| Literature DB >> 29743811 |
Yonghong Li1, Chaojun Wei1, Hui Xu1, Jing Jia1, Zhenhong Wei1, Rui Guo1, Yanjuan Jia1, Yu Wu1, Yuanting Li1, Xiaoming Qi1, Zhenhao Li1, Xiaoling Gao1.
Abstract
T helper 17 cells (Th17) constitute a distinct subset of helper T cells with a unique transcriptional profile (STAT3, RORγ, and RORα), cytokine production pattern (IL17 family), and requirement of specific cytokines for their differentiation (TGF-β, IL6, IL21, and IL23). Recent studies involving experimental animals and humans have shown that Th17/IL17 plays a crucial role in host defense against a variety of pathogens, including bacteria and viruses. The underlying mechanisms by which Th17 performs include dendritic cell (DC) regulation, neutrophil recruitment, Th1 modulation, and T regulatory cell (Treg) balance. In recent years, researchers have generated an accumulating wealth of evidence on the role of Th17/IL17 in protective immunity to intracellular bacterial pathogens, such as Mycobacterium tuberculosis and Chlamydia trachomatis, which are one of the most important pathogens that inflict significant socioeconomic burden across the globe. In this article, we reviewed the current literature on the functions and mechanisms by which Th17/IL17 responds to intracellular bacterial infections. A better understanding of Th17/IL17 immunity to pathogens would be crucial for developing effective prophylactics and therapeutics.Entities:
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Year: 2018 PMID: 29743811 PMCID: PMC5884031 DOI: 10.1155/2018/6587296
Source DB: PubMed Journal: Mediators Inflamm ISSN: 0962-9351 Impact factor: 4.711
The major characteristics of pathogenic intracellular bacterial species.
| Serial number | Bacterial species | Gram staining | Facultative/obligatory | Diseases | Function of Th17/IL17 |
|---|---|---|---|---|---|
| 1 |
| Positive | Obligatory | Pulmonary infection, pleurisy, tuberculous pericarditis, bone tuberculosis, tubercular meningitis, tuberculous arthritis | (i) Recruit neutrophils, macrophages, Th1 cells and IFN |
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| 2 |
| Positive | Facultative | Septicemia, meningitis, monocytosis | (i) Promote adaptive CTL responses |
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| 3 | (i) | Negative | Obligatory | Pelvic inflammatory disease, trachoma, pneumoniae | Promote DC functions |
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| 4 | (i) | Negative | Facultative | Typhoid fever, paratyphoid fever, Enteritidis | IL23 is required for protection against the sublethal doses of S. Enteritidis |
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| 5 |
| Negative | Facultative | Tularemia | (i) Regulate the IL12-Th1 cell pathway |
Figure 1Schematic depiction of Th17/IL17 immunoregulation mechanisms.