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Clinical Trial Details — Status: Recruiting

Administrative data

NCT number NCT02722772
Other study ID # IAI-ETN-KOA-201613
Secondary ID
Status Recruiting
Phase N/A
First received March 24, 2016
Last updated March 29, 2016
Start date February 2016
Est. completion date August 2017

Study information

Verified date February 2016
Source First Affiliated Hospital of Harbin Medical University
Contact Zhiyi Zhang, Ph.D
Phone +86-451-85552350
Email zhangzhiyi_rheu@163.com
Is FDA regulated No
Health authority China: Food and Drug Administration
Study type Interventional

Clinical Trial Summary

Primary aim: evaluate efficacy of intra-articular injection of etanercept for moderate and severe knee osteoarthritis.

Second aim: investigate the potentiality of serum cytokines (TNF-α, L1-α, IL1-β, MMP1, MMP13) to predict the response of intra-articular injection of etanercept for moderate and severe knee osteoarthritis.


Description:

1. Background:

Osteoarthritis (osteoarthritis, OA) is a common joint disease. It is characterized by recurrent joint pain, swelling, increasing of disease status, joint deformity and activity disorders. [1] The pathogenesis of OA has not been fully understood. It may be associated with a variety of factors, such as: mechanics, biochemistry, genetics, and so on. Its main feature is the imbalance between synthesis and catabolism of articular cartilage cells. The imbalance may refer to cell aging, cell apoptosis, local inflammatory factor in joints as well as stress mechanism and so on. [2] OA usually develops in burdened and active joints, such as: the knee, the spine (cervical and lumbar spine), hip and ankle, hand joints, etc. The first session of The National Health and Nutrition Survey (The first National Health and Nutrition Examination Survey, NHANESI) found that 12% of people in The United States have at least one joint in accordance with the clinical diagnosis of OA. [3] Radiographic result shows that rate of American adults knee OA prevalence is 14% and 37%, and women are more common (4-6). A large study found that at least one joint in people over 55 years have radiographic hand OA, and female prevalence is 67%, male is 55% [7].

The OA in Chinese are more likely happened in elder women than men. Prevalence rate could up to 50% in people over the age of 60, and 80% in 75 years old.

Osteoarthritis patients suffer huge pain, and it cause huge economic burden to the society, and it becomes a serious impact on social productivity and lead to huge economic burden [8].

In the United States, OA cost $ 1, 855 billion per year and in 27 million patients, and women spend $ 6212 per year, male $ 4730 per year [2]; OA cost 1% ~ 2.5% of GDP in the United States, Britain, France, Canada, Australia and other developed countries. There is no burden of economic data of OA in China [9].

Classification criteria of knee osteoarthritis According to the affected areas, OA can be divided into knee OA, hip OA, hand OA (distal interphalangeal joints, the first wrist palm joints), foot OA (first plantar toe joints, heel), etc.

Knee OA is the most common disease in clinical disease. The classification of the knees OA contains clinical criteria, and also clinical and imaging criteria in the modified ACR classification criteria in osteoarthritis classification criteria [10].

Knee osteoarthritis usually occurs with obvious fricatives, bony enlargement, Baker cyst expansion and joint effusion is generally not associated with skin redness [11].

The most common deformity comes out with varus in severe cases, but also it may appear in the early mild disease. That clinically obvious varus may be a predictive factor during the disease progression [12]. That quadriceps become weak is a changeable risk factor for early knees OA disease progression, especially in women (13-14). Muscle atrophy occurs in late stage of disease progression [15] [16]. And it brings huge burden of disease to patients [11].

Treatment of knee OA The aim of the treatment is to relieve pain, prevent and delay the progress of disease, protect the joints function, improve the quality of life. The treatment should be individualized. Full consideration to the patient' illness risk factors should be given, including: joint structure changing, the degree of inflammation and pain, concurrent disease status and other specific situation and condition. Treatment should be given priority to combine non-drug therapy with drug therapy. Operation should be performed when it is necessary [17].

Non-drug therapy include psychosocial intervention [17], decreasing weight [18], reasonable exercise [19], physical therapy which includes heat therapy, spa therapy, etc.), etc.

Drug therapy mainly includes drugs using external, drugs using in whole body and drugs intra-articular injections [17].

Topical drugs include: capsaicin [20], non-steroid anti-inflammatory drugs (NSAIDS) for external use [21] and lidocaine for external use only.

Systemic medicine include: a: non-opiate analgesic. Acetaminophen is the first choice of OA treatment, and the main reason is that the less side effects and good curative effect [22].b: NSAIDS. There are two effect of NSAIDS: anti-pain and anti-inflammatory, which is the most commonly used for the control of OA symptoms. The main adverse reactions are gastrointestinal symptoms, renal or liver damage, effect on platelet function, and it may increase the risk of cardiovascular adverse events [23]. c: opioid analgesics. It can be considered if Pain still difficult to control after non-drug and drug treatment.

Drugs injection intra-articular, including: intra-articular injection of glucocorticoid and hyaluronic acid derivatives [24].

Research of TNF-α application in OA: TNF-α and IL1 play an important role in the pathogenesis of osteoarthritis, IL1 - beta often express highly in middle to late course of OA [25 to 28]. In the OA flare course, TNF-α and IL1 alpha will increase significantly; TNF-α has been considered to be one of the important factors associated with the degree of OA inflammatory, and the IL1 alpha has a significant relation with the start of OA inflammatory [29].

2. Aims:

Primary: evaluate efficacy of intra-articular injection of etanercept for moderate and severe knee osteoarthritis Second: investigate the potentiality of serum cytokines (TNF-α, L1-α, IL1-β, MMP1, MMP13) to predict the response of intra-articular injection of etanercept for moderate and severe knee osteoarthritis.

3. Patients:

Recruit Patients of moderate and severe knee osteoarthritis, totally 60 patients (According with classification of "Clinical Image" of 1986 American college of rheumatology criteria in osteoarthritis of the knee )

4. Study Design:

A 12-week, multi-center, open-labeled, randomized study. Moderately and severe knee osteoarthritis patients, total 60 patients (consider expulsion rate 15%)(According with classification of "Clinical Image" of 1986 American college of rheumatology criteria in osteoarthritis of the knee )

The 60 patients will be randomly assigned into two groups:

Etanercept treatment group: Intra-articular injection of etanercept of 25mg/w/joint and health education, exercise and diet guidance; treatment: 5 weeks Routine care group: Health education, exercise and diet guidance; treatment: 5 weeks (If both knees are involved, the more significant symptomatic side is chosen for injection by etanercept)

This study has two stages:

1. Screening/baseline period: - 4 weeks ~ 0 weeks;

Patients should have signed informed consent form (ICF) before participating the study

Obtain the history before treatment, medical records, disease history and demographic information of patients. And also perform pregnancy test (optional), HIV testing (optional), HBV detection (optional), HCV detection (optional), electrocardiogram examination, chest radiograph, PPD test, vital signs, physical examination, blood routine, urine routine and blood biochemical examination, imaging examination (anteroposterior/lateral of X-ray in knee joint, horizontal position/lateral projection/side lateral projection of ultrasound in knee, supine position in knee joint of MRI (optional, sagittal and coronary are commonly used), measure the ESR and CRP and store serum in - 80 ℃ to detect serum protein markers level during baseline period, at the same time, keep the plasma to - 80 ℃.(refer to "9.3 lab operation"). Collect disease assessment result in baseline, and record the VAS pain score, SF12 score, KOOS score, 30 s - CST score, 40 m FPWT score, ultrasonic relative index score and MRI relative index score.

2. Follow-up:baseline to 12 weeks, during this period, two groups of participants will be treated with Intra-articular injection of etanercept of 25 mg/w/joint, health education, exercise and diet guidance or just health education, exercise and diet guidance separately. During this period 4 times follow-up will be performed at 2nd, 4th, 8th, 12th week.

At 2nd week, vital signs will be recorded, pain VAS score, SF12 score, KOOS score, condition of drug combination and adverse events will be recorded.

At 4th week, vital signs will be recorded, and blood routine, urine routine, blood biochemical, the ESR and CRP will be examined and recorded, imaging examination (horizontal position/lateral projection/side lateral projection of ultrasound in knee), and collect basic evaluation results such as: pain VAS score, SF12 score, KOOS score, 30 s - CST score, 40 m FPWT score, ultrasonic relative index score and condition of drug combination and adverse events will be recorded.

At 8th week, 12th week, vital signs, blood routine, urine routine and blood biochemical will be examined and recorded and imaging examination will be performed (horizontal position/lateral projection/side lateral projection of ultrasound in knee or supine position of MRI in knee joint, (optional, and sagittal and coronary will be used as usual)). Measure the ESR and CRP and store serum in - 80 ℃ to detect serum protein markers level during baseline to 8th week and 12th week, at the same time, store plasma to - 80 ℃.(refer to "9.3 lab operation"). Collect disease assessment result, and record the pain VAS score, SF12 score, KOOS score, 30 s - CST score, 40 m FPWT score, ultrasonic index score and MRI relative index score (optional). And condition of drug combination and adverse events will be recorded.

5. Laboratory tests

Main laboratory examination:

Detect the level of TNF-α, L1-α, IL1-β, MMP1, MMP13 levels in patients peripheral blood at baseline period and 4th week, 8th week by using enzyme-linked immunosorbent assay.

6. The curative effect evaluation/check points:

The primary checkpoint: at 8th week and 12th week, changes of pain VAS score, KOOS score relative to the baseline.

The Secondary checkpoints: at 8 weeks and 12 weeks changes of SF-12 score, 30s-CST score, 40 m FPWT score, ultrasound score, MRI score, level of TNF alpha, IL1 alpha, IL1 - beta, MMP1, MMP13 in serum relative to the baseline.

7. Statistical methods:

Based on the curative effect data of patients, analysis by using R software or SAS statistical software:

Calculate the measurement data using t-test and rank test; and rate is calculated using chi-square test.

Perform single factor and multiple factors regression analysis on indicators of baseline prognostic factors of patients (protein markers) and curative effect.


Recruitment information / eligibility

Status Recruiting
Enrollment 60
Est. completion date August 2017
Est. primary completion date July 2017
Accepts healthy volunteers No
Gender Both
Age group N/A and older
Eligibility Inclusion Criteria:

1. Willing and able to give full consent;

2. According with classification of "Clinical Image" of 1986 American college of rheumatology criteria in osteoarthritis of the knee ;

3. Grade II-III of Kellgren-Lawrence (KL) grading system, revealing synovial inflammation or synovial fluid by combining ultrasound and/or MRI

4. Knee pain for at least 1 Month and Pain VAS Score>4 during the last week;

5. Fertile women agreed to adopt effective contraceptive measures during the test.

Exclusion Criteria:

1. Allergic to pharmaceutical ingredients;

2. Received TNFI or other biologics preparation within 3 months;

3. Received physical therapy or articular injection, taking antidepressants or antispasmodic, opioids within 3 months ;

4. Patients with history of knee surgery or upcoming surgery within 10 years;

5. Patients accompanied by other complications or joint disease (such as septic arthritis, osteochondritis desiccans, osteonecrosis,haemochromatosis, ochronosis, etc.);

6. Patients with serious joint deformation or joint deformities;

7. Patients with active or a history of recurrent infections;

8. Patients existing active TB or has a history of active TB;

9. Patients with positive on hepatitis b surface antigen or hepatitis c antibody;

10. Patients with a history of severe lung disease, tumor;

11. Patients with severely abnormal function on liver and kidney (liver enzyme > = 2 times normal, creatinine > = normal);

12. Patients with pregnancy, ready for pregnancy or lactation;

13. Patients with other conditions which not suitable for use of Etanercept.

Study Design

Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment


Intervention

Drug:
Etanercept
Intra-articular injection of etanercept of 25mg/w/joint for 5 weeks.
Other:
Health education, exercise and diet guidance
Health education, exercise and diet guidance in patient; treatment: 5 weeks

Locations

Country Name City State
China The First Affiliated Hospital of Harbin Medical University Harbin Heilongjiang

Sponsors (2)

Lead Sponsor Collaborator
First Affiliated Hospital of Harbin Medical University Shanghai baiying pharmaceutical technology Co., Ltd.

Country where clinical trial is conducted

China, 

References & Publications (28)

Altman R, Asch E, Bloch D, Bole G, Borenstein D, Brandt K, Christy W, Cooke TD, Greenwald R, Hochberg M, et al. Development of criteria for the classification and reporting of osteoarthritis. Classification of osteoarthritis of the knee. Diagnostic and Therapeutic Criteria Committee of the American Rheumatism Association. Arthritis Rheum. 1986 Aug;29(8):1039-49. — View Citation

Baker KR, Xu L, Zhang Y, Nevitt M, Niu J, Aliabadi P, Yu W, Felson D. Quadriceps weakness and its relationship to tibiofemoral and patellofemoral knee osteoarthritis in Chinese: the Beijing osteoarthritis study. Arthritis Rheum. 2004 Jun;50(6):1815-21. — View Citation

Bradley JD, Brandt KD, Katz BP, Kalasinski LA, Ryan SI. Comparison of an antiinflammatory dose of ibuprofen, an analgesic dose of ibuprofen, and acetaminophen in the treatment of patients with osteoarthritis of the knee. N Engl J Med. 1991 Jul 11;325(2):87-91. — View Citation

Chang A, Hochberg M, Song J, Dunlop D, Chmiel JS, Nevitt M, Hayes K, Eaton C, Bathon J, Jackson R, Kwoh CK, Sharma L. Frequency of varus and valgus thrust and factors associated with thrust presence in persons with or at higher risk of developing knee osteoarthritis. Arthritis Rheum. 2010 May;62(5):1403-11. doi: 10.1002/art.27377. — View Citation

Dahaghin S, Bierma-Zeinstra SM, Ginai AZ, Pols HA, Hazes JM, Koes BW. Prevalence and pattern of radiographic hand osteoarthritis and association with pain and disability (the Rotterdam study). Ann Rheum Dis. 2005 May;64(5):682-7. Epub 2004 Sep 16. Erratum in: Ann Rheum Dis. 2005 Aug;64(8):1248. — View Citation

Dillon CF, Rasch EK, Gu Q, Hirsch R. Prevalence of knee osteoarthritis in the United States: arthritis data from the Third National Health and Nutrition Examination Survey 1991-94. J Rheumatol. 2006 Nov;33(11):2271-9. Epub 2006 Oct 1. — View Citation

Dreiser RL, Tisne-Camus M. DHEP plasters as a topical treatment of knee osteoarthritis--a double-blind placebo-controlled study. Drugs Exp Clin Res. 1993;19(3):117-23. — View Citation

Felson DT, Naimark A, Anderson J, Kazis L, Castelli W, Meenan RF. The prevalence of knee osteoarthritis in the elderly. The Framingham Osteoarthritis Study. Arthritis Rheum. 1987 Aug;30(8):914-8. — View Citation

Firestein GS, Kelley's Textbook of Rheumatology(Chinese Version). 9th ed. 2015: p.1756

Firestein GS, Kelley's Textbook of Rheumatology(Chinese Version). 9th ed. 2015: p.1765-1768.

Ge Z, Hu Y, Heng BC, Yang Z, Ouyang H, Lee EH, Cao T. Osteoarthritis and therapy. Arthritis Rheum. 2006 Jun 15;55(3):493-500. Review. — View Citation

Goldring MB. The role of the chondrocyte in osteoarthritis. Arthritis Rheum. 2000 Sep;43(9):1916-26. Review. — View Citation

Hunter DJ, Felson DT. Osteoarthritis. BMJ. 2006 Mar 18;332(7542):639-42. Review. — View Citation

Ikeda S, Tsumura H, Torisu T. Age-related quadriceps-dominant muscle atrophy and incident radiographic knee osteoarthritis. J Orthop Sci. 2005;10(2):121-6. — View Citation

Jordan JM, Helmick CG, Renner JB, Luta G, Dragomir AD, Woodard J, Fang F, Schwartz TA, Abbate LM, Callahan LF, Kalsbeek WD, Hochberg MC. Prevalence of knee symptoms and radiographic and symptomatic knee osteoarthritis in African Americans and Caucasians: the Johnston County Osteoarthritis Project. J Rheumatol. 2007 Jan;34(1):172-80. — View Citation

Kotlarz H, Gunnarsson CL, Fang H, Rizzo JA. Insurer and out-of-pocket costs of osteoarthritis in the US: evidence from national survey data. Arthritis Rheum. 2009 Dec;60(12):3546-53. doi: 10.1002/art.24984. — View Citation

Lawrence RC, Felson DT, Helmick CG, Arnold LM, Choi H, Deyo RA, Gabriel S, Hirsch R, Hochberg MC, Hunder GG, Jordan JM, Katz JN, Kremers HM, Wolfe F; National Arthritis Data Workgroup. Estimates of the prevalence of arthritis and other rheumatic conditions in the United States. Part II. Arthritis Rheum. 2008 Jan;58(1):26-35. doi: 10.1002/art.23176. — View Citation

Loeser RF, Goldring SR, Scanzello CR, Goldring MB. Osteoarthritis: a disease of the joint as an organ. Arthritis Rheum. 2012 Jun;64(6):1697-707. doi: 10.1002/art.34453. Epub 2012 Mar 5. Review. — View Citation

McCarberg B, Tenzer P. Complexities in the pharmacologic management of osteoarthritis pain. Curr Med Res Opin. 2013 May;29(5):539-48. doi: 10.1185/03007995.2013.785391. Epub 2013 Apr 3. Review. — View Citation

McCarthy GM, McCarty DJ. Effect of topical capsaicin in the therapy of painful osteoarthritis of the hands. J Rheumatol. 1992 Apr;19(4):604-7. — View Citation

Messier SP, Loeser RF, Mitchell MN, Valle G, Morgan TP, Rejeski WJ, Ettinger WH. Exercise and weight loss in obese older adults with knee osteoarthritis: a preliminary study. J Am Geriatr Soc. 2000 Sep;48(9):1062-72. — View Citation

Petrella RJ, DiSilvestro MD, Hildebrand C. Effects of hyaluronate sodium on pain and physical functioning in osteoarthritis of the knee: a randomized, double-blind, placebo-controlled clinical trial. Arch Intern Med. 2002 Feb 11;162(3):292-8. — View Citation

Rai MF, Rachakonda PS, Manning K, Vorwerk B, Brunnberg L, Kohn B, Schmidt MF. Quantification of cytokines and inflammatory mediators in a three-dimensional model of inflammatory arthritis. Cytokine. 2008 Apr;42(1):8-17. doi: 10.1016/j.cyto.2008.02.004. Epub 2008 Mar 17. — View Citation

Segal NA, Glass NA, Torner J, Yang M, Felson DT, Sharma L, Nevitt M, Lewis CE. Quadriceps weakness predicts risk for knee joint space narrowing in women in the MOST cohort. Osteoarthritis Cartilage. 2010 Jun;18(6):769-75. doi: 10.1016/j.joca.2010.02.002. Epub 2010 Feb 11. — View Citation

Slemenda C, Brandt KD, Heilman DK, Mazzuca S, Braunstein EM, Katz BP, Wolinsky FD. Quadriceps weakness and osteoarthritis of the knee. Ann Intern Med. 1997 Jul 15;127(2):97-104. — View Citation

Solomon SD, McMurray JJ, Pfeffer MA, Wittes J, Fowler R, Finn P, Anderson WF, Zauber A, Hawk E, Bertagnolli M; Adenoma Prevention with Celecoxib (APC) Study Investigators. Cardiovascular risk associated with celecoxib in a clinical trial for colorectal adenoma prevention. N Engl J Med. 2005 Mar 17;352(11):1071-80. Epub 2005 Feb 15. — View Citation

Topp R, Woolley S, Hornyak J 3rd, Khuder S, Kahaleh B. The effect of dynamic versus isometric resistance training on pain and functioning among adults with osteoarthritis of the knee. Arch Phys Med Rehabil. 2002 Sep;83(9):1187-95. — View Citation

Towle CA, Hung HH, Bonassar LJ, Treadwell BV, Mangham DC. Detection of interleukin-1 in the cartilage of patients with osteoarthritis: a possible autocrine/paracrine role in pathogenesis. Osteoarthritis Cartilage. 1997 Sep;5(5):293-300. — View Citation

* Note: There are 28 references in allClick here to view all references

Outcome

Type Measure Description Time frame Safety issue
Other Adverse event Type and frequency of adverse event 2 weeks, 4 weeks, 8 weeks and 12 weeks Yes
Primary Pain VAS score(Pain Visual Analogue Scale/Score) Changes from the baseline to 8 weeks and 12 weeks to evaluate the treatment efficacy baseline to 8 weeks and 12 weeks No
Primary KOOS score(The Knee injury and Osteoarthritis Score) Changes from the baseline to 8 weeks and 12 weeks to evaluate the treatment efficacy baseline to 8 weeks and 12 weeks No
Secondary 30s-CST score(30 seconds Sit/chair Test) Changes from the baseline to 8 weeks and 12 weeks to evaluate the activity of knee joint baseline to 8 weeks and 12 weeks No
Secondary 40m FPWT score(40 meters fast walking test) Changes from the baseline to 8 weeks and 12 weeks to evaluate the activity of knee joint baseline to 8 weeks and 12 weeks No
Secondary Assessment score under ultrasound Changes from the baseline to 8 weeks and 12 weeks to evaluate the changes of patients' inner-structure of knee baseline to 8 weeks and 12 weeks No
Secondary Assessment score under MRI Changes from the baseline to 8 weeks and 12 weeks to evaluate the changes of patients' inner-structure of knee baseline to 8 weeks and 12 weeks No
Secondary TNF-a?IL1-a?IL1-ß?MMP1?MMP13 level in serum Changes from the baseline to 8 weeks and 12 weeks to evaluate patients' inflammatory level baseline to 8 weeks and 12 weeks No
Secondary SF-12 score(MOS 12-item Short Form Health Survey) Changes from the baseline to 8 weeks and 12 weeks to evaluate patients' health condition baseline to 8 weeks and 12 weeks No
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