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3. Expression of a type B RIFIN in Plasmodium falciparum merozoites and gametes

Author

Mwakalinga Steven B, Wang Christian W, Bengtsson Dominique C, Turner Louise, Dinko Bismarck, Lusingu John P, Arnot David E, Sutherland Colin J, Theander Thor G, and Lavstsen Thomas

Subjects
Arctic medicine. Tropical medicine, RC955-962, Infectious and parasitic diseases, RC109-216
Abstract

Abstract Background The ability of Plasmodium falciparum to undergo antigenic variation, by switching expression among protein variants encoded by multigene families, such as var, rif and stevor, is key to the survival of this parasite in the human host. The RIFIN protein family can be divided into A and B types based on the presence or absence of a 25 amino acid motif in the semi-conserved domain. A particular type B RIFIN, PF13_0006, has previously been shown to be strongly transcribed in the asexual and sexual stages of P. falciparum in vitro. Methods Antibodies to recombinant PF13_0006 RIFIN were used in immunofluorescence and confocal imaging of 3D7 parasites throughout the asexual reproduction and sexual development to examine the expression of PF13_0006. Furthermore, reactivity to recombinant PF13_0006 was measured in plasma samples collected from individuals from both East and West African endemic areas. Results The PF13_0006 RIFIN variant appeared expressed by both released merozoites and gametes after emergence. 7.4% and 12.1% of individuals from East and West African endemic areas, respectively, carry plasma antibodies that recognize recombinant PF13_0006, where the antibody responses were more common among older children. Conclusions The stage specificity of PF13_0006 suggests that the diversity of RIFIN variants has evolved to provide multiple specialized functions in different stages of the parasite life cycle. These data also suggest that RIFIN variants antigenically similar to PF13_0006 occur in African parasite populations.

Published
2012
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4. Identification of a major rif transcript common to gametocytes and sporozoites of Plasmodium falciparum

Author

Hermsen Cornelus C, Sharp Sarah, Schwank Samana, Sutherland Colin J, Mwakalinga Steven B, Wang Christian W, Sauerwein Robert W, Theander Thor G, and Lavstsen Thomas

Subjects
Arctic medicine. Tropical medicine, RC955-962, Infectious and parasitic diseases, RC109-216
Abstract

Abstract Background The Plasmodium falciparum parasite is transmitted in its sexual gametocyte stage from man to mosquito and as asexual sporozoites from mosquito to man. Developing gametocytes sequester preferentially in the bone marrow, but mature stage gametocytes are released to the bloodstream. Sexual stage parasite surface proteins are of interest as candidate target antigens for transmission blocking vaccines. Methods In this study, the transcript profiles of rif and var genes, known to encode surface antigens in asexual blood stage parasites, were investigated at different stages of 3D7/NF54 gametocytogenesis and in sporozoites. Results Gametocytes exhibited a rif transcript profile unlinked to the rif and var transcript profile of the asexual progenitors. At stage V, mature gametocytes produced high levels of a single rif gene, PF13_0006, which also dominated the rif transcript profile of sporozoites. All var genes appeared to be silenced in sporozoites. Conclusions The most prominent variant surface antigen transcribed in both gametocytes and sporozoites of 3D7/NF54 is a single variant of the RIFIN protein family. This discovery may lead to the identification of the parasites binding ligands responsible for the adhesion during sexual stages and potentially to novel vaccine candidates.

Published
2010
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5. Mapping clusters of chikungunya and dengue transmission in northern Tanzania using disease exposure and vector data

Author

KAJEGUKA, DEBORA C., KAAYA, ROBERT D., DESROCHERS, RACHELLE, IRANPOUR, MAHMOOD, KAVISHE, REGINALD A., MWAKALINGA, STEVEN, SCHIØLER, KARIN L., ALIFRANGIS, MICHAEL, LINDSAY, L. ROBBIN, DIBERNARDO, ANTONIA, MOSHA, FRANKLIN W., KULKARNI, MANISHA A., KAJEGUKA, DEBORA C., KAAYA, ROBERT D., DESROCHERS, RACHELLE, IRANPOUR, MAHMOOD, KAVISHE, REGINALD A., MWAKALINGA, STEVEN, SCHIØLER, KARIN L., ALIFRANGIS, MICHAEL, LINDSAY, L. ROBBIN, DIBERNARDO, ANTONIA, MOSHA, FRANKLIN W., and KULKARNI, MANISHA A.

Abstract

Background: Dengue and chikungunya are mosquito-borne viral diseases that are of public health importance throughout the tropical and subtropical regions of the world. Seasonal variations in transmission of these viruses have been suggested owing to the ecology of their mosquito vectors. However, little is known about the epidemiology of the diseases Tanzania. To address this gap, seasonal community-based cross-sectional surveys were undertaken to identify potential clusters of transmission in Hai district in northern Tanzania. Methods: Epidemiological and entomological data from two cross-sectional surveys were used to examine the spatial pattern of dengue and chikungunya transmission. Six villages namely, Boma Ng’ombe, Magadini, Rundugai, Nshara and Kware were involved in the study. Serological measures of dengue and chikungunya virus infections were derived using enzyme-linked immunosorbent assays, and all participants were geo-referenced to the household level using a global positioning system. Potential clusters of individual exposed to dengue and chikungunya virus , as well as clusters of Aedes mosquitoes in the wet and dry seasons were detected using SaTScan. All significant clusters (with p≤0.05) were mapped using ArcGIS. Results: A large, widely dispersed cluster of chikungunya exposed individuals was detected spanning Rundugai and parts of Magadini villages (RR = 2.58, p= 0.01), while no significant clustering was observed in the dry season. Spatial clusters of Aedes aegypti were detected in Rundugai in both the wet and dry seasons (RR = 2.56, p< 0.001 and RR = 2.24, p=0.05, respectively). In the dry season a small cluster was also detected in Kware (RR = 2.25, p=0.05). No significant clusters of dengue were detected in both seasons. Conclusion: Clusters of chikungunya-exposed individuals and Aedes mosquitoes indicate on-going transmission of chikungunya virus in Hai district of northern Tanzania.

Published
2018

6. Mapping clusters of chikungunya and dengue transmission in northern Tanzania using disease exposure and vector data

Author

Kajeguka, Debora C., Kaaya, Robert D., Desrochers, Rachelle, Iranpour, Mahmood, Kavishe, Reginald A., Mwakalinga, Steven, Schiøler, Karin L., Alifrangis, Michael, Lindsay, L. Robbin, Dibernardo, Antonia, Mosha, Franklin W., and Kulkarni, Manisha A.

Subjects
Clusters, Dengue, parasitic diseases, Spatial, dengue, chikungunya, spatial, clusters, vector data, Tanzania, Chikungunya, Tanzania, Vector data
Abstract

Background: Dengue and chikungunya are mosquito-borne viral diseases that are of public health importance throughout the tropical and subtropical regions of the world. Seasonal variations in transmission of these viruses have been suggested owing to the ecology of their mosquito vectors. However, little is known about the epidemiology of the diseases Tanzania. To address this gap, seasonal community-based cross-sectional surveys were undertaken to identify potential clusters of transmission in Hai district in northern Tanzania. Methods: Epidemiological and entomological data from two cross-sectional surveys were used to examine the spatial pattern of dengue and chikungunya transmission. Six villages namely, Boma Ng’ombe, Magadini, Rundugai, Nshara and Kware were involved in the study. Serological measures of dengue and chikungunya virus infections were derived using enzyme-linked immunosorbent assays, and all participants were geo-referenced to the household level using a global positioning system. Potential clusters of individual exposed to dengue and chikungunya virus, as well as clusters of Aedes mosquitoes in the wet and dry seasons were detected using SaTScan. All significant clusters (with p≤0.05) were mapped using ArcGIS. Results: A large, widely dispersed cluster of chikungunya exposed individuals was detected spanning Rundugai and parts of Magadini villages (RR = 2.58, p= 0.01), while no significant clustering was observed in the dry season. Spatial clusters of Aedes aegypti were detected in Rundugai in both the wet and dry seasons (RR = 2.56, p< 0.001 and RR = 2.24, p=0.05, respectively). In the dry season a small cluster was also detected in Kware (RR = 2.25, p=0.05). No significant clusters of dengue were detected in both seasons. Conclusion: Clusters of chikungunya-exposed individuals and Aedes mosquitoes indicate on-going transmission of chikungunya virus in Hai district of northern Tanzania.

Published
2017

8. A VAR2CSA:CSP conjugate capable of inducing dual specificity antibody responses

Author

Kavishe Reginald Adolph, Janitzek Christoph Mikkel, Salanti Ali, Theander Thor Grundtvig, Mwakalinga Steven Boniface, Nielsen Morten Agertoug, Matondo Sungwa, Sander Adam Frederik, and Thrane Susan

Subjects
0301 basic medicine, Bacterial superglue, Plasmodium falciparum, Protozoan Proteins, Antibodies, Protozoan, Antigens, Protozoan, Enzyme-Linked Immunosorbent Assay, Circumsporozoite protein, Malaria vaccine, VAR2CSA, CSP conjugate [DBL1x-DBL2x-ID2a], Mice, 03 medical and health sciences, Antigen, Conjugate vaccine, CSP-SpyCatcher, Malaria Vaccines, parasitic diseases, Animals, Mice, Inbred BALB C, Vaccines, Conjugate, biology, Immunogenicity, Antibody titer, Articles, General Medicine, Flow Cytometry, Malaria vaccine, Circumsporozoite protein, VAR2CSA, CSP SpyCatcher, SpyTag-DBL1x-DBL2x-ID2a, bacterial superglue, DBL1x-DBL2x-ID2a:CSP conjugate, SpyTag-DBL1x-DBL2x-ID2a, Virology, 030104 developmental biology, Antibody Formation, Immunology, biology.protein, Female, Antibody, Peptides, Conjugate
Abstract

Background: Vaccine antigens targeting specific P. falciparum parasite stages are under pre-clinical and clinical development. It seems plausible that vaccine with multiple specificities will offer higher protection. With this hypothesis, we exploited the Spy- Tag/SpyCatcher conjugation system to make a, post expression, dual antigen conjugate vaccine, comprising two clinically tested antigen candidates (CSP and VAR2CSA). Methods: The DBL1x-DBL2x-ID2a region of VAR2CSA was genetically fused with SpyTag at N-terminus. The full-length CSP antigen was genetically fused to C-terminal SpyCatcher peptide. The covalent interaction between SpyTag/ SpyCatcher enables the formation of DBL1x-DBL2x-ID2a:CSP conjugate vaccine. Immunogenicity and quality of antibody responses induced by the conjugate vaccine, as well as a control CSP-SpyCatcher vaccine, was tested in BALB/c mice. Results: Serum samples obtained from mice immunized with the conjugate vaccine were able to recognize both untagged DBL1x-DBL2x-ID2a as well as CSP antigen. Moreover, the geometric mean anti-CSP antibody titer was 1.9-fold higher in serum (at day 35 and 55 post-first immunization) from mice immunized with the conjugate vaccine, as compared to mice receiving the control vaccine. Conclusion: The data obtained in this study serves as proof-of-concept for the simultaneous induction of antibodies directed against individual antigen components in a dual stage anti-malaria vaccine. Keywords: Malaria vaccine, Circumsporozoite protein, VAR2CSA, CSP SpyCatcher, SpyTag-DBL1x-DBL2x-ID2a, bacterial superglue, DBL1x-DBL2x-ID2a:CSP conjugate

Published
2017

9. A VAR2CSA:CSP conjugate capable of inducing dual specificity antibody responses

Author

Matondo, Sungwa, Thrane, Susan, Janitzek, Christoph Mikkel, Kavishe, Reginald Adolph, Mwakalinga, Steven Boniface, Theander, Thor Grundtvig, Salanti, Ali, Nielsen, Morten Agertoug, Pedersen, Adam Frederik Sander, Matondo, Sungwa, Thrane, Susan, Janitzek, Christoph Mikkel, Kavishe, Reginald Adolph, Mwakalinga, Steven Boniface, Theander, Thor Grundtvig, Salanti, Ali, Nielsen, Morten Agertoug, and Pedersen, Adam Frederik Sander

Abstract

Background: Vaccine antigens targeting specific P. falciparum parasite stages are under pre-clinical and clinical development. It seems plausible that vaccine with multiple specificities will offer higher protection. With this hypothesis, we exploited the Spy-Tag/SpyCatcher conjugation system to make a, post expression, dual antigen conjugate vaccine, comprising two clinically tested antigen candidates (CSP and VAR2CSA). Methods: The DBL1x-DBL2x-ID2a region of VAR2CSA was genetically fused with SpyTag at N-terminus. The full-length CSP antigen was genetically fused to C-terminal SpyCatcher peptide. The covalent interaction between SpyTag/SpyCatcher enables the formation of DBL1x-DBL2x-ID2a:CSP conjugate vaccine. Immunogenicity and quality of antibody responses induced by the conjugate vaccine, as well as a control CSP-SpyCatcher vaccine, was tested in BALB/c mice. Results: Serum samples obtained from mice immunized with the conjugate vaccine were able to recognize both untagged DBL1x-DBL2x-ID2a as well as CSP antigen. Moreover, the geometric mean anti-CSP antibody titer was 1.9-fold higher in serum (at day 35 and 55 post-first immunization) from mice immunized with the conjugate vaccine, as compared to mice receiving the control vaccine. Conclusion: The data obtained in this study serves as proof-of-concept for the simultaneous induction of antibodies directed against individual antigen components in a dual stage anti-malaria vaccine.

Published
2017

10. Cellulose filtration of blood from malaria patients for improving ex vivo growth of Plasmodium falciparum parasites

Author

Mkumbaye, Sixbert I, Minja, Daniel T R, Jespersen, Jakob S, Alifrangis, Michael, Kavishe, Reginald A, Mwakalinga, Steven B, Lusingu, John P, Theander, Thor G, Lavstsen, Thomas, Wang, Christian W, Mkumbaye, Sixbert I, Minja, Daniel T R, Jespersen, Jakob S, Alifrangis, Michael, Kavishe, Reginald A, Mwakalinga, Steven B, Lusingu, John P, Theander, Thor G, Lavstsen, Thomas, and Wang, Christian W

Abstract

BACKGROUND: Establishing in vitro Plasmodium falciparum culture lines from patient parasite isolates can offer deeper understanding of geographic variations of drug sensitivity and mechanisms of malaria pathogenesis and immunity. Cellulose column filtration of blood is an inexpensive, rapid and effective method for the removal of host factors, such as leucocytes and platelets, significantly improving the purification of parasite DNA in a blood sample.METHODS: In this study, the effect of cellulose column filtration of venous blood on the initial in vitro growth of P. falciparum parasite isolates from Tanzanian children admitted to hospital was tested. The parasites were allowed to expand in culture without subcultivation until 5 days after admission or the appearance of dead parasites and parasitaemia was determined daily. To investigate whether the filtration had an effect on clonality, P. falciparum merozoite surface protein 2 genotyping was performed using nested PCR on extracted genomic DNA, and the var gene transcript levels were investigated, using quantitative PCR on extracted RNA, at admission and 4 days of culture.RESULTS: The cellulose-filtered parasites grew to higher parasitaemia faster than non-filtered parasites seemingly due to a higher development ratio of ring stage parasites progressing into the late stages. Cellulose filtration had no apparent effect on clonality or var gene expression; however, evident differences were observed after only 4 days of culture in both the number of clones and transcript levels of var genes compared to the time of admission.CONCLUSIONS: Cellulose column filtration of parasitized blood is a cheap, applicable method for improving cultivation of P. falciparum field isolates for ex vivo based assays; however, when assessing phenotype and genotype of cultured parasites, in general, assumed to represent the in vivo infection, caution is advised.

Published
2017

12. The Severity of Plasmodium falciparum Infection Is Associated with Transcript Levels of var Genes Encoding Endothelial Protein C Receptor-Binding P. falciparum Erythrocyte Membrane Protein 1

Author

Mkumbaye, Sixbert I., primary, Wang, Christian W., additional, Lyimo, Eric, additional, Jespersen, Jakob S., additional, Manjurano, Alphaxard, additional, Mosha, Jacklin, additional, Kavishe, Reginald A., additional, Mwakalinga, Steven B., additional, Minja, Daniel T. R., additional, Lusingu, John P., additional, Theander, Thor G., additional, and Lavstsen, Thomas, additional

Published
2017
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14. Plasma Ang2 and ADAM17 levels are elevated during clinical malaria; Ang2 level correlates with severity and expression of EPCR-binding PfEMP1

Author

Petersen, Jens E V, Mkumbaye, Sixbert I, Vaaben, Anna V, Manjurano, Alphaxard, Lyimo, Eric, Kavishe, Reginald A, Mwakalinga, Steven B, Mosha, Jacklin, Minja, Daniel T R, Lusingu, John P A, Theander, Thor G, Lavstsen, Thomas, Wang, Christian W, Petersen, Jens E V, Mkumbaye, Sixbert I, Vaaben, Anna V, Manjurano, Alphaxard, Lyimo, Eric, Kavishe, Reginald A, Mwakalinga, Steven B, Mosha, Jacklin, Minja, Daniel T R, Lusingu, John P A, Theander, Thor G, Lavstsen, Thomas, and Wang, Christian W

Abstract

The pathogenesis of Plasmodium falciparum malaria involves a complex interplay between parasite adhesion and inflammatory response that includes release of cytokines and activation of the endothelium with accompanying release of Angiopoitin 2 (Ang2) to the plasma. A-disintegrin and metalloproteinase 17 (ADAM17) is a protein responsible for releasing cytokines, including Tumor Necrosis Factor α (TNFα), and shedding of adhesion proteins. In this study, we show that plasma levels of ADAM17 are increased in Tanzanian children hospitalized with a malaria infection compared with asymptomatic children but similar to children hospitalized with other infectious diseases. The plasma levels of ADAM17 decreased during recovery after an acute malaria episode. Plasma levels of Ang2 were associated with markers of malaria severity and levels of var transcripts encoding P. falciparum Erythrocyte Membrane Protein 1 (PfEMP1) containing Cysteine Rich Inter Domain Region α1 (CIDRα1) domains predicted to bind Endothelial Protein C receptor (EPCR). ADAM17 levels were not associated with expression of var genes encoding different PfEMP1 types when controlling for age. These data are the first to report ADAM17 plasma levels in malaria-exposed individuals, and support the notion that parasite sequestration mediated by EPCR-binding PfEMP1 is associated with endothelial activation and pathology in severe paediatric malaria.

Published
2016

15. Oral candida infection among HIV patients at Kilimanjaro Christian Medical Centrein northern, Tanzania

Author

NGASALA, GWAKISA, MGABO, MASEKE R., MREMA, JOHN G., SABUNI, JANET, MWAKALINGA, STEVEN, KAJEGUKA, DEBORA C., NGASALA, GWAKISA, MGABO, MASEKE R., MREMA, JOHN G., SABUNI, JANET, MWAKALINGA, STEVEN, and KAJEGUKA, DEBORA C.

Abstract

Background: Oral candidiasis has been a global health challenge especially in immunocompromised patients particularly with HIV infection. Though the incidence and prevalence of opportunistic infections have been reduced due to the use of anti-retroviral therapy (ART), oral candidiasis remains the most frequently HIV-associated oral lesion in Tanzania. This study aimed at determining the prevalence of oral candida infection in HIV positive patients and investigate the relationship between oral manifestations and the level of immunosuppression. Method: This study was carried out at Kilimanjaro Christian Medical Centre in Moshi, Tanzania. The study included 314 HIV patients with complete clinical results records who were diagnosed with HIV and who were on ARV and attending the hospital for care and treatment. Results: Prevalence of oral candida was 42.0% (132/314). Age group 6-27 years accounted for half of the infections (49/98). A significantly higher prevalence of candida infection (66.7%; 24/36) was obseved among patients with <200 cells/µl than in those with 200-500 cells/µl or >500 cells/µl (Chi-square χ2=14.9, p=0.001). The mean CD4+T-cell counts in HIV patients infected with oral candida was lower (523±35) than patients without oral candida infection (645±31 cells/µl), (ANOVA, p= 0.009). The mean CD4+ T-cell count among HIV patients on ART and those not on ART was not statistically different. Conclusion: The prevalence of oral candida infection was significantly higher in patients with CD4+ cell counts less than 200 cells/µl.

Published
2016

16. Group A Streptococcus pharyngitis among schoolchildren in Mbulu District, Tanzania

Author

Makuka, Fatuma I., Mwakalinga, Steven, Mattaka, Hassan H., Kipanyula, Maulilio J., Manjurano, Alphaxard, Makuka, Fatuma I., Mwakalinga, Steven, Mattaka, Hassan H., Kipanyula, Maulilio J., and Manjurano, Alphaxard

Abstract

Streptococcal pharyngitis continues to be one of the most common childhood illnesses throughout the world. Recent evidence indicates an increased incidence of group A Streptococcal (GAS) infections, which is a significant cause of mortality and morbidity on the global scale. The objective of this study was to determine prevalence of group A Streptococcus infection among primary schoolchildren in Mbulu district, northern Tanzania. This study was carried out in five primary schools, namely Mangisha, Gunyoda, Kainam, Hyloto and Tsaayo. GAS pharyngitis was diagnosed clinically and confirmed by laboratory investigation using a rapid test. A total of 320 study participants were recruited in the study. Overall, more than half (53.8%) of the children were females. The overall prevalence of Group a Streptococcal infection was 6.9% (95%CI [4.4-10.2]). The highest frequency of GAS infection was observed among children at Hyloto primary school (14.3%) while, none of the children in Tsaayo had GAS infection. This study potentially indicates that group A Streptococcal infection prevalent among schoolchildren in Mbulu district calling for the need of education to create awareness of the condition in the community.

Published
2016

17. Prevalence of dengue and chikungunya virus infections in north-eastern Tanzania:a cross sectional study among participants presenting with malaria-like symptoms

Author

Kajeguka, Debora C, Kaaya, Robert D, Mwakalinga, Steven, Ndossi, Rogathe, Ndaro, Arnold, Chilongola, Jaffu O, Mosha, Franklin W, Schiøler, Karin L, Kavishe, Reginald A, Alifrangis, Michael, Kajeguka, Debora C, Kaaya, Robert D, Mwakalinga, Steven, Ndossi, Rogathe, Ndaro, Arnold, Chilongola, Jaffu O, Mosha, Franklin W, Schiøler, Karin L, Kavishe, Reginald A, and Alifrangis, Michael

Abstract

BACKGROUND: In spite of increasing reports of dengue and chikungunya activity in Tanzania, limited research has been done to document the general epidemiology of dengue and chikungunya in the country. This study aimed at determining the sero-prevalence and prevalence of acute infections of dengue and chikungunya virus among participants presenting with malaria-like symptoms (fever, headache, rash, vomit, and joint pain) in three communities with distinct ecologies of north-eastern Tanzania.METHODS: Cross sectional studies were conducted among 1100 participants (aged 2-70 years) presenting with malaria-like symptoms at health facilities at Bondo dispensary (Bondo, Tanga), Hai hospital (Hai, Kilimanjaro) and TPC hospital (Lower Moshi). Participants who were malaria negative using rapid diagnostic tests (mRDT) were screened for sero-positivity towards dengue and chikungunya Immunoglobulin G and M (IgG and IgM) using ELISA-based kits. Participants with specific symptoms defined as probable dengue and/or chikungunya by WHO (fever and various combinations of symptoms such as headache, rash, nausea/vomit, and joint pain) were further screened for acute dengue and chikungunya infections by PCR.RESULTS: Out of a total of 1100 participants recruited, 91.2 % (n = 1003) were malaria negative by mRDT. Out of these, few of the participants (<5 %) were dengue IgM or IgG positive. A total of 381 participants had fever out of which 8.7 % (33/381) met the defined criteria for probable dengue, though none (0 %) was confirmed to be acute cases. Chikungunya IgM positives among febrile participants were 12.9 % (49/381) while IgG positives were at 3.7 % (14/381). A total of 74.2 % (283/381) participants met the defined criteria for probable chikungunya and 4.2 % (11/263) were confirmed by PCR to be acute chikungunya cases. Further analyses revealed that headache and joint pain were significantly associated with chikungunya IgM seropositivity.CONCLUSION: In north

Published
2016

18. Plasma Ang2 and ADAM17 levels are elevated during clinical malaria; Ang2 level correlates with severity and expression of EPCR-binding PfEMP1

Author

Petersen, Jens E. V., primary, Mkumbaye, Sixbert I., additional, Vaaben, Anna V., additional, Manjurano, Alphaxard, additional, Lyimo, Eric, additional, Kavishe, Reginald A., additional, Mwakalinga, Steven B., additional, Mosha, Jacklin, additional, Minja, Daniel T. R., additional, Lusingu, John P. A., additional, Theander, Thor G., additional, Lavstsen, Thomas, additional, and Wang, Christian W., additional

Published
2016
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20. Prevalence of dengue and chikungunya virus infections in north-eastern Tanzania: a cross sectional study among participants presenting with malaria-like symptoms

Author

Kajeguka, Debora C., primary, Kaaya, Robert D., additional, Mwakalinga, Steven, additional, Ndossi, Rogathe, additional, Ndaro, Arnold, additional, Chilongola, Jaffu O., additional, Mosha, Franklin W., additional, Schiøler, Karin L., additional, Kavishe, Reginald A., additional, and Alifrangis, Michael, additional

Published
2016
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23. Expression of a type B RIFIN in Plasmodium falciparum merozoites and gametes

Author

Mwakalinga, Steven B, Wang, Christian W, Bengtsson, Dominique C, Turner, Louise, Dinko, Bismarck, Lusingu, John P, Arnot, David E, Sutherland, Colin J, Theander, Thor G, Lavstsen, Thomas, Mwakalinga, Steven B, Wang, Christian W, Bengtsson, Dominique C, Turner, Louise, Dinko, Bismarck, Lusingu, John P, Arnot, David E, Sutherland, Colin J, Theander, Thor G, and Lavstsen, Thomas

Abstract

BACKGROUND: The ability of Plasmodium falciparum to undergo antigenic variation, by switching expression among protein variants encoded by multigene families, such as var, rif and stevor, is key to the survival of this parasite in the human host. The RIFIN protein family can be divided into A and B types based on the presence or absence of a 25 amino acid motif in the semi-conserved domain. A particular type B RIFIN, PF13_0006, has previously been shown to be strongly transcribed in the asexual and sexual stages of P. falciparum in vitro. METHODS: Antibodies to recombinant PF13_0006 RIFIN were used in immunofluorescence and confocal imaging of 3D7 parasites throughout the asexual reproduction and sexual development to examine the expression of PF13_0006. Furthermore, reactivity to recombinant PF13_0006 was measured in plasma samples collected from individuals from both East and West African endemic areas. RESULTS: The PF13_0006 RIFIN variant appeared expressed by both released merozoites and gametes after emergence. 7.4% and 12.1% of individuals from East and West African endemic areas, respectively, carry plasma antibodies that recognize recombinant PF13_0006, where the antibody responses were more common among older children. CONCLUSIONS: The stage specificity of PF13_0006 suggests that the diversity of RIFIN variants has evolved to provide multiple specialized functions in different stages of the parasite life cycle. These data also suggest that RIFIN variants antigenically similar to PF13_0006 occur in African parasite populations.

Published
2012

24. Antibodies against PfEMP1, RIFIN, MSP3 and GLURP are acquired during controlled Plasmodium falciparum malaria infections in naïve volunteers

Author

Turner, Louise, Wang, Christian W, Lavstsen, Thomas, Mwakalinga, Steven B, Sauerwein, Robert W, Hermsen, Cornelus C, Theander, Thor G, Turner, Louise, Wang, Christian W, Lavstsen, Thomas, Mwakalinga, Steven B, Sauerwein, Robert W, Hermsen, Cornelus C, and Theander, Thor G

Abstract

Antibodies to polymorphic antigens expressed during the parasites erythrocytic stages are important mediators of protective immunity against P. falciparum malaria. Therefore, polymorphic blood stage antigens like MSP3, EBA-175 and GLURP and variant surface antigens PfEMP1 and RIFIN are considered vaccine candidates. However, to what extent these antibodies to blood stage antigens are acquired during naive individuals' first infections has not been studied in depth. Using plasma samples collected from controlled experimental P. falciparum infections we show that antibodies against variant surface antigens, PfEMP1 and RIFIN as well as MSP3 and GLURP, are acquired during a single short low density P. falciparum infection in non-immune individuals including strain transcendent PfEMP1 immune responses. These data indicate that the immunogenicity of the variant surface antigens is similar to the less diverse merozoite antigens. The acquisition of a broad and strain transcendent repertoire of PfEMP1 antibodies may reflect a parasite strategy of expressing most or all PfEMP1 variants at liver release optimizing the likelihood of survival and establishment of chronic infections in the new host.

Published
2011

25. Identification of a major rif transcript common to gametocytes and sporozoites of Plasmodium falciparum

Author

Wang, Christian W, Mwakalinga, Steven B, Sutherland, Colin J, Schwank, Samana, Sharp, Sarah, Hermsen, Cornelus C, Sauerwein, Robert W, Theander, Thor G, Lavstsen, Thomas, Wang, Christian W, Mwakalinga, Steven B, Sutherland, Colin J, Schwank, Samana, Sharp, Sarah, Hermsen, Cornelus C, Sauerwein, Robert W, Theander, Thor G, and Lavstsen, Thomas

Abstract

Udgivelsesdato: 2010-May-28, BACKGROUND: The Plasmodium falciparum parasite is transmitted in its sexual gametocyte stage from man to mosquito and as asexual sporozoites from mosquito to man. Developing gametocytes sequester preferentially in the bone marrow, but mature stage gametocytes are released to the bloodstream. Sexual stage parasite surface proteins are of interest as candidate target antigens for transmission blocking vaccines. METHODS: In this study, the transcript profiles of rif and var genes, known to encode surface antigens in asexual blood stage parasites, were investigated at different stages of 3D7/NF54 gametocytogenesis and in sporozoites. RESULTS: Gametocytes exhibited a rif transcript profile unlinked to the rif and var transcript profile of the asexual progenitors. At stage V, mature gametocytes produced high levels of a single rif gene, PF13_0006, which also dominated the rif transcript profile of sporozoites. All var genes appeared to be silenced in sporozoites. CONCLUSIONS: The most prominent variant surface antigen transcribed in both gametocytes and sporozoites of 3D7/NF54 is a single variant of the RIFIN protein family. This discovery may lead to the identification of the parasites binding ligands responsible for the adhesion during sexual stages and potentially to novel vaccine candidates.

Published
2010

26. Low density parasitaemia, red blood cell polymorphisms and Plasmodium falciparum specific immune responses in a low endemic area in northern Tanzania

Author

Shekalaghe, Seif, Alifrangis, Michael, Mwanziva, Charles, Enevold, Anders, Mwakalinga, Steven Boniface, Mkali, Humphrey, Kavishe, Reginald, Manjurano, Alphaxard, Sauerwein, Robert, Drakeley, Chris, Bousema, Teun, Shekalaghe, Seif, Alifrangis, Michael, Mwanziva, Charles, Enevold, Anders, Mwakalinga, Steven Boniface, Mkali, Humphrey, Kavishe, Reginald, Manjurano, Alphaxard, Sauerwein, Robert, Drakeley, Chris, and Bousema, Teun

Abstract

Udgivelsesdato: 2009-null, BACKGROUND: Low density Plasmodium falciparum infections, below the microscopic detection limit, may play an important role in maintaining malaria transmission in low endemic areas as well as contribute to the maintenance of acquired immunity. Little is known about factors influencing the occurrence of sub-microscopic parasitaemia or the relation with immune responses.We investigated possible associations between the occurrence of sub-microscopic P. falciparum parasite carriage and antibody responses to the asexual stage antigens, G6PD deficiency and alpha+-thalassaemia in 464 subjects from a low endemic area in northern Tanzania. METHODS: We used samples collected from two cross sectional surveys conducted during dry and wet season in 2005. Submicroscopic parasitaemia was detected by using quantitative nucleic acid sequence based amplification (QT-NASBA). Genotyping for G6PD and alpha+-thalassaemia were performed by high throughput PCR; the prevalence and level of total IgG antibodies against MSP-1, MSP-2 and AMA-1 were determined by ELISA. RESULTS: Compared to parasite free individuals, individuals carrying sub-microscopic densities of P. falciparum parasites had significantly higher median antibody levels to MSP-1 (p = 0.042) and MSP-2 (p = 0.034) but not to AMA-1 (p = 0.14) while no clear relation between sub-microscopic parasite carriage and G6PD deficiency or alpha+-thalassaemia was observed. CONCLUSION: Our data suggest a role for sub-microscopic parasite densities in eliciting or maintaining humoral immune responses without evidence for a modulating effect of G6PD deficiency or alpha+-thalassaemia.

Published
2009

31. The Severity of Plasmodium falciparumInfection Is Associated with Transcript Levels of varGenes Encoding Endothelial Protein C Receptor-Binding P. falciparumErythrocyte Membrane Protein 1

Author

Mkumbaye, Sixbert I., Wang, Christian W., Lyimo, Eric, Jespersen, Jakob S., Manjurano, Alphaxard, Mosha, Jacklin, Kavishe, Reginald A., Mwakalinga, Steven B., Minja, Daniel T. R., Lusingu, John P., Theander, Thor G., and Lavstsen, Thomas

Abstract

ABSTRACTBy attaching infected erythrocytes to the vascular lining, Plasmodium falciparumparasites leave blood circulation and avoid splenic clearance. This sequestration is central to pathogenesis. Severe malaria is associated with parasites expressing an antigenically distinct P. falciparumerythrocyte membrane protein 1 (PfEMP1) subset mediating binding to endothelial receptors. Previous studies indicate that PfEMP1 adhesins with so-called CIDRα1 domains capable of binding endothelial protein C receptor (EPCR) constitute the PfEMP1 subset associated with severe pediatric malaria. To analyze the relative importance of different subtypes of CIDRα1 domains, we compared Pfemp1transcript levels in children with severe malaria (including 9 fatal and 114 surviving cases), children hospitalized with uncomplicated malaria (n= 42), children with mild malaria not requiring hospitalization (n= 10), and children with parasitemia and no ongoing fever (n= 12). High levels of transcripts encoding EPCR-binding PfEMP1 were found in patients with symptomatic infections, and the abundance of these transcripts increased with disease severity. The compositions of CIDRα1 subtype transcripts varied markedly between patients, and none of the subtypes were dominant. Transcript-level analyses targeting other domain types indicated that subtypes of DBLβ or DBLζ domains might mediate binding phenomena that, in conjunction with EPCR binding, could contribute to pathogenesis. These observations strengthen the rationale for targeting the PfEMP1-EPCR interaction by vaccines and adjunctive therapies. Interventions should target EPCR binding of all CIDRα1 subtypes.

Published
2017
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