Jun-Ling Zhu, Jian-Yao Zhou, Tao Hou, Jian-Zhi Zhao,Guo-Fang Wang, Xiao-Wei Han

Department of Rheumatology, Shaoxing Central Hospital, Zhejiang Province (312030) China

1. Introduction

Ankylosing spondylitis (AS) is a chronic, inflammatory and rheumatological disease involving the axial skeleton, sacroiliac joint, and periphery joints, and its etiology remains obscure[1]. The clinical manifestations of AS mainly include pain, stiffness, spinal mobility limitation, and chest expansion, which has serious impacts on work and quality of life[2]. The prevalence of AS is 1.67% in Asia and 0.2%-0.4% in China[3,4]. Two thirds of these patients will progress into partial or full stiffening of spine several years after onset[5]. Fibronectin and metalloproteinase-3 (MMP-3) are main factors in the inflammation and fibrosis pathology in AS[6,7]. And the aim of this study is to observe the expression of fibronectin and MMP-3 in AS patients and explore related significance.

2. Materials and methods

2.1. Diagnostic criteria

Thirty consecutive patients were diagnosed with AS according to the modified New York classification criteria and CT examination that showed sacroiliitis level was below[8].

2.2. Inclusion criteria

The patients inclusion criteria were listed as follows: (1) between 16 to 69 years old, (2) conformed AS diagnosis according to diagnostic criteria[8]; (3) had not received sulfasalazine,methotrexate, thalidomide and glucocorticoid for at least four weeks prior participation of the study; (4) voluntarily signed the informed consent form. This study was approved by the Ethical Committee of Shaoxing Central Hospital.

2.3. Exclusion criteria

Patients were excluded as follows: (1) had other rheumatoid diseases that require treatment with sulfasalazine, methotrexate,thalidomide, leflunomide and glucocorticoid; (2) women in pregnancy or lactation stage; (3) patients who were hypersensitive to the testing drug; (4) complicated with serious primary diseases of heart, lung, liver, kidney system, or had mental diseases.

2.4. Drop-out criteria

The patients (1) did not conform to inclusion criteria during the research process; (2) did not take medicines according to the research; (3) had evident side effects and cannot recover spontaneously after another 1 week of treatment.

2.5. Patients

A total of 30 confirmed AS patients that visited out-patient or inpatient Department of Rheumatology of Shaoxing Central Hospital from May 2015 to March 2017 were enrolled in this study, and they were diagnosed according to the above mentioned AS diagnostic criteria. And 30 healthy volunteers were also enrolled as the normal control group in this research.

2.6. Treatment

2.7. Detection of fibronectin and MMP-3

Fibronectin and MMP-3 in the venous blood of AS patients were measured by ELISA method before and after the research respectively. The fibronectin and MMP-3 reagent kits were bought from Nanjing Jiancheng Bioengineering Institute. And the specific operation processes were conduceted according to the instructions.Fibronectin and MMP-3 in the venous blood of healthy volunteers patients were measured only once before the research.

2.8. Clinical data collection

Bath ankylosing spondylitis disease activity index (BASDAI),bath ankylosing spondylitis functional index, bath ankylosing spondylitis metrology index, patient’s global assessment, spinal pain,general pain and night pain were used for scoring (1-10) patients with AS. Physical examination, blood and urine tests, erythrocyte sedimentation rate (ESR) and C-reactive protein (CRP) measurement were observed before and after the treatment in AS group.

2.9. Statistical analysis

The measurement data were expressed by mean±standard deviation (mean±SD). Statistical comparisons were conducted byt-test. Pearson’s linear-correlation analysis was used to determine relationships between parameters. Statistical analysis was carried out using SPSS version 13.0 software. Statistical significance was considered atP＜0.05.

3.Results

3.1. General materials

In AS group, 1 patient withdrew from the research because of poor response, and 1 patient withdrew from the study for increasing liver enzymes. Finally 28 cases finished the research, including 21 male and 7 female with a mean age of (33.50±10.82) years. The mean duration of illness was (12.68±6.12) years, with HLA-B27 positive in 23 cases and negative in 5 cases. And all 30 healthy volunteers in the normal control group finished blood measuring in this study.

3.2. Changes of fibronectin and MMP-3 levels in venous blood of AS group

Fibronectin and MMP-3 in venous blood of AS patients were significant higher than that in the normal control group (P＜0.05,Table 1). Three months after treated with sulfasalazine, the level of fibronectin and MMP-3 in the AS group were significant lower than that before treatment (P＜0.05, Table 1).

Table 1Detection of fibronectin and MMP-3 in peripheral blood of AS patients at baseline (mean±SD).

3.3. Lab examination

Levels of ESR and CRP in AS group were significantly decreased compared to that before treatment (P＜0.05, Table 2).

Table 2Changes of ESR and CRP of AS patients related to baseline (mean±SD).

3.4. Changes of clinical data of AS patients compared to baseline

After treated by sulfasalazine for 3 months, scores of BASDAI,global assessment, spine pain, night pain and general pain in AS group were significantly improved compared with that before treatment (P＜0.05). And scores of bath ankylosing spondylitis functional index and bath ankylosing spondylitis metrology index in the AS group were of no evident change compared with that before treatment (P＞0.05, Table 3).

3.5. Correlation detection

Pearson’s linear-correlation analysis showed that serum fibronectin level had a positive correlation with BASDAI, global assessment,spine pain, night pain, general pain, ESR and CRP (r=0.635, 0.562,0.431, 0.470, 0.536, 0.528, 0.469,P＜0.05); serum MMP-3 level had a positive correlation with BASDAI, global assessment, spine pain, night pain, general pain, ESR and CRP (r=0.521, 0.507, 0.463,0.514, 0.476, 0.531, 0.502,P＜0.05).

4. Discussion

AS is a chronic inflammatory disease that affects 1% of the general population. As one of the most severe types of spondyloarthropathy disease, AS normally affects the spinal vertebrae and sacroiliac joints, which can cause debilitating pain and loss of mobility. A total of 90% of patients with AS are HLA-B27 positive. Traditional therapies include nonsteroidal anti-inflammatory drugs or adrenal cortical hormones, but they can only alleviate the symptoms and cannot improve symptoms[9,10]. Clinically, sulfasalazine,methotrexate and leflunomide were used to treat peripheral arthritis of AS effectively, but failed in therapeutic course. Sulfasalazine continues to be frequently prescribed as one kind of nonbiologic disease-modifying antirheumatic drugs to treat AS, despite of an unclear efficacy profile[11,12]. Some studies have suggested that sulfasalazine can improve peripheral joint disease[13-15], and it is also effective in treating the spinal symptoms in patients without associated peripheral joint disease[16,17]. In our study, sulfasalazine was used to treat the patients and the results showed that scores of BASDAI, global assessment, spine pain, night pain and general pain were significantly improved (P＜0.05) compared with baseline values. It showed that sulfasalazine could largely achieve a therapeutic purpose for AS patients.

Fibrosis is important in the pathology change of AS and it can lead to bone destruction and joint deformation[18]. Fibrosis is a chronic and progressive process characterized by an excessive deposition of extracellular matrix components, such as collagen and fibronectins. It is believed to follow chronic tissue inflammation and ultimately leads to organ scarring and subsequent loss of function.Excessive collagen is a biological marker of fibrosis, and its expression is regulated by many kinds of cytokines[19]. The increase of extracellular matrix in the tissue, with fibronectin and collagen being the major components, can ultimately lead to development of fibrosis. Fibronectin has been shown to co-localize with aggregations of fibroblasts[20]. Matrix MMP-3 can degrade proteoglycan, collagen type III, IV, IX, XI and other protein substrates in extracellular matrix[21]. In this research, we aimed to investigate the expression of collagen and MMP-3 and its significance in AS patients.

Our study showed that the serum level of both fibronectin and MMP-3 in AS patients were significantly higher than that in normal control group (P＜0.05). The possible reason is that thelocal or system inflammation activated fibroblasts and synovial cells produced more fibronectin and MMP-3. After treatment,the expression of fibronectin and MMP-3 were both significantly decreased, indicating that the fibronectin and MMP-3 level could reflect the disease activity of AS. What’s more, both serum fibronectin and MMP-3 level had a positive correlation with BASDAI, global assessment, spine pain, night pain, general pain, ESR and CRP, showing that serum fibronectin and MMP-3 correlated with the onset of AS. It showed fibronectin and MMP-3 played an important regulatory role in the fibrosis pathogenesis of AS.

Table 3Changes of clinical data of AS patients compared to baseline (mean±SD).

In conclusion, our study showed that the expression of fibronectin and MMP-3 in AS patients were significantly higher than that in the normal control group, and they all decreased significantly after treatment. It indicates that both fibronectin and MMP-3 are correlated closely with the onset of AS.

[1] Sveälv BG, Täng MS, Klingberg E, Forsblad-d’Elia H, Bergfeldt L. Prevalence of diastolic dysfunction in patients with ankylosing spondylitis: A cross-sectional study.Scand J Rheumatol2015; 44(2): 111-117.

[2] Martindale J, Shukla R, Goodacre J. The impact of ankylosing spondylitis/axial spondyloarthritis on work productivity.Best Pract Res Clin Rheumatol2015; 29(3): 512-523.

[3] Dean LE, Jones GT, MacDonald AG, Downham C, Sturrock RD,Macfarlane GJ. Global prevalence of ankylosing spondylitis.Rheumatology2014; 53(4): 650-657.

[4] Li Z, Wong S, Shen JX, Chan M, Wu W. The role of microRNAS in ankylosing spondylitis.Medicine2016; 95(14): e3325.

[5] Yang CH, Huang F. Immunogenetics and pathogenesis of ankylosing spondylitis.Curr Immnol2007; 27: 265-268.

[6] Klavdianou K, Liossis SN, Sakkas L, Daoussis D. The role of Dickkopf-1 in joint remodeling and fibrosis: A link connecting spondyloarthropathies and scleroderma?Semin Arthritis Rheum2017; 46(4): 430-438.

[7] Fan JP, Zhao J, Shao J, Wei XZ, Zhu XD, Li M. I-BET151 inhibits expression of RANKL, OPG, MMP3 and MMP9 in ankylosing spondylitisin vivoandin vitro.Exp Ther Med2017; 14(5): 4602-4606.

[8] Van der linden S, Valkenburg HA, Cats A. Evaluation of diagnostic criteria for ankylosing spondylitis. A propsposal for modification of the New York criteria.Arthritis Rheum1984; 27: 361-368.

[9] Kroon F, Landewe R, Dougados M, van der Heijde D. Continuous NSAID use reverts the effects of inflammation on radiographic progression in patients with ankylosing spondylitis.Ann Rheum Dis2012; 71(10): 1623-1629.

[10] Yang EZ, Cao LL, Zhang GW, Lian XF, Xu JG. Transpseudarthrosis osteotomy with interbody fusion for kyphotic spinal pseudarthrosis in ankylosing spondylitis by a single posterior approach: A retrospective study and a brief relevant literature review.Biomed Res Int2017; 10(8):40-48.

[11] Tam HW, Yeo KJ, Leong PY, Chen CH, Li YC, Ma CM, et al.Sulfasalazine might reduce risk of cardiovascular diseases in patients with ankylosing spondylitis: A nationwide population-based retrospective cohort study.Int J Rheum Dis2017; 20(3): 363-370.

[12] Mitulescu TC, Stavaru C, Voinea LM, Banica LM, Matache C,Predeteanu D. The role of Vitamin D in immuno-inflammatory responses in ankylosing spondylitis patients with and without acute anterior uveitis.J Med Life2016; 9(1): 26-33.

[13] Hou ZD, Xiao ZY, Gong Y, Zhang YP, Zeng QY. Arylamine N-acetyltransferase polymorphisms in Han Chinese patients with ankylosing spondylitis and their correlation to the adverse drug reactions to sulfasalazine.BMC Pharmacol Toxicol2014; 21(11): 156-158.

[14] Xiao P, Pang C, Zhu X, Wu X. Clinical research for curing ankylosing spondylitis through combining etanercept, thalidomide and sulfasalazine.Pak J Pharm Sci2015; 28(1 Suppl): 359-362.

[15] Damjanov N, Shehhi WA, Huang F, Kotak S, Burgos-Vargas R, Shirazy K, et al. Assessment of clinical efficacy and safety in a randomized double-blind study of etanercept and sulfasalazine in patients with ankylosing spondylitis from Eastern/Central Europe, Latin America, and Asia.Rheumatol Int2016; 36(5): 643-651.

[16] Dougados M, Boumier P, Amor B. Sulphasalazine in ankylosing spondylitis: a double blind controlled study in 60 patients.Br Med J (Clin Res Ed)1986; 293: 911-914.

[17] Braun J, Zochling J, Baraliakos X, Alten R, Burmester G, Grasedyck K, et al. Efficacy of sulfasalazine in patients with inflammatory back pain due to undifferentiated spondyloarthritis and early ankylosing spondylitis: a multicentre randomised controlled trial.Ann Rheum Dis2006; 65: 1147-1153.

[18] Bron JL, de Vries MK, Snieders MN, van der Horst-Bruinsma IE, van Royen BJ. Discovertebral (Andersson) lesions of the spine in ankylosing spondylitis revisited.Clin Rheumatol2009; 28: 883-892.

[19] Leeming DJ, Byrjalsen I, Jimenez W, Christiansen C, Karsdal MA.Protein fingerprinting of the extracellular matrix remodeling in a rat model of liver fibrosis-a serological evaluation.Liver Int2013; 33: 439-447.

[20] Van Assche G, Geboes K, Rutgeerts P. Medical therapy for Crohn’s diseases strictures.Inflamm Bowel Dis2004; 10: 55-60.

[21] Visse R, Nagase H. Matrix metalloproteinases and tissue inhibitors of metalloproteinases structure, function, and biochemistry.Circ Res2003;92(8): 827-839.