Mycobacterium Tuberculosis Proteome Microarray for Global Studies of Protein Function and Immunogenicity

Deng, Jiao-Yu; Bi, Lijun; Zhou, Lin; Guo, Shujuan; Fleming, Joy; Jiang, He‐wei; Zhou, Ying; Gu, Jia; Zhong, Qian; Wang, Zongxiu; Liu, Zhonghui; Deng, Rui-Ping; Gao, Jing; Chen, Tao; Li, Wenjuan; Wang, Jingfang; Wang, Xude; Li, Haicheng; Ge, Feng; Zhu, Guofeng; Zhang, Hainan; Gu, Jing; Wu, Fanlin; Zhang, Zhiping; Wang, Dianbing; Hang, Haiying; Yang, Li; Cheng, Li; He, Xiang; Tao, Sheng-Ce; Zhang, Xian-En

doi:10.1016/j.celrep.2014.11.023

Cited by 75 publications

(65 citation statements)

References 58 publications

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“…Rv2031c (hspX) was also previously identified using a Mtb proteomic level microarray with printing of unpurified Mtb proteins generated in E. coli lysate (6). Interestingly, we did not identify shared candidate proteins with an independent recent microarray study that was based on printing proteins generated in a Saccharomyces cerevisiae system (47). Overall, we have validated the value of some previously known serological biomarkers and further identified some new TB biomarker candidates.…”

Section: M-hd-nappa -Conceptmentioning

confidence: 50%

Identification of Antibody Targets for Tuberculosis Serology using High-Density Nucleic Acid Programmable Protein Arrays

Song

Wallstrom

et al. 2017

Molecular & Cellular Proteomics

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Better and more diverse biomarkers for the development of simple point-of-care tests for active tuberculosis (TB), a clinically heterogeneous disease, are urgently needed. We generated a proteomic Mycobacterium tuberculosis (Mtb) High-Density Nucleic Acid Programmable Protein Array (HD-NAPPA) that used a novel multiplexed strategy for expedited high-throughput screening for antibody responses to the Mtb proteome. We screened sera from HIV uninfected and coinfected TB patients and controls (n ‫؍‬ 120) from the US and South Africa (SA) using the multiplex HD-NAPPA for discovery, followed by deconvolution and validation through single protein HD-NAPPA with biologically independent samples (n ‫؍‬ 124). We verified the top proteins with enzyme-linked immunosorbent assays (ELISA) using the original screening and validation samples (n ‫؍‬ 244) and heretofore untested samples (n ‫؍‬ 41). We identified 8 proteins with TB biomarker value; four (Rv0054, Rv0831c, Rv2031c and Rv0222) of these were previously identified in serology studies, and four (Rv0948c, Rv2853, Rv3405c, Rv3544c) were not known to elicit antibody responses. Using ELISA data, we created classifiers that could discriminate patients' TB status according to geography (

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Section: M-hd-nappa -Conceptmentioning

confidence: 50%

Identification of Antibody Targets for Tuberculosis Serology using High-Density Nucleic Acid Programmable Protein Arrays

Song

Wallstrom

et al. 2017

Molecular & Cellular Proteomics

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“…Antibodies from five donors from this study were shipped to TB Healthcare (China), which commercialized the assay. The assay was run as previously described (29). Briefly, the Mtb proteome microarrays were blocked for 1 h at RT with blocking buffer (3% BSA in 1× PBS, 0.1% Tween-20, pH 7.4) in a shaker.…”

Section: Methodsmentioning

confidence: 99%

“…To determine if the antigen targets of the protective antibodies were proteinaceous in nature, we panned antibodies from three protective donors and two nonprotective donors (24 and 26) against an Mtb proteome chip (29). The five pools of antibodies made multiple detectable binding responses against a variety of recombinantly expressed Mtb antigens (Dataset S1).…”

Section: Significancementioning

confidence: 99%

Latently and uninfected healthcare workers exposed to TB make protective antibodies against Mycobacterium tuberculosis

Wang

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

124

125

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The role of Igs in natural protection against infection by Mycobacterium tuberculosis (Mtb), the causative agent of TB, is controversial. Although passive immunization with mAbs generated against mycobacterial antigens has shown protective efficacy in murine models of infection, studies in B cell-depleted animals only showed modest phenotypes. We do not know if humans make protective antibody responses. Here, we investigated whether healthcare workers in a Beijing TB hospital-who, although exposed to suprainfectious doses of pathogenic Mtb, remain healthy-make antibody responses that are effective in protecting against infection by Mtb. We tested antibodies isolated from 48 healthcare workers and compared these with 12 patients with active TB. We found that antibodies from 7 of 48 healthcare workers but none from active TB patients showed moderate protection against Mtb in an aerosol mouse challenge model. Intriguingly, three of seven healthcare workers who made protective antibody responses had no evidence of prior TB infection by IFN-γ release assay. There was also good correlation between protection observed in vivo and neutralization of Mtb in an in vitro human whole-blood assay. Antibodies mediating protection were directed against the surface of Mtb and depended on both immune complexes and CD4+ T cells for efficacy. Our results indicate that certain individuals make protective antibodies against Mtb and challenge paradigms about the nature of an effective immune response to TB.TB | antibodies | immune complex | humoral immunity | TB restrictors

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“…The field as a whole has a promising outlook with broad chemical diversity being displayed in newly identified lead compounds. Phenotypic screening is by and large the most successful tool in this renaissance of discovery [112, 151, 152], empowered greatly by advances in genomic and structural knowledge of druggable targets [153]. The most common targets identified in TB via typical phenotypic whole-cell screening are Mmpl3, DprE1 and QcrB [150, 154, 155] and it comes as no surprise that many of the advanced drugs under review and undergoing optimization hit these molecular targets.…”

Section: New Drugsmentioning

confidence: 99%

Advances in Drug Discovery and Development for Pediatric Tuberculosis

Hoagland¹,

Zhao²,

Lee

2016

MRMC

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Pediatric tuberculosis is an underappreciated global epidemic estimated to afflict around half a million children worldwide. This problem has historically been overlooked, due in part to their low social status and the difficulty in diagnosis of tuberculosis in children. Children are more susceptible to tuberculosis infection and disease progression, including rapid dissemination into extra-pulmonary infection sites. Treatment of pediatric tuberculosis infections has been traditionally built around agents used to treat the adult disease, but the disease pathology, drug pharmacokinetics and the safety window in children differs from the adult disease. This produces additional concerns for drug discovery and development of new agents. This review examines: (i) the safety concerns for current front and second line agents used to treat complex drug resistant infections and how this knowledge can be used to identify, prioritize and dose agents that may be better tolerated in pediatric populations; (ii) the chemistry and suitability of new drugs in the clinical development pipeline for tuberculosis for the treatment of pediatric infections indicating several new agents may offer significant improvements for the treatment of multi-drug resistant tuberculosis in children.

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Mycobacterium Tuberculosis Proteome Microarray for Global Studies of Protein Function and Immunogenicity

Cited by 75 publications

References 58 publications

Identification of Antibody Targets for Tuberculosis Serology using High-Density Nucleic Acid Programmable Protein Arrays

Identification of Antibody Targets for Tuberculosis Serology using High-Density Nucleic Acid Programmable Protein Arrays

Latently and uninfected healthcare workers exposed to TB make protective antibodies against Mycobacterium tuberculosis

Advances in Drug Discovery and Development for Pediatric Tuberculosis

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