Publication

• Title: Video Laryngoscopy vs Direct Laryngoscopy on Successful First-Pass Orotracheal Intubation Among ICU Patients: A Randomized Clinical Trial
• Acronym: MACMAN
• Year: 2017
• Journal published in: JAMA
• Citation: Lascarrou JB, Boisrame-Helms J, Bailly A, et al; Clinical Research in Intensive Care and Sepsis (CRICS) Group. Video laryngoscopy vs direct laryngoscopy on successful first-pass orotracheal intubation among ICU patients: a randomized clinical trial. JAMA. 2017;317(5):483-493.

Context & Rationale

• Background

  • Tracheal intubation in the ICU is frequent and physiologically hazardous, with high rates of hypoxaemia, cardiovascular collapse, and cardiac arrest.
  • First-pass success is a plausible, modifiable driver of safety because repeated attempts increase duration of apnoea and airway trauma and may compound haemodynamic instability.
  • Videolaryngoscopy improves glottic visualisation in operating theatres, but effectiveness and safety in ICU intubations were uncertain given different case-mix (hypoxaemia, shock), operator mix, and urgency.
  • Prior ICU data were dominated by observational studies and small trials, with inconsistent signals for first-pass success and limited harms reporting.
• Research Question/Hypothesis

  • In adults requiring ICU orotracheal intubation, does first-attempt use of a Macintosh-blade videolaryngoscope (McGrath MAC) increase successful first-pass intubation compared with standard Macintosh direct laryngoscopy?
  • Hypothesis underpinning sample size: videolaryngoscopy would increase first-pass success from 65% to 80% (15% absolute improvement).
• Why This Matters

  • Routine adoption of videolaryngoscopy in critical care has major implications for procurement, training, and airway algorithms.
  • A neutral or harmful effect would shift emphasis to physiology-first airway bundles and targeted device use (anticipated difficulty, supervision), rather than universal deployment.
  • Clarifying whether improved laryngeal view translates into clinically meaningful first-pass success in ICU patients is essential before extrapolating from theatre evidence.

Design & Methods

• Research Question: In adult ICU patients requiring orotracheal intubation, does first-attempt McGrath MAC videolaryngoscopy (indirect view) improve first-pass success compared with Macintosh direct laryngoscopy?
• Study Type: Multicentre, parallel-group, investigator-initiated, unblinded randomised clinical trial; 7 adult ICUs in France; May 2015 to January 2016.
• Population:
  • Setting: adult ICU patients requiring orotracheal intubation, for any indication.
  • Inclusion: adults (≥18 years) requiring orotracheal intubation in ICU.
  • Key exclusions: pregnancy; contraindication to orotracheal intubation; nasotracheal intubation; fibreoptic intubation planned; no time for inclusion/randomisation; previous study inclusion; protected persons (guardianship/curatorship); persons deprived of liberty; no health insurance; refusal.
  • Operator strata: randomisation stratified by centre and operator status (expert vs non-expert).
  • Expert definition: ≥5 years ICU experience, or ≥1 year ICU experience after ≥2 years of anaesthesiology training.
• Intervention:
  • Device: McGrath MAC videolaryngoscope (Covidien).
  • First-pass technique: indirect view on the screen mandated for the first attempt.
  • Adjuncts on first attempt: no endotracheal tube stylet and no gum elastic bougie.
  • After first-attempt failure: repeat laryngoscopy or alternative airway technique at the operator’s discretion, consistent with local guidelines; subsequent laryngoscopy attempts could use videolaryngoscopy with indirect or direct view.
• Comparison:
  • Device: standard Macintosh direct laryngoscope.
  • Adjuncts on first attempt: no endotracheal tube stylet and no gum elastic bougie.
  • After first-attempt failure: repeat laryngoscopy or alternative airway technique at the operator’s discretion, consistent with local guidelines.
• Blinding: Unblinded (operators and bedside staff); primary endpoint objective (capnography-confirmed), but open-label delivery could influence process measures and some complication reporting.
• Statistics: A total of 370 patients were required to detect a 15% absolute increase in first-pass success (from 65% to 80%) with 90% power (type II error 10%) at a 2-sided 5% significance level; primary analysis was intention-to-treat using a mixed-effects logistic regression model (centre random effect; group and operator status fixed effects); missing primary endpoint counted as failure; secondary outcomes were not adjusted for multiplicity.
• Follow-Up Period: Peri-intubation outcomes during the procedure and up to 1 hour post-intubation; ICU outcomes followed to day 28 (mortality and other follow-up data reported in the supplement).

Key Results

This trial was not stopped early. Recruitment met the planned sample size (371 randomised; target 370); no interim stopping was reported.

Outcome	McGrath MAC videolaryngoscopy	Macintosh direct laryngoscopy	Effect	p value / 95% CI	Notes
Successful first-pass orotracheal intubation (primary; intention-to-treat)	126/186 (67.7%)	130/185 (70.3%)	Absolute difference −2.5%	95% CI −11.9 to 6.9; P=0.60	Success required waveform capnography for ≥4 breaths.
Successful first-pass orotracheal intubation (per-protocol)	126/183 (68.9%)	130/182 (71.4%)	Absolute difference −2.5%	95% CI −12.3 to 6.4; P=0.54	Per-protocol population n=365.
Glottic view: Cormack–Lehane grade I	133/176 (75.6%)	93/177 (52.5%)	Absolute difference 23.1%	95% CI 13.3 to 32.7; P<0.001	Better visualisation with videolaryngoscopy did not translate into higher first-pass success.
Time to successful intubation (min; median [IQR])	3.9 (2.8 to 7.0)	3.8 (2.4 to 6.4)	Median difference 0.0 min	95% CI −0.6 to 0.4; P=0.74	Measured from start of anaesthetic induction to capnography confirmation.
Any life-threatening complication (prespecified composite)	24/180 (13.3%)	17/179 (9.5%)	Absolute difference 3.8%	95% CI −2.7 to 10.4; P=0.25	Composite included severe hypoxaemia, severe cardiovascular collapse, cardiac arrest, and death.
Severe life-threatening complication (post hoc composite)	17/179 (9.5%)	5/179 (2.8%)	Absolute difference 6.7%	95% CI 1.8 to 11.6; P=0.01	Post hoc severity categorisation; no multiplicity adjustment across secondary outcomes.
Day-28 mortality	66/185 (35.7%)	67/184 (36.4%)	Absolute difference −0.7%	95% CI −10.5 to 9.1; P=0.88	Follow-up outcome; trial not powered for mortality.

• Videolaryngoscopy improved glottic view (Cormack–Lehane grade I 75.6% vs 52.5%) but did not improve first-pass success (67.7% vs 70.3%).
• Sensitivity analysis (intention-to-treat) adjusting for MACOCHA >4 showed no difference in first-pass failure (aOR for videolaryngoscopy 1.10; 95% CI 0.69 to 1.75; P=0.69).
• In the per-protocol MACOCHA subgroup analysis, first-pass success remained similar in MACOCHA >4 (64.9% videolaryngoscopy vs 67.7% direct; absolute difference 2.9%; 95% CI −19.6 to 25.4; interaction P=0.55).

Internal Validity

• Randomisation and allocation:
  • Centralised, computer-generated randomisation (software), using permuted blocks of 4 and stratified by centre and operator status (expert vs non-expert).
  • Analytic approach matched the stratified design (mixed-effects logistic regression with centre random effect; group and operator status fixed effects).
• Dropout or exclusions:
  • 371 patients randomised (186 videolaryngoscopy; 185 direct laryngoscopy).
  • Primary endpoint missing in 5 participants; per protocol, these were counted as first-pass failures.
  • Per-protocol analysis included 365 participants (183 videolaryngoscopy; 182 direct laryngoscopy).
• Performance and detection bias:
  • Unblinded intervention and bedside outcome recording introduce potential performance bias (operator behaviour) and detection bias for clinician-judgement outcomes.
  • Primary outcome definition was objective and pre-specified (capnography-confirmed first pass).
  • Many complications were defined using physiologic thresholds (e.g., oxygen saturation and blood pressure), limiting subjectivity; some events (e.g., aspiration, airway trauma) remain susceptible to reporting differences.
• Protocol adherence:
  • Allocated device was used for the first attempt in 183/186 (98.4%) in the videolaryngoscopy group and 182/185 (98.4%) in the direct laryngoscopy group.
  • Induction and preoxygenation were protocol-guided but clinician-selected; key elements were similar between groups (e.g., etomidate 89.1% vs 90.7%; succinylcholine 78.3% vs 75.8%; bag-valve-mask preoxygenation 51.6% vs 52.5%).
  • Mandated technique differences (indirect view for videolaryngoscopy first attempt; no stylet/bougie on first attempt in either group) enhanced between-group separation but may not reflect all contemporary videolaryngoscopy practices.
• Baseline characteristics:
  • Overall severity was high and balanced (SAPS II mean 58.0 vs 57.7; SOFA median 7 vs 7; PaO₂:FiO₂ median 95 vs 91).
  • Indications for intubation were similar (acute respiratory failure 65.6% vs 63.8%; coma 23.1% vs 24.3%).
• Heterogeneity:
  • Seven ICUs with broad indications and variable physiology (shock, hypoxaemia) increase pragmatic relevance but add clinical heterogeneity.
  • Most intubations were performed by non-experts (84.4% vs 83.2%), reflecting typical ICU workforce structures but potentially increasing sensitivity to learning-curve effects.
• Timing:
  • Randomisation occurred at the time of the intubation procedure, with immediate application of allocated device.
  • Time-to-success was defined from the start of anaesthetic induction, not laryngoscope insertion, which may dilute device-related differences in “laryngoscopy time”.
• Separation of the variable of interest:
  • Laryngeal view was substantially better with videolaryngoscopy (Cormack–Lehane grade I 75.6% vs 52.5%; P<0.001).
  • Despite improved view, rescue bougie use after first-attempt failure was more common with videolaryngoscopy (12.0% vs 5.5%; P=0.03), suggesting challenges with tube delivery/catheterisation.
  • Time to successful intubation was similar (median 3.9 vs 3.8 minutes; P=0.74), indicating that improved view did not produce procedural efficiency gains in this setting.
• Outcome assessment:
  • Primary outcome was clearly defined and objectively verified.
  • Complication composites were prespecified, but the “severe life-threatening” composite was post hoc, reducing robustness of inference for that signal.
• Statistical rigor:
  • Planned sample size achieved (371 randomised vs 370 planned).
  • Primary analysis followed intention-to-treat with prespecified handling of missing primary endpoint (counted as failure).
  • Secondary outcomes were not adjusted for multiplicity, so individual secondary P values should be interpreted as exploratory.

Conclusion on Internal Validity: Overall, internal validity appears moderate-to-strong given robust randomisation, minimal attrition, and an objective primary endpoint; however, open-label delivery and extensive, unadjusted secondary comparisons (including a post hoc “severe” composite) limit confidence in some secondary and harm inferences.

External Validity

• Population representativeness:
  • High-severity adult ICU population (SAPS II ~58; PaO₂:FiO₂ ~90–95), broadly reflective of many ICU intubations in high-income systems.
  • Exclusions (e.g., “no time for inclusion/randomisation”, planned fibreoptic/nasotracheal intubation, pregnancy) reduce applicability to crash intubations and selected airway pathologies.
• Applicability:
  • Device-specific (McGrath MAC) and technique-specific (indirect view mandated on first attempt; no stylet/bougie on first attempt), which may not map to current practice in some ICUs that routinely use stylets or different videolaryngoscope designs.
  • Operator-mix (majority non-expert intubators) enhances relevance to training environments; effects may differ where intubations are performed predominantly by airway experts.
  • Centres were in France with guideline-informed practice (e.g., general anaesthesia with hypnotic and neuromuscular blockade); transferability to systems with different drug availability, staffing, and airway pathways is uncertain.

Conclusion on External Validity: External validity is moderate: findings are most generalisable to routine ICU intubations in resourced centres using Macintosh-blade videolaryngoscopy with mixed-experience operators, but extrapolation to crash scenarios, other device designs, or different adjunct strategies is less secure.

Strengths & Limitations

• Strengths:
  • Multicentre, pragmatic ICU trial with broad indications and high illness severity.
  • Central randomisation with stratification by centre and operator status.
  • Objective, clinically relevant primary endpoint (capnography-confirmed first-pass success).
  • High protocol delivery for first attempt (≈98% received allocated device) and minimal missingness for the primary endpoint.
• Limitations:
  • Unblinded design may influence operator behaviour and reporting of some complications.
  • Mandated technique (indirect view on first attempt; no stylet/bougie on first attempt) may not reflect optimised or contemporary videolaryngoscopy practice in all ICUs.
  • Control first-pass success was higher than expected (observed ~70% vs assumed 65%), reducing power to detect smaller benefits than the prespecified 15% absolute increase.
  • Secondary outcomes were not multiplicity-adjusted, and the “severe life-threatening complications” signal was based on a post hoc composite definition.

Interpretation & Why It Matters

• Clinical practice

  • Routine first-attempt McGrath MAC videolaryngoscopy (as delivered in this trial) did not improve first-pass success compared with Macintosh direct laryngoscopy.
  • Improved visualisation alone is an insufficient surrogate for success in ICU intubation, where tube delivery, apnoea tolerance, and haemodynamic instability are dominant constraints.
• Mechanistic signal

  • The combination of better view (Cormack–Lehane grade I 75.6% vs 52.5%) and higher post-first-attempt bougie use (12.0% vs 5.5%) supports a “see more, struggle to pass” interpretation for Macintosh-blade videolaryngoscopy when used indirectly without a stylet on first attempt.
  • This underscores that device design and adjunct strategy (stylet shaping, bougie use, external laryngeal manipulation) are integral to effectiveness, not optional add-ons.
• Implementation & safety

  • The neutral primary outcome and uncertain secondary harm signal reinforce the need to implement videolaryngoscopy alongside physiologically optimised airway bundles, minimised attempts, and structured training/supervision.
  • Device adoption decisions should be made on patient-centred endpoints (first-pass success and complications), not laryngeal view alone.

Controversies & Subsequent Evidence

• Post hoc severe-complication signal:
  • The higher rate of “severe life-threatening complications” with videolaryngoscopy (9.5% vs 2.8%; P=0.01) was derived from a post hoc severity categorisation, within a framework of multiple unadjusted secondary outcomes, increasing the probability of a chance finding and limiting causal inference.¹
• Correspondence on definitions and technique (what was really being tested):
  • Time-to-success was measured from start of anaesthetic induction rather than from laryngoscope insertion, potentially obscuring device-specific effects on laryngoscopy duration and apnoea exposure.
  • For a Macintosh-blade videolaryngoscope, mandating indirect view for first attempt and prohibiting stylet/bougie on the first attempt was challenged as potentially suboptimal and not reflective of common videolaryngoscopy technique, raising concerns about whether the intervention was “videolaryngoscopy as typically practised” versus a constrained technique.
  • The authors’ reply emphasised a pragmatic comparison with symmetrical adjunct restrictions on the first attempt, and argued that improved view without improved first-pass success reflected real-world constraints in ICU intubation.²³⁴⁵
• Subsequent RCT evidence shifted the evidential centre of gravity:
  • In the single-centre ICU FELLOW trial, first-pass success did not differ (68.9% vs 65.8%; unadjusted P=0.68), aligning with MACMAN’s neutral primary outcome despite improved view with videolaryngoscopy.⁶
  • In the larger multicentre DEVICE trial of critically ill adults, videolaryngoscopy improved first-attempt success (85.1% vs 70.8%; absolute risk difference 14.3 points; 95% CI 9.9 to 18.7) with similar severe complications (21.4% vs 20.9%; difference 0.5 points; 95% CI −3.9 to 4.9), implying that context, operator factors, and device/technique implementation materially influence clinical effect.⁷
• Meta-analytic synthesis:
  • Systematic reviews generally report higher first-pass success with videolaryngoscopy outside the operating theatre but emphasise heterogeneity across devices, operator experience, and setting, and inconsistent effects on patient-centred outcomes—consistent with MACMAN’s “better view, same first-pass success” phenotype and later trial-to-trial variability.⁸⁹
• Guideline trajectory:
  • Recent guidance increasingly recommends videolaryngoscopy availability (and often first-line use) for ICU intubation, but places equal emphasis on training, physiologic optimisation, and minimising attempts—principles that sit alongside MACMAN’s device-specific neutral primary outcome and highlight that “videolaryngoscopy” is an implementation strategy, not a single invariant intervention.^10111213

Summary

• In 371 ICU intubations, first-attempt McGrath MAC videolaryngoscopy did not improve first-pass success versus Macintosh direct laryngoscopy (67.7% vs 70.3%).
• Videolaryngoscopy markedly improved laryngeal view (Cormack–Lehane grade I 75.6% vs 52.5%) but did not reduce time to successful intubation (median 3.9 vs 3.8 minutes).
• Overall life-threatening complications were not significantly different; a post hoc “severe” composite was higher with videolaryngoscopy (9.5% vs 2.8%), warranting cautious interpretation.
• Mortality to day 28 was similar (35.7% vs 36.4%); the trial was not powered for survival endpoints.
• MACMAN is a landmark ICU airway trial because it demonstrates that improved glottic exposure is not a sufficient surrogate for first-pass success, and that device effects depend on technique and context.

Further Reading

Other Trials

• 2023Prekker ME, et al. Video versus direct laryngoscopy for tracheal intubation of critically ill adults. N Engl J Med. 2023;389(5):418-429.
• 2016Janz DR, Semler MW, Lentz RJ, et al. Randomized trial of video laryngoscopy for endotracheal intubation of critically ill adults. Crit Care Med. 2016;44(11):1980-1987.
• 2016Driver BE, Prekker ME, Klein LR, et al. Direct versus video laryngoscopy using the C-MAC for emergency intubation. Acad Emerg Med. 2016;23(8):953-960.
• 2015Silverberg MJ, Li N, Kory P, et al. Video laryngoscopy versus direct laryngoscopy for endotracheal intubation in the intensive care unit: a randomized trial. Crit Care Med. 2015;43(3):636-641.

Systematic Review & Meta Analysis

• 2024McDougall GG, Lichtman AD, Liu J, McNarry AF, Patel DA, Kearney E. Video laryngoscopy compared with direct laryngoscopy in critically ill patients: systematic review and trial sequential analysis. Crit Care Med. 2024;52(11):1674-1685.
• 2022Hansel J, Rogers K, Lewis SR, et al. Videolaryngoscopy versus direct laryngoscopy for adult patients requiring tracheal intubation. Cochrane Database Syst Rev. 2022;4:CD011136.
• 2018Arulkumaran N, Lowe J, Ions R, Mendoza M, Bennett V, Dunser M, et al. Videolaryngoscopy vs direct laryngoscopy for emergency orotracheal intubation outside the operating room: a systematic review and meta-analysis. Br J Anaesth. 2018;120(4):712-724.
• 2018Cabrini L, Landoni G, Baiardo Redaelli M, et al. Tracheal intubation in critically ill patients: a comprehensive systematic review of randomized trials. Crit Care. 2018;22(1):6.

Observational Studies

• 2021Russotto V, Myatra SN, Laffey JG, et al. Adverse peri-intubation events in critically ill patients: the INTUBE Study. JAMA. 2021;325(12):1164-1172.
• 2013De Jong A, Molinari N, Terzi N, et al. Early identification of patients at risk of difficult intubation in the ICU: development and validation of the MACOCHA score in a multicenter cohort study. Am J Respir Crit Care Med. 2013;187(8):832-839.
• 2012Simpson GD, Ross MJ, McKeown DW, Ray DC. Tracheal intubation in the critically ill: a multi-centre national study of practice and complications. Br J Anaesth. 2012;108(5):792-799.
• 2010Jaber S, Jung B, Corne P, et al. An intervention to decrease complications related to endotracheal intubation in the intensive care unit: a prospective, multiple-center study. Intensive Care Med. 2010;36(2):248-255.

Guidelines

• 2023Society of Critical Care Medicine. Clinical practice guidelines for rapid sequence intubation in the critically ill adult patient. Crit Care Med. 2023;51(10):1411-1430.
• 2022Apfelbaum JL, Hagberg CA, Connis RT, et al. 2022 American Society of Anesthesiologists Practice Guidelines for Management of the Difficult Airway. Anesthesiology. 2022;136(1):31-81.
• 2021Kornas RL, Owyang CG, Sakles JC, Foley LJ, Mosier JM; on behalf of Society for Airway Management’s Special Projects Committee. Evaluation and management of the physiologically difficult airway: consensus recommendations from Society for Airway Management. Anesth Analg. 2021;132(2):395-405.
• 2018Higgs A, McGrath BA, Goddard C, et al. Guidelines for management of tracheal intubation in critically ill adults. Br J Anaesth. 2018;120(2):323-352.

Overall Takeaway

MACMAN is “landmark” because it challenged an intuitive assumption—better glottic view equals better intubation success—in the physiologically high-risk ICU context. It showed that Macintosh-blade videolaryngoscopy (as delivered: indirect first-pass view without a stylet/bougie) did not improve first-pass success versus direct laryngoscopy, while highlighting that device effects are tightly coupled to technique, operator factors, and implementation context.

Bibliography

• 1O'Gara B, Talmor D. Video laryngoscopy in the intensive care unit: seeing is believing but that does not mean it's true. JAMA. 2017;317(5):479-480.
• 2Loh KW, Tan RA. Intubation With Video Laryngoscopy vs Direct Laryngoscopy. JAMA. 2017;317(20):2130-2131.
• 3Xue FS, Liu YY, Li HX, Yang GZ, Xu YC. Intubation With Video Laryngoscopy vs Direct Laryngoscopy. JAMA. 2017;317(20):2131-2132.
• 4Saddawi-Konefka D, Baker KH, Wiener-Kronish JP. Intubation With Video Laryngoscopy vs Direct Laryngoscopy. JAMA. 2017;317(20):2132-2133.
• 5Lascarrou JB, Boisrame-Helms J, Bailly A, et al. Intubation With Video Laryngoscopy vs Direct Laryngoscopy. JAMA. 2017;317(20):2133-2134.
• 6Janz DR, Semler MW, Lentz RJ, et al. Randomized trial of video laryngoscopy for endotracheal intubation of critically ill adults. Crit Care Med. 2016;44(11):1980-1987.
• 7Prekker ME, et al. Video versus direct laryngoscopy for tracheal intubation of critically ill adults. N Engl J Med. 2023;389(5):418-429.
• 8Arulkumaran N, Lowe J, Ions R, Mendoza M, Bennett V, Dunser M, et al. Videolaryngoscopy vs direct laryngoscopy for emergency orotracheal intubation outside the operating room: a systematic review and meta-analysis. Br J Anaesth. 2018;120(4):712-724.
• 9McDougall GG, Lichtman AD, Liu J, McNarry AF, Patel DA, Kearney E. Video laryngoscopy compared with direct laryngoscopy in critically ill patients: systematic review and trial sequential analysis. Crit Care Med. 2024;52(11):1674-1685.
• 10Higgs A, McGrath BA, Goddard C, et al. Guidelines for management of tracheal intubation in critically ill adults. Br J Anaesth. 2018;120(2):323-352.
• 11Kornas RL, Owyang CG, Sakles JC, Foley LJ, Mosier JM; on behalf of Society for Airway Management’s Special Projects Committee. Evaluation and management of the physiologically difficult airway: consensus recommendations from Society for Airway Management. Anesth Analg. 2021;132(2):395-405.
• 12Apfelbaum JL, Hagberg CA, Connis RT, et al. 2022 American Society of Anesthesiologists Practice Guidelines for Management of the Difficult Airway. Anesthesiology. 2022;136(1):31-81.
• 13Society of Critical Care Medicine. Clinical practice guidelines for rapid sequence intubation in the critically ill adult patient. Crit Care Med. 2023;51(10):1411-1430.