Your search keyword '"Hikaru Nagaoka"' showing total 37 results

1. Antibody responses in Burkinabe children against P. falciparum proteins associated with reduced risk of clinical malaria

Author

Takaaki Yuguchi, Benedicta O. Dankyi, Rattanaporn Rojrung, Hikaru Nagaoka, Bernard N. Kanoi, Alfred B. Tiono, Issa Nebie, Alphonse Ouedraogo, Kazutoyo Miura, Jetsumon Sattabongkot, Sodiomon B. Sirima, Takafumi Tsuboi, and Eizo Takashima

Subjects

Plasmodium falciparum, blood-stage, serology, wheat germ cell-free system, AlphaScreen, Burkinabe children, Immunologic diseases. Allergy, RC581-607

Abstract

Individuals residing in malaria-endemic regions with high disease transmission can develop semi-immunity within five years of age. Although understanding the target of the IgGs in this age group helps discover novel blood-stage vaccine candidates and serological markers, it has not been well elucidated due to limited accessibility to plasmodial antigens and samples. This study presents the first comprehensive analysis of antibody levels in plasma obtained from Burkinabe children (n=80, aged 0 to 5 years) to 1307 Plasmodium falciparum proteins expressed by the eukaryotic wheat germ cell-free system. Antibody levels were measured by AlphaScreen. We found that 98% of antigens were immunoreactive. The number of reactive antigens by the individual was correlated with increasing age. The most significant increases in seroprevalence occur during the first 2 years of life. By correlating antibody levels and the number of clinical malaria during a 1-year follow-up period, we identified 173 potential protein targets which might be associated with clinical immunity. These results provide valuable insights into how children acquired semi-immunity to malaria in their early lives.

Published

2025

2. Pfs230 Domain 7 is targeted by a potent malaria transmission-blocking monoclonal antibody

Author

Maartje R. Inklaar, Roos M. de Jong, Ezra T. Bekkering, Hikaru Nagaoka, Felix L. Fennemann, Karina Teelen, Marga van de Vegte-Bolmer, Geert-Jan van Gemert, Rianne Stoter, C. Richter King, Nicholas I. Proellochs, Teun Bousema, Eizo Takashima, Takafumi Tsuboi, and Matthijs M. Jore

Subjects

Immunologic diseases. Allergy, RC581-607, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Malaria transmission-blocking vaccines (TBVs) aim to induce antibodies that block Plasmodium parasite development in the mosquito midgut, thus preventing mosquitoes from becoming infectious. While the Pro-domain and first of fourteen 6-Cysteine domains (Pro-D1) of the Plasmodium gamete surface protein Pfs230 are known targets of transmission-blocking antibodies, no studies to date have discovered other Pfs230 domains that are functional targets. Here, we show that a murine monoclonal antibody (mAb), 18F25.1, targets Pfs230 Domain 7. We generated a subclass-switched complement-fixing variant, mAb 18F25.2a, using a CRISPR/Cas9-based hybridoma engineering method. This subclass-switched mAb 18F25.2a induced lysis of female gametes in vitro. Importantly, mAb 18F25.2a potently reduced P. falciparum infection of Anopheles stephensi mosquitoes in a complement-dependent manner, as assessed by standard membrane feeding assays. Together, our data identify Pfs230 Domain 7 as target for transmission-blocking antibodies and provide a strong incentive to study domains outside Pfs230Pro-D1 as TBV candidates.

Published

2023

3. GATS tag system is compatible with biotin labelling methods for protein analysis

Author

Kohdai Yamada, Fumiya Soga, Soh Tokunaga, Hikaru Nagaoka, Tatsuhiko Ozawa, Hiroyuki Kishi, Eizo Takashima, and Tatsuya Sawasaki

Subjects

Medicine, Science

Abstract

Abstract Polypeptide tags and biotin labelling technologies are widely used for protein analyses in biochemistry and cell biology. However, many peptide tag epitopes contain lysine residues (or amino acids) that are masked after biotinylation. Here, we propose the GATS tag system without a lysine residue and with high sensitivity and low non-specific binding using a rabbit monoclonal antibody against Plasmodium falciparum glycosylphosphatidylinositol (GPI)-anchored micronemal antigen (PfGAMA). From 14 monoclonal clones, an Ra3 clone was selected as it recognized an epitope—TLSVGVQNTF—without a lysine residue; this antibody and epitope tag set was called the GATS tag system. Surface plasmon resonance analysis showed that the tag system had a high affinity of 8.71 × 10–9 M. GATS tag indicated a very low background with remarkably high sensitivity and specificity in immunoblotting using the lysates of mammalian cells. It also showed a high sensitivity for immunoprecipitation and immunostaining of cultured human cells. The tag system was highly sensitive in both biotin labelling methods for proteins using NHS-Sulfo-biotin and BioID (proximity-dependent biotin identification) in the human cells, as opposed to a commercially available tag system having lysine residues, which showed reduced sensitivity. These results showed that the GATS tag system is suitable for methods such as BioID involving labelling lysine residues.

Published

2023

4. The Need for Novel Asexual Blood-Stage Malaria Vaccine Candidates for Plasmodium falciparum

Author

Eizo Takashima, Hitoshi Otsuki, Masayuki Morita, Daisuke Ito, Hikaru Nagaoka, Takaaki Yuguchi, Ifra Hassan, and Takafumi Tsuboi

Subjects

antigen discovery, asexual blood stage, malaria, vaccine, Plasmodium falciparum, Microbiology, QR1-502

Abstract

Extensive control efforts have significantly reduced malaria cases and deaths over the past two decades, but in recent years, coupled with the COVID-19 pandemic, success has stalled. The WHO has urged the implementation of a number of interventions, including vaccines. The modestly effective RTS,S/AS01 pre-erythrocytic vaccine has been recommended by the WHO for use in sub-Saharan Africa against Plasmodium falciparum in children residing in moderate to high malaria transmission regions. A second pre-erythrocytic vaccine, R21/Matrix-M, was also recommended by the WHO on 3 October 2023. However, the paucity and limitations of pre-erythrocytic vaccines highlight the need for asexual blood-stage malaria vaccines that prevent disease caused by blood-stage parasites. Few asexual blood-stage vaccine candidates have reached phase 2 clinical development, and the challenges in terms of their efficacy include antigen polymorphisms and low immunogenicity in humans. This review summarizes the history and progress of asexual blood-stage malaria vaccine development, highlighting the need for novel candidate vaccine antigens/molecules.

Published

2024

5. Identification of novel Plasmodium vivax proteins associated with protection against clinical malaria

Author

Ramin Mazhari, Eizo Takashima, Rhea J. Longley, Shazia Ruybal-Pesantez, Michael T. White, Bernard N. Kanoi, Hikaru Nagaoka, Benson Kiniboro, Peter Siba, Takafumi Tsuboi, and Ivo Mueller

Subjects

malaria, Plasmodium vivax, vaccine, antibody, naturally acquired immunity, protective immunity, Microbiology, QR1-502

Abstract

As progress towards malaria elimination continues, the challenge posed by the parasite species Plasmodium vivax has become more evident. In many regions co-endemic for P. vivax and Plasmodium falciparum, as transmission has declined the proportion of cases due to P. vivax has increased. Novel tools that directly target P. vivax are thus warranted for accelerated elimination. There is currently no advanced vaccine for P. vivax and only a limited number of potential candidates in the pipeline. In this study we aimed to identify promising P. vivax proteins that could be used as part of a subunit vaccination approach. We screened 342 P. vivax protein constructs for their ability to induce IgG antibody responses associated with protection from clinical disease in a cohort of children from Papua New Guinea. This approach has previously been used to successfully identify novel candidates. We were able to confirm previous results from our laboratory identifying the proteins reticulocyte binding protein 2b and StAR-related lipid transfer protein, as well as at least four novel candidates with similar levels of predicted protective efficacy. Assessment of these P. vivax proteins in further studies to confirm their potential and identify functional mechanisms of protection against clinical disease are warranted.

Published

2023

6. A novel asexual blood-stage malaria vaccine candidate: PfRipr5 formulated with human-use adjuvants induces potent growth inhibitory antibodies

Author

Eizo Takashima, Hikaru Nagaoka, Ricardo Correia, Paula M. Alves, António Roldão, Dennis Christensen, Jeffrey A. Guderian, Akihisa Fukushima, Nicola K. Viebig, Hilde Depraetere, and Takafumi Tsuboi

Subjects

asexual blood-stage malaria vaccine, PfRipr5, Plasmodium falciparum, adjuvant, Alhydrogel, GLA-SE, Immunologic diseases. Allergy, RC581-607

Abstract

PfRipr is a highly conserved asexual-blood stage malaria vaccine candidate against Plasmodium falciparum. PfRipr5, a protein fragment of PfRipr inducing the most potent inhibitory antibodies, is a promising candidate for the development of next-generation malaria vaccines, requiring validation of its potential when formulated with adjuvants already approved for human use. In this study, PfRipr5 antigen was efficiently produced in a tank bioreactor using insect High Five cells and the baculovirus expression vector system; purified PfRipr5 was thermally stable in its monomeric form, had high purity and binding capacity to functional monoclonal anti-PfRipr antibody. The formulation of purified PfRipr5 with Alhydrogel®, GLA-SE or CAF®01 adjuvants accepted for human use showed acceptable compatibility. Rabbits immunized with these formulations induced comparable levels of anti-PfRipr5 antibodies, and significantly higher than the control group immunized with PfRipr5 alone. To investigate the efficacy of the antibodies, we used an in vitro parasite growth inhibition assay (GIA). The highest average GIA activity amongst all groups was attained with antibodies induced by immunization with PfRipr5 formulated with CAF®01. Overall, this study validates the potential of adjuvanted PfRipr5 as an asexual blood-stage malaria vaccine candidate, with PfRipr5/CAF®01 being a promising formulation for subsequent pre-clinical and clinical development.

Published

2022

7. High-Throughput Antibody Profiling Identifies Targets of Protective Immunity against P. falciparum Malaria in Thailand

Author

Ifra Hassan, Bernard N. Kanoi, Hikaru Nagaoka, Jetsumon Sattabongkot, Rachanee Udomsangpetch, Takafumi Tsuboi, and Eizo Takashima

Subjects

malaria, wheat germ cell-free system, immunoscreening, AlphaScreen, Microbiology, QR1-502

Abstract

Malaria poses a significant global health challenge, resulting in approximately 600,000 deaths each year. Individuals living in regions with endemic malaria have the potential to develop partial immunity, thanks in part to the presence of anti-plasmodium antibodies. As efforts are made to optimize and implement strategies to reduce malaria transmission and ultimately eliminate the disease, it is crucial to understand how these interventions impact naturally acquired protective immunity. To shed light on this, our study focused on assessing antibody responses to a carefully curated library of P. falciparum recombinant proteins (n = 691) using samples collected from individuals residing in a low-malaria-transmission region of Thailand. We conducted the antibody assays using the AlphaScreen system, a high-throughput homogeneous proximity-based bead assay that detects protein interactions. We observed that out of the 691 variable surface and merozoite stage proteins included in the library, antibodies to 268 antigens significantly correlated with the absence of symptomatic malaria in an univariate analysis. Notably, the most prominent antigens identified were P. falciparum erythrocyte membrane protein 1 (PfEMP1) domains. These results align with our previous research conducted in Uganda, suggesting that similar antigens like PfEMP1s might play a pivotal role in determining infection outcomes in diverse populations. To further our understanding, it remains critical to conduct functional characterization of these identified proteins, exploring their potential as correlates of protection or as targets for vaccine development.

Published

2023

8. Recruitment of Irgb6 to the membrane is a direct trigger for membrane deformation

Author

Hiroshi Yamada, Tadashi Abe, Hikaru Nagaoka, Eizo Takashima, Ryo Nitta, Masahiro Yamamoto, and Kohji Takei

Subjects

IFN-inducible GTPase, Irgb6, GTPase, membrane, T. gondii, Microbiology, QR1-502

Abstract

Irgb6 is a member of interferon γ-induced immunity related GTPase (IRG), and one of twenty “effector” IRGs, which coordinately attack parasitophorous vacuole membrane (PVM), causing death of intracellular pathogen. Although Irgb6 plays a pivotal role as a pioneer in the process of PVM disruption, the direct effect of Irgb6 on membrane remained to be elucidated. Here, we utilized artificial lipid membranes to reconstitute Irgb6-membrane interaction in vitro, and revealed that Irgb6 directly deformed the membranes. Liposomes incubated with recombinant Irgb6 were drastically deformed generating massive tubular protrusions in the absence of guanine nucleotide, or with GMP-PNP. Liposome deformation was abolished by incubating with Irgb6-K275A/R371A, point mutations at membrane targeting residues. The membrane tubules generated by Irgb6 were mostly disappeared by the addition of GTP or GDP, which are caused by detachment of Irgb6 from membrane. Binding of Irgb6 to the membrane, which was reconstituted in vitro using lipid monolayer, was stimulated at GTP-bound state. Irgb6 GTPase activity was stimulated by the presence of liposomes more than eightfold. Irgb6 GTPase activity in the absence of membrane was also slightly stimulated, by lowering ionic strength, or by increasing protein concentration, indicating synergistic stimulation of the GTPase activity. These results suggest that membrane targeting of Irgb6 and resulting membrane deformation does not require GTP, but converting into GTP-bound state is crucial for detaching Irgb6 from the membrane, which might coincident with local membrane disruption.

Published

2022

9. Meta-Analysis of Human Antibodies Against Plasmodium falciparum Variable Surface and Merozoite Stage Antigens

Author

Eizo Takashima, Bernard N. Kanoi, Hikaru Nagaoka, Masayuki Morita, Ifra Hassan, Nirianne M. Q. Palacpac, Thomas G. Egwang, Toshihiro Horii, Jesse Gitaka, and Takafumi Tsuboi

Subjects

Plasmodium falciparum, variable surface antigens, PfEMP1, RIFIN, malaria immunity, PCA, Immunologic diseases. Allergy, RC581-607

Abstract

Concerted efforts to fight malaria have caused significant reductions in global malaria cases and mortality. Sustaining this will be critical to avoid rebound and outbreaks of seasonal malaria. Identifying predictive attributes that define clinical malaria will be key to guide development of second-generation tools to fight malaria. Broadly reactive antibodies against variable surface antigens that are expressed on the surface of infected erythrocytes and merozoites stage antigens are targets of naturally acquired immunity and prime candidates for anti-malaria therapeutics and vaccines. However, predicting the relationship between the antigen-specific antibodies and protection from clinical malaria remains unresolved. Here, we used new datasets and multiple approaches combined with re-analysis of our previous data to assess the multi-dimensional and complex relationship between antibody responses and clinical malaria outcomes. We observed 22 antigens (17 PfEMP1 domains, 3 RIFIN family members, merozoite surface protein 3 (PF3D7_1035400), and merozoites-associated armadillo repeats protein (PF3D7_1035900) that were selected across three different clinical malaria definitions (1,000/2,500/5,000 parasites/µl plus fever). In addition, Principal Components Analysis (PCA) indicated that the first three components (Dim1, Dim2 and Dim3 with eigenvalues of 306, 48, and 29, respectively) accounted for 66.1% of the total variations seen. Specifically, the Dim1, Dim2 and Dim3 explained 52.8%, 8.2% and 5% of variability, respectively. We further observed a significant relationship between the first component scores and age with antibodies to PfEMP1 domains being the key contributing variables. This is consistent with a recent proposal suggesting that there is an ordered acquisition of antibodies targeting PfEMP1 proteins. Thus, although limited, and further work on the significance of the selected antigens will be required, these approaches may provide insights for identification of drivers of naturally acquired protective immunity as well as guide development of additional tools for malaria elimination and eradication.

Published

2022

10. Asexual Blood-Stage Malaria Vaccine Candidate PfRipr5: Enhanced Production in Insect Cells

Author

Ricardo Correia, Bárbara Fernandes, Rute Castro, Hikaru Nagaoka, Eizo Takashima, Takafumi Tsuboi, Akihisa Fukushima, Nicola K. Viebig, Hilde Depraetere, Paula M. Alves, and António Roldão

Subjects

malaria asexual blood-stage vaccine, PfRipr5, insect cells, baculovirus expression vector system, low temperature, improved production, Biotechnology, TP248.13-248.65

Abstract

The malaria asexual blood-stage antigen PfRipr and its most immunogenic fragment PfRipr5 have recently risen as promising vaccine candidates against this infectious disease. Continued development of high-yielding, scalable production platforms is essential to advance the malaria vaccine research. Insect cells have supplied the production of numerous vaccine antigens in a fast and cost-effective manner; improving this platform further could prove key to its wider use. In this study, insect (Sf9 and High Five) and human (HEK293) cell hosts as well as process-optimizing strategies (new baculovirus construct designs and a culture temperature shift to hypothermic conditions) were employed to improve the production of the malaria asexual blood-stage vaccine candidate PfRipr5. Protein expression was maximized using High Five cells at CCI of 2 × 106 cell/mL and MOI of 0.1 pfu/cell (production yield = 0.49 mg/ml), with high-purity PfRipr5 binding to a conformational anti-PfRipr monoclonal antibody known to hold GIA activity and parasite PfRipr staining capacity. Further improvements in the PfRipr5 expression were achieved by designing novel expression vector sequences and performing a culture temperature shift to hypothermic culture conditions. Addition of one alanine (A) amino acid residue adjacent to the signal peptide cleavage site and a glycine-serine linker (GGSGG) between the PfRipr5 sequence and the purification tag (His6) induced a 2.2-fold increase in the expression of secreted PfRipr5 over using the expression vector with none of these additions. Performing a culture temperature shift from the standard 27–22°C at the time of infection improved the PfRipr5 expression by up to 1.7 fold. Notably, a synergistic effect was attained when combining both strategies, enabling to increase production yield post-purification by 5.2 fold, with similar protein quality (i.e., purity and binding to anti-PfRipr monoclonal antibody). This work highlights the potential of insect cells to produce the PfRipr5 malaria vaccine candidate and the importance of optimizing the expression vector and culture conditions to boost the expression of secreted proteins.

Published

2022

11. The Lipid-Binding Defective Dynamin 2 Mutant in Charcot-Marie-Tooth Disease Impairs Proper Actin Bundling and Actin Organization in Glomerular Podocytes

Author

Eriko Hamasaki, Natsuki Wakita, Hiroki Yasuoka, Hikaru Nagaoka, Masayuki Morita, Eizo Takashima, Takayuki Uchihashi, Tetsuya Takeda, Tadashi Abe, Ji-Won Lee, Tadahiro Iimura, Moin A Saleem, Naohisa Ogo, Akira Asai, Akihiro Narita, Kohji Takei, and Hiroshi Yamada

Subjects

dynamin, podocyte, actin, bundle, GTPase, CMT, Biology (General), QH301-705.5

Abstract

Dynamin is an endocytic protein that functions in vesicle formation by scission of invaginated membranes. Dynamin maintains the structure of foot processes in glomerular podocytes by directly and indirectly interacting with actin filaments. However, molecular mechanisms underlying dynamin-mediated actin regulation are largely unknown. Here, biochemical and cell biological experiments were conducted to uncover how dynamin modulates interactions between membranes and actin in human podocytes. Actin-bundling, membrane tubulating, and GTPase activities of dynamin were examined in vitro using recombinant dynamin 2-wild-type (WT) or dynamin 2-K562E, which is a mutant found in Charcot-Marie-Tooth patients. Dynamin 2-WT and dynamin 2-K562E led to the formation of prominent actin bundles with constant diameters. Whereas liposomes incubated with dynamin 2-WT resulted in tubule formation, dynamin 2-K562E reduced tubulation. Actin filaments and liposomes stimulated dynamin 2-WT GTPase activity by 6- and 20-fold, respectively. Actin-filaments, but not liposomes, stimulated dynamin 2-K562E GTPase activity by 4-fold. Self-assembly-dependent GTPase activity of dynamin 2-K562E was reduced to one-third compared to that of dynamin 2-WT. Incubation of liposomes and actin with dynamin 2-WT led to the formation of thick actin bundles, which often bound to liposomes. The interaction between lipid membranes and actin bundles by dynamin 2-K562E was lower than that by dynamin 2-WT. Dynamin 2-WT partially colocalized with stress fibers and actin bundles based on double immunofluorescence of human podocytes. Dynamin 2-K562E expression resulted in decreased stress fiber density and the formation of aberrant actin clusters. Dynamin 2-K562E colocalized with α-actinin-4 in aberrant actin clusters. Reformation of stress fibers after cytochalasin D-induced actin depolymerization and washout was less effective in dynamin 2-K562E-expressing cells than that in dynamin 2-WT. Bis-T-23, a dynamin self-assembly enhancer, was unable to rescue the decreased focal adhesion numbers and reduced stress fiber density induced by dynamin 2-K562E expression. These results suggest that the low affinity of the K562E mutant for lipid membranes, and atypical self-assembling properties, lead to actin disorganization in HPCs. Moreover, lipid-binding and self-assembly of dynamin 2 along actin filaments are required for podocyte morphology and functions. Finally, dynamin 2-mediated interactions between actin and membranes are critical for actin bundle formation in HPCs.

Published

2022

12. Identification of Novel Malaria Transmission-Blocking Vaccine Candidates

Author

Eizo Takashima, Mayumi Tachibana, Masayuki Morita, Hikaru Nagaoka, Bernard N. Kanoi, and Takafumi Tsuboi

Subjects

immuno-profiling, malaria, Plasmodium, reverse vaccinology, transmission-blocking vaccine (TBV), wheat germ cell-free system (WGCFS), Microbiology, QR1-502

Abstract

Control measures have significantly reduced malaria morbidity and mortality in the last two decades; however, the downward trends have stalled and have become complicated by the emergence of COVID-19. Significant efforts have been made to develop malaria vaccines, but currently only the RTS,S/AS01 vaccine against Plasmodium falciparum has been recommended by the WHO, for widespread use among children in sub-Saharan Africa. The efficacy of RTS,S/AS01 is modest, and therefore the development of more efficacious vaccines is still needed. In addition, the development of transmission-blocking vaccines (TBVs) to reduce the parasite transmission from humans to mosquitoes is required toward the goal of malaria elimination. Few TBVs have reached clinical development, and challenges include low immunogenicity or high reactogenicity in humans. Therefore, novel approaches to accelerate TBV research and development are urgently needed, especially novel TBV candidate discovery. In this mini review we summarize the progress in TBV research and development, novel TBV candidate discovery, and discuss how to accelerate novel TBV candidate discovery.

Published

2021

13. Characterization of Naturally Acquired Immunity to a Panel of Antigens Expressed in Mature P. falciparum Gametocytes

Author

Michelle K. Muthui, Eizo Takashima, Brian R. Omondi, Christine Kinya, William I. Muasya, Hikaru Nagaoka, Kennedy W. Mwai, Benedict Orindi, Juliana Wambua, Teun Bousema, Chris Drakeley, Andrew M. Blagborough, Kevin Marsh, Philip Bejon, and Melissa C. Kapulu

Subjects

Plasmodium falciparum, naturally acquired immunity, mature gametocytes, seroepidemiology, malaria transmission, Microbiology, QR1-502

Abstract

IntroductionNaturally acquired immune responses against antigens expressed on the surface of mature gametocytes develop in individuals living in malaria-endemic areas. Evidence suggests that such anti-gametocyte immunity can block the development of the parasite in the mosquito, thus playing a role in interrupting transmission. A better comprehension of naturally acquired immunity to these gametocyte antigens can aid the development of transmission-blocking vaccines and improve our understanding of the human infectious reservoir.MethodsAntigens expressed on the surface of mature gametocytes that had not previously been widely studied for evidence of naturally acquired immunity were identified for protein expression alongside Pfs230-C using either the mammalian HEK293E or the wheat germ cell-free expression systems. Where there was sequence variation in the candidate antigens (3D7 vs a clinical isolate PfKE04), both variants were expressed. ELISA was used to assess antibody responses against these antigens, as well as against crude stage V gametocyte extract (GE) and AMA1 using archived plasma samples from individuals recruited to participate in malaria cohort studies. We analyzed antibody levels (estimated from optical density units using a standardized ELISA) and seroprevalence (defined as antibody levels greater than three standard deviations above the mean levels of a pool of malaria naïve sera). We described the dynamics of antibody responses to these antigens by identifying factors predictive of antibody levels using linear regression models.ResultsOf the 25 antigens selected, seven antigens were produced successfully as recombinant proteins, with one variant antigen, giving a total of eight proteins for evaluation. Antibodies to the candidate antigens were detectable in the study population (N = 216), with seroprevalence ranging from 37.0% (95% CI: 30.6%, 43.9%) for PSOP1 to 77.8% (95% CI: 71.6%, 83.1%) for G377 (3D7 variant). Responses to AMA1 and GE were more prevalent than those to the gametocyte proteins at 87.9% (95% CI: 82.8%, 91.9%) and 88.3% (95% CI: 83.1%, 92.4%), respectively. Additionally, both antibody levels and breadth of antibody responses were associated with age and concurrent parasitaemia.ConclusionAge and concurrent parasitaemia remain important determinants of naturally acquired immunity to gametocyte antigens. Furthermore, we identify novel candidates for transmission-blocking activity evaluation.

Published

2021

14. Plasmodium yoelii Erythrocyte Binding Like Protein Interacts With Basigin, an Erythrocyte Surface Protein

Author

Takaaki Yuguchi, Bernard N. Kanoi, Hikaru Nagaoka, Toyokazu Miura, Daisuke Ito, Hiroyuki Takeda, Takafumi Tsuboi, Eizo Takashima, and Hitoshi Otsuki

Subjects

Plasmodium yoelii, PyEBL, basigin, invasion, protein-protein interaction, CD147, Microbiology, QR1-502

Abstract

Erythrocyte recognition and invasion is critical for the intra-erythrocytic development of Plasmodium spp. parasites. The multistep invasion process involves specific interactions between parasite ligands and erythrocyte receptors. Erythrocyte-binding-like (EBL) proteins, type I integral transmembrane proteins released from the merozoite micronemes, are known to play an important role in the initiation and formation of tight junctions between the apical end of the merozoite and the erythrocyte surface. In Plasmodium yoelii EBL (PyEBL), a single amino acid substitution in the putative Duffy binding domain dramatically changes parasite growth rate and virulence. This suggests that PyEBL is important for modulating the virulence of P. yoelii parasites. Based on these observations, we sought to elucidate the receptor of PyEBL that mediates its role as an invasion ligand. Using the eukaryotic wheat germ cell-free system, we systematically developed and screened a library of mouse erythrocyte proteins against native PyEBL using AlphaScreen technology. We report that PyEBL specifically interacts with basigin, an erythrocyte surface protein. We further confirmed that the N-terminal cysteine-rich Duffy binding-like region (EBL region 2), is responsible for the interaction, and that the binding is not affected by the C351Y mutation, which was previously shown to modulate virulence of P. yoelii. The identification of basigin as the putative PyEBL receptor offers new insights into the role of this molecule and provides an important base for in-depth studies towards developing novel interventions against malaria.

Published

2021

15. Global Repertoire of Human Antibodies Against Plasmodium falciparum RIFINs, SURFINs, and STEVORs in a Malaria Exposed Population

Author

Bernard N. Kanoi, Hikaru Nagaoka, Michael T. White, Masayuki Morita, Nirianne M. Q. Palacpac, Edward H. Ntege, Betty Balikagala, Adoke Yeka, Thomas G. Egwang, Toshihiro Horii, Takafumi Tsuboi, and Eizo Takashima

Subjects

Plasmodium falciparum, RIFIN, STEVOR, SURFIN, naturally acquired immunity, Immunologic diseases. Allergy, RC581-607

Abstract

Clinical immunity to malaria develops after repeated exposure to Plasmodium falciparum parasites. Broadly reactive antibodies against parasite antigens expressed on the surface of infected erythrocytes (variable surface antigens; VSAs) are candidates for anti-malaria therapeutics and vaccines. Among the VSAs, several RIFIN, STEVOR, and SURFIN family members have been demonstrated to be targets of naturally acquired immunity against malaria. For example, RIFIN family members are important ligands for opsonization of P. falciparum infected erythrocytes with specific immunoglobulins (IgG) acquiring broad protective reactivity. However, the global repertoire of human anti-VSAs IgG, its variation in children, and the key protective targets remain poorly understood. Here, we report wheat germ cell-free system-based production and serological profiling of a comprehensive library of A-RIFINs, B-RIFINs, STEVORs, and SURFINs derived from the P. falciparum 3D7 parasite strain. We observed that >98% of assayed proteins (n = 265) were immunogenic in malaria-exposed individuals in Uganda. The overall breadth of immune responses was significantly correlated with age but not with clinical malaria outcome among the study volunteers. However, children with high levels of antibodies to four RIFINs (PF3D7_0201000, PF3D7_1254500, PF3D7_1040600, PF3D7_1041100), STEVOR (PF3D7_0732000), and SURFIN 1.2 (PF3D7_0113600) had prospectively reduced the risk of developing febrile malaria, suggesting that the 5 antigens are important targets of protective immunity. Further studies on the significance of repeated exposure to malaria infection and maintenance of such high-level antibodies would contribute to a better understanding of susceptibility and naturally acquired immunity to malaria.

Published

2020

16. Blood-stage malaria vaccines: post-genome strategies for the identification of novel vaccine candidates

Author

Edward H. Ntege, Eizo Takashima, Masayuki Morita, Hikaru Nagaoka, Tomoko Ishino, and Takafumi Tsuboi

Subjects

antibody profiling, malaria vaccine, plasmodium falciparum, post-genome, protein array, reverse vaccinology, wheat germ cell-free protein synthesis system, Internal medicine, RC31-1245

Abstract

Introduction: An efficacious malaria vaccine is necessary to advance the current control measures towards malaria elimination. To-date, only RTS,S/AS01, a leading pre-erythrocytic stage vaccine completed phase 3 trials, but with an efficacy of 28–36% in children, and 18–26% in infants, that waned over time. Blood-stage malaria vaccines protect against disease, and are considered effective targets for the logical design of next generation vaccines to improve the RTS,S field efficacy. Therefore, novel blood-stage vaccine candidate discovery efforts are critical, albeit with several challenges including, high polymorphisms in vaccine antigens, poor understanding of targets of naturally protective immunity, and difficulties in the expression of high AT-rich plasmodial proteins. Areas covered: PubMed (www.ncbi.nlm.nih.gov/pubmed) was searched to review the progress and future prospects of malaria vaccine research and development. We focused on post-genome vaccine candidate discovery, malaria vaccine development, sequence diversity, pre-clinical and clinical trials. Expert commentary: Post-genome high-throughput technologies using wheat germ cell-free protein synthesis technology and immuno-profiling with sera from malaria patients with clearly defined outcomes are highlighted to overcome current challenges of malaria vaccine candidate discovery.

Published

2017

17. The N-Terminal Region of Plasmodium falciparum MSP10 Is a Target of Protective Antibodies in Malaria and Is Important for PfGAMA/PfMSP10 Interaction

Author

Hikaru Nagaoka, Bernard N. Kanoi, Kana Jinoka, Masayuki Morita, Thangavelu U. Arumugam, Nirianne M. Q. Palacpac, Thomas G. Egwang, Toshihiro Horii, Takafumi Tsuboi, and Eizo Takashima

Subjects

malaria, Plasmodium falciparum, blood-stage vaccine, PfMSP10, PfGAMA, Immunologic diseases. Allergy, RC581-607

Abstract

Clinical manifestation of malaria is mainly due to intra-erythrocytic development of Plasmodium parasites. Plasmodium falciparum merozoites, the invasive form of the blood-stage parasite, invade human erythrocytes in a complex but rapid process. This multi-step progression involves interactions between parasite and human host proteins. Here we show that antibodies against a vaccine antigen, PfGAMA, co-immunoprecipitate with PfMSP10. This interaction was validated as direct by surface plasmon resonance analysis. We then demonstrate that antibodies against PfMSP10 have growth inhibitory activity against cultured parasites, with the region PfMSP10 R1 that is critical for its interaction with PfGAMA being the key target. We also observe that the PfMSP10 R1 region is highly conserved among African field isolates. Lastly, we show that high levels of antibodies against PfMSP10 R1 associate with reduced risk to clinical malaria in children resident in a malaria endemic region in northern Uganda. Put together, these findings provide for the first time the functional context of the important role of PfGAMA/PfMSP10 interaction in erythrocyte invasion and unveil a novel asexual blood-stage malaria vaccine target for attenuating P. falciparum merozoite invasion.

Published

2019

18. Pfs230 Domain 7 is targeted by a potent malaria transmissionblocking monoclonal antibody.

Author

Inklaar, Maartje R., de Jong, Roos M., Bekkering, Ezra T., Hikaru Nagaoka, Fennemann, Felix L., Teelen, Karina, van de Vegte-Bolmer, Marga, van Gemert, Geert-Jan, Stoter, Rianne, King, C. Richter, Proellochs, Nicholas I., Bousema, Teun, Eizo Takashima, Takafumi Tsuboi, and Jore, Matthijs M.

Subjects

MONOCLONAL antibodies, ANOPHELES stephensi, OVUM, MALARIA, MALARIA vaccines

Abstract

Malaria transmission-blocking vaccines (TBVs) aim to induce antibodies that block Plasmodium parasite development in the mosquito midgut, thus preventing mosquitoes from becoming infectious. While the Pro-domain and first of fourteen 6-Cysteine domains (Pro-D1) of the Plasmodium gamete surface protein Pfs230 are known targets of transmission-blocking antibodies, no studies to date have discovered other Pfs230 domains that are functional targets. Here, we show that a murine monoclonal antibody (mAb), 18F25.1, targets Pfs230 Domain 7. We generated a subclass-switched complement-fixing variant, mAb 18F25.2a, using a CRISPR/Cas9-based hybridoma engineering method. This subclass-switched mAb 18F25.2a induced lysis of female gametes in vitro. Importantly, mAb 18F25.2a potently reduced P. falciparum infection of Anopheles stephensi mosquitoes in a complementdependent manner, as assessed by standard membrane feeding assays. Together, our data identify Pfs230 Domain 7 as target for transmission-blocking antibodies and provide a strong incentive to study domains outside Pfs230Pro-D1 as TBV candidates. [ABSTRACT FROM AUTHOR]

Published

2023

19. GATS Tag System for Protein Analysis with Biotin Labelling Methods

Author

Kohdai Yamada, Fumiya Soga, Soh Tokunaga, Hikaru Nagaoka, Tatsuhiko Ozawa, Hiroyuki Kishi, Eizo Takashima, and Tatsuya Sawasaki

Abstract

Polypeptide tags and biotin labelling technologies are widely used for protein analyses in biochemistry and cell biology. Although biotin labelling reacts with a lysine residue, many peptide tag epitopes have lysine residue(s). Here, we propose the GATS tag system without a lysine residue and with high sensitivity and low non-specific binding using a rabbit monoclonal antibody against Plasmodium falciparum glycosylphosphatidylinositol (GPI)- anchored micronemal antigen (PfGAMA). From 14 monoclonal clones, an Ra3 clone was selected as it recognized an epitope—TLSVGVQNTF—without a lysine residue; this antibody and epitope tag set was called the GATS tag system. Surface plasmon resonance analysis showed that the tag system had a high affinity of 8.71 × 10-9 M. GATS tag indicated a very low background with remarkably high sensitivity and specificity in immunoblotting using the lysates of mammalian cells. It also showed a high sensitivity for immunoprecipitation and immunostaining of cultured human cells. The tag system was highly sensitive in both biotin labelling methods for proteins using NHS-Sulfo-biotin and BioID (proximity-dependent biotin identification) in the human cells, as opposed to a commercially available tag system having lysine residues, which showed reduced sensitivity. These results showed that the GATS tag system is suitable for methods such as BioID involving labelling lysine residues.

Published

2022

20. Dynamin 1 is important for microtubule organization and stabilization in glomerular podocytes

Author

The Mon La, Hiromi Tachibana, Shun‐Ai Li, Tadashi Abe, Sayaka Seiriki, Hikaru Nagaoka, Eizo Takashima, Tetsuya Takeda, Daisuke Ogawa, Shin‐ichi Makino, Katsuhiko Asanuma, Masami Watanabe, Xuefei Tian, Shuta Ishibe, Ayuko Sakane, Takuya Sasaki, Jun Wada, Kohji Takei, and Hiroshi Yamada

Subjects

Male, 0301 basic medicine, Microtubule bundle formation, endocrine system, podocyte, Immunoelectron microscopy, Endocytic cycle, macromolecular substances, Kidney, Biochemistry, Podocyte, microtubules, Mice, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, primary process, Tubulin, Microtubule, dynamin, Genetics, medicine, Animals, Molecular Biology, Cells, Cultured, Dynamin I, Dynamin, Mice, Knockout, Podocytes, Chemistry, Epithelial Cells, Endocytosis, Rats, Cell biology, Mice, Inbred C57BL, Nocodazole, 030104 developmental biology, medicine.anatomical_structure, Acetylation, biological phenomena, cell phenomena, and immunity, Microtubule-Associated Proteins, 030217 neurology & neurosurgery, Biotechnology

Abstract

Dynamin 1 is a neuronal endocytic protein that participates in vesicle formation by scission of invaginated membranes. Dynamin 1 is also expressed in the kidney; however, its physiological significance to this organ remains unknown. Here, we show that dynamin 1 is crucial for microtubule organization and stabilization in glomerular podocytes. By immunofluorescence and immunoelectron microscopy, dynamin 1 was concentrated at microtubules at primary processes in rat podocytes. By immunofluorescence of differentiated mouse podocytes (MPCs), dynamin 1 was often colocalized with microtubule bundles, which radially arranged toward periphery of expanded podocyte. In dynamin 1-depleted MPCs by RNAi, alpha-tubulin showed a dispersed linear filament-like localization, and microtubule bundles were rarely observed. Furthermore, dynamin 1 depletion resulted in the formation of discontinuous, short acetylated alpha-tubulin fragments, and the decrease of microtubule-rich protrusions. Dynamins 1 and 2 double-knockout podocytes showed dispersed acetylated alpha-tubulin and rare protrusions. In vitro, dynamin 1 polymerized around microtubules and cross-linked them into bundles, and increased their resistance to the disassembly-inducing reagents Ca(2+)and podophyllotoxin. In addition, overexpression and depletion of dynamin 1 in MPCs increased and decreased the nocodazole resistance of microtubules, respectively. These results suggest that dynamin 1 supports the microtubule bundle formation and participates in the stabilization of microtubules.

Published

2020

21. Antibodies against a short region of PfRipr inhibit Plasmodium falciparum merozoite invasion and PfRipr interaction with Rh5 and SEMA7A

Author

Takafumi Tsuboi, Bernard N. Kanoi, Hikaru Nagaoka, Akihisa Fukushima, Masamitsu Aoki, Edward H. Ntege, and Eizo Takashima

Subjects

0301 basic medicine, Protein vaccines, Erythrocytes, Plasmodium falciparum, Protozoan Proteins, lcsh:Medicine, Antigens, Protozoan, Semaphorins, GPI-Linked Proteins, Antibodies, Article, Truncate, Pathogenesis, 03 medical and health sciences, 0302 clinical medicine, Antigens, CD, medicine, Humans, Malaria, Falciparum, Receptor, lcsh:Science, chemistry.chemical_classification, Multidisciplinary, biology, Merozoites, Malaria vaccine, lcsh:R, medicine.disease, Cell biology, Amino acid, Parasite biology, 030104 developmental biology, Gene Expression Regulation, chemistry, biology.protein, lcsh:Q, Antibody, Carrier Proteins, 030217 neurology & neurosurgery, Malaria, Protein Binding, Cysteine

Abstract

Plasmodium falciparum merozoite invasion into erythrocytes is an essential step of the blood-stage cycle, survival of parasites, and malaria pathogenesis. P. falciparum merozoite Rh5 interacting protein (PfRipr) forms a complex with Rh5 and CyRPA in sequential molecular events leading to erythrocyte invasion. Recently we described PfRipr as a conserved protein that induces strain-transcending growth inhibitory antibodies in in vitro assays. However, being a large and complex protein of 1086 amino acids (aa) with 87 cysteine residues, PfRipr is difficult to express in conventional expression systems towards vaccine development. In this study we sought to identify the most potent region of PfRipr that could be developed to overcome difficulties related to protein expression, as well as to elucidate the invasion inhibitory mechanism of anti-PfRipr antibodies. Using the wheat germ cell-free system, Ecto- PfRipr and truncates of approximately 200 aa were expressed as soluble proteins. We demonstrate that antibodies against PfRipr truncate 5 (PfRipr_5: C720-D934), a region within the PfRipr C-terminal EGF-like domains, potently inhibit merozoite invasion. Furthermore, the antibodies strongly block PfRipr/Rh5 interaction, as well as that between PfRipr and its erythrocyte-surface receptor, SEMA7A. Taken together, PfRipr_5 is a potential candidate for further development as a blood-stage malaria vaccine.

Published

2020

22. Identification of Novel Malaria Transmission-Blocking Vaccine Candidates

Author

Takafumi Tsuboi, Masayuki Morita, Mayumi Tachibana, Eizo Takashima, Hikaru Nagaoka, and Bernard N. Kanoi

Subjects

Microbiology (medical), Plasmodium, Computer science, Mini Review, Immunology, Plasmodium falciparum, malaria, transmission-blocking vaccine (TBV), Microbiology, immuno-profiling, wheat germ cell-free system (WGCFS), Cellular and Infection Microbiology, reverse vaccinology, Malaria transmission, parasitic diseases, Malaria Vaccines, Animals, Humans, Malaria, Falciparum, Child, Blocking (radio), SARS-CoV-2, COVID-19, Virology, QR1-502, Identification (information), Infectious Diseases

Abstract

Control measures have significantly reduced malaria morbidity and mortality in the last two decades; however, the downward trends have stalled and have become complicated by the emergence of COVID-19. Significant efforts have been made to develop malaria vaccines, but currently only the RTS,S/AS01 vaccine against Plasmodium falciparum has been recommended by the WHO, for widespread use among children in sub-Saharan Africa. The efficacy of RTS,S/AS01 is modest, and therefore the development of more efficacious vaccines is still needed. In addition, the development of transmission-blocking vaccines (TBVs) to reduce the parasite transmission from humans to mosquitoes is required toward the goal of malaria elimination. Few TBVs have reached clinical development, and challenges include low immunogenicity or high reactogenicity in humans. Therefore, novel approaches to accelerate TBV research and development are urgently needed, especially novel TBV candidate discovery. In this mini review we summarize the progress in TBV research and development, novel TBV candidate discovery, and discuss how to accelerate novel TBV candidate discovery.

Published

2021

23. Malaria transmission-blocking vaccines: wheat germ cell-free technology can accelerate vaccine development

Author

Tomoko Ishino, Hikaru Nagaoka, Mayumi Tachibana, Takafumi Tsuboi, Eizo Takashima, Kazutoyo Miura, Masayuki Morita, Bernard N. Kanoi, Minami Baba, and Motomi Torii

Subjects

0301 basic medicine, Databases, Factual, Plasmodium falciparum, Immunology, Protozoan Proteins, Cell free, 03 medical and health sciences, Immunogenicity, Vaccine, 0302 clinical medicine, Malaria transmission, Malaria elimination, Malaria Vaccines, parasitic diseases, Drug Discovery, Humans, Medicine, 030212 general & internal medicine, Malaria, Falciparum, Triticum, Pharmacology, Cell-Free System, biology, business.industry, Malaria vaccine, Immunogenicity, Wheat germ, biology.organism_classification, medicine.disease, Recombinant Proteins, Malaria, Germ Cells, 030104 developmental biology, Molecular Medicine, business

Abstract

Introduction: Highly effective malaria vaccines are essential component toward malaria elimination. Although the leading malaria vaccine, RTS,S/AS01, with modest efficacy is being evaluated in a pilot feasibility trial, development of a malaria transmission-blocking vaccine (TBV) could make a major contribution toward malaria elimination. Only a few TBV antigens have reached pre-clinical or clinical development but with several challenges including difficulties in the expression of malaria recombinant proteins and low immunogenicity in humans. Therefore, novel approaches to accelerate TBV research to preclinical development are critical to generate an efficacious TBV.Areas covered: PubMed was searched to review the progress and future prospects of malaria TBV research and development. We also reviewed registered trials at ClinicalTrials.gov as well as post-genome TBV candidate discovery research including our efforts.Expert opinion: Wheat germ cell-free protein synthesis technology can accelerate TBV development by overcoming some current challenges of TBV research.

Published

2019

24. PfMSA180 is a novel Plasmodium falciparum vaccine antigen that interacts with human erythrocyte integrin associated protein (CD47)

Author

Eizo Takashima, Chisa Sasaoka, Hikaru Nagaoka, Daisuke Ito, Takafumi Tsuboi, Rachanee Udomsangpetch, Bernard N. Kanoi, Jetsumon Sattabongkot, Takaaki Yuguchi, Masayuki Morita, and Tomoko Ishino

Subjects

0301 basic medicine, Erythrocytes, Integrin, Plasmodium falciparum, Protozoan Proteins, Antibodies, Protozoan, lcsh:Medicine, CD47 Antigen, Plasmodium, Article, Microbiology, 03 medical and health sciences, Mice, 0302 clinical medicine, Antigen, Malaria Vaccines, medicine, Animals, Humans, Malaria, Falciparum, lcsh:Science, Multidisciplinary, biology, Malaria vaccine, Merozoites, CD47, lcsh:R, medicine.disease, biology.organism_classification, 030104 developmental biology, Antibody Formation, biology.protein, lcsh:Q, Rabbits, Antibody, 030217 neurology & neurosurgery, Malaria

Abstract

Malaria symptoms and pathology are initiated by invasion of host erythrocytes by Plasmodium merozoites in a complex process that involves interactions between parasite and host erythrocyte proteins. Erythrocyte invasion presents attractive targets for malaria vaccine and drug development. Recently it was observed that antibodies against PfMSA180 (PF3D7_1014100) are associated with protection from symptomatic malaria, suggesting that this protein is a target of naturally acquired protective antibodies. Here we characterize PfMSA180, a ~170 kDa merozoite surface antigen that is potentially involved in erythrocyte invasion. PfMSA180 synthesized by the wheat germ cell-free system was used to raise antibodies in rabbits. Growth inhibition assays revealed that parasite invasion is inhibited by antibodies to the PfMSA180 C-terminal region, which contains an erythrocyte-binding domain. Surface plasmon resonance analysis showed that PfMSA180 specifically interacts with human erythrocyte integrin associated protein (CD47), suggesting that PfMSA180 plays a role during merozoite invasion of erythrocytes. Polymorphism analysis revealed that pfmsa180 is highly conserved among field isolates. We show that naturally acquired PfMSA180-specific antibodies responses are associated with protective immunity in a malaria-exposed Thai population. In sum, the data presented here supports further evaluation of the conserved erythrocyte-binding C-terminal region of PfMSA180 as an asexual blood-stage malaria vaccine candidate.

Published

2019

25. PV1 Protein from Plasmodium falciparum Exhibits Chaperone-Like Functions and Cooperates with Hsp100s

Author

Kyosuke Shinohara, Rio Midorikawa, Eizo Takashima, Ken Morishima, Manami Nakamura, Keiichi Noguchi, Kazuaki Hakamada, Masaaki Sugiyama, Hikaru Nagaoka, Akihiro Kawamoto, Masafumi Yohda, and Rintaro Inoue

Subjects

0301 basic medicine, Plasmodium falciparum, malaria, Protozoan Proteins, Catalysis, Article, Inorganic Chemistry, lcsh:Chemistry, 03 medical and health sciences, 0302 clinical medicine, Tetramer, Humans, Physical and Theoretical Chemistry, Molecular Biology, Structural unit, lcsh:QH301-705.5, Spectroscopy, translocon, Heat-Shock Proteins, chaperone unfolding, biology, Chemistry, Organic Chemistry, A protein, General Medicine, biology.organism_classification, Translocon, Computer Science Applications, Cell biology, Structure and function, 030104 developmental biology, lcsh:Biology (General), lcsh:QD1-999, Chaperone (protein), transport, biology.protein, 030217 neurology & neurosurgery

Abstract

Plasmodium falciparum parasitophorous vacuolar protein 1 (PfPV1), a protein unique to malaria parasites, is localized in the parasitophorous vacuolar (PV) and is essential for parasite growth. Previous studies suggested that PfPV1 cooperates with the Plasmodium translocon of exported proteins (PTEX) complex to export various proteins from the PV. However, the structure and function of PfPV1 have not been determined in detail. In this study, we undertook the expression, purification, and characterization of PfPV1. The tetramer appears to be the structural unit of PfPV1. The activity of PfPV1 appears to be similar to that of molecular chaperones, and it may interact with various proteins. PfPV1 could substitute CtHsp40 in the CtHsp104, CtHsp70, and CtHsp40 protein disaggregation systems. Based on these results, we propose a model in which PfPV1 captures various PV proteins and delivers them to PTEX through a specific interaction with HSP101.

Published

2020

26. Leveraging the wheat germ cell-free protein synthesis system to accelerate malaria vaccine development

Author

Hikaru Nagaoka, Bernard N. Kanoi, Takafumi Tsuboi, Masayuki Morita, and Eizo Takashima

Subjects

Cell-free protein synthesis, biology, Cell-Free System, Malaria vaccine, Reverse vaccinology, Plasmodium falciparum, Wheat germ, Antigens, Protozoan, Computational biology, biology.organism_classification, medicine.disease, Infectious Diseases, Protein Biosynthesis, parasitic diseases, Malaria Vaccines, medicine, Parasitology, Malaria, Falciparum, Malaria, Triticum

Abstract

Vaccines against infectious diseases have had great successes in the history of public health. Major breakthroughs have occurred in the development of vaccine-based interventions against viral and bacterial pathogens through the application of classical vaccine design strategies. In contrast the development of a malaria vaccine has been slow. Plasmodium falciparum malaria affects millions of people with nearly half of the world population at risk of infection. Decades of dedicated research has taught us that developing an effective vaccine will be time consuming, challenging, and expensive. Nevertheless, recent advancements such as the optimization of robust protein synthesis platforms, high-throughput immunoscreening approaches, reverse vaccinology, structural design of immunogens, lymphocyte repertoire sequencing, and the utilization of artificial intelligence, have renewed the prospects of an accelerated discovery of the key antigens in malaria. A deeper understanding of the major factors underlying the immunological and molecular mechanisms of malaria might provide a comprehensive approach to identifying novel and highly efficacious vaccines. In this review we discuss progress in novel antigen discoveries that leverage on the wheat germ cell-free protein synthesis system (WGCFS) to accelerate malaria vaccine development.

Published

2020

27. Characterization of a Plasmodium falciparum PHISTc protein, PF3D7_0801000, in blood- stage malaria parasites

Author

Eizo Takashima, Bernard N. Kanoi, Nirianne Marie Q. Palacpac, Takafumi Tsuboi, Toshihiro Horii, Takahiro Nakata, Masayuki Morita, Hikaru Nagaoka, and Thomas G. Egwang

Subjects

0301 basic medicine, 030231 tropical medicine, Population, Plasmodium falciparum, Protozoan Proteins, Antibodies, Protozoan, 03 medical and health sciences, 0302 clinical medicine, Immune system, Antigen, parasitic diseases, Malaria Vaccines, medicine, Coding region, Parasite hosting, Malaria, Falciparum, education, education.field_of_study, biology, Merozoites, 030108 mycology & parasitology, medicine.disease, biology.organism_classification, Virology, Infectious Diseases, biology.protein, Parasitology, Antibody, Malaria

Abstract

During intraerythrocytic development Plasmodium falciparum deploys numerous proteins to support erythrocyte invasion, intracellular growth and development, as well as host immune evasion. Since these proteins are key for parasite intraerythrocytic survival and propagation, they represent attractive targets for antimalarial vaccines. In this study we sought to characterize a member of the PHISTc family of proteins, PF3D7_0801000, as a potential vaccine target. Using the wheat germ cell-free system we expressed the N-terminal region of PF3D7_0801000 (G93-L494, PF3D7_0801000N) and generated specific immune sera. We observed that PF3D7_0801000 localizes in merozoites, and antibodies against PF3D7_0801000N modestly inhibit P. falciparum parasite growth in in vitro culture. Sliding window analysis of the coding sequence revealed that pf3d7_0801000n is relatively conserved among African parasite isolates. Antibody profiles in a malaria-exposed Ugandan population revealed that PF3D7_0801000N is strongly immunoreactive with antibody acquisition increasing with age. Taken together, these findings suggest the need for further evaluation of PF3D7_0801000 for its role in merozoite invasion and utility as an asexual blood-stage vaccine candidate antigen.

Published

2020

28. Global Repertoire of Human Antibodies Against Plasmodium falciparum RIFINs, SURFINs, and STEVORs in a Malaria Exposed Population

Author

Masayuki Morita, Adoke Yeka, Eizo Takashima, Takafumi Tsuboi, Nirianne Marie Q. Palacpac, Michael T. White, Thomas G. Egwang, Edward H. Ntege, Betty Balikagala, Bernard N. Kanoi, Toshihiro Horii, and Hikaru Nagaoka

Subjects

Male, 0301 basic medicine, lcsh:Immunologic diseases. Allergy, Adolescent, Immunology, Plasmodium falciparum, Protozoan Proteins, STEVOR, Antibodies, Protozoan, Antigens, Protozoan, SURFIN, Serology, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Immune system, Antigen, Immunity, parasitic diseases, medicine, Humans, Immunology and Allergy, Uganda, Prospective Studies, naturally acquired immunity, Malaria, Falciparum, Child, Original Research, biology, Membrane Proteins, biology.organism_classification, medicine.disease, Acquired immune system, Immunity, Innate, 030104 developmental biology, Antibody Formation, biology.protein, RIFIN, Female, Antibody, lcsh:RC581-607, Malaria, 030215 immunology

Abstract

Clinical immunity to malaria develops after repeated exposure to Plasmodium falciparum parasites. Broadly reactive antibodies against parasite antigens expressed on the surface of infected erythrocytes (variable surface antigens; VSAs) are candidates for anti-malaria therapeutics and vaccines. Among the VSAs, several RIFIN, STEVOR, and SURFIN family members have been demonstrated to be targets of naturally acquired immunity against malaria. For example, RIFIN family members are important ligands for opsonization of P. falciparum infected erythrocytes with specific immunoglobulins (IgG) acquiring broad protective reactivity. However, the global repertoire of human anti-VSAs IgG, its variation in children, and the key protective targets remain poorly understood. Here, we report wheat germ cell-free system-based production and serological profiling of a comprehensive library of A-RIFINs, B-RIFINs, STEVORs, and SURFINs derived from the P. falciparum 3D7 parasite strain. We observed that >98% of assayed proteins (n = 265) were immunogenic in malaria-exposed individuals in Uganda. The overall breadth of immune responses was significantly correlated with age but not with clinical malaria outcome among the study volunteers. However, children with high levels of antibodies to four RIFINs (PF3D7_0201000, PF3D7_1254500, PF3D7_1040600, PF3D7_1041100), STEVOR (PF3D7_0732000), and SURFIN 1.2 (PF3D7_0113600) had prospectively reduced the risk of developing febrile malaria, suggesting that the 5 antigens are important targets of protective immunity. Further studies on the significance of repeated exposure to malaria infection and maintenance of such high-level antibodies would contribute to a better understanding of susceptibility and naturally acquired immunity to malaria.

Published

2020

29. PV1, a novel Plasmodium falciparum merozoite dense granule protein, interacts with exported protein in infected erythrocytes

Author

Masayuki Morita, Bernard N. Kanoi, Tadahiro Iimura, Kazuaki Tokunaga, Takafumi Tsuboi, Eizo Takashima, Motomi Torii, Hikaru Nagaoka, Daisuke Ito, Takahiro Nakata, Ji-Won Lee, and Edward H. Ntege

Subjects

0301 basic medicine, Erythrocytes, Immunoprecipitation, Plasmodium falciparum, Protozoan Proteins, lcsh:Medicine, Plasma protein binding, Article, 03 medical and health sciences, 0302 clinical medicine, Cytosol, Animals, Humans, lcsh:Science, Microscopy, Multidisciplinary, biology, Chemistry, lcsh:R, Translocon, biology.organism_classification, Transport protein, Cell biology, Protein Transport, 030104 developmental biology, Merozoite dense granule, lcsh:Q, Dense granule, 030217 neurology & neurosurgery, Protein Binding

Abstract

Upon invasion, Plasmodium falciparum exports hundreds of proteins across its surrounding parasitophorous vacuole membrane (PVM) to remodel the infected erythrocyte. Although this phenomenon is crucial for the parasite growth and virulence, elucidation of precise steps in the export pathway is still required. A translocon protein complex, PTEX, is the only known pathway that mediates passage of exported proteins across the PVM. P. falciparum Parasitophorous Vacuolar protein 1 (PfPV1), a previously reported parasitophorous vacuole (PV) protein, is considered essential for parasite growth. In this study, we characterized PfPV1 as a novel merozoite dense granule protein. Structured illumination microscopy (SIM) analyses demonstrated that PfPV1 partially co-localized with EXP2, suggesting the protein could be a PTEX accessory molecule. Furthermore, PfPV1 and exported protein PTP5 co-immunoprecipitated with anti-PfPV1 antibody. Surface plasmon resonance (SPR) confirmed the proteins’ direct interaction. Additionally, we identified a PfPV1 High-affinity Region (PHR) at the C-terminal side of PTP5 where PfPV1 dominantly bound. SIM analysis demonstrated an export arrest of PTP5ΔPHR, a PTP5 mutant lacking PHR, suggesting PHR is essential for PTP5 export to the infected erythrocyte cytosol. The overall results suggest that PfPV1, a novel dense granule protein, plays an important role in protein export at PV.

Published

2018

30. The N-Terminal Region of Plasmodium falciparum MSP10 Is a Target of Protective Antibodies in Malaria and Is Important for PfGAMA/PfMSP10 Interaction

Author

Bernard N. Kanoi, Hikaru Nagaoka, Thangavelu U. Arumugam, Toshihiro Horii, Takafumi Tsuboi, Thomas G. Egwang, Masayuki Morita, Nirianne Marie Q. Palacpac, Eizo Takashima, and Kana Jinoka

Subjects

0301 basic medicine, lcsh:Immunologic diseases. Allergy, Immunology, Plasmodium falciparum, malaria, Context (language use), Biology, Plasmodium, 03 medical and health sciences, 0302 clinical medicine, PfGAMA, parasitic diseases, medicine, Immunology and Allergy, Parasite hosting, Malaria vaccine, medicine.disease, biology.organism_classification, Virology, blood-stage vaccine, 030104 developmental biology, biology.protein, Protective antibody, Antibody, PfMSP10, lcsh:RC581-607, Malaria, 030215 immunology

Abstract

Clinical manifestation of malaria is mainly due to intra-erythrocytic development of Plasmodium parasites. Plasmodium falciparum merozoites, the invasive form of the blood-stage parasite, invade human erythrocytes in a complex but rapid process. This multi-step progression involves interactions between parasite and human host proteins. Here we show that antibodies against a vaccine antigen, PfGAMA, co-immunoprecipitate with PfMSP10. This interaction was validated as direct by surface plasmon resonance analysis. We then demonstrate that antibodies against PfMSP10 have growth inhibitory activity against cultured parasites, with the region PfMSP10 R1 that is critical for its interaction with PfGAMA being the key target. We also observe that the PfMSP10 R1 region is highly conserved among African field isolates. Lastly, we show that high levels of antibodies against PfMSP10 R1 associate with reduced risk to clinical malaria in children resident in a malaria endemic region in northern Uganda. Put together, these findings provide for the first time the functional context of the important role of PfGAMA/PfMSP10 interaction in erythrocyte invasion and unveil a novel asexual blood-stage malaria vaccine target for attenuating P. falciparum merozoite invasion.

Published

2019

31. Initial phospholipid-dependent Irgb6 targeting to

Author

Youngae, Lee, Hiroshi, Yamada, Ariel, Pradipta, Ji Su, Ma, Masaaki, Okamoto, Hikaru, Nagaoka, Eizo, Takashima, Daron M, Standley, Miwa, Sasai, Kohji, Takei, and Masahiro, Yamamoto

Subjects

Male, Mice, Knockout, Ubiquitin, Ubiquitination, Fibroblasts, Immunity, Innate, Recombinant Proteins, Host-Parasite Interactions, Mice, Inbred C57BL, Interferon-gamma, Mice, parasitic diseases, Vacuoles, Animals, Female, Toxoplasma, Cells, Cultured, Phospholipids, Toxoplasmosis, Research Articles, Monomeric GTP-Binding Proteins, Protein Binding, Research Article

Abstract

Irgb6 has a role in the cell-autonomous response against T. gondii and involves ubiquitination and breakdown of vacuoles via binding of a specific phospholipid on the parasitophorous vacuole membrane., Toxoplasma gondii is an obligate intracellular protozoan parasite capable of infecting warm-blooded animals by ingestion. The organism enters host cells and resides in the cytoplasm in a membrane-bound parasitophorous vacuole (PV). Inducing an interferon response enables IFN-γ–inducible immunity-related GTPase (IRG protein) to accumulate on the PV and to restrict parasite growth. However, little is known about the mechanisms by which IRG proteins recognize and destroy T. gondii PV. We characterized the role of IRG protein Irgb6 in the cell-autonomous response against T. gondii, which involves vacuole ubiquitination and breakdown. We show that Irgb6 is capable of binding a specific phospholipid on the PV membrane. Furthermore, the absence of Irgb6 causes reduced targeting of other effector IRG proteins to the PV. This suggests that Irgb6 has a role as a pioneer in the process by which multiple IRG proteins access the PV. Irgb6-deficient mice are highly susceptible to infection by a strain of T. gondii avirulent in wild-type mice.

Published

2019

32. Identification of domains within Pfs230 that elicit transmission blocking antibody responses

Author

Masayuki Morita, Motomi Torii, C. Richter King, Takafumi Tsuboi, Mayumi Tachibana, Hikaru Nagaoka, Tomoko Ishino, Carole A. Long, Kazutoyo Miura, Luwen Zhou, and Eizo Takashima

Subjects

030231 tropical medicine, Plasmodium falciparum, Protozoan Proteins, Antibodies, Protozoan, Antigens, Protozoan, Enzyme-Linked Immunosorbent Assay, Cleavage (embryo), Immunofluorescence, Article, law.invention, 03 medical and health sciences, Mice, 0302 clinical medicine, Immunogenicity, Vaccine, law, parasitic diseases, Malaria Vaccines, medicine, Animals, Humans, 030212 general & internal medicine, Malaria, Falciparum, Antibodies, Blocking, Wheat germ cell-free system, Antiserum, General Veterinary, General Immunology and Microbiology, biology, medicine.diagnostic_test, Public Health, Environmental and Occupational Health, Transmission-blocking vaccine, biology.organism_classification, Molecular biology, Recombinant Proteins, Malaria, Blot, Disease Models, Animal, Infectious Diseases, Immunoglobulin G, Pfs230, biology.protein, Recombinant DNA, Molecular Medicine, Antibody, Cysteine

Abstract

A transmission-blocking vaccine (TBV) against Plasmodium falciparum is likely to be a valuable tool in a malaria eradication program. Pfs230 is one of the major TBV candidates, and multiple Pfs230-based vaccines induced antibodies, which prevented oocyst formation in mosquitoes as determined by a standard membrane-feeding assay (SMFA). Pfs230 is a >300 kDa protein consisting of 14 cysteine motif (CM) domains, and the size and cysteine-rich nature of the molecule have hampered its production as an intact protein. Except for one early study with maltose-binding protein fusion Pfs230 constructs expressed in Esherichia coli, all other studies have focused on only the first four CM domains in the Pfs230 molecule. To identify all possible TBV candidate domains, we systematically produced either single-CM-domain (a total of 14), 2-CM-domain (7), or 4-CM-domain (6) recombinant protein fragments using a eukaryotic wheat germ cell-free expression system (WGCFS). In addition, two more constructs which covered previously published regions, and an N-terminal prodomain construct spanning the natural cleavage site of Pfs230 were produced. Antisera against each fragment were generated in mice and we evaluated the reactivity to native Pfs230 protein by Western blots and immunofluorescence assay (IFA), and functionality by SMFA. All 30 WGCFS-produced Pfs230 constructs were immunogenic in mice. Approximately half of the mouse antibodies specifically recognized native Pfs230 by Western blots with variable band intensities. Among them, seven antibodies showed higher reactivities against native Pfs230 determined by IFA. Interestingly, antibodies against all protein fragments containing CM domain 1 displayed strong inhibitions in SMFA, while antibodies generated using constructs without CM domain 1 showed no inhibition. The results strongly support the concept that future Pfs230-based vaccine development should focus on the Pfs230 CM domain 1.

Published

2018

33. Anti-MSP11 IgG inhibits Plasmodium falciparum merozoite invasion into erythrocytes in vitro

Author

Motomi Torii, Masayuki Morita, Hikaru Nagaoka, Satoru Takeo, Eizo Takashima, Takafumi Tsuboi, Jetsumon Sattabongkot, Tomoko Ishino, Tatsuhiro Tohmoto, and Rachanee Udomsangpetch

Subjects

0301 basic medicine, Erythrocytes, 030231 tropical medicine, Plasmodium falciparum, Protozoan Proteins, Antibodies, Protozoan, Fluorescent Antibody Technique, Antigens, Protozoan, Enzyme-Linked Immunosorbent Assay, Immunofluorescence, 03 medical and health sciences, 0302 clinical medicine, parasitic diseases, medicine, Humans, Malaria, Falciparum, Asymptomatic Infections, Rhoptry, biology, medicine.diagnostic_test, Malaria vaccine, Merozoites, 030108 mycology & parasitology, medicine.disease, biology.organism_classification, Thailand, Virology, In vitro, Infectious Diseases, Rhoptry neck, Immunoglobulin G, biology.protein, Parasitology, Antibody, Malaria

Abstract

Merozoite surface proteins (MSPs) are considered as promising blood-stage malaria vaccine candidates. MSP3 has long been evaluated for its vaccine candidacy, however, the candidacy of other members of MSP3 family is insufficiently characterized. Here, we investigated Plasmodium falciparum MSP11 (PF3D7_1036000), a member of the MSP3 family, for its potential as a blood-stage vaccine candidate. The full-length protein (MSP11-FL) as well as the N-terminal half-MSP11 (MSP11-N), known to be unique among the MSP3 family members, were expressed by wheat germ cell-free system, and used to raise antibodies in rabbit. Immunoblot analysis of schizont lysates probed with anti-MSP11-N antibodies detected double bands at approximately 40 and 60 kDa, consistent with the previous report thus confirming antibodies specificity. However, inconsistent with previously reported merozoite's surface localization, immunofluorescence assay (IFA) revealed that MSP11 likely localizes to rhoptry neck of merozoites in mature schizonts. After invasion, MSP11 localized to parasitophorous vacuole and thereafter in Maurer's clefts in trophozoites. Anti-MSP11-FL antibody levels were significantly higher in asymptomatic than symptomatic P. falciparum cases in malaria low endemic Thailand. This reconfirmed that anti-MSP11 antibodies play an important role in protection against clinical malaria, as previously reported. Furthermore, in vitro growth inhibition assay revealed that anti-MSP11-FL rabbit antibodies biologically function by inhibiting merozoite invasion of erythrocytes. These findings further support the vaccine candidacy of MSP11.

Published

2018

34. Docking model of the nicotinic acetylcholine receptor and nitromethylene neonicotinoid derivatives with a longer chiral substituent and their biological activities

Author

Yoshihiro Shuto, Hisashi Nishiwaki, Takuya Kubo, Miki Akamatsu, Satoshi Yamauchi, and Hikaru Nagaoka

Subjects

Steric effects, Insecticides, Stereochemistry, Molecular Sequence Data, Clinical Biochemistry, Substituent, Quantitative Structure-Activity Relationship, Pharmaceutical Science, Ether, Receptors, Nicotinic, Methylation, Biochemistry, chemistry.chemical_compound, Thioether, Imidazolidine, Houseflies, Aplysia, Drug Discovery, Animals, Phenyl group, Amino Acid Sequence, Molecular Biology, Organic Chemistry, Nitro Compounds, Molecular Docking Simulation, Nicotinic acetylcholine receptor, chemistry, Docking (molecular), Molecular Medicine, Female

Abstract

In the present study, nitromethylene neonicotinoid derivatives possessing substituents that contain a sulfur atom, oxygen atom or aromatic ring at position 5 on the imidazolidine ring were synthesized to evaluate their affinity for the nicotinic acetylcholine receptor (nAChR) and their insecticidal activity against adult female houseflies. Comparing the receptor affinity of the alkylated derivative with the receptor affinity of compounds possessing either ether or thioether groups revealed that conversion of the carbon atom to a sulfur atom did not influence the receptor affinity, whereas conversion to an oxygen atom was disadvantageous for the receptor affinity. The receptor affinity of compounds possessing a benzyl or phenyl group was lower than that of the unsubstituted compound. Analysis of the three-dimensional quantitative structure-activity relationship using comparative molecular field analysis demonstrated that steric hindrance of the receptor should exist around the C3 of an n-butyl group attached at position 5 on the imidazolidine ring. A docking study of the nAChR-ligand model suggested that the ligand-binding region expands as the length of the substituent increases by brushing against the amino acids that form the binding region. The insecticidal activity of the compounds was positively correlated with the receptor affinity by considering logP and the number of heteroatoms, including sulfur and oxygen atoms, in the substituents, suggesting that the insecticidal activity is influenced by the receptor affinity, hydrophobicity, and metabolic stability of the compounds.

Published

2015

35. Blood-stage malaria vaccines: post-genome strategies for the identification of novel vaccine candidates

Author

Hikaru Nagaoka, Masayuki Morita, Takafumi Tsuboi, Tomoko Ishino, Edward H. Ntege, and Eizo Takashima

Subjects

0301 basic medicine, Immunology, Blood stage malaria, Antibodies, Protozoan, Antigens, Protozoan, Disease, Genome, 03 medical and health sciences, 0302 clinical medicine, Malaria elimination, parasitic diseases, Drug Discovery, Malaria Vaccines, medicine, Humans, 030212 general & internal medicine, Pharmacology, biology, Malaria vaccine, Reverse vaccinology, Plasmodium falciparum, biology.organism_classification, medicine.disease, 030104 developmental biology, Molecular Medicine, Genome, Protozoan, Malaria

Abstract

An efficacious malaria vaccine is necessary to advance the current control measures towards malaria elimination. To-date, only RTS,S/AS01, a leading pre-erythrocytic stage vaccine completed phase 3 trials, but with an efficacy of 28-36% in children, and 18-26% in infants, that waned over time. Blood-stage malaria vaccines protect against disease, and are considered effective targets for the logical design of next generation vaccines to improve the RTS,S field efficacy. Therefore, novel blood-stage vaccine candidate discovery efforts are critical, albeit with several challenges including, high polymorphisms in vaccine antigens, poor understanding of targets of naturally protective immunity, and difficulties in the expression of high AT-rich plasmodial proteins. Areas covered: PubMed ( www.ncbi.nlm.nih.gov/pubmed ) was searched to review the progress and future prospects of malaria vaccine research and development. We focused on post-genome vaccine candidate discovery, malaria vaccine development, sequence diversity, pre-clinical and clinical trials. Expert commentary: Post-genome high-throughput technologies using wheat germ cell-free protein synthesis technology and immuno-profiling with sera from malaria patients with clearly defined outcomes are highlighted to overcome current challenges of malaria vaccine candidate discovery.

Published

2017

36. Initial phospholipid-dependent Irgb6 targeting to Toxoplasma gondii vacuoles mediates host defense

Author

Miwa Sasai, Ji Su Ma, Eizo Takashima, Masahiro Yamamoto, Youngae Lee, Ariel Pradipta, Daron M. Standley, Masaaki Okamoto, Hiroshi Yamada, Kohji Takei, and Hikaru Nagaoka

Subjects

0303 health sciences, Ecology, biology, Effector, Health, Toxicology and Mutagenesis, Toxoplasma gondii, Plant Science, GTPase, Plasma protein binding, Vacuole, biology.organism_classification, Biochemistry, Genetics and Molecular Biology (miscellaneous), Cell biology, 03 medical and health sciences, 0302 clinical medicine, Ubiquitin, Cytoplasm, Interferon, biology.protein, medicine, 030217 neurology & neurosurgery, 030304 developmental biology, medicine.drug

Abstract

Toxoplasma gondii is an obligate intracellular protozoan parasite capable of infecting warm-blooded animals by ingestion. The organism enters host cells and resides in the cytoplasm in a membrane-bound parasitophorous vacuole (PV). Inducing an interferon response enables IFN-γ–inducible immunity-related GTPase (IRG protein) to accumulate on the PV and to restrict parasite growth. However, little is known about the mechanisms by which IRG proteins recognize and destroy T. gondii PV. We characterized the role of IRG protein Irgb6 in the cell-autonomous response against T. gondii, which involves vacuole ubiquitination and breakdown. We show that Irgb6 is capable of binding a specific phospholipid on the PV membrane. Furthermore, the absence of Irgb6 causes reduced targeting of other effector IRG proteins to the PV. This suggests that Irgb6 has a role as a pioneer in the process by which multiple IRG proteins access the PV. Irgb6-deficient mice are highly susceptible to infection by a strain of T. gondii avirulent in wild-type mice.

Published

2019

37. Synthesis of imidacloprid derivatives with a chiral alkylated imidazolidine ring and evaluation of their insecticidal activity and affinity to the nicotinic acetylcholine receptor

Author

Miki Akamatsu, Hikaru Nagaoka, Yoshihiro Shuto, Satoshi Yamauchi, Akira Kato, Hisashi Nishiwaki, and Mituhiro Kuriyama

Subjects

Models, Molecular, Insecticides, Quantitative structure–activity relationship, Alkylation, Stereochemistry, Molecular Sequence Data, Clinical Biochemistry, Substituent, Quantitative Structure-Activity Relationship, Pharmaceutical Science, Receptors, Nicotinic, Imidazolidines, Ring (chemistry), Biochemistry, Neonicotinoids, chemistry.chemical_compound, Imidazolidine, Houseflies, Drug Discovery, Animals, Receptor, Molecular Biology, Alkyl, chemistry.chemical_classification, Dose-Response Relationship, Drug, Molecular Structure, Chemistry, Organic Chemistry, Imidazoles, Nitro Compounds, Nicotinic acetylcholine receptor, Molecular Medicine, Female, Sequence Alignment

Abstract

A series of imidacloprid (IMI) derivatives with an alkylated imidazolidine ring were asymmetrically synthesized to evaluate their insecticidal activity against adult female housefly, Musca domestica, and affinity to the nicotinic acetylcholine receptor of the flies. The bulkier the alkyl group, the lower was the receptor affinity, but the derivatives methylated and ethylated at the R-5-position of the imidazolidine ring were equipotent to the unsubstituted compound. Quantitative structure–activity relationship (QSAR) analysis of the receptor affinity demonstrated that the introduction of a substituent into the imidazolidine ring was fundamentally disadvantageous, but the introduction of a substituent at the R-5-position was permissible in the case of its small size. The binding model of the synthesized derivatives with the receptor supported the QSAR analysis, indicating the existence of space for a short alkyl group around the R-5-position in the ligand-binding site. In addition, positive correlation was observed between the insecticidal activity and receptor affinity, suggesting that the receptor affinity was the primary factor in influencing the insecticidal activity even if the imidazolidine ring was modified.

Published

2012