)
Physical examination will be performed. Any new medical issues or symptoms that have arisen
will be assessed. Blood will be collected for P. falciparum testing. Participants with
parasitaemia or anaemia will be treated according to national guidelines. Blood will be
collected and stored for measurement of antibodies against P. falciparum circumsporozoite
(anti-circumsporozoite) until shipment to the reference laboratory. Urine will be collected
from women of child-bearing age for immediate pregnancy test.
Before vaccination, the on-going eligibility of the volunteer will be reviewed. All
participants will attend the clinic for vaccination visits, will be observed closely for at
least 30 minutes following the administration of each study vaccine.
Follow up assessments
Follow-up assessments (visits not involving vaccination) will be done at month 3 and month 6
after the first vaccination.
Blood tests
Blood will be drawn at the time points indicated in the schedule of procedures and the
following laboratory assays performed:
At screening:
- Haematology: haemoglobin (Hb), leukocytes (white blood cells [WBC]) and platelets (PLT).
- Biochemistry: alanine aminotransferase (ALT), aspartate aminotransferase (AST) and
creatinine (CREA).
- Diagnostic serology: HBsAg, HCV antibodies, HIV antibodies (Counselling will be given
prior to testing blood for these blood-borne viruses)
- P. falciparum testing
At M0, D0: P. falciparum testing, Haematology: Hb, WBC, PLT, Biochemistry: ALT, AST, CREA,
anti-circumsporozoite antibody; Pharmacokinetics (piperaquine and primaquine drug levels will
be assessed if additional data are required) At M0, D1: Pharmacokinetics (piperaquine and
primaquine drug levels) At M0, D2: Pharmacokinetics (piperaquine drug levels) At M0, D7:
Haematology: Hb, WBC, PLT; Biochemistry: ALT, AST, CREA; Pharmacokinetics (piperaquine drug
levels) At M1, D0: P. falciparum testing, anti-circumsporozoite antibody; Pharmacokinetics
(piperaquine drug levels) At M1, D1: Pharmacokinetics (piperaquine and primaquine drug
levels) At M1, D2: Pharmacokinetics (piperaquine drug levels) At M1, D7: Haematology: Hb,
WBC, PLT; Biochemistry: ALT, AST, CREA; Pharmacokinetics (piperaquine drug levels) At M2, D0:
P. falciparum testing, anti-circumsporozoite antibody; Pharmacokinetics (piperaquine drug
levels) At M2, D1: Pharmacokinetics (piperaquine and primaquine drug levels) At M2, D2:
Pharmacokinetics (piperaquine drug levels) At M2, D7: Haematology: Hb, WBC, PLT;
Biochemistry: ALT, AST, CREA; Pharmacokinetics (piperaquine drug levels) At M3: P. falciparum
testing, Haematology: Hb, WBC, PLT; Biochemistry: ALT, AST, CREA; anti-circumsporozoite
antibody At M6: P. falciparum testing, anti-circumsporozoite antibody
