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下一代利什曼原虫接种疗法:重新审视用于选择基因工程减毒活疫苗的分子靶点

Next-Generation Leishmanization: Revisiting Molecular Targets for Selecting Genetically Engineered Live-Attenuated .

作者信息

Moreira Paulo O L, Nogueira Paula M, Monte-Neto Rubens L

机构信息

Biotechnology Applied to Pathogens (BAP), Instituto René Rachou, Fundação Oswaldo Cruz, Fiocruz Minas, Belo Horizonte 30190-009, Brazil.

出版信息

Microorganisms. 2023 Apr 16;11(4):1043. doi: 10.3390/microorganisms11041043.


DOI:10.3390/microorganisms11041043
PMID:37110466
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10145799/
Abstract

Despite decades of research devoted to finding a vaccine against leishmaniasis, we are still lacking a safe and effective vaccine for humans. Given this scenario, the search for a new prophylaxis alternative for controlling leishmaniasis should be a global priority. Inspired by leishmanization-a first generation vaccine strategy where live parasites are inoculated in the skin to protect against reinfection-live-attenuated vaccine candidates are promising alternatives due to their robust elicited protective immune response. In addition, they do not cause disease and could provide long-term protection upon challenge with a virulent strain. The discovery of a precise and easy way to perform CRISPR/Cas-based gene editing allowed the selection of safer null mutant live-attenuated parasites obtained by gene disruption. Here, we revisited molecular targets associated with the selection of live-attenuated vaccinal strains, discussing their function, their limiting factors and the ideal candidate for the next generation of genetically engineered live-attenuated vaccines to control leishmaniasis.

摘要

尽管数十年来致力于寻找抗利什曼病疫苗的研究,但我们仍然缺乏一种对人类安全有效的疫苗。在这种情况下,寻找控制利什曼病的新预防方法应成为全球优先事项。受利什曼原虫接种法(一种第一代疫苗策略,将活寄生虫接种到皮肤中以预防再次感染)的启发,减毒活疫苗候选物因其能引发强大的保护性免疫反应而成为有前景的替代方案。此外,它们不会引起疾病,并且在受到强毒株攻击时可提供长期保护。基于CRISPR/Cas的基因编辑精确且简便方法的发现,使得通过基因破坏获得更安全的无功能突变减毒活寄生虫成为可能。在此,我们重新审视了与减毒活疫苗株选择相关的分子靶点,讨论了它们的功能、限制因素以及用于控制利什曼病的下一代基因工程减毒活疫苗的理想候选物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7358/10145799/6bb7247aad7d/microorganisms-11-01043-g001.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7358/10145799/6bb7247aad7d/microorganisms-11-01043-g001.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7358/10145799/6bb7247aad7d/microorganisms-11-01043-g001.jpg

相似文献

[1]
Next-Generation Leishmanization: Revisiting Molecular Targets for Selecting Genetically Engineered Live-Attenuated .

Microorganisms. 2023-4-16

[2]
From classical approaches to new developments in genetic engineering of live attenuated vaccine against cutaneous leishmaniasis: potential and immunization.

Front Public Health. 2024

[3]
Revival of Leishmanization and Leishmanin.

Front Cell Infect Microbiol. 2021-3-17

[4]
Centrin Gene-Deleted Parasites Generate Skin Resident Memory T-Cell Immune Response Analogous to Leishmanization.

Front Immunol. 2022

[5]
Biomarkers of safety and immune protection for genetically modified live attenuated leishmania vaccines against visceral leishmaniasis - discovery and implications.

Front Immunol. 2014-5-23

[6]
Leishmania major p27 gene knockout as a novel live attenuated vaccine candidate: Protective immunity and efficacy evaluation against cutaneous and visceral leishmaniasis in BALB/c mice.

Vaccine. 2019-4-29

[7]
Generation of growth arrested Leishmania amastigotes: a tool to develop live attenuated vaccine candidates against visceral leishmaniasis.

Vaccine. 2014-6-30

[8]
A second generation leishmanization vaccine with a markerless attenuated Leishmania major strain using CRISPR gene editing.

Nat Commun. 2020-7-10

[9]
Live vaccination tactics: possible approaches for controlling visceral leishmaniasis.

Front Immunol. 2014-3-31

[10]
The potential of live attenuated vaccines against Cutaneous Leishmaniasis.

Exp Parasitol. 2020-2-3

引用本文的文献

[1]
Kharon Is Crucial for Morphology but Does Not Impair In Vitro Infection.

Pathogens. 2025-3-25

[2]
CRISPR/Cas9-mediated deletion of a kinetoplast-associated gene attenuates virulence in Leishmania major parasites.

Med Microbiol Immunol. 2025-3-25

[3]
From classical approaches to new developments in genetic engineering of live attenuated vaccine against cutaneous leishmaniasis: potential and immunization.

Front Public Health. 2024

[4]
Live attenuated-nonpathogenic and DNA structures as promising vaccine platforms against leishmaniasis: innovations can make waves.

Front Microbiol. 2024-4-3

[5]
Immunization with -Deficient Does Not Protect against Homologous Challenge.

Vaccines (Basel). 2024-3-15

[6]
Preliminary Information of Iranian Lizard Promastigote Transcriptome Sequencing by Next Generation Sequencing (NGS) Method.

Iran J Parasitol. 2023

本文引用的文献

[1]
Drug resistance in Leishmania: does it really matter?

Trends Parasitol. 2023-4

[2]
Vaccination with Formulation of Nanoparticles Loaded with Leishmania amazonensis Antigens Confers Protection against Experimental Visceral Leishmaniasis in Hamster.

Vaccines (Basel). 2023-1-2

[3]
Centrin-deficient Leishmania mexicana confers protection against Old World visceral leishmaniasis.

NPJ Vaccines. 2022-12-3

[4]
Visceral leishmaniasis in the COVID-19 pandemic era.

Trans R Soc Trop Med Hyg. 2023-2-1

[5]
Promastigote-to-Amastigote Conversion in spp.-A Molecular View.

Pathogens. 2022-9-15

[6]
The History of Live Attenuated Gene-Deleted Vaccine Candidates.

Pathogens. 2022-4-2

[7]
Immune Responses in Leishmaniasis: An Overview.

Trop Med Infect Dis. 2022-3-31

[8]
The Leishmania donovani Ortholog of the Glycosylphosphatidylinositol Anchor Biosynthesis Cofactor PBN1 Is Essential for Host Infection.

mBio. 2022-6-28

[9]
Targeted Deletion of Centrin in Using CRISPR-Cas9-Based Editing.

Front Cell Infect Microbiol. 2021

[10]
Centrin-deficient Leishmania mexicana confers protection against New World cutaneous leishmaniasis.

NPJ Vaccines. 2022-3-2

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