R. Richle scite author profile

The late blood stages of the human malaria parasite, Plasmodium falciparum, carry a major surface antigen, p190, of molecular weight (Mr) 190,000. This antigenically variable protein is actively processed, first as the parasite matures and again when it is released into the blood stream and invades a new erythrocyte to initiate a cycle of growth. It elicits a strong immune response in man; all tested adult sera from endemic areas have antibodies against this protein. Our evidence indicates that purified p190 can alter the course of parasitaemia in monkeys with falciparum malaria. We have also succeeded in cloning part of the gene for p190 and expressing it in Escherichia coli. To this end we have developed a new technique, antibody select, which greatly simplifies final identification of expressing clones.

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Immunization with a Plasmodium falciparum merozoite surface antigen induces a partial immunity in monkeys.

Perrin¹,

Merkli²,

Gabra³

et al. 1985

J. Clin. Invest.

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Saimiri monkeys immunized with a Plasmodium falciparum merozoite polypeptide of 41 kD mol wt are resistant to a blood challenge infection that induces a fulminant infection in control monkeys. The sera of the immunized monkeys reacted, as shown by the indirect immunofluorescence technique, with the apical part of the merozoites from five isolates or clones of P. falciparum. Whether the immunogen was dissolved in nonionic detergent (NP-40) or in sodium dodecyl sulfate (SDS) had a marked influence on the level of protection in immunized monkeys. Thus, monkeys immunized with the antigen solubilized in a nonionic detergent developed much lower parasitemia than monkeys immunized with denatured antigen (antigen eluted from SDS polyacrylamide gel electrophoresis).

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Antimalarial immunity in Saimiri monkeys. Immunization with surface components of asexual blood stages.

Perrin¹,

Merkli²,

Loche³

et al. 1984

186

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Plasmodium falciparum polypeptides of 200 and 140 K mol wt exposed at the surface of merozoites and/or schizonts were purified by affinity chromatography and by electroelution from sodium dodecyl sulfate-polyacrylamide gel electrophoresis. Monkeys were separated into three groups of four and immunized either with one of the two polypeptides or with saline (control). After intravenous challenge with 2.5 X 10(7) P. falciparum asexual blood stages, two monkeys of the control group had to be treated and two recovered spontaneously after peak parasitemia of 9 and 11%. The four monkeys immunized with the 140 K polypeptide recovered without treatment after peak parasitemia between 1.5 and 4.5%. Monkeys immunized with the 200 K polypeptide had similar peak parasitemia except one monkey who suffered from a large skin excoriation and who recovered spontaneously after a peak parasitemia of 11%. Prechallenge sera of the immunized monkeys reacted only with the polypeptide used for immunization except for one serum of the 140 K group, which precipitated an additional polypeptide of 39 K, and a polypeptide of 31 K weakly precipitated by the four sera of monkeys immunized with the 200 K polypeptide. The relatedness between the 200 and 140 K polypeptides was investigated using tryptic digestion and reverse phase chromatography. No clear analogy was found between the two polypeptides, which suggests that immunization with either of two independent surface components of P. falciparum asexual blood stages is able to induce at least a partial protective immunity in immunized hosts.

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Mode of action of the 2-nitroimidazole derivative benznidazole

Polak

Richle

1978

Annals of Tropical Medicine & Parasitology

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The inhibitory effect of a drug combination on the development of mefloquine resistance inPlasmodium berghei

Merkli

Richle

Peters

1980

Annals of Tropical Medicine & Parasitology

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R. Richle

Major surface antigen gene of a human malaria parasite cloned and expressed in bacteria

Immunization with a Plasmodium falciparum merozoite surface antigen induces a partial immunity in monkeys.

Antimalarial immunity in Saimiri monkeys. Immunization with surface components of asexual blood stages.

Mode of action of the 2-nitroimidazole derivative benznidazole

The inhibitory effect of a drug combination on the development of mefloquine resistance inPlasmodium berghei

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