Immunity to malaria using the rodent malaria parasite Plasmodium chabaudi chabaudi AS as a model of the human malaria Plasmodium falciparum

The role of IFN in acquisition of immunity against erythrocyte forms of P.c. chabaudi AS was studied. Inbred NIH mice given the construct 7 days before malaria infection, showed a significant delay in the onset and in the level of the recrudescent parasitaemia in comparison with controls. No differences, however, were observed in the recrudescent parasitaemia between the groups. NIH mice infected with malaria 3 days after or on the same day as the administration of the IFN construct, showed a primary peak of infection similar to controls, but the resolution of this patent parasitaemia occurred 1 or 2 days earlier in the experimental mice when compared with controls. In the same experiment, mice given the construct 10 days before malaria infection had a similar course of infection as controls. Simultaneous inoculation with two S. typhimurium constructs: IFN and TNF, 8 days before malaria infection resulted in a course of parasitaemia similar to that observed in mice given the IFN construct alone. On the other hand, inoculation of 'susceptible' inbred A/J mice with S. typhimurium/IFN 3 or 8 days before malaria infection had no effect on the course of the parasitaemia when compared with controls. The immune mechanisms involved in the better control of the malaria infection of NIH mice given S. typhimurium/ IFN, seem to be independent of nitric oxide (NO) production, since increased levels of the molecule were demonstrable around the peak of the primary parasitaemia in control groups but not in experimental mice. In the latter basal levels of serum NO were observed from the period after the S. typhimurium/ IFN inoculation until up to three days after the peak of the parasitaemia

Genotype comparison of Plasmodium vivax and Plasmodium falciparum clones from pregnant and non-pregnant populations in North-west Colombia

ABSTARCT: Placental malaria is the predominant pathology secondary to malaria in pregnancy, causing substantial maternal and infant morbidity and mortality in tropical areas. While it is clear that placental parasites are phenotypically different from those in the peripheral circulation, it is not known whether unique genotypes are associated specifically with placental infection or perhaps more generally with pregnancy. In this study, genetic analysis was performed on Plasmodium vivax and Plasmodium falciparum parasites isolated from peripheral and placental blood in pregnant women living in North-west Colombia, and compared with parasites causing acute malaria in non-pregnant populations. Methods: A total of 57 pregnant women at delivery with malaria infection confirmed by real-time PCR in peripheral or placental blood were included, as well as 50 pregnant women in antenatal care and 80 men or non-pregnant women with acute malaria confirmed by a positive thick smear for P. vivax or P. falciparum. Five molecular markers per species were genotyped by nested PCR and capillary electrophoresis. Genetic diversity and the fixation index FST per species and study group were calculated and compared. Results: Almost all infections at delivery were asymptomatic with significantly lower levels of infection compared with the groups with acute malaria. Expected heterozygosity for P. vivax molecular markers ranged from 0.765 to 0.928 and for P. falciparum markers ranged from 0.331 to 0.604. For P. vivax infections, the genetic diversity was similar amongst the four study groups and the fixation index from each pairwise comparison failed to show significant genetic differentiation. For P. falciparum, no genetic differentiation was observed between placental and peripheral parasites from the same woman at delivery, but the parasites isolated at delivery showed significant genetic differentiation compared with parasites isolated from subjects with acute malaria. Conclusions: In North-west Colombia, P. vivax parasites have high genetic diversity that is equivalent in pregnant and non-pregnant populations as well as in symptomatic and asymptomatic infections. For P. falciparum, the overall genetic diversity is lower, with specific genotypes associated with asymptomatic infections at delivery

Detection of submicroscopic infection with Plasmodium spp., using classical and molecular techniques in pregnant patients from Córdoba, Colombia

ABSTRACT: Gestational malaria affects both the mother and the development of her embryo or fetus. Rapid diagnosis and timely and effective treatment are required to prevent complications and deaths. Objective: To compare thick blood smear with nested PCR and real-time PCR (qRT-PCR) for the diagnosis of submicroscopic infections with Plasmodium falciparum and P. vivax. Methodology: 21 women with clinical manifestations of malaria, including both pregnant and non-pregnant, were studied in Puerto Libertador, Córdoba, Colombia. Peripheral blood specimens were obtained from all of them; umbilical cord and placenta blood specimens were taken in the pregnant ones. DNA was extracted and amplified for nested PCR or qRT-PCR. Statistical analysis was done using Graphpad PRISM and EPIDAT softwares. Results: The three techniques were satisfactory for the detection of Plasmodium falciparum and P. vivax in peripheral blood and in the umbilical cord and placenta specimens. Molecular tests were 100% sensitive and specific. Two submicroscopic cases of P. falciparum infection were detected with the two PCR techniques. Conclusion: qRT-PCR is advantageous over nested PCR because its standardization is shorter, it requires lesser infrastructure and it allows the quantification of DNA.RESUMEN: La malaria gestacional afecta a las madres y al embrión o feto en desarrollo; requiere diagnóstico rápido y tratamiento oportuno y efectivo para evitar las complicaciones y muertes. Objetivo: comparar las técnicas de gota gruesa, PCR anidada y PCR en tiempo real (qRT-PCR), para diagnosticar infecciones submicroscópicas por Plasmodium falciparum y P. vivax. Metodología: se estudiaron 21 mujeres con manifestaciones clínicas de malaria, incluyendo gestantes y no gestantes, en Puerto Libertador, Córdoba, Colombia; de todas se obtuvieron muestras de sangre periférica y, en las gestantes, de placenta y cordón umbilical. Se extrajo el ADN y se lo amplificó por PCR anidada y cuantitativa (qRT-PCR). Para el análisis estadístico se usaron los programas Graphpad PRISM y EPIDAT. Resultados: las tres técnicas diagnosticaron satisfactoriamente la presencia de P. falciparum y P. vivax en sangre periférica, cordón y placenta. Las pruebas moleculares presentaron sensibilidad y especificidad del 100%; dos casos de infección por P. falciparum no identificados por gota gruesa (submicroscópicos) se diagnosticaron con las dos técnicas de PCR. Conclusión: la qRT-PCR es ventajosa en comparación con la PCR anidada porque su estandarización es más corta, requiere menos infraestructura y permite cuantificar el ADN

Now ICT malaria Pf/Pv ® versus microscopy (thick-smear, thin smear) for diagnosis of malaria in Urabá (Colombia)

ABSTRACT: To date, there are only three reports from Colombia about the malaria diagnostic test Now ICT Malaria Pf / Pv ® (NowICT). The results from these studies showed major differences in sensitivity and specificity. Objective: To evaluate the diagnostic performance of NowICT compared to thick smear for the diagnosis of Plasmodium infection in matched blood samples from mothers (maternal peripheral blood), umbilical cord and placenta. Methods: We used a closed (blinded/masked) and parallel design for the evaluation of a diagnostic test. The sample size was calculated with statistical and epidemiological parameters; this consisted of 131 thick smears from maternal peripheral blood. Blood samples from placenta and umbilical cord were also studied (386 samples tested in total). Results: The sensitivity of Now ICT for detection of P. vivax was below 70% in any of the samples (maternal blood, placental blood or cord blood). The specificity was greater than 99%. Values for P. falciparum infection were not calculated since too few cases were detected. Conclusions: Now ICT Malaria Pf / Pv ® is not a useful diagnostic tool in Colombia since the sensitivity for the most frequent species in the country, P. vivax, is poor. This interpretation is consistent with the WHO’s general conclusions about the state of development of rapid diagnostic tests for malaria.RESUMEN: Solo conocemos tres informes para Colombia de la prueba diagnóstica de malaria Now ICT Malaria Pf/Pv ® (NowICT); esos estudios tuvieron resultados de sensibilidad y especificidad muy diferentes. Objetivo: evaluar la capacidad diagnóstica de NowICT frente a la gota gruesa para el diagnóstico de infección plasmodial en sangres periférica materna, del cordón umbilical y placentaria. Metodología: diseño paralelo y enmascarado para evaluación de una prueba diagnóstica. El tamaño de la muestra se calculó con parámetros epidemiológicos y estadísticos y fue de 131 muestras de sangre periférica materna; también se examinaron sendas muestras de sangre placentaria y de cordón umbilical. Resultados: se evaluaron en total 386 muestras. La sensibilidad de NowICT para P. vivax no alcanzó 70% en ninguna de las fuentes (madre, placenta, cordón). La especificidad mínima fue de 99%. Los valores para P. falciparum no se calcularon porque los casos fueron pocos. Conclusión: Now ICT malaria Pf/Pv® no es una herramienta diagnóstica útil en Colombia porque su sensibilidad para P. vivax es muy deficiente y en el país esta especie es la que predomina en la generación de malaria en humanos. Esta interpretación concuerda con las conclusiones generales de la OMS sobre el estado de desarrollo de las pruebas diagnósticas rápidas para malaria

Functional antibodies against VAR2CSA in nonpregnant populations from Colombia exposed to Plasmodium falciparum and Plasmodium vivax

RESUMEN: En el embarazo, se observa inmunidad dependiente de la paridad en respuesta a la infección placentaria con Plasmodium falciparum. Los anticuerpos reconocen el antígeno de superficie, VAR2CSA, expresado en glóbulos rojos infectados e inhiben la citoadherencia al tejido placentario. En la mayoría de los entornos de endemicidad del paludismo, los anticuerpos contra VAR2CSA se observan predominantemente en las mujeres multigravidias y con poca frecuencia en hombres, niños y mujeres nulligráficas. Sin embargo, en Colombia, se detectaron anticuerpos contra múltiples constructos de VAR2CSA entre hombres y niños con infección aguda por P. falciparum y Plasmodium vivax. La mayoría de los hombres y niños (> 60%) tenían altos niveles de IgG contra tres dominios recombinantes de VAR2CSA: DBL5ε, DBL3X e ID1-ID2. Sorprendentemente, estos anticuerpos se observaron sólo en mujeres embarazadas, hombres y niños expuestos a P. falciparum oa P. vivax. Además, los anticuerpos anti-VAR2CSA son de alta avidez e inhiben eficazmente la adherencia de glóbulos rojos infectados al condroitín sulfato A in vitro, lo que sugiere que son específicos y funcionales. Estos resultados inesperados sugieren que puede haber diferencias genotípicas o fenotípicas en los parásitos de esta región o en la respuesta del huésped a la infección por P. falciparum o P. vivax fuera del embarazo. Estos hallazgos pueden tener relevancia clínica significativa para la fisiopatología y el resultado de las infecciones de malaria en esta región.ABSTRACT: In pregnancy, parity-dependent immunity is observed in response to placental infection with Plasmodium falciparum. Antibodies recognize the surface antigen, VAR2CSA, expressed on infected red blood cells and inhibit cytoadherence to the placental tissue. In most settings of malaria endemicity, antibodies against VAR2CSA are predominantly observed in multigravid women and infrequently in men, children, and nulligravid women. However, in Colombia, we detected antibodies against multiple constructs of VAR2CSA among men and children with acute P. falciparum and Plasmodium vivax infection. The majority of men and children (>60%) had high levels of IgGs against three recombinant domains of VAR2CSA: DBL5ε, DBL3X, and ID1-ID2. Surprisingly, these antibodies were observed only in pregnant women, men, and children exposed either to P. falciparum or to P. vivax. Moreover, the anti-VAR2CSA antibodies are of high avidity and efficiently inhibit adherence of infected red blood cells to chondroitin sulfate A in vitro, suggesting that they are specific and functional. These unexpected results suggest that there may be genotypic or phenotypic differences in the parasites of this region or in the host response to either P. falciparum or P. vivax infection outside pregnancy. These findings may hold significant clinical relevance to the pathophysiology and outcome of malaria infections in this region

Malaria: Efficacy of Mefloquine According to Nutritional Status and Alellic Variations of the CYP3A4 Gen

RESUMEN: Introducción: hay poca información sobre las relaciones entre la falla de la terapia antimalárica y algunos factores del hospedero (estado nutricional, fenotipo y genotipo del citocromo CYP450 que metaboliza el medicamento antipalúdico). Objetivo: explorar si la falla terapéutica de la mefloquina dada a pacientes con malaria falciparum no complicada se puede explicar por la influencia del estado nutricional del enfermo y del fenotipo y genotipo de su citocromo CYP3A4. Materiales y métodos: estudio de casos y controles no pareado. Pacientes: hombres y mujeres adultos, de Turbo y El Bagre (Antioquia, Colombia). Resultados: se evaluó la respuesta terapéutica en 46 enfermos; hubo solo tres fallas (6,5%); por la muy baja ocurrencia de falla terapéutica (n = 3/46), los resultados se presentan en forma descriptiva para los 46 pacientes. La relación dextrometorfano/3-metoximorfinano fue 0,39 (mediana); 20% fueron metabolizadores lentos. Las concentraciones sanguíneas medianas de mefloquina a las 24 horas (C24h) y al día 14 (Cd14) fueron 1.363 + 397 ng/mL y 978 + 106 ng/mL, respectivamente. Los 46 pacientes presentaron el alelo CYP3A4*2 (silvestre). Conclusión: no se pudo evaluar con profundidad la relación entre la respuesta a la terapia antimalárica, por una parte y, por otra, la actividad del CYP450 y el estado nutricional, pero hubo hallazgos que justifican la evaluación y control de las características del hospedero en estudios posteriores de farmacocinética antimalárica.ABSTRACT: Introduction: Information on the relationship between treatment failure in malaria and factors of the host (nutritional status, phenotype and genotype of cytochrome CYP450) involved in the metabolism of antimalarials is scarce. Objective: To explore whether treatment failure of mefloquine administered to patients with noncomplicated falciparum malaria can be explained in terms of the patient’s nutritional status and the CYP3A4 phenotype and genotype. Materials and methods: Non-matched case-control study. Patients were adult males and females, inhabitants of Turbo and El Bagre (Antioquia, Colombia). Results: The therapeutic response was assessed in 46 patients, and there were only three failures (6.5%); due to the rare occurrence of therapeutic failure (n = 3/46), results are presented in a descriptive way for the 46 patients. The dextrometorphan/3-methoxymorphinan ratio was 0.39 (median); 20% of the patients were slow metabolizers. The blood concentrations of mefloquine at 24 hours (C24h) and at day 14 (Cd14) were (median) 1.363 ± 397 ng/mL and 978 ± 106 ng/mL, respectively. All 46 patients had the wild CYP3A4*2 allele. Conclusion: We were unable to assess in depth the relationship between the response to mefloquine, on the one hand and, on the other, CYP450 activity and nutritional status. However, there were findings that justify the assessment and control of the characteristics of the host in subsequent studies of antimalarial pharmacokineti

Eficacia de tres esquemas con Cloroquina – Primaquina para el tratamiento de la malaria por Plasmodium vivax en Colombia

Plasmodium vivax malaria is an important cause of morbility in Central and South America. In Colombia this is the most prevalent malaria infection representing 75 % of the reported cases. To define the efficacy of the chloroquine and primaquine regimen to eliminate hypnozoites and prevent relapses, we a conducted a random controlled clinical trial of three primaquine regimens in an open-label study. We evaluated the anti-relapse efficacy of a total primaquine dose of 45, 105 and 210 mg administered at 15mg/day in 210 adults with P. vivax infection from the Northwestern region of Colombia. Cure rates for blood stage vivax malaria by day 28 of followup were 100 % in all groups. Post-treatment reappearance of parasitaemia during the 6 months of following up was 45 %, 36,6 % and 17,6 % respectively, for each group. When compared to other groups, administration of 210 mg was a significant protection factor for reappearance of parasitaemia in an endemic area.L a malaria por Plasmodiun vivax es una de las principales causas de morbilidad en centro y sur América. En Colombia es la más prevalente y representa el 75 % de los casos reportados. La primaquina (PQ) es la única droga disponible de uso clínico para eliminar los hipnozoitos y prevenir recaídas en la malaria por P. vivax. Se hizo un ensayo clínico aleatorio controlado sin placebo y no ciego. Se estudió la eficacia antirrecaída de tres esquemas de tratamiento con dosis total de PQ (45, 105 y 210 mg) suministrados en dosis de 15 mg/día, en 210 adultos con diagnóstico de P. vivax en dos municipios de Antioquia (Colombia). Todos los pacientes recibieron una dosis total de 1.500 mg de cloroquina [CQ] en tres días (600 mg el día 1 y 450 mg los días 2 y 3). Los pacientes tuvieron una respuesta clínica adecuada del 100 % al tratamiento CQ+PQ hasta el día 28, en los tres grupos. El porcentaje de recurrencias durante los seis meses de seguimiento fue de 45 %, 36,6 % y 17,6 % para los grupos con 45, 105 y 210 mg de PQ respectivamente. El tratamiento convencional (210 mg) fue un factor de protección para las recurrencias cuando se comparó con los esquemas de 45 y 105 mg respectivamente. El tratamiento convencional sigue siendo el tratamiento más eficaz para prevenir las recaídas en la malaria por P. vivax en una zona endémica