Interleukin-37: A crucial cytokine with multiple roles in disease and potentially clinical therapy (Review)

Wang, Limin; Quan, Yanchun; Yue, Yongfang; Heng, Xueyuan; Che, Fengyuan

doi:10.3892/ol.2018.7982

Cited by 42 publications

(65 citation statements)

References 87 publications

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“…Accumulated data have implicated that IL‐37 plays an important role in regulating both innate and adaptive immune responses (Tawfik, Nasef, Omar, & Ghaly, ; Zhao et al, ). In addition, growing bodies of data have revealed that IL‐37 is capable of suppressing the production of inflammatory cytokines, for instance, tumor necrosis factor‐α (TNF‐α) and IL‐6 (L. Wang, Quan, et al, ; L. Wang, Wang, et al, ). A recent study by Yu et al () has shown the evidence that IL‐37 is reduced in GDM placentas and serum and could protect pregnant women from the development of GDM.…”

Section: Introductionmentioning

confidence: 99%

Dysregulation of microRNA‐657 influences inflammatory response via targeting interleukin‐37 in gestational diabetes mellitus

Wang

et al. 2018

Journal Cellular Physiology

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A number of studies have implicated that microRNAs (miRNAs) play a critical role in the development of gestational diabetes mellitus (GDM). However, the role of miR-657 in GDM remains vague up to date. We aim to investigate the modifying effect of miR-657 on GDM, which will provide new insight into the pathogenesis of GDM and may help to identify new diagnostic or therapeutic targets for GDM. Increased expression of miR-657 but decreased expression of interleukin-37 (IL-37) was observed in patients with GDM. Besides, negative association between miR-657 and IL-37 was demonstrated in this study. miR-657 could targetedly regulate IL-37 and enhance the proliferation of mononuclear macrophages. Moreover, miR-657 promoted the generation of inflammatory cytokines (IL-6 and tumor necrosis factor-α [TNF-α]) and activation of nuclear factor κB (NF-κB) in lipopolysaccharide-induced mononuclear macrophages, while its effect was significantly inhibited when exogenous recombinant IL-37 was administrated into cells.Accordingly, dysregulation of miR-657 contributes to the pathogenesis of GDM via IL-37/NF-κB signaling axis. K E Y W O R D S gestational diabetes mellitus, IL-37, inflammation, microRNA, NF-κB J Cell Physiol. 2019;234:7141-7148.wileyonlinelibrary.com/journal/jcp

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Section: Introductionmentioning

confidence: 99%

Dysregulation of microRNA‐657 influences inflammatory response via targeting interleukin‐37 in gestational diabetes mellitus

Wang

et al. 2018

Journal Cellular Physiology

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“…The combined comparison of in silico analysis and in vivo data appear in conflict with regard to the finding that a significant reduction in IL37 expression was observed in PBMCs from MS patients undergoing exacerbation of the disease in the in silico analysis whereas augmented levels of IL37 were observed in the circulation of MS patients suffering an exacerbation. These apparently conflicting results may be explained by the fact that in the in silico analysis only the production of IL37 from PBMC was evaluated, whereas measurement of the circulating levels of IL37 also takes into account the production of IL37 from other non-immune sources including uterus and gastrointestinal cells for example [17]. Although our study is the first to demonstrate increased levels of IL37 during relapses of MS, two previous studies found augmented blood levels of IL37 in Iranian patients suffering from RR-MS and NMO.…”

Section: Discussionmentioning

confidence: 99%

“…IL37 is a cytokine belonging to the IL1 family that was originally discovered by in silico research [15]. IL37 can be found in the cytoplasm and nucleus [16] and is detectable in many human cells, including monocytes; natural killer (NK) cells; stimulated B cells; and tissues such as thymus, bone marrow, lymph nodes, colon, lung, and uterus [17]. The human IL37 gene is located on chromosome 2 and undergoes alternative splicing.…”

Section: Introductionmentioning

confidence: 99%

In Silico and In Vivo Analysis of IL37 in Multiple Sclerosis Reveals Its Probable Homeostatic Role on the Clinical Activity, Disability, and Treatment with Fingolimod

et al. 2019

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We evaluated the in silico expression and circulating levels of interleukin (IL)37 in patients with different forms of multiple sclerosis (MS) and also upon treatment with different disease-modifying drugs. The combined interpretation of the resulting data strengthens and extends the current emerging concept that endogenous IL37 plays an important role in determining onset and progression of MS. The in silico analysis revealed that production of IL37 from cluster of differentiation (CD)4+ T cells from MS patients was reduced in vitro as compared to healthy controls. The analysis of the datasets also demonstrated that "higher" levels of IL37 production from PBMC entailed significant protection from MS relapses. In addition, the in vivo part of the study showed that IL37 was selectively augmented in the sera of MS patients during a relapse and that treatment with the high potency disease-modifying drug fingolimod significantly increased the frequency of patients with circulating blood levels of IL37 (6/9, 66%) as compared to patients receiving no treatment (n = 48) or platform therapy (n = 59) who had levels of IL37 below the limit of the sensitivity of the assay. This finding therefore anticipates that fingolimod may at least partially exert its beneficial effects in MS by upregulating the production of IL37.

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“…It has been discussed that such a biological function of interleukin-37 could be captured as a clinically successful therapeutic target for the treatment of periodontal inflammation and cancers. 92,93 To explore other similarities between shared epigenome alterations in both periodontitis and cancer, methylation-specific PCR for E-cadherin and cyclooxygenase-2 was performed. 94 while in the breast neoplastic tissue, the gene-silencing detection rate was 38% and 35%, respectively.…”

Section: Peri Odontal Pathog En S and Infl Ammatory Re S P On S E Pmentioning

confidence: 99%

Epigenetic reprogramming in periodontal disease: Dynamic crosstalk with potential impact in oncogenesis

Barros

Fahimipour

Tarran

et al. 2019

Periodontology 2000

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Periodontitis is a chronic multifactorial inﬂammatory disease associated with microbial dysbiosis and characterized by progressive destruction of the periodontal tissues. Such chronic infectious inflammatory disease is recognized as a major public health problem worldwide with measurable impact in systemic health. It has become evident that the periodontal disease phenotypes are not only determined by the microbiome effect, but the extent of the tissue response is also driven by the host genome and epigenome patterns responding to various environmental exposures. More recently there is mounting evidence indicating that epigenetic reprogramming in response to combined intrinsic and environmental exposures, might be particularly relevant due its plasticity and potential application towards precision health. The complex epigenetic crosstalk is reflected in the prognosis and progress of periodontal diseases and may also lead to a favorable landscape for cancer development. This review discusses epigenomics modifications focusing on the role of DNA methylation and pathways linking microbial infection and inflammatory pathways, which are also associated with carcinogenesis. There is a more clear vision whereas 'omics' technologies applied to unveil relevant epigenetic factors could play a significant role in the treatment of periodontal disease in a personalized mode, evidencing that public health approach should coexist with precision individualized treatment.

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Interleukin-37: A crucial cytokine with multiple roles in disease and potentially clinical therapy (Review)

Cited by 42 publications

References 87 publications

Dysregulation of microRNA‐657 influences inflammatory response via targeting interleukin‐37 in gestational diabetes mellitus

Dysregulation of microRNA‐657 influences inflammatory response via targeting interleukin‐37 in gestational diabetes mellitus

In Silico and In Vivo Analysis of IL37 in Multiple Sclerosis Reveals Its Probable Homeostatic Role on the Clinical Activity, Disability, and Treatment with Fingolimod

Epigenetic reprogramming in periodontal disease: Dynamic crosstalk with potential impact in oncogenesis

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