KLF9 positively regulates TRIM33 to inhibit abnormal synovial fibroblast proliferation, migration as well as inflammation in rheumatoid arthritis

Dan, Huang; Tao, Lihua; Du, Xiuri

doi:10.1002/iid3.696

Cited by 5 publications

(9 citation statements)

References 34 publications

(63 reference statements)

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“…Another study by Das also confirmed that overexpression of KLF2 down‐regulated the expression of MMP9, thus reducing joint inflammation and cartilage injury 122 . Following the foregoing, KLF9 is down‐regulated in MH7A cells (human rheumatoid arthritis fibroblasts) induced by TNF‐α, while the enhancement of KLF9 can inhibit the release of pro‐inflammatory factors (IL‐1β, IL‐6, IL‐8, iNOS and COX‐2) 123,124 . Tripartite motif containing gene 33 (TRIM33) is a member of TRIM family containing E3 ubiquitin ligase, which can inhibit the secretion of inflammatory factors by synovial fibroblasts 124,125 .…”

Section: Role Of Klfs In Bone Diseasesmentioning

confidence: 83%

“…The luciferase report found that the luciferase activity in MH7A cells transduced by TRIM33‐WT and si‐KLF9 decreased, whereas the enrichment of TRIM33 was observed after adding anti‐KLF9 125 . The above results suggest that overexpression of KLF9 increases the enrichment of TRIM33, while down‐regulation of KLF9 weakens the inhibitory effect of TRIM33 on inflammatory response, indicating that KLF9 may partially inhibit inflammation in RA by positively regulating TRIM33 124 . Furthermore, Wang et al 126 .…”

Section: Role Of Klfs In Bone Diseasesmentioning

confidence: 93%

“…125 The above results suggest that overexpression of KLF9 increases the enrichment of TRIM33, while down-regulation of KLF9 weakens the inhibitory effect of TRIM33 on inflammatory response, indicating that KLF9 may partially inhibit inflammation in RA by positively regulating TRIM33. 124 Furthermore, Wang et al 126 KLF4 and KLF7, on the other hand, support the inflammatory reaction in RA. It is reported that TNFα induced RA synovial cells exhibited significant levels of KLF4 expression, and luciferase assay revealed that KLF4 trans-activated the inflammatory factor iNOS promoter and encouraged its expression.…”

Section: Klfs and Inflammationmentioning

confidence: 99%

“…It follows that KLF9 may inhibit RA‐FLS proliferation by encouraging apoptosis and autophagy. Additionally, KLF9 positively regulated TRIM33 expression to prevent TNF‐α induced abnormal proliferation and migration of MH7A cells 124 . Same as KLF9, inhibition of KLF10 can eliminate the suppressive effect of PDLIM2 on RA‐FLS, which shows that the activity of FLS is significantly increased, FLS migration is increased, the expression of Bcl‐2 is increased, the expression of apoptosis‐related proteins (Bax, Cyto‐C and Cleaved caspase 3) is decreased, and the expressions of inflammatory factors and MMPs (MMP2 and MMP9) are markedly increased.…”

Section: Role Of Klfs In Bone Diseasesmentioning

confidence: 99%

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KLF transcription factors in bone diseases

Wang,

Han,

Dmitrii

et al. 2024

J Cellular Molecular Medi

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Krüppel‐like factors (KLFs) are crucial in the development of bone disease. They are a family of zinc finger transcription factors that are unusual in containing three highly conserved zinc finger structural domains interacting with DNA. It has been discovered that it engages in various cell functions, including proliferation, apoptosis, autophagy, stemness, invasion and migration, and is crucial for the development of human tissues. In recent years, the role of KLFs in bone physiology and pathology has received adequate attention. In addition to regulating the normal growth and development of the musculoskeletal system, KLFs participate in the pathological process of the bones and joints and are intimately linked to several skeletal illnesses, such as osteoarthritis (OA), rheumatoid arthritis (RA), osteoporosis (OP) and osteosarcoma (OS). Consequently, targeting KLFs has emerged as a promising therapeutic approach for an array of bone disorders. In this review, we summarize the current literature on the importance of KLFs in the emergence and regulation of bone illnesses, with a particular emphasis on the pertinent mechanisms by which KLFs regulate skeletal diseases. We also discuss the need for KLFs‐based medication‐targeted treatment. These endeavours offer new perspectives on the use of KLFs in bone disorders and provide prognostic biomarkers, therapeutic targets and possible drug candidates for bone diseases.

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Section: Role Of Klfs In Bone Diseasesmentioning

confidence: 83%

Section: Role Of Klfs In Bone Diseasesmentioning

confidence: 93%

Section: Klfs and Inflammationmentioning

confidence: 99%

Section: Role Of Klfs In Bone Diseasesmentioning

confidence: 99%

See 2 more Smart Citations

KLF transcription factors in bone diseases

Wang,

Han,

Dmitrii

et al. 2024

J Cellular Molecular Medi

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“…KLF transcription factors are crucial regulators of inflammatory conditions, such as neutrophil/endothelial cell‐driven inflammation 32,33 . As a prominent member of the KLF family, KLF9 has been demonstrated to trigger lipopolysaccharide (LPS)‐induced pulmonary inflammation, 34 TNF‐α‐induced synovial fibroblast inflammation, 35 and high glucose‐induced trophoblast inflammation 36 . Especially, KLF9 overexpression in the lungs of COPD mice and CSE‐treated BEAS‐2B cells has been identified in our study, which is consistent with a previous study reporting KLF9 elevation in the end‐stage lung of COPD 10 .…”

Section: Discussionmentioning

confidence: 99%

Mechanism of KLF9 in airway inflammation in chronic obstructive pulmonary

Gu,

Wang,

et al. 2023

Immunity Inflam & Disease

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BackgroundChronic obstructive pulmonary disease (COPD) is an airway‐associated lung disorder, resulting in airway inflammation. This article aimed to explore the role of the krüppel‐like factor 9 (KLF9)/microRNA (miR)‐494‐3p/phosphatase and tensin homolog (PTEN) axis in airway inflammation and pave a theoretical foundation for the treatment of COPD.MethodsThe COPD mouse model was established by exposure to cigarette smoke, followed by measurements of total cells, neutrophils, macrophages, and hematoxylin and eosin staining. The COPD cell model was established on human lung epithelial cells BEAS‐2B using cigarette smoke extract. Cell viability was assessed by cell counting kit‐8 assay. miR‐494‐3p, KLF9, PTEN, and NLR family, pyrin domain containing 3 (NLRP3) levels in tissues and cells were measured by quantitative real‐time polymerase chain reaction or Western blot assay. Inflammatory factors (TNF‐α/IL‐6/IL‐8/IFN‐γ) were measured by enzyme‐linked immunosorbent assay. Interactions among KLF9, miR‐494‐3p, and PTEN 3′UTR were verified by chromatin immunoprecipitation and dual‐luciferase assays.ResultsKLF9 was upregulated in lung tissues of COPD mice. Inhibition of KLF9 alleviated airway inflammation, reduced intrapulmonary inflammatory cell infiltration, and repressed NLRP3 expression. KLF9 bound to the miR‐494‐3p promoter and increased miR‐494‐3p expression, and miR‐494‐3p negatively regulated PTEN expression. miR‐494‐3p overexpression or Nigericin treatment reversed KLF9 knockdown‐driven repression of NLRP3 inflammasome and inflammation.ConclusionKLF9 bound to the miR‐494‐3p promoter and repressed PTEN expression, thereby facilitating NLRP3 inflammasome‐mediated inflammation.

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KLF9 positively regulates TRIM33 to inhibit abnormal synovial fibroblast proliferation, migration as well as inflammation in rheumatoid arthritis

Dan

Tao

2022

Immunity Inflam & Disease

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Background Rheumatoid arthritis (RA) can cause irreversible joint injury and serious disability. This study aimed to investigate how TRIM33 regulated by KLF9 affects the aggressive behaviors of synovial fibroblasts induced by tumor necrosis factor‐α (TNF‐α). Materials and Methods TNF‐α‐induced MH7A cells were used to simulate the in vitro model of RA. TRIM33 and KLF9 expression in TNF‐α‐challenged MH7A cells and transfection efficiency were analyzed via real‐time reverse transcription polymerase chain reaction together with western blot. The viability, proliferation, invasion, and migration of TNF‐α‐induced MH7A cells after transfection was respectively detected by CCK‐8, EdU staining, transwell, and wound‐healing assays. The expression of invasion and migration‐related proteins and inflammation‐related proteins was determined by western blot and the levels of inflammatory factors were detected by enzyme‐linked immunosorbent assay. The combination between TRIM33 and KLF9 was substantiated through dual‐luciferase reporter assay and chromatin immunoprecipitation. Results TRIM33 and KLF9 expression in TNF‐α‐challenged MH7A cells was downregulated. TRIM33 elevation inhibited TNF‐α‐elicited proliferation, metastasis as well as inflammation of MH7A cells. Moreover, KLF9 was combined with TRIM33 and KLF9 promoted transcription of TRIM33. The inhibitory effect of TRIM33 overexpression on proliferation, invasion and migration and inflammation of MH7A cells induced by TNF‐α was alleviated by the downregulation of KLF9. Conclusion KLF9 positively regulates TRIM33 to suppress the abnormal MH7A cell proliferation, migration, and reduce inflammation upon exposure to TNF‐α, which was reversed by inhibiting KLF9.

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KLF9 positively regulates TRIM33 to inhibit abnormal synovial fibroblast proliferation, migration as well as inflammation in rheumatoid arthritis

Cited by 5 publications

References 34 publications

KLF transcription factors in bone diseases

KLF transcription factors in bone diseases

Mechanism of KLF9 in airway inflammation in chronic obstructive pulmonary

KLF9 positively regulates TRIM33 to inhibit abnormal synovial fibroblast proliferation, migration as well as inflammation in rheumatoid arthritis

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