Your search keyword '"Adams Jh"' showing total 13 results

1. Naturally acquired antibodies against Plasmodium vivax pre-erythrocytic stage vaccine antigens inhibit sporozoite invasion of human hepatocytes in vitro.

Author

Ntumngia FB, Kolli SK, Annamalai Subramani P, Barnes SJ, Nicholas J, Ogbondah MM, Barnes BB, Salinas ND, Thawornpan P, Tolia NH, Chootong P, and Adams JH

Subjects

Animals, Humans, Plasmodium vivax, Sporozoites metabolism, Protozoan Proteins metabolism, Antigens, Protozoan, Membrane Proteins metabolism, Erythrocytes metabolism, Hepatocytes metabolism, Antibodies, Protozoan, Plasmodium falciparum metabolism, Malaria, Vivax, Vaccines

Abstract

In Plasmodium vivax, the most studied vaccine antigens are aimed at blocking merozoite invasion of erythrocytes and disease development. Very few studies have evaluated pre-erythrocytic (PE) stage antigens. The P. vivax circumsporozoite protein (CSP), is considered the leading PE vaccine candidate, but immunity to CSP is short-lived and variant specific. Thus, there is a need to identify other potential candidates to partner with CSP in a multivalent vaccine to protect against infection and disease. We hypothesize that sporozoite antigens important for host cell infection are considered potential targets. In this study, we evaluated the magnitude and quality of naturally acquired antibody responses to four P. vivax PE antigens: sporozoite surface protein 3 (SSP3), sporozoite protein essential for traversal 1 (SPECT1), cell traversal protein of ookinetes and sporozoites (CelTOS) and CSP in plasma of P. vivax infected patients from Thailand. Naturally acquired antibodies to these antigens were prevalent in the study subjects, but with significant differences in magnitude of IgG antibody responses. About 80% of study participants had antibodies to all four antigens and only 2% did not have antibodies to any of the antigens. Most importantly, these antibodies inhibited sporozoite infection of hepatocytes in vitro. Significant variations in magnitude of antigen-specific inhibitory antibody responses were observed with individual samples. The highest inhibitory responses were observed with anti-CelTOS antibodies, followed by anti-SPECT1, SSP3 and CSP antibodies respectively. These data highlight the vaccine potential of these antigens in protecting against hepatocyte infection and the need for a multi-valent pre-erythrocytic vaccine to prevent liver stage development of P. vivax sporozoites., (© 2024. The Author(s).)

Published

2024

2. Characterization of Duffy Binding Protein II-specific CD4 + T cell responses in Plasmodium vivax patients.

Author

Thawornpan P, Malee C, Kochayoo P, Wangriatisak K, Leepiyasakulchai C, Ntumngia FB, De SL, Adams JH, and Chootong P

Subjects

Humans, Carrier Proteins, Epitopes, T-Lymphocyte, Cross-Sectional Studies, Antigens, Protozoan, Protozoan Proteins genetics, Cytokines metabolism, Antibodies, Protozoan, Plasmodium vivax genetics, Malaria, Vivax parasitology

Abstract

Plasmodium vivax Duffy Binding Protein region II (PvDBPII) is a leading vaccine candidate against blood-stage vivax malaria. Anti-PvDBPII antibodies potentially block parasite invasion by inhibition of erythrocyte binding. However, knowledge of PvDBPII-specific T cell responses is limited. Here, to assess the responses of PvDBPII-specific CD4 + T cells in natural P. vivax infection, three cross-sectional studies were conducted in recovered subjects. In silico analysis was used for potential T cell epitope prediction and selection. PBMCs from P. vivax subjects were stimulated with selected peptides and examined for cytokine production by ELISPOT or intracellular cytokine staining. Six dominant T cell epitopes were identified. Peptide-driven T cell responses showed effector memory CD4 + T cell phenotype, secreting both IFN-γ and TNF-α cytokines. Single amino acid substitutions in three T cell epitopes altered levels of IFN-γ memory T cell responses. Seropositivity of anti-PvDBPII antibodies were detected during acute malaria (62%) and persisted up to 12 months (11%) following P. vivax infection. Further correlation analysis showed four out of eighteen subjects had positive antibody and CD4 + T cell responses to PvDBPII. Altogether, PvDBPII-specific CD4 + T cells were developed in natural P. vivax infections. Data on their antigenicity could facilitate development of an efficacious vivax malaria vaccine., (© 2023. The Author(s).)

Published

2023

3. Protein KIC5 is a novel regulator of artemisinin stress response in the malaria parasite Plasmodium falciparum.

Author

Simmons CF, Gibbons J, Zhang M, Oberstaller J, Pires CV, Casandra D, Wang C, Seyfang A, Otto TD, Rayner JC, and Adams JH

Subjects

Drug Resistance genetics, Mutation, Protozoan Proteins genetics, Protozoan Proteins metabolism, Antimalarials pharmacology, Artemisinins therapeutic use, Plasmodium falciparum drug effects, Plasmodium falciparum genetics, Plasmodium falciparum metabolism

Abstract

Artemisinin combination therapies (ACTs) have led to a significant decrease in Plasmodium falciparum malaria mortality. This progress is now threatened by emerging artemisinin resistance (ART-R) linked originally in SE Asia to polymorphisms in the Kelch propeller protein (K13) and more recently to several other seemingly unrelated genetic mutations. To better understand the parasite response to ART, we are characterizing a P. falciparum mutant with altered sensitivity to ART that was created via piggyBac transposon mutagenesis. The transposon inserted near the putative transcription start site of a gene defined as a "Plasmodium-conserved gene of unknown function," now functionally linked to K13 as the Kelch13 Interacting Candidate 5 protein (KIC5). Phenotype analysis of the KIC5 mutant during intraerythrocytic asexual development identified transcriptional changes associated with DNA stress response and altered mitochondrial metabolism, linking dysregulation of the KIC5 gene to the parasite's ability to respond to ART exposure. Through characterization of the KIC5 transcriptome, we hypothesize that this gene may be essential under ART exposure to manage gene expression of the wild-type stress response at early ring stage, thereby providing a better understanding of the parasite's processes that can alter ART sensitivity., (© 2023. The Author(s).)

Published

2023

4. Interferon-γ signal drives differentiation of T-bet hi atypical memory B cells into plasma cells following Plasmodium vivax infection.

Author

Kochayoo P, Thawornpan P, Wangriatisak K, Changrob S, Leepiyasakulchai C, Khowawisetsut L, Adams JH, and Chootong P

Subjects

B-Lymphocytes, Humans, Immunoglobulin G, Immunologic Memory, Interferon-gamma, Memory B Cells, Plasma Cells, Plasmodium vivax, Malaria, Malaria, Vivax

Abstract

For development of a long-lasting protective malaria vaccine, it is crucial to understand whether Plasmodium-induced memory B cells (MBCs) or plasma cells develop and stably contribute to protective immunity, or on the contrary the parasite suppresses antibody responses by inducing MBC dysfunction. The expansion of T-bet hi atypical MBCs is described in chronic Plasmodium falciparum-exposed individuals. However, it remains unclear whether accumulation of T-bet hi atypical MBCs is indicative of a protective role or rather an impaired function of the immune system in malaria. Here, the phenotypic and functional features of T-bet hi atypical MBCs were studied in P. vivax patients living in an area of low malaria transmission. During P. vivax infection, the patients produced a twofold higher frequency of T-bet hi atypical MBCs compared to malaria non-exposed individuals. This distinct atypical MBC subset had a switched IgG phenotype with overexpression of activation markers and FcRL5, and decreased Syk phosphorylation upon BCR stimulation. Post-infection, expansion of T-bet hi IgG + atypical MBCs was maintained for at least 3 months. Further studies of the contribution of T-bet hi atypical MBC function to humoral immunity showed that synergizing IFN-γ with TLR7/8 and IL-21 signals was required for their differentiation into plasma cells and antibody secretion., (© 2022. The Author(s).)

Published

2022

5. Author Correction: Structural basis for neutralization of Plasmodium vivax by naturally acquired human antibodies that target DBP.

Author

Urusova D, Carias L, Huang Y, Nicolete VC, Popovici J, Roesch C, Salinas ND, Dechavanne S, Witkowski B, Ferreira MU, Adams JH, Gross ML, King CL, and Tolia NH

Abstract

An amendment to this paper has been published and can be accessed via a link at the top of the paper.

Published

2019

6. Structural basis for neutralization of Plasmodium vivax by naturally acquired human antibodies that target DBP.

Author

Urusova D, Carias L, Huang Y, Nicolete VC, Popovici J, Roesch C, Salinas ND, Dechavanne S, Witkowski B, Ferreira MU, Adams JH, Gross ML, King CL, and Tolia NH

Subjects

Amino Acid Sequence, Antibodies, Monoclonal chemistry, Antibodies, Neutralizing chemistry, Antigens, Protozoan genetics, Antigens, Protozoan metabolism, Binding Sites, Crystallography, X-Ray, Duffy Blood-Group System metabolism, Epitopes, B-Lymphocyte, Erythrocytes metabolism, Erythrocytes parasitology, Genetic Variation, Humans, Malaria Vaccines immunology, Malaria, Vivax parasitology, Malaria, Vivax prevention & control, Plasmodium vivax genetics, Protein Binding, Protozoan Proteins genetics, Protozoan Proteins metabolism, Receptors, Cell Surface genetics, Receptors, Cell Surface metabolism, Antibodies, Monoclonal immunology, Antibodies, Neutralizing immunology, Antigens, Protozoan chemistry, Antigens, Protozoan immunology, Plasmodium vivax immunology, Protozoan Proteins chemistry, Protozoan Proteins immunology, Receptors, Cell Surface chemistry, Receptors, Cell Surface immunology

Abstract

The Plasmodium vivax Duffy-binding protein (DBP) is a prime target of the protective immune response and a promising vaccine candidate for P. vivax malaria. Naturally acquired immunity (NAI) protects against malaria in adults residing in infection-endemic regions, and the passive transfer of malarial immunity confers protection. A vaccine that replicates NAI will effectively prevent disease. Here, we report the structures of DBP region II in complex with human-derived, neutralizing monoclonal antibodies obtained from an individual in a malaria-endemic area with NAI. We identified protective epitopes using X-ray crystallography, hydrogen-deuterium exchange mass spectrometry, mutational mapping and P. vivax invasion studies. These approaches reveal that naturally acquired human antibodies neutralize P. vivax by targeting the binding site for Duffy antigen receptor for chemokines (DARC) and the dimer interface of P. vivax DBP. Antibody binding is unaffected by polymorphisms in the vicinity of epitopes, suggesting that the antibodies have evolved to engage multiple polymorphic variants of DBP. The human antibody epitopes are broadly conserved and are distinct from previously defined epitopes for broadly conserved murine monoclonal antibodies. A library of globally conserved epitopes of neutralizing human antibodies offers possibilities for rational design of strain-transcending DBP-based vaccines and therapeutics against P. vivax.

Published

2019

7. Unraveling the Plasmodium vivax sporozoite transcriptional journey from mosquito vector to human host.

Author

Roth A, Adapa SR, Zhang M, Liao X, Saxena V, Goffe R, Li S, Ubalee R, Saggu GS, Pala ZR, Garg S, Davidson S, Jiang RHY, and Adams JH

Subjects

Animals, Anopheles parasitology, Gene Expression Profiling, Host-Pathogen Interactions genetics, Humans, Insect Vectors parasitology, Malaria parasitology, Malaria, Vivax parasitology, Mosquito Vectors genetics, Parasites, Plasmodium vivax pathogenicity, Salivary Glands parasitology, Sporozoites pathogenicity, Sporozoites physiology, Plasmodium vivax genetics, Plasmodium vivax physiology, Sporozoites genetics

Abstract

Malaria parasites transmitted by mosquito bite are remarkably efficient in establishing human infections. The infection process requires roughly 30 minutes and is highly complex as quiescent sporozoites injected with mosquito saliva must be rapidly activated in the skin, migrate through the body, and infect the liver. This process is poorly understood for Plasmodium vivax due to low infectivity in the in vitro models. To study this skin-to-liver-stage of malaria, we used quantitative bioassays coupled with transcriptomics to evaluate parasite changes linked with mammalian microenvironmental factors. Our in vitro phenotyping and RNA-seq analyses revealed key microenvironmental relationships with distinct biological functions. Most notable, preservation of sporozoite quiescence by exposure to insect-like factors coupled with strategic activation limits untimely activation of invasion-associated genes to dramatically increase hepatocyte invasion rates. We also report the first transcriptomic analysis of the P. vivax sporozoite interaction in salivary glands identifying 118 infection-related differentially-regulated Anopheles dirus genes. These results provide important new insights in malaria parasite biology and identify priority targets for antimalarial therapeutic interventions to block P. vivax infection.

Published

2018

8. Persistence of Long-lived Memory B Cells specific to Duffy Binding Protein in individuals exposed to Plasmodium vivax.

Author

Changrob S, McHenry AM, Nyunt MH, Sattabongkot J, Han ET, Adams JH, and Chootong P

Subjects

Adult, Aged, Antibodies, Protozoan immunology, Antibody Formation immunology, B-Lymphocytes metabolism, Cohort Studies, Cross-Sectional Studies, Duffy Blood-Group System, Female, Humans, Immunity, Humoral physiology, Malaria blood, Male, Middle Aged, Phenotype, Plasmodium vivax genetics, Plasmodium vivax immunology, Polymorphism, Genetic genetics, Protozoan Proteins genetics, Receptors, Cell Surface genetics, B-Lymphocytes immunology, Malaria Vaccines immunology, Malaria, Vivax immunology

Abstract

The major challenge in designing a protective Duffy binding protein region II (DBPII)-based vaccine against blood-stage vivax malaria is the high number of polymorphisms in critical residues targeted by binding-inhibitory antibodies. Here, longevity of antibody and memory B cell response (MBCs) to DBL-TH variants, DBL-TH2, -TH4, -TH5, -TH6 and -TH9 were analyzed in P. vivax-exposed individuals living in a low malaria transmission area of southern Thailand. Antibody to DBL-TH variants were significantly detected during P. vivax infection and it was persisted for up to 9 months post-infection. However, DBL-TH-specific MBC responses were stably maintained longer than antibody response, at least 3 years post-infection in the absence of re-infection. Phenotyping of B cell subsets showed the expansion of activated and atypical MBCs during acute and recovery phase of infection. While the persistence of DBL-TH-specific MBCs was found in individuals who had activated and atypical MBC expansion, anti-DBL-TH antibody responses was rapidly declined in plasma. The data suggested that these two MBCs were triggered by P. vivax infection, its expansion and stability may have impact on antibody responses. Our results provided evidence for ability of DBPII variant antigens in induction of long-lasting MBCs among individuals who were living in low malaria endemicity.

Published

2018

9. An engineered vaccine of the Plasmodium vivax Duffy binding protein enhances induction of broadly neutralizing antibodies.

Author

Ntumngia FB, Pires CV, Barnes SJ, George MT, Thomson-Luque R, Kano FS, Alves JRS, Urusova D, Pereira DB, Tolia NH, King CL, Carvalho LH, and Adams JH

Subjects

Animals, Antibody Formation, Enzyme-Linked Immunosorbent Assay, Erythrocytes metabolism, Mice, Mice, Inbred BALB C, Protein Binding, Antibodies, Neutralizing immunology, Antibodies, Protozoan immunology, Antigens, Protozoan immunology, Erythrocytes immunology, Malaria Vaccines immunology, Protein Engineering methods, Protozoan Proteins immunology, Receptors, Cell Surface immunology

Abstract

Plasmodium vivax invasion into human reticulocytes is a complex process. The Duffy binding protein (DBP) dimerization with its cognate receptor is vital for junction formation in the invasion process. Due to its functional importance, DBP is considered a prime vaccine candidate, but variation in B-cell epitopes at the dimer interface of DBP leads to induction of strain-limited immunity. We believe that the polymorphic residues tend to divert immune responses away from functionally conserved epitopes important for receptor binding or DBP dimerization. As a proof of concept, we engineered the vaccine DEKnull to ablate the dominant Bc epitope to partially overcome strain-specific immune antibody responses. Additional surface engineering on the next generation immunogen, DEKnull-2, provides an immunogenicity breakthrough to conserved protective epitopes. DEKnull-2 elicits a stronger broadly neutralizing response and reactivity with long-term persistent antibody responses of acquired natural immunity. By using novel engineered DBP immunogens, we validate that the prime targets of protective immunity are conformational epitopes at the dimer interface. These successful results indicate a potential approach that can be used generally to improve efficacy of other malaria vaccine candidates.

Published

2017

10. Chemogenomic profiling of Plasmodium falciparum as a tool to aid antimalarial drug discovery.

Author

Pradhan A, Siwo GH, Singh N, Martens B, Balu B, Button-Simons KA, Tan A, Zhang M, Udenze KO, Jiang RH, Ferdig MT, Adams JH, and Kyle DE

Subjects

Drug Discovery methods, Drug Resistance, Multiple drug effects, Drug Resistance, Multiple genetics, Mutagenesis, Insertional drug effects, Plasmodium falciparum genetics, Protozoan Proteins genetics, Antimalarials pharmacology, Plasmodium falciparum drug effects

Abstract

The spread of Plasmodium falciparum multidrug resistance highlights the urgency to discover new targets and chemical scaffolds. Unfortunately, lack of experimentally validated functional information about most P. falciparum genes remains a strategic hurdle. Chemogenomic profiling is an established tool for classification of drugs with similar mechanisms of action by comparing drug fitness profiles in a collection of mutants. Inferences of drug mechanisms of action and targets can be obtained by associations between shifts in drug fitness and specific genetic changes in the mutants. In this screen, P. falciparum, piggyBac single insertion mutants were profiled for altered responses to antimalarial drugs and metabolic inhibitors to create chemogenomic profiles. Drugs targeting the same pathway shared similar response profiles and multiple pairwise correlations of the chemogenomic profiles revealed novel insights into drugs' mechanisms of action. A mutant of the artemisinin resistance candidate gene - "K13-propeller" gene (PF3D7_1343700) exhibited increased susceptibility to artemisinin drugs and identified a cluster of 7 mutants based on similar enhanced responses to the drugs tested. Our approach of chemogenomic profiling reveals artemisinin functional activity, linked by the unexpected drug-gene relationships of these mutants, to signal transduction and cell cycle regulation pathways.

Published

2015

11. An excess of cosmic ray electrons at energies of 300-800 GeV.

Author

Chang J, Adams JH, Ahn HS, Bashindzhagyan GL, Christl M, Ganel O, Guzik TG, Isbert J, Kim KC, Kuznetsov EN, Panasyuk MI, Panov AD, Schmidt WK, Seo ES, Sokolskaya NV, Watts JW, Wefel JP, Wu J, and Zatsepin VI

Abstract

Galactic cosmic rays consist of protons, electrons and ions, most of which are believed to be accelerated to relativistic speeds in supernova remnants. All components of the cosmic rays show an intensity that decreases as a power law with increasing energy (for example as E(-2.7)). Electrons in particular lose energy rapidly through synchrotron and inverse Compton processes, resulting in a relatively short lifetime (about 10(5) years) and a rapidly falling intensity, which raises the possibility of seeing the contribution from individual nearby sources (less than one kiloparsec away). Here we report an excess of galactic cosmic-ray electrons at energies of approximately 300-800 GeV, which indicates a nearby source of energetic electrons. Such a source could be an unseen astrophysical object (such as a pulsar or micro-quasar) that accelerates electrons to those energies, or the electrons could arise from the annihilation of dark matter particles (such as a Kaluza-Klein particle with a mass of about 620 GeV).

Published

2008

12. Comparative genomics of the neglected human malaria parasite Plasmodium vivax.

Author

Carlton JM, Adams JH, Silva JC, Bidwell SL, Lorenzi H, Caler E, Crabtree J, Angiuoli SV, Merino EF, Amedeo P, Cheng Q, Coulson RM, Crabb BS, Del Portillo HA, Essien K, Feldblyum TV, Fernandez-Becerra C, Gilson PR, Gueye AH, Guo X, Kang'a S, Kooij TW, Korsinczky M, Meyer EV, Nene V, Paulsen I, White O, Ralph SA, Ren Q, Sargeant TJ, Salzberg SL, Stoeckert CJ, Sullivan SA, Yamamoto MM, Hoffman SL, Wortman JR, Gardner MJ, Galinski MR, Barnwell JW, and Fraser-Liggett CM

Subjects

Amino Acid Motifs, Animals, Artemisinins metabolism, Artemisinins pharmacology, Atovaquone metabolism, Atovaquone pharmacology, Cell Nucleus genetics, Chromosomes genetics, Conserved Sequence genetics, Erythrocytes parasitology, Evolution, Molecular, Haplorhini parasitology, Humans, Isochores genetics, Ligands, Malaria, Vivax metabolism, Multigene Family, Plasmodium vivax drug effects, Plasmodium vivax pathogenicity, Plasmodium vivax physiology, Sequence Analysis, DNA, Species Specificity, Synteny genetics, Genome, Protozoan genetics, Genomics, Malaria, Vivax parasitology, Plasmodium vivax genetics

Abstract

The human malaria parasite Plasmodium vivax is responsible for 25-40% of the approximately 515 million annual cases of malaria worldwide. Although seldom fatal, the parasite elicits severe and incapacitating clinical symptoms and often causes relapses months after a primary infection has cleared. Despite its importance as a major human pathogen, P. vivax is little studied because it cannot be propagated continuously in the laboratory except in non-human primates. We sequenced the genome of P. vivax to shed light on its distinctive biological features, and as a means to drive development of new drugs and vaccines. Here we describe the synteny and isochore structure of P. vivax chromosomes, and show that the parasite resembles other malaria parasites in gene content and metabolic potential, but possesses novel gene families and potential alternative invasion pathways not recognized previously. Completion of the P. vivax genome provides the scientific community with a valuable resource that can be used to advance investigation into this neglected species.

Published

2008

13. Volume of the infarct in the anterior lobe of the monkey's pituitary gland shortly after stalk section.

Author

ADAMS JH, DANIEL PM, and PRICHARD MM

Subjects

Animals, Humans, Haplorhini, Infarction, Pituitary Gland, Pituitary Gland, Anterior

Published

1963