Delimitação ecológica dos anofelíneos do subgênero Kerteszia na região costeira do sul do Brasil

The present work is part of the studies carried out by the Serviço Nacional de Malária in cooperation with technicians of the Instituto Oswaldo Cruz in coastal region of Southern Brazil, from 1949 to 1953. in view of the floristic unity existing among the associations studied in the various working stations, distributed at random and somewhat far from each other, and considering that the identity of those associations has been established, the authors suggest the generalization of the problem "bromeliad - kerteszia" in similar associations of the remaining pluvial formation in the southern coast of Brazil. The present contribution is an attempt to the bio-ecological maping of the three malaria vectors responsible for the widespread malaria outbreaks in the southern coastal region of Brazil.

O comportamento dos Anofelinos do subgênero Kerteszia, no sul do Brasil e o efeito do inseticida DDT

Informações sobre o comportamento dos Kerteszia obtidas nos Estados de São Paulo, Paraná e Santa Catarina, foram comparadas entre si e com dados relativos a outros anofelinos neotrópicos e etiópicos. Das conclusões obtidas destacam-se: 1. Em seguida ao pôr do sol os Kerteszia tornam-se mais ativos nas copas das árvores da mata a ao anoitecer, quando começam a se inverter as diferenças microclimáticas existentes entre a floresta e ao ar livre, passam a predominar nas áreas abertas; 2. nas localidades não dedetizadas não existe grande diferença entre a proporção dos Kerteszia que se alimenta dentro das casas e a que tem sido observada para o A. gambiae, na África. Entretanto, memso antes do aparecimento do DDT, os Kerteszia não eram mosquitos endófilos. Para os anofelinos ditos zoófilos, como o A. strodei, a relação entre o número de mosquitos capturados simultaneamente no peridomicílio e dentro de casa, é pelo menos duas vezes mais elevada; 3. Alguns dados sobre a ação impedidora ('deterrency") do DDT, para os kerteszia, mostram que ela é elevadíssima, outros são da mesma ordem de grandeza dos observados para o A. gambiae. Foi verificado que os Kerteszia evitam entrar mesmo em casas com muito pouco inseticida; 4. Apenas uma pequena proporção dos Kerteszia, que se alimenta dentro das casas, pousa nas paredes; a maioria voa diretamente para as pessoas e depois para fora. O tempo de permanência nas superfícies dedetizadas é o mesmo que tem sido observado para outros anofelinos, geralmente inferior a 10 minutos; 5. Ao contrário da maioria dos transmissores de malária a atividade dos Kerteszia, fora da mata, concentra-se nas primeiras horas da noite, quando há maior probabilidade de existir pessoas fora de casa; 6. o estudo do contato homem-mosquito ("man-bitting rate") mostrou que, mesmo nas casas não dedetizadas, esse contato é quase sempre maior fora dos domicilios. Nas localidades dedetizadas a componente externa, desse contato, pode ser até 10 vezes mais elevada. O que, logicamente, resulta do horário de atividade; 7. Os trabalhos de profilaxia do antigo Serviços Nacional de Malária já haviam mostrado que, mesmo com distribuição de medicamentos, essa diminuição dos contatos homem-mosquito dentro das casas e a ação tóxica do inseticida, são suficientes para impedir a transmissão da malária. Fato que, juntamente com os dados das capturas extradomiciliares, sugere a realização de pesquisas visando encontrar medidas capazes de diminuir a densidade dos kerteszia nas áreas freqüentadas pela população humana.

Efeito da dieta láctea na supressão da parasitemia e no desenvolvimento da imunidade humoral durante o curso da infecção malárica em camundongos

Estudou-se o efeito da dieta láctea, por um período de 150 dias em camundongos infectados com diferentes números das formas sangüíneas de Plasmodium berghei, e observou-se o desenvolvimento da imunidade humoral nestes animais pela dosagem das imunoglobulinas das classes IgG e IgM no soro, usando o teste de imunofluorescência indireta. Os resultados indicam que a administração do leite, como único alimento em camundongos, protege-os cotnra infecção malárica fatal, independentemente do número de parasitas inoculados. Os animais desenvolveram altos níveis de anticorpos IgG, os quais persistiram no soro por longo período de tempo. Contudo, os anticorpos IgM somente foram detectáveis no soro durante as primeiras duas semanas de infecção. O P. berghei continua presente na circulação periférica, após dois meses de infecção, uma vez que o sangue destes animasi inoculados em camundongos mantidos em dieta norma, produziu infecção fatal nos recipientes. No entanto, ao exame microscópico não foi possível detectar o parasita da malária no sangue periférico destes animais. O protozoário esteve presente no baço e fígado dos camundongos durante todo o tempo de duração da pesquisa. A presença contínua do P. berghei nestes animais, em nível de infecção subclínica, ofereceu ao hospedeiro o desenvolvimento de uma imunidade sólida contra subseqüente infecção. Esta imunidade adquirida esteve presente, nestes animais, até cinco meses após a infecção.

Mosquitos no Parque Nacional da Serra dos Orgãos, Estado do Rio de Janeiro, Brasil: II. Distribuição vertical

Em prosseguimento aos estudos sobre a ecologia de culicídeos que vimos realizando no Parque Nacional da Serra dos Orgãos (PNSO), apresentamos nesta oportunidade a sua distribuição vertical. Por meio de capturas feitas em isca humana concomitantemente ao nível do solo e nas imediações da copa das árvores, estabelecemos as tendências das espécies que ali ocorreram de março de 1981 a fevereiro de 1982, por se alimentarem de sangue na copa da floresta ou junto ao solo. A distribuição é analisada comparativamente em ambos os níveis levando-se em consideração as variações de temperatura, umidade, precipitações pluviométricas e estações do ano. Dentre as espécies com nítida preferência à acrodendrofilia encontramos alguns importantes transmissores de doenças: Anopheles cruzii - malária humana e simiana; Culex nigripalpus - encefalite de São Luis (SLE); Haemagogus leucocelaenus e Haemagogus capricornii - febre amarela silvestre, todas também sendo obtidas, embora em menor número, a nível do solo. Os sabetíneos - Wyeomyia Knabi, Phoniomyia theobaldi, Sabethes tarsopus, Sabethes quasicyaneus, Sabethes chloropterus - completam a relação das principais espécies que preferem a copa. Por outro lado, Aedes fluviatilis, Trichoprosopon digitatum, Tr. similis, Tr. frontosus, Tr. theobaldi, Wy, arthrostigma, Wy. aporonoma, Wy. personata, Wy undulata, Wy. mystes, Limatus durhami, Li. pseudomethisticus, Sa. identicus e Sa. undosus foram capturados em grande maioria próximo ao solo.

Effects of immigration on the prevalence of malaria in rural areas of the Amazon basin of Brazil

Epidemiological studies were conducted on malaria in three rural areas of the Amazon basin in the State of Rondônia: the town of Costa Marques, Forte Príncipe da Beira (Fort), and an immigrant settlement in the nearby forest. These studies were instituted to document the malaria problem and to describe the role of immigration on its distribution and prevalence. Hospital records in the town show that the number of malaria cases increased five fold from 1983 to 1987 and that the predominant malaria parasite changel from Plasmodium vivax to P. falciparum. Increased malaria followed increased immigration and colonization of the forest. A series of epidemiologic studies suggested the linkage between malaria and immigration as the prevalence of malaria was 1-2% at the Fort, a stable community, 8-9% at Costa Marques, a growing community, and 14-26% in the new settlements in the forest.

Malaria vaccine development using synthetic peptides as a technical platform.

The review covers the development of synthetic peptides as vaccine candidates for Plasmodium falciparum- and Plasmodium vivax-induced malaria from its beginning up to date and the concomitant progress of solid phase peptide synthesis (SPPS) that enables the production of long peptides in a routine fashion. The review also stresses the development of other complementary tools and actions in order to achieve the long sought goal of an efficacious malaria vaccine.

Kinetics of antigen specific and non-specific polyclonal B-cell responses during lethal Plasmodium yoelii malaria

In order to study the kinetics and composition of the polyclonal B-cell activation associated to malaria infection, antigen-specific and non-specific B-cell responses were evaluated in the spleens of mice infected with Plasmodium yoelii 17 XL or injected with lysed erythrocytes or plasma from P. yoelii infected mice or with P. falciparum culture supernatants. Spleen/body weigth ratio, numbers of nucleated spleen cells and Immunoglobulin-containing and Immunoglobulin-secreting cells increased progressively during the course of infection,in parallel to the parasitemia. A different pattern of kinetics was observed when anti-sheep red blood cell and anti-trinitrophenylated-sheep red blood cell plaque forming cells response were studied: maximum values were observed at early stages of infection, whereas the number of total Immunoglobulin-containing and Immunoglobulin-secreting cells were not yet altered. Conversely, at the end of infection, when these latter values reached their maximum, the anti-sheep red blood cell and anti-trinitrophenylated-sheep red blood cell specific responses were normal or even infranormal. In mice injected with Plasmodium-derived material, a higher increase in antigen-specific PFC was observed, as compared to the increase of Immunoglobulin-containing and Immunoglobulin-secreting cell numbers. This suggested a "preferential" (antigen-plus mitogen-induced) stimulation of antigen-specific cells rather than a generalized non-specific (mitogen-induced) triggering of B-lymphocytes. On the basis of these and previous results, it is suggested that polyclonal B-cell activation that takes place during the course of infection appears as a result of successive waves of antigen-specific B-cell activation.

Malaria seroepidemiology: comparison between indirect fluorescent antibody test and enzyme immunoassay using bloodspot eluates

Blood sampling on filter paper is a current practice seroepidemiological studies by indirect fluorescent antibody test (IFAT). There is, however, scant comparative information about the use of bloodspot eluates for detection of malarial IgG antibodies simultaneously by IFAT and enzyme immunoassay (ELISA). Here we report data obtained by both serological methods done on 219 bloodspot eluate samples collected in a rural community in Brazilian Amazon Basin (Alto Paraíso, Ariquemes municipality) where malaria is endemic. Plasmodium falciparum and P. vivax thick smear antigens were used in the IFAT; a detergent-soluble P. falciparum antigen was prepared for ELISA. Substantial agreement of results (Kappa coefficient k = 0.686) was observed when P. falciparum antigen was used in both tests, and IFAT titers were found to be strongly correlated ELISA antibody units (Spearman correlation coeficient rs = 0.818, p < 0.0001). Only moderate agreement (k = 0.467) between IFAT with P. vivax antigen and ELISA with P. falciparum antigen was observed. Spearman correlation coefficient value between quantitative results (IFAT titers and ELISA antibody units) in this case was numerically lowe (rs = 0.540, p < 0.0001). Our results suggest that, with P. falciparum antigen, both IFAT and ELISA performed on bloodspot eluates are equivalent for seropidemiological purposes.

A malaria merozoite surface protein (MSP1)-structure, processing and function

Merozoite surface protein-1 (MSP-1, also referred to as P195, PMMSA or MSA 1) is one of the most studied of all malaria proteins. The proteins. The protein is found in all malaria species investigated and structural studies on the gene indicate that parts of the molecule are well-conserved. Studies on Plasmodium falciparum have shown that the protein is in a processed form on the merozoite surface, a result of proteolytic cleavage of the large percursor molecule. Recent studies have identified some of these cleavage sites. During invasion of the new red cell most of the MSP1 molecule is shed from the parasite surface except for a small C-terminal fragment which can be detected in ring stages. Analysis of the structure of this fragment suggests that it contains two growth factor-like domains that may have a functional role.

The role of cytokines in Plasmodium vivax malaria

The cytokine tumor necrosis factor and other as yet unidentified factor(s) which together mediate the killing of intraerythrocytic malaria parasites are transiently elevated in sera during paroxysms in human Plasmodium vivax infections in non-immunes. These factors which included TNF and parasite killing factor(s) are associated with the clinical disease in malaria to the extent that their transient presence in infection sera coincided with paroxysms, the most pronounced clinical disturbances of P. vivax malaria and secondly because their levels were markedly lower in paroxysm sera of semi-immune patients who were resident of an endemic area. Further, a close parallel was obtained between serum TFN levels and changes in body temperature that occur during a P. vivax paroxysm in non-immune patients, suggesting a causative role for TNF in the fever in malaria. P. vivax rarely if ever cause complicated clinical syndromes. Nevertheles serum TFN levels reached in acutely ill P. vivax patients were as high as in patients suffering from cerebral complications of P. falciparum malaria as reported in studies from the Gambia. Cytokine profiles and other changes accompanying clinical disease in P. vivax and P. falciparum malaria are compared in this paper with a view to discussing the potential role of cytokines in the causation of disease in malaria.

Molecular approaches to malaria and Babesisosis diagnosis

The development of additional methods for detecting and identifuing Babesia and Plasmodium infections may be useful in disease monitoring, management and control efforts. To preliminarily evaluate sunthetic peptide-based serodiagnosis, a hydrophilic sequence (DDESEFDKEK)was selected from published BabR gene of B. bovis. Immunization of rabbits and cattle with the hemocyanin-conjugated peptide elicited antibody responses that specifically detected both P. falciparum and B. bovis antigens by immunofluorescence and Western blots. Using a dot-ELISA with this peptide, antisera from immunized and naturally-infected cattle, and immunized rodents, were specifically detected. Reactivity was weak and correlated with peptide immunization or infection. DNA-based detection using repetitive DNA was species-specific in dot-blot formats for B. bovis DNA, and in both dot-blot and in situ formats for P. falciparum; a streamlined enzymelinked synthetic DNA assay for P. falciparum detected 30 parasites/mm(cúbicos) from patient blood using either colorimetric (2-15 h color development) or chemiluminescent detection (0.5-6-min. exposures). Serodiagnostic and DNA hybridization methods may be complementary in the respective detection of both chronic and acute infections. However, recent improvements in the polymerase chain reaction (PCR) make feasible a more sensitive and uniform approach to the diagnosis of these and other infectious disease complexes, with appropriate primers and processing methods. An analysis of ribosomal DNA genes of Plasmodium and Toxoplasma identified Apicomplexa-conserved sequence regions. Specific and distinctive PCR profiles were obtained for primers spanning the internal transcribed spacer locus for each of several Plasmodium and Babesia species.

Human IgG responses against the N-terminal region of Merozoite Surface Protein 1 of Plasmodium vivax

The complete primary structure of the gene encoding the Merozoite Surface Protein 1 of Plasmodium vivax (PvMSP-1) revealed the existence of interspecies conserved regions among the analogous proteins of other Plasmodia species. Here, three DNA recombinant clones expressing 50, 200 and 500 amino acids from the N-terminal region of the PvMSP-1 protein were used on ELISA and protein immunoblotting assays to look at the IgG antibody responses of malaria patients from the Brasilian amazon region of Rondônia. The results showed the existance of P. vivax and P. falciparum IgG antibodies directed against PvMSP-1 antigenic determinants expressed in the clones containing the first 200 and the following 500 amino acids of the molecule, but not within the one expressing the most N-terminal 50 amino acids. Interestingly, there was no correlation between the levels of these IgG antibodies and the previous number of malaria infections.

A recombinant hybrid protein as antigen for an anti-blood stage malaria vaccine: a study on the conservation of a protective component

Recently we have shown that two hybrid proteins expressed in Escherichia coli confer protective immunity to Aotus monkeys against an experimental Plasmodium falciparum infection (Knapp et al., 1992). Both hybrid proteins carry a sequence containing amino acids 631 to 764 of the serine stretch protein SERP (Knapp et al., 1989b). We have studied the diversity of this SERP region in field isolates of P. falciparum. Genomic DNA was extracted from the blood of six donors from different endemic areas of Brazil and West Africa. The SERP region encoding amino acids 630 to 781 was amplified by polymerase chain reaction (PCR) and sequenced. Only conserved amino acid substitutions in maximally two positions of the analyzed SERP fragment could be detected which supports the suitability of this SERP region as a component of anti-blood stage malaria vaccine.

Basic biochemical investigations as rationale for the design of original antimalarial drugs. An example of phospholipid metabolism

The future of antimalarial chemotherapy is particulary alarming in view of the spread of parasite cross-resistances to drugs that are not even structurally related. Only the availability of new pharmacological models will make it possible to select molecules with novel mechanisms of action, thus delaving resistance and allowing the development of new chemotherapeutic strategies. We reached this objective in mice. Our approach is hunged on fundamental and applied research begun in 1980 to investigate to phospholipid (PL) metabolism of intraerythrocytic Plasmodium. This metabolism is abundant, specific and indispensable for the production of Plasmodium membranes. Any drug to interfere with this metabolism blocks parasitic development. The most effective interference yet found involves blockage of the choline transporter, which supplies Plasmodium with choline for the synthesis of phosphatidylcholine, its major PL, this is a limiting step in the pathway. The drug sensitivity thereshold is much lower for the parasite, which is more dependent on this metabolism than host cells. The compounds show in vitro activity against P. falciparum at 1 to 10 nM. They show a very low toxicity against a lymphblastoid cell line, demonstrating a total abscence of correlation between growth inhibition of parasites and lymphoblastoid cells. They show antimalarial activity in vivo, in the P. berghei or P. chabaudi/mouse system, at doses 20-to 100-fold lower than their in acute toxicity limit. The bioavailability of a radiolabeled form of the product seemed to be advantageous (slow blood clearance and no significant concentration in tissues). Lastly, the compounds are inexpensive to produce. They are stable and water-soluble.

Mefloquine resistant malaria in cameroon and correlation with resistance quinine

Based on the results of in vitro sensitivity of Plasmodium falciparum to chloroquine, quinine and mefloquine, and evaluation of drug consumption conducted in 1987-1988 in four areas in the noth and south-west of Cameron, two opposite situations were encountered in this country. In northern Cameron where mefloquine resistance is prevalent a close correlation was found between the responses of P. falciparum to mefloquine and to quinine, but not between mefloquine and chloroquine. In the south, where chloroquine resistance is highly prevalent, no correlation was found neither between mefloquine and chloroquine nor mefloquine and quinine, but the responses to quinine and chloroquine appear partly correlated. These lead to formulate the hypothesis of a "southern" type of P. falciparum submitted to a high chloroquine drug pressure inducing a secondary cross resistance, whilst a "northern"type submitted to a relatively high and abortive quinine drug pressure inducing a primary quinine resistance and a secondary cross resistance with mefloquine.