Isorhamnetin Downregulates MMP2 and MMP9 to Inhibit Development of Rheumatoid Arthritis through SRC/ERK/CREB Pathway

LIU Xiao-rong; LI Shuo-fu; MEI Wen-ya; LIU Xiang-dan; ZHOU Ri-bao

doi:10.1007/s11655-023-3753-6

Your Location：

Home >

Browse articles >

Isorhamnetin Downregulates MMP2 and MMP9 to Inhibit Development of Rheumatoid Arthritis through SRC/ERK/CREB Pathway

Original Article | Updated：2024-03-22

- Isorhamnetin Downregulates MMP2 and MMP9 to Inhibit Development of Rheumatoid Arthritis through SRC/ERK/CREB Pathway
- Chinese Journal of Integrative Medicine Vol. 30, Issue 4, Pages: 299-310(2024)
- Affiliations：
  
  1.College of Pharmacy, Hunan University of Chinese Medicine, Changsha (410208), China
  2.Department of Orthopaedics, The First Hospital of Hunan University of Chinese Medicine, Changsha(410007), China
- Author bio：
  
  Dr. LIU Xiao-rong, E-mail: smile20221204@163.com
- Funds：
- DOI：10.1007/s11655-023-3753-6
  CLC：
- Published：01 April 2024，
  
  Published Online：12 January 2024，
  
  Accepted：29 June 2023
Scan for full text
LIU Xiao-rong, LI Shuo-fu, MEI Wen-ya, et al. Isorhamnetin Downregulates MMP2 and MMP9 to Inhibit Development of Rheumatoid Arthritis through SRC/ERK/CREB Pathway. [J]. Chinese Journal of Integrative Medicine 30(4):299-310(2024)
DOI：

LIU Xiao-rong, LI Shuo-fu, MEI Wen-ya, et al. Isorhamnetin Downregulates MMP2 and MMP9 to Inhibit Development of Rheumatoid Arthritis through SRC/ERK/CREB Pathway. [J]. Chinese Journal of Integrative Medicine 30(4):299-310(2024) DOI： 10.1007/s11655-023-3753-6.

摘要

目的:

为了研究异鼠李素对类风湿性关节炎 (RA) 病理的影响.

方法:

将肿瘤坏死因子 (TNF) -α诱导的成纤维细胞样滑膜细胞 (FLS) 暴露于额外的异鼠李素 (10、20 和 40 μmol/L) . 将基质金属蛋白酶-2 (MMP2) 或 MMP9 或 SRC 的过表达载体转染至细胞内以探索它们在异鼠李素介导的 RA-FLS 功能中的作用. 对 RA-FLS 的活力、迁移和侵袭进行了评估. 此外

还建立了胶原蛋白诱导的关节炎 (CIA) 大鼠模型. 将大鼠随机分为sham组、CIA组、低剂量组、中剂量组和高剂量组 (每组 5 只)

分别给予生理盐水或额外的异鼠李素 (2、10 和 20 mg/kg)

连续 4 周. 计算CIA大鼠的关节炎指数并测定滑膜组织炎症. 在RA-FLS和滑膜组织测定MMP2、MMP9、TNF-α、白细胞介素-6 (IL-6) 和IL-1β的水平

以及测定SRC、细胞外调节激酶 (ERK) 和环磷酸腺苷反应元件结合蛋白 (CREB) 的磷酸化水平. 分子对接还被用于异鼠李素与 SRC 的结合.

结果:

在体外研究中

异鼠李素抑制了 RA-FLS 的活力、迁移研究中

异鼠李素抑制了 RA-FLS 的活力、迁移和侵袭研究中

异鼠李素抑制了 RA-FLS 的活力、迁移和侵袭 (

0.05) . 异鼠李素降低了RA-FLS 中 MMP2、MMP9、TNF-α、IL-6 和 IL-1β 的水平 (

0.05) . 过表达 MMP2 或过表达MMP9 可逆转异鼠李素对 RA-FLS迁移和侵袭

以及TNF-α、IL-6和 IL-1β 水平的抑制 (

0.05) . 此外

异鼠李素与 SRC 结合

并减少了 SRC、ERK 和 CREB 的磷酸化水平 (

0.05) . SRC 的过表达逆转了异鼠李素对RA-FLS活力、迁移和侵袭的抑制作用

以及对MMP2和MMP9的负调控 (

0.05) . 在体内研究中

异鼠李素降低了关节炎指数评分 (

0.05)

减轻了滑膜炎. 异鼠李素降低了滑膜组织中 MMP2、MMP9、TNF-α、IL-6和IL-1β 的水平

以及 SRC、ERK 和 CREB 的磷酸化水平 (

0.05) . 值得注意的是

浓度越高

异鼠李素的抑制作用越明显 (

0.05) .

结论:

异鼠李素通过调节SRC/ERK/CREB和MMP2/MMP9信号通路发挥抗RA作用

表明异鼠李素可能是一种潜在的RA治疗剂.

Abstract

Objective:

To investigate the effect of isorhamnetin on the pathology of rheumatoid arthritis (RA).

Methods:

Tumor necrosis factor (TNF)-α-induced fibroblast-like synoviocytes (FLS) was exposed to additional isorhamnetin (10

20 and 40 μmol/L). Overexpression vectors for matrix metalloproteinase-2 (MMP2) or MMP9 or SRC were transfected to explore their roles in isorhamnetin-mediated RA-FLS function. RA-FLS viability

migration

and invasion were evaluated. Moreover

a collagen-induced arthritis (CIA) rat model was established. Rats were randomly divided to sham

CIA

low-

medium-

and high-dosage groups using a random number table (

=5 in each group) and administed with normal saline or additional isorhamnetin [2

and 20 mg/(kg•day)] for 4 weeks

respectively. Arthritis index was calculated and synovial tissue inflammation was determined in CIA rats. The levels of MMP2

MMP9

TNF-α

interleukin-6 (IL-6)

and IL-1β

as well as the phosphorylation levels of SRC

extracellular regulated kinase (ERK)

and cyclic adenosine monophosphate response element-binding (CREB)

were detected in RA-FLS and synovial tissue. Molecular docking was also used to analyze the binding of isorhamnetin to SRC.

Results:

in vitro

studies

isorhamnetin inhibited RA-FLS viability

migration and invasion (

0.05). Isorhamnetin downregulated the levels of MMP2

MMP9

TNF-α

IL-6

and IL-1β in RA-FLS (

0.05). The overexpression of either MMP2 or MMP9 reversed isorhamnetin-inhibited RA-FLS migration and invasion

as well as the levels of TNF-α

IL-6

and IL-1β (

0.05). Furthermore

isorhamnetin bound to SRC and reduced the phosphorylation of SRC

ERK

and CREB (

0.05). SRC overexpression reversed the inhibitory effect of isorhamnetin on RA-FLS viability

migration and invasion

as well as the negative regulation of MMP2 and MMP9 (

0.05). In

in vivo

studies

isorhamnetin decreased arthritis index scores (

0.05) and alleviated synovial inflammation. Isorhamnetin reduced the levels of MMP2

MMP9

TNF-α

IL-6

and IL-1β

as well as the phosphorylation of SRC

ERK

and CREB in synovial tissue (

0.05). Notably

the inhibitory effect of isorhamnetin was more pronounced at higher concentrations (

0.05).

Conclusion:

Isorhamnetin exhibited anti-RA effects through modulating SRC/ERK/CREB and MMP2/MMP9 signaling pathways

suggesting that isorhamnetin may be a potential therapeutic agent for RA.

关键词

Keywords

rheumatoid arthritisisorhamnetinSRC/ERK/CREBmatrix metalloproteinase

references

More>

Views

Downloads

CSCD

Alert me when the article has been cited

Submit

Tools

Publicity Resources

Mechanism of Gentisic Acid on Rheumatoid Arthritis Based on miR-19b-3p/RAF1 Axis

Prevalence and Factors Associated with Concomitant Chinese Medicine Use by Rheumatoid Arthritis Patients in A Multi-Ethnic Asian Population

Inokosterone Is a Potential Drug Target of Estrogen Receptor 1 in Rheumatoid Arthritis Patients:Analysis from Active Ingredient of Cyathula Officinalis

Deciphering Potential Correlations between New Biomarkers and Pattern Classification in Chinese Medicine by Bioinformatics:Two Examples of Rheumatoid Arthritis*

Chinese Herbal Formula Ermiao Powder (二妙散) Regulates Cholinergic Anti-inflammatory Pathway in Rats with Rheumatoid Arthritis

Related Author

No data

Related Institution

Department of Traditional Chinese Medicine, Zunyi Medical and Pharmaceutical College

Centre for Quantitative Medicine, Duke-NUS Medical School

Medicine Academic Clinical Program, Division of Medicine, Singapore General Hospital

Department of Rheumatology and Immunology, Singapore General Hospital

Duke-NUS Medical School

Address：1 Caochang, xiyuan, Beijing, People's Republic of China Postal code：100091
Tel：010-62886827, 62877592 Fax：010-62874291
Technical support is provided by Beijing Founder electronics co., LTD 京ICP备05067934号-1 京公网安备11010802024621
It is recommended to read the content of this site in Chrome&IE9+. Please switch to extreme mode in browser 360.
Cookies We use cookies to help provide and enhance our service and tailor content. By continuing, you agree to the use of cookies.

⁰