Effects of Transcranial Direct Current Stimulation (tDCS) Plus Language Therapy for Naming in Subacute Left Hemisphere Stroke

Johns Hopkins University1 site in 1 country58 target enrollmentJune 15, 2016

ConditionsStroke

Overview

Phase: Not Applicable
Intervention: Not specified
Conditions: Stroke
Sponsor: Johns Hopkins University
Enrollment: 58
Locations: 1
Primary Endpoint: Change in Accuracy of Naming Untrained Pictures (Philadelphia Naming Test (PNT)) Pre-treatment to 1 Week Post-treatment
Status: Completed
Last Updated: 3 years ago

Overview Investigators Eligibility Criteria Outcomes Sites Similar Trials

Overview

Brief Summary

The investigators will study the effects of transcranial direct current (tDCS) stimulation during language therapy for naming in individuals with aphasia in the acute and subacute post stroke period. Naming difficulties are a persistent and common symptom in aphasia after left-hemisphere (LH) stroke. Behavioral therapy (speech and language therapy; SALT) is the mainstay treatment for post stroke aphasia. Transcranial direct cortical stimulation (tDCS) is a promising adjunct to traditional SALT. tDCS is a safe, non-invasive, non-painful electrical stimulation of the brain which modulates cortical excitability by application of weak electrical currents in the form of direct current brain polarization. It is usually administered via saline-soaked surface sponge electrodes attached to the scalp and connected to a direct current stimulator with low intensities. Most studies are conducted in the chronic phase after stroke. Because neuroplasticity is greatest early after stroke, there is reason to believe tDCS might be most effective in the acute-subacute period. However, only two studies have evaluated tDCS paired with language therapy in group studies of acute to subacute aphasic stroke patients and only one of these was sham-controlled. Furthermore, no studies (of which we are aware) have combined tDCS with therapy to facilitate naming in post stroke aphasia, as shown to be effective in studies of chronic stroke. In this study, the investigators will evaluate whether tDCS combined with SALT improves naming in individuals with aphasia in the acute and subacute post stroke period, more than SALT alone in a randomized, double-blind, sham-controlled trial. The investigators will test the hypothesis that anodal tDCS (A-tDCS) over a targeted region and computer-delivered SALT is associated with greater gains in accuracy in naming pictures, compared to sham combined with the same computer-delivered SALT in post stroke aphasia.

Detailed Description

After informed consent is received, a neurological examination will be performed and multiple screening assessments will be conducted including a tDCS and MRI safety screening. If the participant passes the initial screening portion, speech and language diagnostic testing will be conducted during the same visit (Visit 1). During the next visit (Visit 2), participants will undergo a second baseline assessment of naming ability and assessment of connected speech. On that visit, participants who have no contraindication for MRI (and agree to have MRI) will be randomized to (1) functional magnetic resonance (fMRI) electrode placement or (2) structural electrode placement. All participants who have no contraindication will have structural and resting state functional connectivity MRI (rsfcMRI). Those randomized to fMRI electrode placement will also participate in the naming paradigm during the MRI. The third visit will include electrode positioning and tDCS treatment administration. Participants will receive 15 sessions (Visits 3-17) of tDCS + SALT administration. At the beginning of Visit 3, eligible participants will be randomized to receive either A-tDCS (1 milli amp (mA)) or sham-tDCS (placebo) for 15 sessions (20-minutes per each 45-minute behavioral treatment session) over the course of three weeks. A computer-delivered naming treatment will be coupled with the stimulation. The computer-delivered treatment task will be 45-minutes in total length, so that it will commence at the same time as the tDCS administration and continue for another 25-minutes after the tDCS has ceased. To assess cardiovascular arousal, blood pressure and heart rate will be measured before and after each session. Additionally, discomfort ratings will be recorded following the end of each session using the Wong-Baker FACES Pain Rating Scale and a weekly neurological exam will be administered by a neurologist. Neither the participant nor the clinician monitoring and setting up the treatment will have knowledge of the treatment condition (A-tDCS versus sham). Utilizing a computerized picture naming assessment, all participants will be assessed at several different time points throughout the experiment: twice immediately before and twice the week immediately following the fifteenth and final treatment session; twice at five weeks follow-up after the end of treatment; and twice at 20 weeks after the end of treatment. Participants who agree to participate in the MRI portion of the study (and have none of the additional exclusion criteria for MRI) will have structural and rsfcMRI at Visit 2, following the 15th treatment session (Week 1 after the end of treatment), and at 5 weeks after the end of treatment.

Registry

clinicaltrials.gov

Start Date

June 15, 2016

End Date

April 1, 2022

Last Updated

3 years ago

Study Type

Interventional

Study Design

Parallel

Sex

All

Investigators

Sponsor

Johns Hopkins University

Responsible Party

Sponsor

Eligibility Criteria

Inclusion Criteria

•Participant Inclusion Criteria
•Participants must satisfy the following inclusion criteria to be considered eligible for entry into this study:
•Participants must have sustained an acute ischemic left hemisphere stroke.
•Participants must be fluent speakers of English by self-report.
•Participants must be capable of giving informed consent or indicating another to provide informed consent.
•Participants must be age 18 or older.
•Participants must be premorbidly right handed.
•Participants must be within 3 months of onset of stroke.
•Participants must have an aphasia diagnosis as confirmed by the Western Aphasia Battery-Revised.
•Participants must achieve at least 65% accuracy on screening task (comparable to treatment task) on 1 of 3 attempts

Exclusion Criteria

•Participant Exclusion Criteria
•Participants with any of the following characteristics will not be eligible for entry into this study:
•Previous neurological or psychiatric disease, including previous symptomatic stroke.
•Seizures during the previous 12 months.
•Uncorrected visual loss or hearing loss by self-report.
•Use of medications that lower the seizure threshold (e.g., methylphenidate, amphetamine salts).
•Use of N-methyl-D-aspartate (NMDA) antagonists (e.g., memantine).
•History of brain surgery or any metal in the head.
•Scalp sensitivity (per participant report).

Outcomes

Primary Outcomes

Change in Accuracy of Naming Untrained Pictures (Philadelphia Naming Test (PNT)) Pre-treatment to 1 Week Post-treatment

Time Frame: 2 consecutive days immediately before treatment and 2 consecutive days within 1 week after the end of treatment

The purpose of this measure was to determine whether A-tDCS coupled with SALT will improve naming performance of participants with post stroke aphasia more effectively than SALT alone (i.e., the sham condition). The PNT is a 175-item picture naming test where a person earns one point per each correct answer. Scores range from 0-175 with higher scores associated with better performance. The outcome measure was the difference between the average of administrations on two consecutive days immediately before treatment and administrations on two consecutive days within 1 week after the end of treatment.

Secondary Outcomes

Change in Efficiency of Picture Description Pre-treatment to 1 Week Post-treatment(Immediately before and within 1 week after treatment)
Change in Stroke Impact Scale (SIS) Pre-treatment to 5 Weeks Post-treatment(Immediately before and 5 weeks after treatment)
Change in Content of Picture Description Pre-treatment to 20-weeks Post-treatment(Immediately before and at 20 weeks after treatment)
Change in Accuracy of Naming Untrained Pictures (Philadelphia Naming Test) Pre-treatment to 5-weeks Post-treatment(The PNT will be administered at baseline and at 5 weeks post treatment.)
Change in Content of Picture Description Pre-treatment to 1 Week Post-treatment(Immediately before and within 1 week after treatment)
Change in Efficiency of Picture Description Pre-treatment to 5 Weeks Post-treatment(Immediately before and at 5 weeks after treatment)
Change in Stroke Impact Scale (SIS) Pre-treatment to Post-treatment(Immediately before and within 1 week after treatment)
Change in Accuracy of Naming Untrained Pictures (Philadelphia Naming Test) Pre-treatment to 20-weeks Post-treatment(The PNT will be administered at baseline and at 20 weeks post treatment.)
Change in Content of Picture Description Pre-treatment to 5 Weeks Post-treatment(Immediately before and at 5 weeks after treatment)
Change in the Efficiency of Picture Description Pre-treatment to 20 Weeks Post-treatment(Immediately before and at 20 weeks after treatment)
Change in Stroke Impact Scale (SIS) Pre-treatment to 20 Weeks Post-treatment(Immediately before and 20 weeks after treatment)