Publication

• Title: Efficacy and safety of minocycline in patients with acute ischaemic stroke (EMPHASIS): a multicentre, double-blind, randomised controlled trial
• Acronym: EMPHASIS
• Year: 2026
• Journal published in: The Lancet
• Citation: Lu Y, Guan L, Wu J, Zhang M, Huang R, Li J, et al; EMPHASIS investigators. Efficacy and safety of minocycline in patients with acute ischaemic stroke (EMPHASIS): a multicentre, double-blind, randomised controlled trial. Lancet. 2026 Jan 30:S0140-6736(25)01862-8.

Context & Rationale

• Background

  • Even in the reperfusion era, a large proportion of patients with acute ischaemic stroke (AIS) remain disabled; adjunctive strategies targeting secondary injury pathways remain a major unmet need.
  • Post-ischaemic injury evolves over hours–days via neuroimmune activation, matrix metalloproteinase (MMP) activity, blood–brain barrier dysfunction, oedema, and secondary neuronal/glial injury.
  • Minocycline is a lipophilic tetracycline with pleiotropic anti-inflammatory and MMP-inhibitory actions; early human studies and meta-analyses suggested possible functional benefit, but evidence was limited by small sample sizes and heterogeneous designs.
• Research Question/Hypothesis

  • In adults with imaging-confirmed AIS treated within 72 hours of onset, does a 4.5-day course of enteral minocycline improve 90-day functional outcomes compared with placebo, without excess intracranial haemorrhage or other serious harms?
• Why This Matters

  • Minocycline is inexpensive, widely available, and potentially scalable in health systems with limited access to reperfusion therapies.
  • A positive signal in a late window (hours–days) would support “cerebro-/cytoprotection” approaches targeting glia/vasculature and subacute injury biology, rather than hyperacute neuronal salvage alone.

Design & Methods

• Research Question: Among adults with AIS within 72 hours, does minocycline plus routine care increase the proportion achieving mRS 0–1 at 90 days versus placebo plus routine care?
• Study Type: Multicentre, double-blind, randomised, placebo-controlled, parallel-group trial (58 hospitals in China); investigator-initiated; no interim efficacy analyses.
• Population:
  • Setting: In-hospital acute stroke care across 58 centres.
  • Key inclusion: age 18–80 years; imaging-confirmed AIS; randomisation ≤72 h from onset; NIHSS 4–25 and NIHSS 1a ≤1; first-ever stroke or pre-stroke mRS ≤1.
  • Key exclusions: tetracycline allergy; pregnancy/breastfeeding; severe renal or hepatic insufficiency; active bacterial infection; bleeding tendency or recent surgery; other protocol-defined exclusions.
• Intervention:
  • Study drug: minocycline 200 mg loading dose orally within 30 min of randomisation, then 100 mg every 12 h for 4 days (total treatment duration 4.5 days); administration via feeding tube if dysphagic.
  • Co-interventions: routine AIS management permitted, including intravenous thrombolysis and/or thrombectomy if clinically indicated.
  • Key prohibited co-interventions: other tetracyclines; edaravone–dexborneol; selected anti-inflammatory/immune-modulating therapies (eg, colchicine, tocilizumab, immunosuppressants); systemic retinoids (vitamin A derivatives).
• Comparison:
  • Study drug: matching placebo capsules on the same schedule (200 mg loading-equivalent then 100 mg-equivalent every 12 h for 4 days).
  • Background care: routine AIS management as above, with the same protocol-defined prohibited co-interventions.
• Blinding: Double-blind (participants, clinical teams, investigators, and outcome assessors); identical-appearing study drug; 90-day mRS adjudicated by an independent blinded panel.
• Statistics: A total of 1672 patients were required to detect an 8% absolute increase in mRS 0–1 at 90 days (from 60% to 68%) with 90% power at a two-sided 5% significance level, allowing for 10% loss to follow-up; primary analysis in a modified intention-to-treat population (randomised and received ≥1 dose) with complete-case analysis for the primary endpoint; prespecified sensitivity analyses included multiple imputation and worst-case imputation for missing primary outcomes.
• Follow-Up Period: 90 ± 7 days (with additional assessments at 24 h and day 6 or discharge).

Key Results

This trial was not stopped early. No interim efficacy analyses were performed.

Outcome	Minocycline	Placebo	Effect	p value / 95% CI	Notes
mRS 0–1 at 90 days (primary)	447/850 (52.6%)	403/851 (47.4%)	RR 1.11	95% CI 1.03–1.20; p=0.0061	Complete-case mITT (mRS missing: 12 vs 11)
Ordinal mRS shift at 90 days	0: 22.9%; 1: 29.6%; 2: 19.8%; 3: 16.5%; 4: 6.8%; 5: 2.7%; 6: 1.6%	0: 20.6%; 1: 26.8%; 2: 20.4%; 3: 20.9%; 4: 6.0%; 5: 2.9%; 6: 2.4%	cOR 1.19	95% CI 1.03–1.38; p=0.018	cOR >1 indicates shift towards better (lower) mRS
mRS 0–2 at 90 days	615/850 (72.4%)	577/851 (67.8%)	RR 1.07	95% CI 1.02–1.12; p=0.0056	Complete-case mITT
mRS 0–3 at 90 days	755/850 (88.8%)	755/851 (88.7%)	RR 1.00	95% CI 0.97–1.03; p=0.94	Complete-case mITT
NIHSS change baseline → 24 h	0 (0 to 0)	0 (0 to 0)	β −0.07	95% CI −0.20 to 0.06; p=0.32	NIHSS missing: 15 vs 8
NIHSS change baseline → day 6	−2 (−3 to 0)	−1 (−3 to 0)	β −0.28	95% CI −0.50 to −0.05; p=0.015	NIHSS missing: 21 vs 18
Early neurological deterioration at 24 h	52/848 (6.1%)	54/850 (6.3%)	RR 0.97	95% CI 0.64–1.47; p=0.89	Defined by NIHSS worsening; missing: 14 vs 12
Early neurological deterioration at day 6	56/842 (6.7%)	66/840 (7.9%)	RR 0.85	95% CI 0.59–1.21; p=0.36	Missing: 20 vs 22
hs-CRP change baseline → day 6 (mg/L)	0 (−1.20 to 1.97)	0.20 (−0.94 to 3.73)	β −2.72	95% CI −5.64 to 0.19; p=0.067	hs-CRP missing: 172 vs 184
Stroke recurrence at 90 days	51/862 (5.9%)	47/862 (5.5%)	HR 1.09	95% CI 0.73–1.62; p=0.68	Time-to-event analysis; safety population
Composite vascular events at 90 days	59/862 (6.8%)	52/862 (6.0%)	HR 1.14	95% CI 0.79–1.65; p=0.49	Composite endpoint; safety population
Symptomatic intracranial haemorrhage at day 6	3/859 (0.3%)	0/861 (0%)	Not reported	Not reported	Heidelberg-based definition; rare events
Any bleeding event at 90 days	63/862 (7.3%)	69/862 (8.0%)	HR 0.90	95% CI 0.64–1.27; p=0.56	Safety population
All-cause death at 90 days	14/862 (1.6%)	20/862 (2.3%)	HR 0.69	95% CI 0.35–1.36; p=0.28	Safety population
Serious adverse events (during trial follow-up)	40/862 (4.6%)	51/862 (5.9%)	Not reported	p=0.24	Effect estimate not reported; trial not powered for rare harms

• Minocycline increased the proportion of patients achieving functional independence (mRS 0–1) at 90 days (52.6% vs 47.4%; RR 1.11; 95% CI 1.03–1.20; p=0.0061) and favoured an ordinal mRS shift (cOR 1.19; 95% CI 1.03–1.38; p=0.018).
• Early neurological recovery signals were modest and temporally delayed (NIHSS improvement at day 6 but not at 24 h), and inflammatory marker reduction (hs-CRP) did not reach conventional statistical significance.
• Major safety outcomes were broadly similar between groups (bleeding, mortality), with very low rates of symptomatic intracranial haemorrhage.

Internal Validity

• Randomisation and Allocation: Centralised computer-generated randomisation stratified by study site with a fixed block size of four; allocation implemented via unique drug bottle numbers.
• Drop out or exclusions: 90-day mRS available for 850/862 (98.6%) in the minocycline group and 851/862 (98.7%) in the placebo group; 23/1724 (1.3%) did not complete 90-day follow-up (4 withdrew consent; 19 lost to follow-up).
• Post-randomisation exclusions: Per-protocol analysis excluded 48/862 (5.6%) vs 50/862 (5.8%) for major protocol deviations; primary analysis was a complete-case approach within a modified intention-to-treat population.
• Performance/Detection Bias: Double-blind design; 90-day mRS adjudicated by an independent blinded panel; many secondary outcomes were objective (NIHSS, clinical events).
• Protocol Adherence: All randomised participants received at least one dose; treatment discontinuation 12 vs 13; prohibited concomitant medication exposure 16 vs 13.
• Baseline Characteristics: Median age 65.0 (57.0–72.0) vs 65.0 (57.0–71.0); baseline NIHSS 5.0 (4.0–7.0) in both groups; pre-stroke mRS 0 in 739/862 (85.7%) vs 744/862 (86.3%).
• Heterogeneity: 58-centre design; primary models adjusted for pooled study centre (mixed-effects); directionally similar estimates were reported in sensitivity analyses.
• Timing: Median onset-to-treatment time 41.9 h (26.1–52.8) vs 40.5 h (26.5–52.0) (missing for 96 vs 95); treatment initiated ≤24 h in 179/862 (20.8%) vs 175/862 (20.3%), >24–48 h in 375/862 (43.5%) vs 396/862 (45.9%), and >48–72 h in 308/862 (35.7%) vs 291/862 (33.8%).
• Dose: Loading 200 mg within 30 min of randomisation followed by 100 mg every 12 h for 4 days (enteral route; feeding tube permitted).
• Separation of the Variable of Interest: Reperfusion therapy use 114/862 (13.2%) vs 130/862 (15.1%); major protocol deviations similar (48 vs 50) and treatment discontinuation similar (12 vs 13).
• Outcome Assessment: NIHSS missing at 24 h for 15 vs 8 and at day 6 for 21 vs 18; hs-CRP at day 6 missing for 172 vs 184.
• Statistical Rigor: Achieved enrolment exceeded target (1724 vs 1672); no interim efficacy analyses; prespecified missing-data sensitivity analyses reported (multiple imputation; worst-case imputation).

Conclusion on Internal Validity: Overall, internal validity appears moderate to strong, supported by robust blinding, balanced baseline characteristics, high follow-up completeness, and prespecified analyses; the principal vulnerabilities relate to the complete-case approach for the primary endpoint and the modest event rates for safety outcomes.

External Validity

• Population Representativeness: Adults aged 18–80 with predominantly mild-to-moderate AIS (median NIHSS 5) and pre-stroke independence; conducted exclusively in China.
• Applicability: Enteral minocycline is inexpensive and logistically simple, potentially attractive in systems without ready access to reperfusion; applicability to very severe stroke (NIHSS >25), very minor stroke (NIHSS <4), older patients (>80), and different ethnic/genetic backgrounds remains uncertain.
• Practice Context: Low use of reperfusion therapies (13–15%) suggests findings primarily reflect outcomes in patients not receiving thrombolysis/thrombectomy; translation to high-thrombectomy populations is not established.

Conclusion on External Validity: Generalisability is moderate for patients resembling the enrolled cohort (mild–moderate AIS, largely non-reperfused, age ≤80), but is limited for very severe/minor strokes, older populations, and non-Chinese health systems and case-mix.

Strengths & Limitations

• Strengths: Large multicentre sample (n=1724); double-blind, placebo-controlled design; prespecified statistical plan and sensitivity analyses; high 90-day outcome completeness; central blinded adjudication of mRS; pragmatic background care with reperfusion therapies permitted.
• Limitations: Single-country population and age cap at 80 years; predominantly mild-to-moderate strokes (median NIHSS 5) with low reperfusion rates; primary endpoint analysed as complete-case; substantial missingness for some biomarkers (hs-CRP) and secondary outcomes were not consistently positive (eg, mRS 0–3, vascular events); quality-of-life endpoint (EQ-5D) was prespecified but not reported.

Interpretation & Why It Matters

• Clinical signal

  • Enteral minocycline was associated with a statistically significant improvement in 90-day functional outcome (mRS 0–1 and ordinal shift), with broadly similar safety event rates.
  • The magnitude and pattern (delayed NIHSS improvement) is compatible with an anti-inflammatory/vasculoprotective mechanism rather than immediate reperfusion-like salvage.
• Implementation considerations

  • Oral/enteral administration and 72-hour enrolment window increase practical feasibility, but also mean results apply to a late-treated population.
  • In critically ill or dysphagic patients, enteral absorption and drug delivery logistics may differ; intravenous formulations (tested in earlier studies) may be relevant for future protocols.
• Position within acute stroke care

  • Findings support renewed evaluation of adjunct “cerebro-/cytoprotection” alongside reperfusion and best medical therapy.
  • Replication and mechanistic validation (biomarkers/imaging) are key before routine adoption.

Controversies & Other Evidence

• Randomisation and missing-data sensitivity: Fixed block randomisation can increase predictability at the site level; the primary analysis excluded 23 randomised participants with missing 90-day mRS (complete-case), and sensitivity analyses highlighted dependence on missing-data assumptions.¹
• Mechanism and outcome coherence: The observed 90-day functional benefit was accompanied by modest early neurological changes and no clearly significant reduction in hs-CRP, raising questions about the most relevant biological pathway and the optimal biomarkers for effect confirmation.¹
• Late treatment window as a “cerebro-/cytoprotection” test case: EMPHASIS deliberately targeted a subacute therapeutic window (≤72 h) consistent with delayed neuroimmune and vascular injury biology; this frames minocycline as a potential cerebroprotective adjunct rather than classic hyperacute neuroprotection.²³
• Prior evidence base: Earlier small trials and meta-analyses suggested possible benefit but were limited by sample size, design heterogeneity, and imprecision; EMPHASIS provides the largest blinded, placebo-controlled dataset to date, but the effect size and generalisability warrant independent confirmation.⁴
• Guideline position: Major contemporary AIS guidelines focus on reperfusion, physiological optimisation, and complication prevention; they do not yet provide an implementation pathway for routine minocycline neuro-/cerebroprotection in AIS care.⁵

Summary

• EMPHASIS randomised 1724 adults with imaging-confirmed AIS within 72 h (median NIHSS 5) to enteral minocycline vs placebo for 4.5 days.
• Primary outcome favoured minocycline: mRS 0–1 at 90 days 52.6% (447/850) vs 47.4% (403/851); RR 1.11; 95% CI 1.03–1.20; p=0.0061.
• Ordinal functional recovery also favoured minocycline (cOR 1.19; 95% CI 1.03–1.38; p=0.018), but broader disability-free survival thresholds (mRS 0–3) and vascular events were unchanged.
• Safety outcomes were broadly similar, with very low symptomatic intracranial haemorrhage and no statistically significant differences in bleeding or mortality.
• The trial supports late-window cerebro-/cytoprotection as a plausible strategy, but replication and mechanistic corroboration are needed before routine adoption.

Further Reading

Other Trials

• 2007Lampl Y, Boaz M, Gilad R, et al. Minocycline treatment in acute stroke: an open-label, evaluator-blinded study. Neurology. 2007;69:1404–1410.
• 2012Padma Srivastava MV, Bhasin A, Bhatia R, et al. Efficacy of minocycline in acute ischemic stroke: a single-blinded, placebo-controlled trial. Neurol India. 2012;60:23–28.
• 2013Kohler E, Prentice DA, Bates TR, et al. Intravenous minocycline in acute stroke: a randomized, controlled pilot study and meta-analysis. Stroke. 2013;44:2493–2499.
• 2015Amiri-Nikpour MR, Nazarbaghi S, Hamdi-Holasou M, Rezaei Y. An open-label evaluator-blinded clinical study of minocycline neuroprotection in ischemic stroke: gender-dependent effect. Acta Neurol Scand. 2015;131:45–50.
• 2017Shamsaei G, Mohammadi P. Effect of oral minocycline on clinical recovery process in patients with acute ischemic stroke: a randomized clinical trial. Jundishapur J Nat Pharm Prod. 2017;12(3):e63792.

Systematic Review & Meta Analysis

• 2018Malhotra K, Chang JJ, Khunger A, et al. Minocycline for acute stroke treatment: a systematic review and meta-analysis of randomized clinical trials. J Neurol. 2018;265:1871–1879.
• 2018Sheng Z, Liu Y, Li H, et al. Efficacy of minocycline in acute ischemic stroke: a systematic review and meta-analysis of rodent and clinical studies. Front Neurol. 2018;9:1103.
• 2019Singh R, Augustin SJ, Jane M, Cheong JMY, Haur LS, Choo TB. Does minocycline improve recovery after acute ischemic stroke? J Stroke Med. 2019;2:40–46.
• 2020Naderi Y, Sabetghadam S, Naderi A, et al. Neuroprotective effects of minocycline on focal cerebral ischemia injury: a systematic review and meta-analysis. Neural Regen Res. 2020;15:1524–1531.
• 2020Ortiz JF, Ruxmohan S, Saxena A, et al. Minocycline and magnesium as neuroprotective agents for ischemic stroke: a systematic review. Cureus. 2020;12:e12339.

Observational Studies

• 2023Bani-Sadr A, et al. Blood–brain barrier permeability and kinetics of circulating inflammatory markers after ischemic stroke. Neurology. 2023; published online.
• 2024Huang JA, et al. Matrix metalloproteinase-9 upregulation may predict hemorrhagic transformation after endovascular thrombectomy. Front Neurol. 2024;15:1400270.
• 2016Li J, Zhao X, Meng X, et al. High-sensitivity C-reactive protein predicts recurrent stroke and poor functional outcome in patients with minor stroke or transient ischaemic attack. Stroke. 2016;47:2025–2031.
• 2015von Kummer R, Broderick JP, Campbell BC, et al. The Heidelberg Bleeding Classification: classification of bleeding events after ischemic stroke and reperfusion therapy. Stroke. 2015;46:2981–2986.
• 2026Wang F, et al. Blood–brain barrier permeability dynamics after acute ischaemic stroke and association with haemorrhagic transformation. J Am Heart Assoc. 2026; published online.

Guidelines

• 2026Prabhakaran S, Gonzalez NR, et al. 2026 Guideline for the Early Management of Patients With Acute Ischemic Stroke: a guideline from the American Heart Association/American Stroke Association. Stroke. 2026 Jan 26. Online ahead of print.
• 2024Meschia JF, et al. 2024 Guideline for the Primary Prevention of Stroke: a guideline from the American Heart Association/American Stroke Association. Stroke. 2024; published online.
• 2018Powers WJ, Rabinstein AA, Ackerson T, et al. 2018 Guidelines for the Early Management of Patients With Acute Ischemic Stroke. Stroke. 2018;49:e46–e110.
• 2021Kleindorfer DO, Towfighi A, Chaturvedi S, et al. 2021 Guideline for the Prevention of Stroke in Patients With Stroke and Transient Ischemic Attack. Stroke. 2021;52:e364–e467.
• 2021Lyden PD, et al. Cerebroprotection for acute ischaemic stroke: looking ahead. Stroke. 2021; published online.

Notes

• Minocycline is an antibiotic; if used off-label for cerebroprotection, antimicrobial stewardship considerations and monitoring for tetracycline-class adverse effects are relevant alongside stroke-specific safety surveillance.

Overall Takeaway

EMPHASIS is the largest blinded, placebo-controlled evaluation of minocycline for AIS to date and reports a statistically significant improvement in 90-day functional outcomes with broadly similar safety event rates. Its late enrolment window (≤72 h) tests a cerebro-/cytoprotection paradigm aligned with subacute neuroimmune and vascular injury biology. While promising for a low-cost, scalable adjunct, the modest effect size, reliance on complete-case primary analysis, and single-country setting mean replication and mechanistic corroboration are required before routine adoption.

Bibliography

• 1Hill MD. Continued hope for late neuroprotection with minocycline. Lancet. 2026 Jan 30;S0140-6736(26)00047-4.
• 2Lu Y, Guan L, Zhang M, et al. Rationale and study design to assess the efficacy and safety of minocycline in patients with moderate to severe acute ischaemic stroke (EMPHASIS). Stroke Vasc Neurol. 2025; published online March 26.
• 3Lyden P. Back Again to the Future: A New Era for Cerebroprotection. Ann Neurol. 2025 Sep 26. Online ahead of print.
• 4Malhotra K, Chang JJ, Khunger A, et al. Minocycline for acute stroke treatment: a systematic review and meta-analysis of randomized clinical trials. J Neurol. 2018;265:1871–1879.
• 5Prabhakaran S, Gonzalez NR, et al. 2026 Guideline for the Early Management of Patients With Acute Ischemic Stroke: a guideline from the American Heart Association/American Stroke Association. Stroke. 2026 Jan 26. Online ahead of print.