Ischemic Stroke Clinical Trial
Official title:
A Phase I Single-Center, Randomized, Double-Blind, Placebo-Controlled Study in Healthy Volunteers to Evaluate the Safety, Tolerability, and Pharmacokinetics of Escalating Single Doses and Multiple Doses of SP-8203
Phase I study in health volunteers to assess the safety, tolerability and pharmacokinetics of escalating single doses and multiple doses of SP-8203
This is a Phase I, single-center, randomized, double-blind, placebo-controlled study of the
safety, tolerability, and PK of escalating single doses and multiple doses of SP 8203 in
healthy adult male and female subjects.
In the SAD Part, the first cohort of 8 subjects will be randomly assigned to receive a single
IV dose of either SP-8203 (n=6) or placebo (n=2). Following medical review of safety, PK, and
biomarker data, subsequent cohorts of 8 new subjects will receive higher single doses of
SP-8203 (6 subjects) or placebo (2 subjects). Dose escalation will continue until a single
MTD of SP-8203 is identified. If a single-dose MTD is not defined within the projected dose
range, additional cohorts of 8 subjects may be added to receive higher doses to achieve the
objectives of the study. Alternate doses may be administered following medical review of the
results of each cohort.
In the MAD Part of the study the first cohort of 8 subjects will receive a single dose of SP
8203 every day and 1 subject will receive a single dose of placebo every day for 7
consecutive days. Doses will be administered at the same time (± 15 minutes) every day.
Following medical review of all safety and biomarker data, subsequent cohorts of 7 drug-naive
subjects will receive higher single doses of SP-8203 (6 subjects) or placebo (2 subject)
every day for 7 consecutive days. Study drug dose-escalation will continue until a
multiple-dose MTD regimen of SP-8203 is identified. If a multiple-dose MTD is not defined
within this range, additional cohorts of 8 subjects may be added to achieve the objectives of
the study. Alternate doses and/or dosing regimens may be administered following medical
review of the safety, biomarker, and PK results of the SAD Part, and prior cohorts in the MAD
Part of the study.
The MTD will be defined as the highest dose that does not lead to unacceptable toxicity in
one or more subjects based on the frequency, nature, and severity of AEs or other safety
parameter abnormalities. The Investigator, Sponsor, and Medical Monitor will jointly assess
the general safety and tolerability of each dose based on available data prior to escalating
to the next higher dose. Successive higher doses will be administered only if previous doses
are adequately tolerated. Intermediate doses may be tested, or a dose level may be repeated,
as appropriate, depending on the safety profile observed.
Each subject will complete Screening, Baseline, Treatment, and Follow-Up Phases. The
Screening Phase will be conducted on an outpatient basis within 30 days, but no sooner than 3
days, prior to the start of the Baseline Phase. The Baseline Phase will consist of admission
to the CRU and final qualification assessments.
In the SAD Part, the Treatment Phase will consist of dosing (after which subjects will be
considered enrolled in the study), postdose safety assessments, and blood and urine
collection for the next 48 hours. Subjects will be discharged approximately 48 hours after
study drug administration, provided all available assessments are clinically acceptable to
the Investigator, and will return for follow-up assessments 2-4 days later. In the MAD Part,
The Treatment Phase will last for 9 days following the first dose. Subjects will be dosed
each morning for 7 consecutive days. Safety assessments will be made, and blood and urine
will be collected prior to, and at prescribed intervals postdose, over the next 9 consecutive
days. Subjects will be discharged approximately 48 hours following the last dose, and will
return for follow-up assessments 2-4 days later.
Safety will be evaluated by physical examination, by evaluation of vital signs, 12 lead ECG,
Holter monitoring, clinical laboratory blood and urine test results, and AE assessments.
Blood samples for determining plasma concentrations of SP 8203 and its metabolites,
assessments of Mn-SOD mRNA, and FRAP biomarkers will be obtained immediately prior to dosing
and at prescribed intervals during the Treatment Phase. Urine samples will be collected
predose and pooled urine samples will be collected postdose for determination of SP 8203
renal clearance and metabolites.
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