Plasmodium Falciparum Malaria Clinical Trial
Official title:
A Proof-of-concept Study to Assess the Effect of (+)-SJ000557733 (SJ733) Against Early Plasmodium Falciparum Blood Stage Infection in Healthy Participants
This is a single-centre, open-label, study using induced blood stage malaria (IBSM) infection
to characterize the activity of (+)-SJ000557733 or SJ733 for short, against early Plasmodium
falciparum blood stage infection. The study will be conducted in two cohorts (n=8 per
cohort). The anticipated efficacious dose range is expected to be within a range of 125 to
600 mg. The dose used in the first cohort was determined on the basis of the safety and PK
data generated in the FIM study (NCT02661373) currently ongoing in United States (US) and
will be 150 mg. Depending on the pharmacodynamics data (effect of SJ733 on parasitaemia)
obtained from this first cohort, the dose in Cohort 2 may be adjusted but will not exceed 600
mg. Based on the PK from all three cohort from the FIM study, the median estimated dose to
obtain the target SJ733 AUC of 13,000 (ug hr/L) is 370 mg. The dose of cohort 2 (≤600mg) is
intended to provide further concentration-response information in the human challenge model.
For Cohort 2 only, a second dose of SJ733 may be administered at peak gametocytaemia to
assess if SJ733 can reduce gametocytes and subsequent infectivity to mosquitoes (a washout of
~15 days post initial SJ733 treatment will be observed). Depending on the data obtained from
the first two cohorts, there may be a subsequent cohort, with the investigated dose of SJ733
to be determined by the Sponsor and Principal Investigator (PI) and endorsed by the Safety
Review Team. Should this third dose be investigated, a substantial amendment including
preliminary data from the first two cohorts will be submitted to the HREC for approval.
Each participant in the cohort will be inoculated on Day 0 with ~2,800 viable Plasmodium
falciparum-infected human erythrocytes (BSPC) administered intravenously. On an outpatient
basis, participants will be monitored daily via phone call and then will attend the clinic
daily (AM) from day 4 (until PCR positive for presence of malaria parasites). Once PCR
positive they will be monitored twice-daily, morning (AM) and evening (PM) until treatment,
for adverse events and the unexpected early onset of symptoms, signs or parasitological
evidence of malaria. Microscopic examination for evidence of parasitaemia may be conducted at
the discretion of the Investigator. On the day designated for commencement of treatment, as
determined by qPCR results, participants will be admitted to the study unit and monitored.
The threshold for commencement of treatment will be when PCR quantification of all
participants is ≥ 5,000 parasites/mL. If the PCR quantification of any participant is ≥ 5,000
parasites/mL, and is accompanied by a clinical symptom score >6, before all participants have
reached the treatment threshold (PCR quantification of ≥ 5,000), then treatment of that
participant will begin within a 24 h period.
Following treatment with SJ733, participants will be followed up as inpatients for at least
72 hours to ensure tolerance of the treatment and clinical response, then on an outpatient
basis if clinically well, for monitoring of safety and clearance of malaria parasites via
PCR. The plasma concentration-time profiles of SJ733 will be assessed from blood samples
collected pre-dose and then following administration of the treatment drug. Wherever
possible, PK sampling will coincide with post-dose blood collection for PCR monitoring of
parasitaemia.
Participants may also be evaluated for the presence of gametocytes in the blood, as
determined by qPCR (amplification of pfs25 gametocyte-specific transcript). Transmission
blocking activity of SJ733 in P. falciparum IBSM infection may be assessed if there are >500
parasites/ml (determined by 18S qPCR) verified as gametocytes by PCR for pfs25 and/or ring
stage marker as appropriate. Transmission studies may be undertaken by direct skin feeding
and/or indirect membrane feeding of mosquitoes. For indirect Membrane Feeding Assays (MFA),
blood will be collected from each participant for membrane feeds using Anopheles vector
mosquitoes. For direct skin feeding assays (DFA), participants will be escorted to the PC3
quarantine insectary facility at QIMR Berghofer Medical Research Institute and asked to allow
Anopheles vector mosquitoes to feed on the volar surface of their forearms, calves or thighs
for a period of 15±5 minutes. Microscopic examination for confirmation of gametocytaemia may
be conducted at the discretion of the Investigator.
If gametocytaemia is detected, in Cohort 2 only, a second same strength dose of SJ733 may be
administered on Day 23, to assess if SJ733 can reduce gametocytes and subsequent infectivity
to mosquitoes. To receive the second SJ733 dose, participants will have >500 parasites/ml
(determined by 18S qPCR) verified as gametocytes by PCR for pfs25 and/or ring stage marker as
appropriate. Membrane feeding and direct skin feeding may occur before and/or after this
second SJ733 dose. Participants receiving the second SJ733 dose will visit the study unit on
the morning of Day 23 for dosing and will be allowed to leave after ~10 hours. Participants
will have blood samples taken during this visit at time-points indicated in the protocol.
Compulsory commencement of treatment with Riamet® (artemether-lumefantrine) will occur 16
days (±3 days) post initial SJ733 treatment unless required earlier (Cohort 1 and Cohort 2 if
not given second SJ733 dose). If a second dose of SJ733 is given in Cohort 2, Riamet®
treatment will occur 11 days (± 3 days) post the second SJ733 treatment unless required
earlier. Early intervention can occur if either poor responses or fast responses are seen
following SJ733 treatment. This is to ensure participant safety and to avoid participant
inconvenience if useful data cannot be obtained. A poor response is defined as a decrease in
parasitaemia of less than 20% from baseline by 3 days post SJ733 treatment. A fast response
occurs when, within the seven day period, two consecutive PCR assessments in 48 hours are
negative. However, pre-emptive treatment with Riamet® can commence whenever deemed necessary
by the Investigator. Participants can be administered the curative Riamet® on site for
initial dosing followed by monitoring, either in clinic, or by telephone for three days to
ensure adherence to Riamet® therapy.
Participants will be treated with a single dose (45 mg) of primaquine (Primacin™) as
described in Section 4.3 in this protocol at the time of their Riamet® treatment if
gametocytes are identified, to ensure complete clearance of any gametocytes present.
Adverse events will be monitored via telephone monitoring, during confinement within the
clinical research unit, and on outpatient review following malaria challenge inoculation and
administration of the antimalarial treatment. Blood samples for safety evaluation, including
for LFT assessment, malaria monitoring, pharmacokinetic determination of drug levels in
plasma and/or blood, and red blood cell antibodies will be drawn at screening and/or baseline
and at nominated times after malaria challenge.
This study includes evaluation of optional, exploratory markers, which require separate
informed consent for participants agreeing to participate in any of these.
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