| Literature DB >> 29697865 |
Sha Zhou1, Qianqian Qi1, Xiaofan Wang1, Lina Zhang1, Lei Xu1, Liyang Dong1, Jifeng Zhu1, Yalin Li1, Xuefeng Wang1, Zhipeng Xu1, Feng Liu1, Wei Hu2, Liang Zhou3, Xiaojun Chen1, Chuan Su1.
Abstract
CD4+ CD25+ Foxp3+ regulatory T cells (Tregs) play a pivotal role in limiting immunopathological damage to host organs after schistosome infection. Transforming growth factor-β (TGF-β) is an essential factor for the periphery conversion of CD4+ CD25- T cells into CD4+ CD25+ Foxp3+ Tregs by inducing the key transcription factor Foxp3. Antigen presenting cells (APCs), which highly express TGF-β, are involved in parasite antigen-induced Treg conversion in peripheral. However, the mechanisms underlying high TGF-β induction in APCs by parasite antigens remain to be clarified during schistosome infection. Here, we demonstrated that Schistosoma japonicum stress protein, heat shock protein 60 (SjHSP60), promoted TGF-β production in macrophages (Mφ). Furthermore, we showed that activation of TLR4-Mal (MyD88 adaptor-like protein) signaling by SjHSP60 is necessary for induction of TGF-β expression in Mφ, which subsequently promoted Treg induction. Our results not only demonstrate a novel mechanism of TGF-β production in Mφ for inducing Tregs in mice with schistosomiasis, but also allude to the possibility of targeting parasite stress protein for potential therapeutics.Entities:
Keywords: Mal; Mφ; TGF-β production; TLR4; Treg induction; schistosomiasis
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Year: 2018 PMID: 29697865 PMCID: PMC6197892 DOI: 10.1111/imcb.12160
Source DB: PubMed Journal: Immunol Cell Biol ISSN: 0818-9641 Impact factor: 5.126