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TNK-PLUS

Intravenous Tenecteplase Prior to Endovascular Treatment for Ischemic Stroke at 4.5 to 24 Hours: The TNK-PLUS Randomized Clinical Trial

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Year of Publication: 2026

Authors: Yunyun Xiong, Fengyuan Che, Hao Wang, ..., Yongjun Wang; for the TNK-PLUS Investigators

Journal: JAMA

Citation: Xiong Y, Che F, Wang H, et al. Intravenous Tenecteplase Prior to Endovascular Treatment for Ischemic Stroke at 4.5 to 24 Hours: The TNK-PLUS Randomized Clinical Trial. JAMA. 2026. doi:10.1001/jama.2026.4292

Link: https://doi.org/10.1001/jama.2026.4292

Clinical Question

In patients with proximal MCA occlusion presenting 4.5–24 hours after stroke onset who have direct access to EVT, does bridging intravenous tenecteplase improve functional outcomes compared to EVT alone?

Bottom Line

Intravenous tenecteplase before endovascular treatment does not improve functional independence at 90 days in patients with proximal MCA occlusion presenting in the 4.5–24-hour window; EVT alone remains the standard of care, and adding tenecteplase may increase bleeding risk.

Major Points

  • Tenecteplase 0.25 mg/kg before EVT did not improve functional independence (mRS 0–2) at 90 days: 44.2% vs 43.2%, adjusted RR 1.01 (95% CI, 0.83–1.24), P = 0.89
  • Risk difference for functional independence was 0.99% (95% CI, −8.84% to 10.83%), confirming no clinically meaningful or statistically significant benefit
  • Symptomatic ICH within 36 hours was numerically higher in the tenecteplase group: 5.1% (10/197) vs 2.6% (5/190)
  • 90-day mortality was numerically lower in the tenecteplase group but not significantly different: 12.7% (25/197) vs 14.2% (27/190)
  • An interim adaptive sample size reestimation showed conditional power of only 0.03 (below the promising zone of 0.33–0.80), confirming futility without requiring sample size expansion
  • Results align with TIMELESS and together indicate that in patients with direct EVT access, adding bridging tenecteplase in the late window provides no additional benefit beyond EVT alone
  • Unlike TRACE-III where thrombolysis benefited patients without EVT access, the availability of EVT appears to negate any incremental benefit of tenecteplase in the late time window

Design

Study Type: Multicenter, prospective, open-label, blinded endpoint (PROBE), phase 3, randomized controlled superiority trial

Randomization: 1

Blinding: Open-label with blinded endpoint assessment; all clinical efficacy and adverse event endpoints evaluated by physicians unaware of treatment allocation; neuroimaging independently adjudicated by central imaging core laboratory

Allocation: 1:1 ratio via centralized web-based system, stratified by LVO site (M1 or M2), block size 4

Enrollment Period: January 25, 2024 – July 21, 2025

Follow-up Duration: 90 days (final follow-up October 14, 2025)

Centers: 40

Countries: China

Sample Size: 391

Analyzed: 391

Analysis: Full analysis set (ITT, all randomly assigned participants) as primary; per-protocol set as secondary (tenecteplase+EVT n=189; EVT alone n=178)

Power Calculation: Estimated conservative effect size of 10% based on TIMELESS and TRACE-III data; minimum sample size 390 (powered for 14% effect), maximum 754 (powered for 10% effect); 2-sided alpha 0.05, power 0.80, anticipated attrition 5%; prespecified interim adaptive sample size reestimation at 273 participants showed conditional power 0.03, outside promising zone (0.33–0.80), so no sample size increase was required

Registration: NCT06221371

Inclusion Criteria

  • Age ≥18 years
  • Acute ischemic stroke with last known well 4.5–24 hours before randomization, including wake-up stroke and unwitnessed onset
  • Pre-stroke mRS score 0–2
  • NIHSS score 6–25
  • Confirmed MCA-M1 or proximal M2 occlusion on CT angiography or MR angiography
  • Ischemic core volume <70 mL (CBF <30% of normal on CT-perfusion or ADC <620×10−6 mm2/s on DWI-MRI)
  • Mismatch ratio (hypoperfused tissue / ischemic core volume) ≥1.8
  • Mismatch volume ≥15 mL (hypoperfused tissue defined as Tmax >6 seconds on CT or MR perfusion)
  • Salvageable brain tissue confirmed on CT-perfusion or MR perfusion-diffusion imaging

Exclusion Criteria

  • No MCA-M1 or proximal M2 occlusion
  • Did not meet target mismatch profile on CTP or MRI with MR perfusion
  • Large infarct on noncontrast CT or MRI (>1/3 MCA territory)
  • Time from onset to randomization <4.5 hours or >24 hours
  • Multiple arterial occlusions
  • Already received thrombolytic therapy at external hospital
  • NIHSS score <6 or >25
  • Chronic occlusion
  • Unable to perform CTP or perfusion-weighted imaging
  • Known coagulation impairment
  • Brain surgery or brain tumor within the last 3 months
  • Active internal bleeding
  • Pre-stroke mRS score >2
  • Declined EVT or intravenous thrombolytic at time of randomization
  • Unlikely to adhere to trial protocol or follow-up

Arms

FieldTenecteplase + EVTControl
N199192
InterventionIntravenous tenecteplase 0.25 mg/kg (maximum dose 25 mg) administered as a single IV bolus over 5–10 seconds immediately after randomization, followed by EVT as soon as possible (stent retriever, aspiration, balloon angioplasty, stent placement, or combination)Endovascular treatment alone without preceding thrombolysis (stent retriever, aspiration, balloon angioplasty, stent placement, or combination)
DurationSingle dose pre-EVT; 90-day follow-up90-day follow-up

Outcomes

OutcomeTypeControlInterventionHR / OR / RRP-value
Functional independence defined as modified Rankin Scale score 0–2 at 90 daysPrimary43.2% (83/192)44.2% (88/199)1.010.89
No disability (mRS ≤1) at 90 days — results not available in source textSecondary
mRS score ≤3 at 90 days — results not available in source textSecondary
Ordinal mRS distribution at 90 days — results not available in source textSecondary
Severe disability or death (mRS 5–6) at 90 days — results not available in source textSecondary
Early neurologic improvement at 72 hours (NIHSS decrease ≥8 points from baseline or NIHSS 0–1) — results not available in source textSecondary
Change in NIHSS score from baseline to day 7 — results not available in source textSecondary
Reperfusion prior to EVT (>50% reperfusion; eTICI 2b50–3) — results not available in source textSecondary
Complete recanalization at 24 hours on CTA or MRA — results not available in source textSecondary
Symptomatic ICH within 36 hours: 5.1% (10/197) tenecteplase+EVT vs 2.6% (5/190) EVT aloneSafety
Death within 90 days: 12.7% (25/197) tenecteplase+EVT vs 14.2% (27/190) EVT aloneSafety
5.1% (10/197)Adverse
2.6% (5/190)Adverse
12.7% (25/197)Adverse
14.2% (27/190)Adverse

Subgroup Analysis

Context from TIMELESS noted in background: patients with M1 occlusion appeared to benefit from tenecteplase, while M2 patients did not in TIMELESS; TNK-PLUS-specific subgroup results by occlusion site (M1 vs proximal M2) are not reported in the available source text.

Criticisms

  • Open-label design may introduce performance bias despite blinded endpoint assessment
  • Conducted exclusively in China at high-volume EVT centers, which may limit generalizability to lower-resource settings or health systems with longer door-to-groin times
  • Interim analysis revealed very low conditional power (0.03), indicating early futility signal; trial continued to minimum prespecified sample size
  • Numerically higher sICH rate in tenecteplase group (5.1% vs 2.6%) raises safety concern not resolvable given the trial was not powered for this endpoint
  • Internal carotid artery and anterior cerebral artery occlusions were excluded, limiting scope; TIMELESS ICA subgroup data suggest ICA occlusion does not benefit anyway
  • Full secondary outcome results not available in the published abstract/early release text

Funding

Unrestricted grant from China Shijiazhuang Pharmaceutical Company Pharmaceutical (Guangzhou), which also manufactured the tenecteplase used in the trial

Based on: TNK-PLUS (JAMA, 2026)

Authors: Yunyun Xiong, Fengyuan Che, Hao Wang, ..., Yongjun Wang; for the TNK-PLUS Investigators

Citation: Xiong Y, Che F, Wang H, et al. Intravenous Tenecteplase Prior to Endovascular Treatment for Ischemic Stroke at 4.5 to 24 Hours: The TNK-PLUS Randomized Clinical Trial. JAMA. 2026. doi:10.1001/jama.2026.4292

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