Safety, Attenuation and Immunogenicity of GAP3KO Administered Via A Stephensi Mosquitoes

This single arm, open-label, phase 1 safety study is designed to evaluate the safety and
tolerability of a genetically attenuated P. falciparum (GAP3KO) that arrests early in the
liver stage of the parasite life cycle. The study will also confirm the attenuation of the
GAP3KO parasites using peripheral blood smears. The secondary objectives of the study are to
evaluate the humoral immune responses to GAP3KO.

A total of 10 healthy, malaria-naïve adult subjects will be enrolled to receive GAP3KO via
the bite of 150-200 GAP3K0-infected A. stephensi mosquitoes under controlled conditions.
Subjects will be evaluated for safety, reactogenicity, and signs and symptoms of malaria to
confirm attenuation for 28 days, including monitoring in a hotel setting 8-18 days post GAP
3KO administration.

Inclusion Criteria:

- Good general health

- No hematologic, hepatic, or renal disease

- Weight greater than 50 kg

- Assessment of Understanding completed and passed prior to enrollment

- Availability and reliable access to trial center

- Females must use two forms of pregnancy prevention

Exclusion Criteria:

- Recent (within 6 months) or planned travel to malaria endemic area

- History of confirmed malaria diagnosis

- Anticipated use of the following:

- Investigational malaria vaccine at any time

- Malaria chemoprophylaxis within 6 months

- Chronic systemic immunosuppressive medications within 6 months

- Blood products or immunoglobulin within 120 days

- Systemic antibiotics with antimalarial effects within 30 days

- Investigational product or vaccine within 30 days

- Live vaccine within 28 days; killed vaccine within 14 days of GAP3KO

- Medications known to significantly interact with chloroquine or Malarone

- History of:

- Sickle cell trait or other hemoglobinopathies

- Splenectomy or functional asplenia

- Systemic anaphylaxis

- Severe allergic reaction to mosquito bites or malaria treatment drugs

- History of chronic or active neurologic disease

- Cardiac disease or stroke

- Clinically significant medical condition, abnormal lab results

- Clinically significant abnormal ECG

- Moderate or high risk for coronary heart disease

- Acute illness

- Pregnant or nursing female

- HIV, Hepatitis B, or Hepatitis C

- Psychiatric condition that precludes compliance with the protocol

- Suspected or known alcohol or drug abuse

- Staff with direct involvement in conduct of the study or GAP activities