| Literature DB >> 34050123 |
Jeffrey D Voigt1, Andrew F Leuchter2, Linda L Carpenter3.
Abstract
Patients with major depressive disorder (MDD) may be refractory to or have contraindications that preclude treatment with antidepressant pharmacotherapies. Alternative therapies such as repetitive transcranial magnetic stimulation (rTMS) continue to evolve, and include theta burst stimulation (TBS), which has advantages over conventional rTMS. The aim of this study was to identify and meta-analyze efficacy data from all randomized controlled trials (RCTs) investigating TBS as a treatment for MDD. Published reports of RCTs (January 1, 2010 to October 23, 2020) were identified via systematic searches in computerized databases, followed by review of individual reports for inclusion. Inclusion criteria included primary diagnosis of MDD ≥ 1 week duration of therapy with ≥10 sessions, and treatment with any form of TBS. The Cochrane GRADE methodology and PRISMA criteria were used for evaluation of individual trials. Data from ten RCTs were included, representing 667 patients. Of these, 8 RCTs compared TBS to sham treatment and one compared TBS to standard rTMS (i.e., high frequency stimulation over left dorsolateral prefrontal cortex [HFL]). Quality of evidence assessment yielded high confidence in the finding of TBS being superior to sham on response measured by the Hamilton Depression Rating Scale (HRSD) (RR = 2.4; 95% CI: 1.27 to 4.55; P = 0.007; I2 = 40%). Comparison of HRSD response rates for TBS versus rTMS produced no statistically significant difference (RR = 1.02; 95% CI: 0.85 to 1.23; P = 0.80; I2 = 0%). The incidence of adverse events between TBS and rTMS was not statistically different. The findings of a positive effect of TBS vs. sham, and noninferiority of TBS vs. standard HFL rTMS support the continued development of TBS to treat depression.Entities:
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Year: 2021 PMID: 34050123 PMCID: PMC8163818 DOI: 10.1038/s41398-021-01441-4
Source DB: PubMed Journal: Transl Psychiatry ISSN: 2158-3188 Impact factor: 6.222
Fig. 1PRISMA flow diagram.
Systematic review process for identification of studies included in the analysis.
studies used in meta-analysis.
| Study | Treatment comparison | Treatment duration | Primary outcome evaluated | Included in Meta-Analysis for these outcomes |
|---|---|---|---|---|
| Blumberger 2018[ | TBS stimulation pattern of triplet 50 Hz bursts, repeated at 5 Hz; 2 s on and 8 s off cycle; TBS total duration for 3 min; 9 s (with 600 stimuli per session) vs.; TMS stimulation pattern of 10 Hz frequency repeated at 4 s on and 26 s off cycling vs.; TMS a total duration of 37.5 min (3000 stimuli per session). Intensity of both at 120% of RMT | 12 weeks | HRSD scores and response (>50% reduction from baseline)/remission (HRSD score <8) | HRSD response TBS vs. TMS. (Fig. HRSD percent change TBS vs. TMS. (Fig. HRSD remission TBS vs. TMS. (Fig. |
| Caeyenberghs 2018[ | TBS stimulation pattern of 50 Hz frequency with a 2 s on 8 s. off cycling. Stimuli were applied at a stimulation intensity of 110% of patient’s RMT. Between 4 daily sessions there was a pause of approximately 15 min each. Each session consisted of 1620 stimuli/session vs.; Sham consisted of a specially designed sham coil identical in form and sound to active coil but did not deliver active stimulation. | 1 week | Percent change in HRSD scores from baseline to 1 week out. | BDI TBS vs. sham. (Fig. |
| Christyakov 2015[ | TBS stimulation pattern of triple-pulse 50 Hz bursts given at a rate of 5 Hz (2 s between each burst cycling and uninterrupted (3,600 stimuli per session) at an intensity of 100% of patient’s RMT vs.; Sham TBS for a period of 10 days (one session per day). Sham consisted of a specially designed coil which produced identical sounds to active but with no stimulus sensation. | 2 weeks | HRSD (21 item) reduction of >50% from baseline (response) | HRSD categorical response TBS vs. sham. (Fig. Adverse events TBS vs. sham. (Fig. |
| Desmyter 2016[ | TBS stimulation pattern of 50 Hz frequency with bursts repeated every 2 s and at an intensity of 110% of patient’s RMT. Resulted in 2 s on and 8 s off cycling. Total of 1,620 stimuli per session. Duration of one week (5 sessions per day for a period of 4 days) vs.; Sham coil looked and sounded exactly the same as active coil but without stimuli. | 1 week | HRSD (17 item) reduction of >50% from baseline (response) | N/A |
| Duprat 2016[ | TBS stimulation pattern of 50 Hz frequency of 54 triplet bursts with a duration of 2 s on and 8 s off cycling. Each session consisted of 1,620 stimulations. Total of 20 TBS sessions spread over 4 days (5 sessions per day; between session pause of 15 min). Stimulation intensity of 110% of patient’s RMT vs.; Sham consisted of identical coil to active placed in same position but without active stimulation. | 1 week | HRSD (17 item) reduction of >50% from baseline (response) | HRSD categorical response TBS vs. sham. (Fig. |
| Li 2014[ | Group 1: TBS stimulation pattern of 50 Hz frequency with 120 s continuous uninterrupted bursts; with a total of 1,800 stimuli/session for 10 daily sessions over a period of 2 weeks vs; Group 2: TBS stimulation pattern of 50 Hz frequency with 2 s bursts on and 8 s off cycling. Total of 1,800 stimuli/session with10 daily sessions over a period of 2 weeks. Both Group 1 and Group 2 TBS were delivered an intensity of 80% of patient’s RMT vs.; Group 3: Sham TBS bursts randomly assigned as per either Group 1 or 2 with same 1,800 stimuli/session for 10 daily sessions over a period of 2 weeks. | 2 weeks | HRSD (17 item) reduction of >50% from baseline (response) | HRSD categorical response TBS vs. sham. (Fig. HRSD percent change TBS vs. sham. (Fig. Adverse events TBS vs. sham. (Fig. |
| Li 2020[ | TBS prolonged stimulation pattern of 50 Hz frequency consisting of 1800 stimuli/session: 10 sessions over a 2 week period (1 session per day; 5 sessions per week) vs.; TMS stimulation pattern of 10 Hz frequency consisting of 1600 stimuli/session: 10 sessions over a 2 week period (1 session per day; 5 sessions per week) vs.; Sham [parameters given as prolonged TBS or TMS randomly assigned; using a sham coil]: 10 sessions over a 2 week period (1 session per day; 5 sessions per week). | 2 weeks | Percent change in HRSD-17 scores from baseline to 2 weeks out. | HRSD categorical response TBS vs. sham. (Fig. HRSD response rate TBS vs. TMS. (Fig. HRSD percent change TBS vs. sham. HRSD percent change TBS vs. TMS. (Fig. HRSD remission TBS vs. TMS. (Fig. |
| Mielacher 2019[ | TBS stimulation consisted of 50 Hz frequency daily sessions [consisting of 2×600 stimuli (1200 stimuli/session) over the left DLPFC] vs.; One active TBS/one sham daily (600 stimuli/session) for a period of 15 sessions over a 3 week period. | 3 weeks | Percent change in HRSD-17 scores from baseline to 3 weeks out. | N/A |
| Plewnia 2014[ | TBS stimulation pattern of 50 Hz frequency in bursts given every 2 s on and 8 s off cycling of left sided TBS (cycling applied a total of 20 times) followed by right sided continuous (40 s) TBS for a total of 1200 stimuli/session. Intensity of both was 80% of patient’s RMT vs.; Sham was accompanied by similar auditory (clicking noise) and somatosensory (pricking, twitches of temporal muscle) artifact. Both TBS and sham were administered over 6 weeks and 30 total sessions. | 6 weeks | MADRS reduction of >50% from baseline (response) | HRSD categorical response TBS vs. sham. (Fig. HRSD percent change TBS vs. sham. (Fig. BDI reduction TBS vs. sham. (Fig. Adverse events TBS vs. sham. (Fig. |
| Prasser 2014[ | TMS stimulation consisted of 1 Hz frequency to right DLPFC (1,000 stimuli/session) immediately followed 10 Hz frequency to left DLPFC (1000 stimuli/session). Intensity of TMS performed at 110% of patient’s RMT; TBS stimulation consisted of 50 Hz frequency 1200 pulses/session continuous TBS applied to right DLPFC immediately followed by 1200 stimuli/session of intermittent TBS to left DLPFC. Intensity of TBS performed at 80% of patient’s RMT; sham [consisted of TBS protocol applied with a sham coil] | 3 weeks | HRSD-21 change between baseline and 3 weeks (response >50% change; and score <11 points remission) | HRSD categorical response TBS vs. sham. (Fig. HRSD percent change TBS vs. TMS. (Fig. Adverse events TBS vs. sham. (Fig. |
BDI Beck Depression Inventory, HRSD Hamilton Rating Scale for Depression, RMT Response Motor Threshold, TBS Theta Burst Stimulation, TMS Transcranial Magnetic Stimulation.
Fig. 6HRSD response rate from baseline TBS vs. TMS.
See descriptor in Fig. 5 above.
Fig. 8HRSD percent change TBS vs. TMS.
See descriptor in Fig. 5 above.
Fig. 9HRSD remission TBS vs. TMS.
See descriptor in Fig. 5 above.
Fig. 5HRSD score ≥50% reduction (categorical response) from baseline TBS vs. sham.
Forest plot displaying effect estimates and confidence interveals for both individual studies and overall meta-analysis. Each study is represented by a block at the point estimate of the intervention effect with a horizontal line extending on each side for the confidence interval. The area of the block indicates the weight assigned to that study in the meta-analysis.
Fig. 11Adverse events TBS vs. sham.
See descriptor in Fig. 5 above.
Fig. 7HRSD percent change TBS vs. sham.
See descriptor in Fig. 5 above.
Fig. 10dBDI response from baseline TBS vs. sham.
See descriptor in Fig. 5 above.
Fig. 2Risk of bias graph.
Aggregate evaluation of bias risks for studies included in the analysis.
Fig. 3Risk of bias summary.
Specific biases as identified for each study included in the analysis.
Fig. 4Funnel plot examining publication bias.
Intervention effect estimate from individual studies on HRSD response reduction from baseline measured against each study size.
Outcomes of other instruments assessed in single RCTs.
| Study | Comparison | Instrument/outcome | Finding |
|---|---|---|---|
| Blumberger 2018[ | rTMS vs. TBS | IDS-30; response ≥50% from baseline | TBS non-inferior to HFL rTMS |
| Blumberger 2018[ | rTMS vs. TBS | QIDS-SR; response ≥50% from baseline | TBS non-inferior to HFL rTMS |
| Blumberger 2018[ | rTMS vs. TBS | BSI-A; response ≥50% from baseline | TBS non-inferior to HFL rTMS |
| Blumberger 2018[ | rTMS vs. TBS | IDS-30; remission <14 | TBS non-inferior to HFL rTMS |
| Blumberger 2018[ | rTMS vs. TBS | QIDS-SR; remission <6 | TBS non-inferior to rTMS |
| Desmyter 2014[ | TBS vs. sham | BSI score | |
| Plewnia 2014[ | TBS vs. sham | MARDS ≤ 50% from baseline; response | |
| Mielacher 2019[ | Once vs. twice daily TBS | HRSD percent reduction |
BSI Beck Scale for Suicide Ideation (Beck & Steer 1991), BSI-A Brief Symptom Inventory-Anxiety subscale (BSI; Derogatis & Melisaratos, 1983); IDS-3 Inventory for Depressive Symptomatology, 30-item (Rush et al. 1996); MADRS Montgomery-Åsberg, Depression Rating Scale (Montgomery & Asberg 1979); QIDS-SR = 16 item Quick Inventory of Depressive Symptomatology (Self-Report version) (Rush et al. 2003).