Felix IL. Clanchy , Federica Borghese , Jonas Bystrom , Attila Balog , Henry Penn , Dobrina N. Hull , Rizgar A. Mageed , Peter C. Taylor , Richard O. Williams
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The expression of immunomodulatory molecules was measured in a murine model of arthritis treated with anti-TNF and the expression of ET-associated molecules was measured in whole blood in rheumatoid arthritis (RA) and ankylosing spondylitis (AS) patients, before and after therapy. The expression of ET-associated genes was also measured in RA patient monocytes before and after therapy, in anti-TNF responders and non-responders. <em>Tnfaip3</em>, <em>Ptpn6</em> and <em>Irak3</em> were differentially expressed in affected paws, spleens, lymph nodes and circulating leucocytes in experimental murine arthritis treated with anti-TNF. Prior to therapy, the expression of <em>TNFAIP3</em>, <em>INPP5D</em>, <em>PTPN6, CD38</em> and <em>SIGIRR</em> in whole blood differed between human healthy controls and RA or AS patients. In blood monocytes from RA patients, the expression of <em>TNFAIP3</em> was significantly reduced by anti-TNF therapy in non-responders. Prior to therapy, anti-TNF non-responders had higher expression of <em>TNFAIP3</em> and <em>SLPI</em>, compared to responders. Although the expression of <em>TNFAIP3</em> was significantly higher in RA non-responders prior to treatment, the post-treatment reduction to a level similar to responders did not coincide with a clinical response to therapy.</p></div>","PeriodicalId":15245,"journal":{"name":"Journal of autoimmunity","volume":"148 ","pages":"Article 103300"},"PeriodicalIF":7.9000,"publicationDate":"2024-08-07","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"https://www.sciencedirect.com/science/article/pii/S0896841124001343/pdfft?md5=25d05f69750e974a5293366990c00329&pid=1-s2.0-S0896841124001343-main.pdf","citationCount":"0","resultStr":"{\"title\":\"Inflammatory disease status and response to TNF blockade are associated with mechanisms of endotoxin tolerance\",\"authors\":\"Felix IL. 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The expression of immunomodulatory molecules was measured in a murine model of arthritis treated with anti-TNF and the expression of ET-associated molecules was measured in whole blood in rheumatoid arthritis (RA) and ankylosing spondylitis (AS) patients, before and after therapy. The expression of ET-associated genes was also measured in RA patient monocytes before and after therapy, in anti-TNF responders and non-responders. <em>Tnfaip3</em>, <em>Ptpn6</em> and <em>Irak3</em> were differentially expressed in affected paws, spleens, lymph nodes and circulating leucocytes in experimental murine arthritis treated with anti-TNF. Prior to therapy, the expression of <em>TNFAIP3</em>, <em>INPP5D</em>, <em>PTPN6, CD38</em> and <em>SIGIRR</em> in whole blood differed between human healthy controls and RA or AS patients. In blood monocytes from RA patients, the expression of <em>TNFAIP3</em> was significantly reduced by anti-TNF therapy in non-responders. Prior to therapy, anti-TNF non-responders had higher expression of <em>TNFAIP3</em> and <em>SLPI</em>, compared to responders. 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引用次数: 0
摘要
内毒素耐受(ET)可下调炎症反应,其机制已在外源性收费样受体配体的反应中得到了很好的描述,但很少有研究关注炎症性疾病中的 ET 相关机制。由于阻断 TNF 可减轻 ET 的发展,因此研究人员测量了抗 TNF 对炎症性自身免疫性疾病中关键 ET 相关分子表达的影响;并使用 ET 生物测定法证实了炎症基因表达的变化。在使用抗肿瘤坏死因子治疗的小鼠关节炎模型中测量了免疫调节分子的表达,并在治疗前后测量了类风湿性关节炎(RA)和强直性脊柱炎(AS)患者全血中 ET 相关分子的表达。在治疗前后,还测量了抗肿瘤坏死因子应答者和非应答者的 RA 患者单核细胞中 ET 相关基因的表达。Tnfaip3、Ptpn6 和 Irak3 在接受抗肿瘤坏死因子治疗的实验性小鼠关节炎患爪、脾脏、淋巴结和循环白细胞中的表达存在差异。治疗前,人类健康对照组与 RA 或 AS 患者全血中 TNFAIP3、INPP5D、PTPN6、CD38 和 SIGIRR 的表达存在差异。在 RA 患者的血液单核细胞中,抗肿瘤坏死因子疗法明显降低了非应答者的 TNFAIP3 表达。在治疗前,抗肿瘤坏死因子无应答者的TNFAIP3和SLPI表达量高于应答者。虽然在治疗前,RA 非应答者的 TNFAIP3 表达量明显较高,但治疗后其表达量降低到与应答者相似的水平,这与临床治疗应答并不一致。
Inflammatory disease status and response to TNF blockade are associated with mechanisms of endotoxin tolerance
The mechanisms of endotoxin tolerance (ET), which down-regulate inflammation, are well described in response to exogenous toll-like receptor ligands, but few studies have focused on ET-associated mechanisms in inflammatory disease. As blocking TNF can attenuate the development of ET, the effect of anti-TNF on the expression of key ET-associated molecules in inflammatory auto-immune disease was measured; changes in inflammatory gene expression were confirmed using an ET bioassay. The expression of immunomodulatory molecules was measured in a murine model of arthritis treated with anti-TNF and the expression of ET-associated molecules was measured in whole blood in rheumatoid arthritis (RA) and ankylosing spondylitis (AS) patients, before and after therapy. The expression of ET-associated genes was also measured in RA patient monocytes before and after therapy, in anti-TNF responders and non-responders. Tnfaip3, Ptpn6 and Irak3 were differentially expressed in affected paws, spleens, lymph nodes and circulating leucocytes in experimental murine arthritis treated with anti-TNF. Prior to therapy, the expression of TNFAIP3, INPP5D, PTPN6, CD38 and SIGIRR in whole blood differed between human healthy controls and RA or AS patients. In blood monocytes from RA patients, the expression of TNFAIP3 was significantly reduced by anti-TNF therapy in non-responders. Prior to therapy, anti-TNF non-responders had higher expression of TNFAIP3 and SLPI, compared to responders. Although the expression of TNFAIP3 was significantly higher in RA non-responders prior to treatment, the post-treatment reduction to a level similar to responders did not coincide with a clinical response to therapy.
期刊介绍:
The Journal of Autoimmunity serves as the primary publication for research on various facets of autoimmunity. These include topics such as the mechanism of self-recognition, regulation of autoimmune responses, experimental autoimmune diseases, diagnostic tests for autoantibodies, as well as the epidemiology, pathophysiology, and treatment of autoimmune diseases. While the journal covers a wide range of subjects, it emphasizes papers exploring the genetic, molecular biology, and cellular aspects of the field.
The Journal of Translational Autoimmunity, on the other hand, is a subsidiary journal of the Journal of Autoimmunity. It focuses specifically on translating scientific discoveries in autoimmunity into clinical applications and practical solutions. By highlighting research that bridges the gap between basic science and clinical practice, the Journal of Translational Autoimmunity aims to advance the understanding and treatment of autoimmune diseases.