Advances in Vaccine Development for Human Lymphatic Filariasis

Lymphatic lariasis is one of the major diseases that belong to the category of neglected tropical illness.Filarial nematodes are the cause of the disease and are transmitted to humans via blood-feeding arthropod vectors. Drugs such as Albendazole, Ivermectin and diethylcarbamazine are administered either individually or in combination to overcome the progress of the lymphatic lariasis. However, these drugs have some disadvantages like temporary hair loss, dizziness, nausea etc. The larial parasites have multifunctional proteins including the Glutathione-s-transferase (GST) enzyme which plays a major role in detoxi cation of endogenous electrophilic compounds. This study aims at the identi cation of a natural molecule that has the potential to bind with the GST enzyme and thus interrupt the detoxi cation process within the larial parasite, Brugia malayi. A medicinal plant Calotropis procera, owing to its anthelmintic properties was searched for the presence of potential phytocompounds. The phytocompounds were docked against the homology modeled GST enzyme using the MOE software. The results were screened and analyzed based on the Lipinski rule of 5. N-octanoate was the phytocompound obtained based on molecular docking, subjected to molecular dynamics. These results require further in vitro and in vivo validation to consider n-octanoate as a potential drug candidate for lymphatic lariasis treatment.

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“…Mass Drug Administration (MDA) is controlling the disease to an extent (Kalyanasundaram et al 2020).…”

Section: Resultsmentioning

confidence: 99%

The potentials of Calotropis procera against filarial elephantiasis: an in-silico approach

et al. 2021

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“…Prophylactic anti-filarial vaccines, replacing or combined with drug therapies, are required to effectively eliminate filarial infections worldwide ( 81 , 82 ). The search for vaccine candidates for filarial infections has been progressive over the years (reviewed in 81 – 83 ), although there are currently no approved consumable vaccines available for filariasis.…”

Section: The Need For Cd8 + T Cell Induction By Prophylactic Filarial Vaccinesmentioning

confidence: 99%

“…The majority of immunization trials against filarial infections in experimental models demonstrate induction of IL-2, IL-4, IL-10, IL-17, and IFN-γ, indicating a balanced Th1/Th2 immunity ( 85 – 90 ). The efficacy of these potential vaccine candidates in different animal models ranges from 45% to 94% ( 83 ). The vaccine formulations usually include filarial antigens such as heat shock protein 12.6 ( 86 – 88 ), abundant larval transcript-2 ( 86 , 88 , 89 , 91 ), tetraspanin large extracellular loop ( 86 – 88 ), vespid allergen homologue ( 89 , 91 ), thioredoxin peroxide ( 86 ), calponin ( 92 ), disorganized muscle protein-1 ( 93 ), and trehalose-6-phosphate phosphatase ( 35 ).…”

Section: The Need For Cd8 + T Cell Induction By Prophylactic Filarial Vaccinesmentioning

confidence: 99%

“…Given this, a very plausible therapeutic approach would be to prime potential prophylactic vaccine candidates to induce sufficient CD8 + T cells and associated memory responses which can have detrimental effects on the establishment of the parasites ( 15 ). Identifying CD8 + T cell epitopes within filarial antigens could be achieved through immunoinformatics predictions and experimental validations or by screening a library of peptides spanning the complete antigen sequence ( 83 ). Recently, our group identified a CD8 + T cell peptide ( 146 KPWENFMRV 154 ) within onchocystatin, as part of a multi-epitope vaccine candidate for onchocerciasis, which demonstrates promising potential based on bioinformatics analysis ( 98 ).…”

Section: The Need For Cd8 + T Cell Induction By Prophylactic Filarial Vaccinesmentioning

confidence: 99%

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Highlighting the Relevance of CD8+ T Cells in Filarial Infections

et al. 2021

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The T cell immune responses in filarial infections are primarily mediated by CD4+ T cells and type 2-associated cytokines. Emerging evidence indicates that CD8+ T cell responses are important for anti-filarial immunity, however, could be suppressed in co-infections. This review summarizes what we know so far about the activities of CD8+ T cell responses in filarial infections, co-infections, and the associations with the development of filarial pathologies.

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“…In part, irradiated larval strategies could not be applied to humans on any scale, and there are far greater regulatory hurdles than in the veterinary setting. Nevertheless, hundreds of candidate antigens have been tested in model systems for filariasis [ 15 , 16 ], schistosomiasis [ 17–19 ], soil-transmitted nematodes [ 20 ] and other human helminth parasites [ 21 ], with trials in endemic populations under way for hookworm and schistosomiasis [ 22 ]. But there remain some fundamental obstacles to achieve fully effective vaccines against human helminth parasites.…”

Section: Introductionmentioning

confidence: 99%

Identifying novel candidates and configurations for human helminth vaccines

Maizels

2021

Expert Review of Vaccines

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Introduction : Human infections with helminth worm parasites are extraordinarily prevalent across tropical and subtropical parts of the world, and control relies primarily on drugs that offer short-term suppression of infection. There is an urgent need for new vaccines that would confer long-lived immunity, protecting children in particular and minimizing community transmission. Areas covered : This article discusses the development of helminth vaccines, from the first successful veterinary vaccines that demonstrated the feasibility of inducing protective immunity to helminths, to more recent initiatives to test human helminth antigens. The field has focussed primarily on evaluating individual antigens that could constitute targets amenable to antibody attack to inhibit parasite establishment. In a new direction, vaccines employing extracellular vesicles released by helminths have also given exciting results. Expert opinion : Taking into account the complex life cycles and sophisticated immune evasion strategies of many helminths, a combination of antigens and approaches designed to target essential functional pathways of the parasite will be required to achieve a high level of protection in future anti-helminth vaccines.

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Advances in Vaccine Development for Human Lymphatic Filariasis

Cited by 35 publications

References 68 publications

The potentials of Calotropis procera against filarial elephantiasis: an in-silico approach

The potentials of Calotropis procera against filarial elephantiasis: an in-silico approach

Highlighting the Relevance of CD8+ T Cells in Filarial Infections

Identifying novel candidates and configurations for human helminth vaccines

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