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Clinical Trial Summary

The overall goal of this proposal is to correlate ultrasound elastography technique with more standard clinically based outcome measures within the setting of a small sample sized group of patients affected by moderate-to- severe, chronic (>6months) midsubstance Achilles tendinopathy (AT).


Clinical Trial Description

The main goal for this pilot level study is to correlate ultrasound elastography technique with more standard clinically based outcome measures within the setting of a small sample sized group of patients affected by moderate-to- severe, chronic (> 6 months) midsubstance Achilles tendinopathy (AT). Investigators will conduct a 24-week, 2-arm randomized controlled pilot study to determine whether novel elastography techniques (AE) and shear wave imaging (SWI), a new quantitative method of ultrasound (US) imaging, correlate with valid clinical outcome measures (VISA-A and conventional US). Methods will be based on recently published clinical trials of autologous blood injections for treating AT and will incorporate novel US outcome measures of Achilles tendon appearance and stiffness, i.e. elasticity. The results of this multi-disciplinary pilot study will be used to help plan a separate larger scaled study to evaluate the effects of platelet-rich plasma (PRP) therapy for Achilles tendinopathy in which elastography will be included as a potential outcome measure and also correlated with standard clinical outcome surveys.

Pain and function will be evaluated by self-report using a validated clinical outcome questionnaire (VISA-A). Disease modification will be assessed by novel US-based AE and SWI methods for stiffness changes (biomechanical) and correlated with morphologic changes using conventional US. A larger study that will evaluate the effects of PRP in healing AT, while correlating with elastography assessment, will include a sham injection arm.

Intervention Subjects assigned to the PRP group will then receive the PRP injection under ultrasound guidance. The injection will take about 15 minutes.

Each subject will undergo a palpatory and ultrasound Achilles tendon exam. Tender areas associated with the Achilles tendon will be identified. Physical exam will be followed by Achilles tendon ultrasound which will serve as visual guidance for injection.

At the injection session, the research nurse will perform a single standard antecubital blood draw (35 mL). The PRP will be obtained from this sample using a two-stage spinning technique: the 1st separates red blood cells from platelets, and the 2nd concentrates the platelets to yield approximately 4 mL of concentrated autologous platelet. This layer of platelet rich plasma will be placed in the syringe by the centrifuge machine.

Platelet counts of subjects' whole blood and PRP processed blood will be analyzed. Platelet counts in whole blood vary by individual. The optimal quantity of platelets and growth factors required for tissue healing is not known, but a clinically effective concentration has been described as being greater than 4 times baseline autologous whole blood platelet concentrations. Therefore, platelet concentration yield may have important implications in clinical outcome correlation. In order to validate consistent platelet concentration yields across subjects, investigators will sample 1 mL of whole blood (approximately one lab Vacutainer) and an additional 1 mL of platelet rich plasma for lab analysis of platelet concentration using a standard lab automated analyzer. This extra 1 ml of whole blood will be drawn at the same time that the 35 ml described above is drawn.

The 3 ml of platelet rich plasma will be injected into the subject's Achilles tendon. The specimens will not be kept or stored. The blood will be analyzed on the same day as the procedure is being performed. This will not require storing of the specimen and prevent erroneous labeling of platelet concentration with a different subject.

After the injections, the subject will rest for 5 minutes. Participants will be given acetaminophen for "as-needed" analgesia and will be telephoned after 3 days to inquire about side effects or adverse events. Subjects will be placed in a boot for two weeks with gradual return to activity. Subjects will also be provided crutches to be non-weight bearing for 24 hours.

Data and Safety Monitoring Plan The data and safety monitoring plan to be implemented in this study consists, in part, of a monthly staff meeting to discuss subject enrollment, safety, and retention. These meetings are intended to monitor participant study flow from initial eligibility assessment to study completion. Standing agenda items for these meetings will be side effects, adverse events and participant retention.

Unanticipated adverse events and complications will be evaluated and treated if necessary by the Principal Investigator and the primary Co-Investigator.

In addition, the following processes will help ensure the timely detection, evaluation and treatment:

1. The Principal Investigator and the primary Co-Investigator will screen subjects for adverse events prior to treatment with PRP. Standardized forms will be used for monitoring and reporting of adverse events. The PI will be immediately available to staff via cell phone in case of a serious adverse event. The PI will immediately report serious adverse events to the UW Research Subjects Advocate using standardized forms. Reports will be made using the subject identification number without other identifying information.

2. Autologous injection of PRP has been found to be safe. The system being used was chosen for its closed system to prevent contamination and for its ease of use. Although safe, internal monitoring of PRP injection safety will also be performed. The study coordinator will assess each PRP injection subject 3 days after treatment with the following question during a brief telephone interview: "Do you think that you have had any side effects from the injection you've received?" [If "Yes"] "Please tell me more about that." Information regarding side effects and adverse events will be made available to the PI, who will decide if the subject requires further medical care.

Investigators do not expect serious adverse events (SAEs) but are well equipped to manage them. Investigators have not seen significant adverse events in combined (UW Radiology and Sports Medicine) clinic use of PRP. Subjects with reactions to acetaminophen or injections have the option to call study personnel at any time. The PI and the primary Co-Investigator will share on-call duty for subjects with adverse events through a pager on a 24/7 basis. Subjects who require significant evaluation and care will be referred to the UW Hospital Emergency Department.

Adverse events from a diagnostic ultrasound are extremely unlikely because ultrasound is considered to have non-significant risk by the FDA. All study procedures will be monitored and documented, and in the unlikely situation where an adverse event occurs, it will be followed to resolution.

The PI(a Board-Certified radiologist) will assess whether the findings should be reported to subjects. Findings that would be reported are those considered clinically relevant. Findings that are considered normal variants (eg. variant anatomy) or clinically insignificant (eg. simple hepatic cyst) will not be reported. Clinically relevant findings will be reported to the subject within 24 hours of the scan, and will also be reported to the subject's physician according to whether the subject has indicated a desire for this in the consent form. ;


Study Design


Related Conditions & MeSH terms


NCT number NCT01911650
Study type Interventional
Source University of Wisconsin, Madison
Contact
Status Completed
Phase N/A
Start date June 2013
Completion date January 10, 2019

See also
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Completed NCT02757664 - Clinical Trial to Evaluate the Adjuvant Effect of Shock Wave Therapy in the Insertional Achilles Tendinopathy N/A
Not yet recruiting NCT03300531 - Impact of Autologous Pure Platelet-rich Plasma in the Treatment of Tendon Disease Phase 2