Your search keyword '"Huanhuan Ning"' showing total 11 results

1. Ag85B with c-di-AMP as mucosal adjuvant showed immunotherapeutic effects on persistent Mycobacterium tuberculosis infection in mice

Author

Xuan Liang, Ruonan Cui, Xue Li, Huanhuan Ning, Jian Kang, Yanzhi Lu, Shan Zhou, Xinying Huang, Yujun Peng, Jingyao Zhang, Shiyun Li, Yanling Ma, and Yinlan Bai

Subjects

Mycobacterium tuberculosis, Ag85B, C-di-AMP, Adjuvant, Immunotherapy, Medicine (General), R5-920, Biology (General), QH301-705.5

Abstract

Tuberculosis (TB), caused by Mycobacterium tuberculosis, remains the leading cause of mortality by a single infectious agent in the world. M. tuberculosis infection could also result in clinical chronic infection, known as latent TB infection (LTBI). Compared to the current limited treatment, several subunit vaccines showed immunotherapeutic effects and were included in clinical trials. In this study, a subunit vaccine of Ag85B with a novel mucosal adjuvant c-di-AMP (Ag85B:c-di-AMP) was delivered intranasally to a persistent M. tuberculosis H37Ra infection mouse model, which also presented the asymptomatic characteristics of LTBI. Compared with Ag85B immunization, Ag85B:c-di-AMP vaccination induced stronger humoral immune responses, significantly higher CD4+ T cells recruitment, enhanced Th1/Th2/Th17 profile response in the lung, decreased pathological lesions of the lung, and reduced M. tuberculosis load in mice. Taken together, Ag85B:c-di-AMP mucosal route immunization provided an immunotherapeutic effect on persistent M. tuberculosis H37Ra infection, and c-di-AMP, as a promising potential mucosal adjuvant, could be further used in therapeutic or prophylactic vaccine strategies for persistent M. tuberculosis infection as well as LTBI.

Published

2024

2. Cyclic di-AMP as endogenous adjuvant enhanced BCG-induced trained immunity and protection against Mycobacterium tuberculosis in mice

Author

Huanhuan Ning, Jian Kang, Yanzhi Lu, Xuan Liang, Jie Zhou, Rui Ren, Shan Zhou, Yong Zhao, Yanling Xie, Lu Bai, Linna Zhang, Yali Kang, Xiaojing Gao, Mingze Xu, Yanling Ma, Fanglin Zhang, and Yinlan Bai

Subjects

Bacillus Calmette-Guérin, cyclic di-AMP, trained immunity, adjuvant, Mycobacterium tuberculosis, Immunologic diseases. Allergy, RC581-607

Abstract

Bacillus Calmette-Guérin (BCG) is a licensed prophylactic vaccine against tuberculosis (TB). Current TB vaccine efforts focus on improving BCG effects through recombination or genetic attenuation and/or boost with different vaccines. Recent years, it was revealed that BCG could elicit non-specific heterogeneous protection against other pathogens such as viruses through a process termed trained immunity. Previously, we constructed a recombinant BCG (rBCG-DisA) with elevated c-di-AMP as endogenous adjuvant by overexpressing di-adenylate cyclase of Mycobacterium tuberculosis DisA, and found that rBCG-DisA induced enhanced immune responses by subcutaneous route in mice after M. tuberculosis infection. In this study, splenocytes from rBCG-DisA immunized mice by intravenous route (i.v) elicited greater proinflammatory cytokine responses to homologous and heterologous re-stimulations than BCG. After M. tuberculosis infection, rBCG-DisA immunized mice showed hallmark responses of trained immunity including potent proinflammatory cytokine responses, enhanced epigenetic changes, altered lncRNA expressions and metabolic rewiring in bone marrow cells and other tissues. Moreover, rBCG-DisA immunization induced higher levels of antibodies and T cells responses in the lung and spleen of mice after M. tuberculosis infection. It was found that rBCG-DisA resided longer than BCG in the lung of M. tuberculosis infected mice implying prolonged duration of vaccine efficacy. Then, we found that rBCG-DisA boosting could prolong survival of BCG-primed mice over 90 weeks against M. tuberculosis infection. Our findings provided in vivo experimental evidence that rBCG-DisA with c-di-AMP as endogenous adjuvant induced enhanced trained immunity and adaptive immunity. What’s more, rBCG-DisA showed promising potential in prime-boost strategy against M. tuberculosis infection in adults.

Published

2022

3. Cyclic-di-AMP Phosphodiesterase Elicits Protective Immune Responses Against Mycobacterium tuberculosis H37Ra Infection in Mice

Author

Yanzhi Lu, Huanhuan Ning, Jian Kang, Guangchun Bai, Lei Zhou, Yali Kang, Zhengfeng Wu, Maolin Tian, Junhao Zhao, Yueyun Ma, and Yinlan Bai

Subjects

Mycobacterium tuberculosis, cyclic-di-AMP, phosphodiesterase, immune response, infection, vaccine, Microbiology, QR1-502

Abstract

Many antigens from Mycobacterium tuberculosis (M. tuberculosis) have been demonstrated as strong immunogens and proved to have application potential as vaccine candidate antigens. Cyclic di-AMP (c-di-AMP) as a bacterial second messenger regulates various bacterial processes as well as the host immune responses. Rv2837c, the c-di-AMP phosphodiesterase (CnpB), was found to be relative to virulence of M. tuberculosis and interference with host innate immune response. In this study, recombinant CnpB was administered subcutaneously to mice. We found that CnpB had strong immunogenicity and induced high levels of humoral response and lung mucosal immunity after M. tuberculosis intranasally infection. CnpB immunization stimulated splenocyte proliferation and the increasing number of activated NK cells but had little effects on Th1/Th2 cellular immune responses in spleens. However, CnpB induced significant Th1/Th2 cellular immune responses with a decreased number of T and B cells in the lungs, and significantly recruits of CD4+ and CD8+ T cells after M. tuberculosis attenuated strain H37Ra infection. Besides, we first reported that CnpB could stimulate IFN-β expression transitorily and inhibit the autophagy of macrophages in vitro. In mice intranasally infection model, CnpB immunization alleviated pathological changes and reduced M. tuberculosis H37Ra loads in the lungs. Thus, our results suggested that CnpB interferes with host innate and adaptive immune responses and confers protection against M. tuberculosis respiratory infection, which should be considered in vaccine development as well as a drug target.

Published

2022

4. c-di-AMP Accumulation Regulates Growth, Metabolism, and Immunogenicity of Mycobacterium smegmatis

Author

Huanhuan Ning, Xuan Liang, Yanling Xie, Lu Bai, Wei Zhang, Lifei Wang, Jian Kang, Yanzhi Lu, Yanling Ma, Guangchun Bai, and Yinlan Bai

Subjects

Mycobacterium smegmatis, M. tuberculosis, c-di-AMP, physiology, immunogenicity, Microbiology, QR1-502

Abstract

Cyclic dimeric adenosine monophosphate (c-di-AMP) is a ubiquitous second messenger of bacteria involved in diverse physiological processes as well as host immune responses. MSMEG_2630 is a c-di-AMP phosphodiesterase (cnpB) of Mycobacterium smegmatis, which is homologous to Mycobacterium tuberculosis Rv2837c. In this study, cnpB-deleted (ΔcnpB), -complemented (ΔcnpB::C), and -overexpressed (ΔcnpB::O) strains of M. smegmatis were constructed to investigate the role of c-di-AMP in regulating mycobacterial physiology and immunogenicity. This study provides more precise evidence that elevated c-di-AMP level resulted in smaller colonies, shorter bacteria length, impaired growth, and inhibition of potassium transporter in M. smegmatis. This is the first study to report that elevated c-di-AMP level could inhibit biofilm formation and induce porphyrin accumulation in M. smegmatis by regulating associated gene expressions, which may have effects on drug resistance and virulence of mycobacterium. Moreover, the cnpB-deleted strain with an elevated c-di-AMP level could induce enhanced Th1 immune responses after M. tuberculosis infection. Further, the pathological changes and the bacteria burden in ΔcnpB group were comparable with the wild-type M. smegmatis group against M. tuberculosis venous infection in the mouse model. Our findings enhanced the understanding of the physiological role of c-di-AMP in mycobacterium, and M. smegmatis cnpB-deleted strain with elevated c-di-AMP level showed the potential for a vaccine against tuberculosis.

Published

2022

5. Subunit Vaccine ESAT-6:c-di-AMP Delivered by Intranasal Route Elicits Immune Responses and Protects Against Mycobacterium tuberculosis Infection

Author

Huanhuan Ning, Wei Zhang, Jian Kang, Tianbing Ding, Xuan Liang, Yanzhi Lu, Chengxuan Guo, Wenjie Sun, Huapeng Wang, Yinlan Bai, and Lixin Shen

Subjects

Mycobacterium tuberculosis, subunit vaccine, ESAT-6, c-di-AMP, mucosal adjuvant, Microbiology, QR1-502

Abstract

Tuberculosis (TB), caused by Mycobacterium tuberculosis (Mtb) infection, remains the most common cause of death from a single infectious disease. More safe and effective vaccines are necessary for preventing the prevalence of TB. In this study, a subunit vaccine of ESAT-6 formulated with c-di-AMP (ESAT-6:c-di-AMP) promoted mucosal and systemic immune responses in spleen and lung. ESAT-6:c-di-AMP inhibited the differentiations of CD8+ T cells as well as macrophages, but promoted the differentiations of ILCs in lung. The co-stimulation also enhanced inflammatory cytokines production in MH-S cells. It was first revealed that ESAT-6 and c-di-AMP regulated autophagy of macrophages in different stages, which together resulted in the inhibition of Mtb growth in macrophages during early infection. After Mtb infection, the level of ESAT-6-specific immune responses induced by ESAT-6:c-di-AMP dropped sharply. Finally, inoculation of ESAT-6:c-di-AMP led to significant reduction of bacterial burdens in lungs and spleens of immunized mice. Our results demonstrated that subunit vaccine ESAT-6:c-di-AMP could elicit innate and adaptive immune responses which provided protection against Mtb challenge, and c-di-AMP as a mucosal adjuvant could enhance immunogenicity of antigen, especially for innate immunity, which might be used for new mucosal vaccine against TB.

Published

2021

6. Recombinant BCG With Bacterial Signaling Molecule Cyclic di-AMP as Endogenous Adjuvant Induces Elevated Immune Responses After Mycobacterium tuberculosis Infection

Author

Huanhuan Ning, Lifei Wang, Jie Zhou, Yanzhi Lu, Jian Kang, Tianbing Ding, Lixin Shen, Zhikai Xu, and Yinlan Bai

Subjects

Mycobacterium tuberculosis, recombinant BCG, cyclic di-AMP, adjuvant, immune response, Immunologic diseases. Allergy, RC581-607

Abstract

Bacillus Calmette-Guerin (BCG) is a live attenuated vaccine against tuberculosis (TB) and remains the most commonly used vaccine worldwide. However, BCG has varied protective efficiency in adults and has safety concerns in immunocompromised population. Thus, effective vaccines are necessary for preventing the prevalence of TB. Cyclic di-AMP (c-di-AMP) is a bacterial second messenger which regulates various cellular processes and host immune response. Previous work found that c-di-AMP regulates bacterial physiological function, pathogenicity and host type I IFN response. In this study, we constructed a recombinant BCG (rBCG) by overexpressing DisA, the diadenylate cyclase of Mycobacterium tuberculosis (Mtb), and observed the physiological changes of rBCG-DisA. The immunological characteristics of rBCG-DisA were investigated on humoral and cellar immune responses in a mice infection model. Our study demonstrated that overexpression of DisA in BCG does not affect the growth but reduces the length of BCG. rBCG-DisA-immunized mice show similar humoral and cellar immune responses in BCG-immunized mice. After Mtb infection, the splenic lymphocytes from both BCG and rBCG-DisA-immunized mice produced more IFN-γ, IL-2, and IL-10 than the un-immunized (UN) mice, while the cytokine levels of the rBCG-DisA group increased significantly than those of the BCG group. The transcription of IFN-β, IL-1β and autophagy related genes (Atgs) were up-regulated in macrophages after treated with c-di-AMP or bacterial infection. The productions of IL-6 were increased after Mtb challenge, especially in the rBCG-DisA-immunized mice. Strikingly, H3K4me3, the epigenetic marker of innate immune memory, was found in both two immunized groups, and the rBCG-DisA group showed stronger expression of H3K4me3 than that of BCG. In addition, the pathological changes of rBCG-DisA immunized mice were similar to that of BCG-immunized mice. The bacterial burdens in the lungs and spleens of BCG- and rBCG-DisA-immunized mice were significantly decreased, but there was no significant difference between the two immunized groups. Together, these results suggested that compared to BCG, rBCG-DisA vaccination, induces stronger immune responses but did not provided additional protection against Mtb infection in this study, which may be related to the innate immunity memory. Hence, c-di-AMP is a promising immunomodulator for a further developed BCG as a better vaccine.

Published

2019

7. [Immune responses induced by subunit vaccine of Ag85B-ESAT-6 delivered by mucosal route to Mycobacterium tuberculosis]

Author

Huanhuan, Ning, Fanglin, Zhang, Jian, Kang, Lifei, Wang, Yanzhi, Lu, Run, Ren, Lu, Bai, Xuan, Liang, Yanling, Xie, and Yinlan, Bai

Subjects

Antigens, Bacterial, Mice, Inbred BALB C, Tumor Necrosis Factor-alpha, Immunity, Mycobacterium tuberculosis, Interleukin-10, Mice, Adjuvants, Immunologic, Bacterial Proteins, Immunoglobulin G, Vaccines, Subunit, Animals, Cytokines, Interleukin-2, Tuberculosis Vaccines

Abstract

Objective To identify the immune responses induced by subunit vaccine of Ag85B-ESAT-6 (AE) fusion protein by mucosal route and the protection against Mycobacterium tuberculosis (MTB) infection in mice. Methods AE and AE with c-di-AMP as adjuvant were inoculated intranasally in mice. The generation of specific IgG, cytokines secreted by Th1 cells (IFN-γ, IL-2) and Th2 cells (IL-10) were detected by ELISA. The transcriptional levels of IFN-γ, IL-2, IL-10, and TNF-α were determined using real-time quantitative PCR. After MTB infection by vein, the antibodies level in mice sera and cytokines secretion of splenocytes were detected by ELISA. Histopathological changes in mice lung was illustrated by HE staining, and bacteria burdens of spleen and lung were counted by colony-forming units (CFUs) on plate. Results AE and AE combined with c-di-AMP via nasal mucosal immunization could induce high level specific antibodies in sera, promote splenocyte proliferation, and lead to increased Th1/Th2 cytokines and TNF-α transcription in spleen and lung, and secret more Th1/Th2 cytokines in spleen. After MTB infection, compared with the control group, the specific antibody levels of AE and AE combined with c-di-AMP immunized mice still increased, with enhanced the Th1/Th2 cellular immune responses, inflammatory response in the lung tissues, and reduced bacteria loads in spleen and lung, especially in mice immunized with AE combined with c-di-AMP. Conclusion Intranasal mucosal vaccination of AE subunit vaccine can induce humoral and cellular immune responses, and provide protection against MTB infection in mice, c-di-AMP as an adjuvant can improve the immunogenicity of AE to a certain extent.

Published

2022

8. Cyclic di-AMP as endogenous adjuvant enhanced BCGinduced trained immunity and protection against Mycobacterium tuberculosis in mice.

Author

Huanhuan Ning, Jian Kang, Yanzhi Lu, Xuan Liang, Jie Zhou, Rui Ren, Shan Zhou, Yong Zhao, Yanling Xie, Lu Bai, Linna Zhang, Yali Kang, Xiaojing Gao, Mingze Xu, Yanling Ma, Fanglin Zhang, and Yinlan Bai

Subjects

MYCOBACTERIUM tuberculosis, BONE marrow cells, GENETIC recombination, VACCINE effectiveness, IMMUNITY

Abstract

Bacillus Calmette-Gue'rin (BCG) is a licensed prophylactic vaccine against tuberculosis (TB). Current TB vaccine efforts focus on improving BCG effects through recombination or genetic attenuation and/or boost with different vaccines. Recent years, it was revealed that BCG could elicit non-specific heterogeneous protection against other pathogens such as viruses through a process termed trained immunity. Previously, we constructed a recombinant BCG (rBCG-DisA) with elevated c-di-AMP as endogenous adjuvant by overexpressing di-adenylate cyclase of Mycobacterium tuberculosis DisA, and found that rBCG-DisA induced enhanced immune responses by subcutaneous route in mice after M. tuberculosis infection. In this study, splenocytes from rBCG-DisA immunized mice by intravenous route (i.v) elicited greater proinflammatory cytokine responses to homologous and heterologous re-stimulations than BCG. After M. tuberculosis infection, rBCG-DisA immunized mice showed hallmark responses of trained immunity including potent proinflammatory cytokine responses, enhanced epigenetic changes, altered lncRNA expressions and metabolic rewiring in bone marrow cells and other tissues. Moreover, rBCG-DisA immunization induced higher levels of antibodies and T cells responses in the lung and spleen of mice after M. tuberculosis infection. It was found that rBCG-DisA resided longer than BCG in the lung of M. tuberculosis infected mice implying prolonged duration of vaccine efficacy. Then, we found that rBCG-DisA boosting could prolong survival of BCG-primed mice over 90 weeks against M. tuberculosis infection. Our findings provided in vivo experimental evidence that rBCGDisA with c-di-AMP as endogenous adjuvant induced enhanced trained immunity and adaptive immunity. What's more, rBCG-DisA showed promising potential in prime-boost strategy against M. tuberculosis infection in adults. [ABSTRACT FROM AUTHOR]

Published

2022

9. Immunological characteristics of Mycobacterium tuberculosis subunit vaccines immunized through different routes

Author

Xingan Wu, Lu Yanzhi, Yinlan Bai, Xu Yanhui, Ying Xue, Huanhuan Ning, Jian Kang, Wang Lifei, and Zhikai Xu

Subjects

0301 basic medicine, animal diseases, medicine.medical_treatment, Injections, Subcutaneous, Guinea Pigs, chemical and pharmacologic phenomena, Biology, complex mixtures, Microbiology, Injections, Intramuscular, Mycobacterium tuberculosis, 03 medical and health sciences, Interferon-gamma, Mice, 0302 clinical medicine, Immune system, Antigen, Adjuvants, Immunologic, Bacterial Proteins, medicine, Animals, Tuberculosis Vaccines, Cell Proliferation, Antigens, Bacterial, Immunity, Cellular, Immunogenicity, bacterial infections and mycoses, biology.organism_classification, Antibodies, Bacterial, Immunity, Humoral, 030104 developmental biology, Infectious Diseases, Immunization, 030220 oncology & carcinogenesis, Humoral immunity, ESAT-6, Immunology, Vaccines, Subunit, Leukocytes, Mononuclear, bacteria, Adjuvant

Abstract

Tuberculosis is chronic infectious disease caused by Mycobacterium tuberculosis (M.tb) that is prevalent worldwide. Several specific antigens, such as Antigen 85B (Ag85B) and 6 kDa early secretory antigenic target (ESAT-6) protein of M.tb, are listed as some of the candidate subunit vaccines against M.tb. ESAT-6, as a virulent factor and differential gene in M.tb, shows insufficient immunogenicity in animal model. In order to investigate the ways to improve the immunogenicity of ESAT-6, we immunized ESAT-6 by subcutaneous and intramuscular routes with different adjuvants. We found that ESAT-6 immunized alone did not induce significant humoral immunity in both immunization routes. However, subcutaneous immunization of ESAT-6 plus incomplete Freund's adjuvant can induce a significant humoral immune response, enhanced proliferation and elevated secretion of IFN-γ from splenocytes. Intramuscular immunization of ESAT-6 plus adjuvant aluminum salt or poly(I:C) did not enhance humoral and cellular immune responses. Therefore, it is concluded that immunization of ESAT-6 subcutaneously plus incomplete Freund's adjuvant induces stronger humoral and cellular immune responses, which can be considered of ESAT-6 as a subunit vaccine in further research against tuberculosis.

Published

2018

10. Genetic determinants involved in the biodegradation of naphthalene and phenanthrene in Pseudomonas aeruginosa PAO1

Author

Jing Qi, Weina Kong, Lixin Shen, Bobo Wang, Jing Li, Huanhuan Ning, and Yingjuan Wang

Subjects

Health, Toxicology and Mutagenesis, Mutant, Gene Expression, Naphthalenes, Biology, medicine.disease_cause, Microbiology, Gene Knockout Techniques, chemistry.chemical_compound, medicine, Environmental Chemistry, Gene, Naphthalene, Pseudomonas aeruginosa, Pseudomonas, Wild type, Promoter, Gene Expression Regulation, Bacterial, General Medicine, Phenanthrenes, Phenanthrene, biology.organism_classification, Pollution, Biodegradation, Environmental, chemistry, Genes, Bacterial

Abstract

Pseudomonas sp. are predominant isolates of degradation-competent strains while very few studies have explored the degradation-related genes and pathways in most of the degrading strains. P. aeruginosa PAO1 was found capable of degrading naphthalene and phenanthrene efficiently. In order to investigate the degradation-related genes of naphthalene and phenanthrene in P. aeruginosa PAO1, a random promoter library of about 5760 strains was constructed. Thirty-two clones for differentially expressed promoters were obtained by screening in the presence of sub-inhibitory concentration of naphthalene and phenanthrene. Among them, 13 genes were up-regulated and 15 were down-regulated in the presence of naphthalene as well as phenanthrene. The four remaining genes have different regulation tendencies by naphthalene or phenanthrene. By comparing the growth between the wild type and mutants as well as the complementations, the roles of seven selected up-regulated genes on naphthalene and phenanthrene degradation were investigated. Five of the seven selected up-regulated genes, like PA2666 and PA4780, were found playing key roles on the degradation in P. aeruginosa PAO1. Also, the results imply that these genes participate in the overlapping part of naphthalene and phenanthrene degradation pathways in PAO1. Results in the article offer the convenience quick method and platform for searching degradation-related genes. It also laid a foundation for understanding of the role of the regulated genes.

Published

2014

11. Determination of Genes Involved in the Resistance of Pseudomonas aeruginosa to Carbapenems

Author

Lixin Shen, Wen Liang, HuanHuan Ning, KangMin Duan, Jing Qi, Yue Zhang, Lin Chen, and Qiao Guo

Subjects

Genetics, Transposable element, Imipenem, Mutation, Pseudomonas aeruginosa, Mutant, Wild type, Mutagenesis (molecular biology technique), biochemical phenomena, metabolism, and nutrition, Biology, bacterial infections and mycoses, medicine.disease_cause, Microbiology, medicine, bacteria, Pharmacology (medical), Gene, medicine.drug

Abstract

To investigate genes involved in the resistance of P. aeruginosa to carbapenems, a transposon mutation library containing more than 30000 clones was constructed and screened with three kinds of carbapenems, imipenem, meropenem and biapenem, for mutants with increased or reduced susceptibility to these antimicrobials. The insertion sites of the transposon were identified by arbitrary PCR and subsequent DNA sequencing. Forty-eight mutants with altered susceptibility to these antimicrobials compared with the wild type PAO1 were identified, 27 mutants demonstrated a reduced susceptibility phenotype and 21 mutants with an increased susceptibility. We identified five overlapping genes between our study and the study of Alvarez-Ortega and Dotsch et al. PA0011, PA0667 and PA3901 knockout mutant and complementary strain were constructed. That the antibiotics susceptibility analysis of these knockout mutants and complementary stains coincide with the mutagenesis mutants and wild type PAO1 respectively demonstrated that the three genes play a role in the carbapenems resistance of PAO1. In this study, 38 novel and unknown genetic determinants involved in susceptibility to carbapenems in PAO1 are found, including 13 class4 genes. Knowledge of novel resistance genes may contribute to understanding the mechanism of carbapenems resistance and discovering new drugs target in P. aeruginosa .

Published

2014