Osteonecrosis of the Hip and Bisphosphonate Treatment

NCT ID: NCT00781261

Last Updated: 2013-01-14

Basic Information

• Recruitment Status: UNKNOWN
• Clinical Phase: PHASE2
• Total Enrollment: 120 participants
• Study Classification: INTERVENTIONAL
• Study Start Date: 2009-08-31
• Study Completion Date: 2013-12-31

Brief Summary

Osteonecrosis of the hip is an important cause of musculoskeletal disability and finding therapeutic solutions has proven to be challenging. Osteonecrosis means death of bone which can occur from the loss of the blood supply or some other means. Although any age group may develop osteonecrosis, most patients are between 20 and 50 years old. The most common risk factor is a history of high steroid treatment for some medical condition. The next most common associated condition is a history of high alcohol use. There are some cases of osteonecrosis that occur in patients that are otherwise completely healthy with no detectable risk factors.

In the earliest stage of the disease, x-rays appear normal and the diagnosis is made using MRI. The advanced stages of osteonecrosis begin when the dead bone starts to fail mechanically through a process of microfractures of the bone. As the disease progresses, the surface begins to collapse until, finally the integrity of the joint is destroyed. A wide range of surgical treatments with variable success rates have been proposed for the treatment of the osteonecrosis to preserve joint integrity, including core decompression, whereby the venous hypertension that ensues is lessened and revascularisation may be induced leading to bone repair. Nonsurgical treatment options are limited and usually result in a poor prognosis. Early stage disease can be treated with protected weight bearing and physiotherapy, however some studies have shown protected weight bearing to be associated with a greater than 85% rate of femoral head collapse. Unfortunately most studies indicate that the risk for disease progression is greater with nonsurgical treatment than with surgical intervention. There are no established pharmaceuticals for the prevention of treatment of osteonecrosis. Evidence is increasing that the nitrogen containing bisphosphonates may be beneficial in the treatment of osteonecrosis. One bisphosphonates (alendronate) has been evaluated in 60 patients diagnosed with osteonecrosis of the hip. Recent clinical studies have shown very promising results. All patients had symptomatic improvement after one year. Although the follow up time ranged from 3 months to 5 years, only 6 patients progressed to the point of needing surgery.

Detailed Description

Osteonecrosis (ON) of the hip is an important cause of musculoskeletal disability and finding therapeutic solutions has proven challenging. Patients who are affected with ON are often relatively young, usually in the third to sixth decade of life. ON of the hip is an increasingly common cause of musculoskeletal disability. It can cause pain with or without loss of function of the joint and often ends in substantial use of health care resources and disability. ON of the hip usually progresses to severe destruction of the femoral head with resultant degeneration of the hip joint, in most cases requiring joint replacement.

Early diagnosis has been made easier using magnetic resonance imaging (MRI), however no common satisfactory therapy has been developed for the early stage of the disease. Early surgery aimed at preserving the femoral head has been proposed, such as vascularised fibula grafting. However, the results of this invasive technique do not seem to be widely reproducible, and more minor interventions such as core drilling have high failure rates. Evidence is increasing that the nitrogen containing bisphosphonates may be beneficial in the treatment of ON. Data from clinical trials with patients with ON of the hip suggested that the bisphosphonate alendronate would reduce pain and disability and may reduce progression to femoral head collapse that usually would require surgical intervention.

With this study we aim to determine the efficacy of bisphosphonate therapy (zoledronic acid) versus placebo for reducing pain and disability in ON of the femoral head necrosis (palliative endpoint) and to investigate the effect of bisphosphonate therapy versus placebo in reducing progression to femoral head collapse and the need for surgical intervention (therapeutic endpoint).

Methods This will be a 2-armed double-blind randomised trial of a) zoledronic acid 5mg annually for 3 doses b) placebo drug infusions. Participants will be recruited primarily from rheumatologists and orthopaedic surgeons from multiple centres in Australia. We plan to include 4 major centres in capital cities in Australia and each centre would recruit approximately 30 participants. Potential participants who meet the eligibility criteria will be identified by their treating Rheumatologists or Orthopaedic surgeons, followed by a screening assessment conducted by the study research staff. Eligible participants will be randomised prior to the start of treatment. Prior to treatment, the study research staff will perform a baseline assessment over the phone, including demographic details, age, sex, duration of symptoms, medical history including prior surgery, trauma and medication use and known risk factors for ON. Furthermore at baseline, the Rheumatologists or Orthopaedic surgeon will perform a clinical evaluation using a slightly modified Harris Hip Score (HHS). The study research staff will contact the participants every 6 months to monitor the participant's condition and evaluate pain and disability. Additionally the participants will have a clinical evaluation and MRI scan at 12 months.

This novel clinical research protocol will aim to provide further evidence of the protective value of alendronate or zoledronic acid in patients with ON of the hip. It will determine whether bisphosphonates slow the progression of symptoms as well as the progression to total collapse of the hip. Additionally it will seek to answer questions regarding the comparative effectiveness and also cost-effectiveness of the use of bisphosphonates in early disease. The results of this study can lead to change in treatment of early disease ON and delay and possibly prevent surgical intervention.

Conditions

Osteonecrosis

Study Design

• Allocation Method: RANDOMIZED
• Intervention Model: PARALLEL
• Primary Study Purpose: PREVENTION
• Blinding Strategy: QUADRUPLE

Study Groups

Control

Subjects in the control group will receive a placebo drug for a 1 year period

Group Type: PLACEBO_COMPARATOR

Placebo

Intervention Type: DRUG

Subjects in the control group will receive a placebo drug for a similar period

Zoledronic Acid

Subjects in this intervention group will be given 5mg Zoledronic acid as a single injection

Group Type: ACTIVE_COMPARATOR

Zoledronic Acid

Intervention Type: DRUG

Subjects in the intervention group B will be given 5mg Zoledronic acid as a single injection.

Interventions

Zoledronic Acid

Subjects in the intervention group B will be given 5mg Zoledronic acid as a single injection.

Intervention Type: DRUG

Placebo

Subjects in the control group will receive a placebo drug for a similar period

Intervention Type: DRUG

Eligibility Criteria

Inclusion Criteria

1. aged between 18-90 years,

2. symptoms of pain and disability in at least one hip joint, or

3. positive MRI findings stage I or II on the ARCO classification

Exclusion Criteria

1. previous hip joint surgery on the affected hip

2. severe pain and disability at rest if treating clinician has recommended surgery

3. radiographic or MRI findings suggestive for stage III and IV on the ARCO classification

4. any iv bisphosphonate within the prior 2 years or any prior use of bisphosphonate preparations, except according to the washout schedule:

• 2 years (if use > 48 weeks),
• 1 year (if used > 8 weeks but < 48 weeks)
• 6 months (if used > 2 weeks but < 8 weeks)
• 2 months (if used < 2 weeks)

5. active primary hyperparathyroidism

6. hypothyroidism, not appropriately controlled with long-term thyroxine therapy

7. history of iritis or uveitis, except due to trauma, and resolved for > 2 years prior to study

8. self-reported history of diabetic nephropathy or retinopathy (if diabetic, Hb A1c > 10%)

9. urine dipstick greater than or equal to 2+ protein at screening

10. AST or ALT greater than twice the upper limit of normal and/or alkaline phosphatase greater than twice the upper limit of normal

11. serum calcium > 2.75 mmol/L (11.0 mg/dL) or < 2.00 mmol/L (8.0 mg/dL)

12. serum 25-hydroxyvitamin D concentrations < 15 ng/L m) baseline renal insufficiency (calculated creatinine clearance less than 40 mL/min and serum creatinine greater than 175 mol/L) at V1

13. a history of invasive malignancy of any organ system, treated or untreated, in the past five years; excluding, basal cell or squamous cell carcinoma of the skin, colonic polyps with non-invasive malignancy which have been removed, ductal carcinoma in-situ (DCIS), and carcinoma in-situ (CIS) of the uterine cervix

14. any candidate patient with severe dental problems or current dental infections and/or any candidate patient with recent or impending dental surgery within three months of dosing

15. women of childbearing potential not using the contraception method(s) specified in this study (specify), as well as women who are breastfeeding

• Minimum Eligible Age: 18 Years
• Maximum Eligible Age: 90 Years
• Eligible Sex: ALL
• Accepts Healthy Volunteers: No

Sponsors

Novartis

INDUSTRY

Sponsor Role: collaborator

University of Sydney

OTHER

Sponsor Role: lead

Responsible Party

Responsibility Role: SPONSOR

Principal Investigators

Philip Sambrook, Prof

Role: PRINCIPAL_INVESTIGATOR

University of Sydney

Locations

Royal North Shore Hospital, Department of Rheumatology

Sydney, New South Wales, Australia

Site Status: RECRUITING

Princess Alexandra Hospital

Brisbane, Queensland, Australia

Site Status: RECRUITING

Royal Brisbane and Womens Hospital

Herston, Queensland, Australia

Site Status: RECRUITING

The Queen Elizabeth Hospital

Adelaide, South Australia, Australia

Site Status: RECRUITING

Cabrini Hospital

Melbourne, Victoria, Australia

Site Status: RECRUITING

Countries

Australia

Central Contacts

Monique Macara

Role: CONTACT

monique.macara@sydney.edu.au

+61294631888

Lyn March

Role: CONTACT

lyn.march@sydney.edu.au

Facility Contacts

Monique Macara

Role: primary

monique.macara@sydney.edu.au

+61294631888

Professor Lyn March

Role: backup

lyn.march@sydney.edu.au

Genni Lynch

Role: primary

Genni_Lynch@health.qld.gov.au

(07) 3176 6640

A/Prof Emma Duncan

Role: primary

e.duncan@uq.edu.au

Janelle McFarlane

Role: backup

j.mcfarlane@uq.edu.au

Catherine Hill, A/Prof

Role: primary

Catherine.Hill@health.sa.gov.au

+618 82226688

Sarah Downie-Doyle

Role: backup

Sarah.Downie-Doyle2@health.sa.gov.au

+618 8133 4029

Rachelle Buchbinder

Role: primary

rachelle.buchbinder@med.monash.edu.au

+613 95081652

Other Identifiers

570989

Identifier Type: -

Identifier Source: org_study_id