Suzetrigine

Suzetrigine (Nav1.8 Non-Opioid Acute Pain)

Evidence grade scale used in this note:

• Confirmed — replicated clinical signals or well-supported mechanism statements
• Supported — single-study or preliminary evidence; directionally consistent
• Reported — observed in trials but not independently confirmed
• Contested — evidence is mixed or interpretation is debated
• Gap — not established in available literature

TL;DR

First-in-class selective Nav1.8 voltage-gated sodium channel inhibitor; FDA approved January 30, 2025 (brand: Journavx) for moderate-to-severe acute pain in adults. Statistically significant pain reduction vs placebo in two Phase 3 RCTs (abdominoplasty n=1,118; bunionectomy n=1,073); comparable efficacy to hydrocodone/acetaminophen (non-inferiority suggested; superiority NOT confirmed). No addiction risk, no respiratory depression, no GI ulceration. No long-term safety data; ~15 months on market as of April 2026.

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Why it matters for Vitals

Vitals relevance:

• First evidence-backed non-opioid option for moderate-to-severe acute pain — directly relevant for pain protocol selection in users avoiding opioids
• Theoretical HRV/autonomic preservation signal vs opioid-based analgesia (not validated in trials — requires clinical review before Vitals coaching use)
• Non-NSAID mechanism for users with GI bleed history, renal impairment, or anticoagulation
• Oral, no device or cold-chain burden — straightforward for outpatient protocol integration

Wearables — evidence boundary: No wearable endpoints were measured in any suzetrigine trial. All HRV/sleep/activity monitoring claims are mechanistic extrapolation. human_signoff_required before any Vitals coaching use.

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Key facts

Field	Detail
Brand name	Journavx
Company	Vertex Pharmaceuticals
Class	Selective Nav1.8 voltage-gated sodium channel blocker
FDA approval	January 30, 2025
Indication	Moderate-to-severe acute pain in adults
Dosing	100 mg loading dose, then 50 mg every 12 hours (oral tablet)
First-in-class	First novel non-opioid acute pain mechanism approved in decades
Clinical trials	2× Phase 3 RCTs (n=1,118; n=1,073) + single-arm Phase 3 (n=256)
Evidence boundary	~15 months on market; no long-term or real-world data

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Mechanism summary

Suzetrigine selectively inhibits the Nav1.8 voltage-gated sodium channel, expressed almost exclusively in peripheral nociceptive neurons (C-fibers and A-delta fibers). Nav1.8 mediates the upstroke of the action potential in pain-sensing neurons and is critical for high-frequency repetitive firing during sustained pain signaling.

Confirmed:

• State-dependent (use-dependent) binding — preferentially targets channels in the inactivated state
• Activity-dependent mechanism: suppresses hyperactive nociceptors while sparing normally functioning neurons
• High selectivity for Nav1.8 over Nav1.5 (cardiac), Nav1.7, and Nav1.9 confirmed preclinically
• No CNS reward pathway activity (non-opioid mechanism)
• No COX inhibition (non-NSAID mechanism)

Distinct from: opioids (mu-receptor agonism), NSAIDs (COX inhibition), non-selective sodium channel blockers (lidocaine).

Evidence gaps: High-resolution cryo-EM structure of the suzetrigine–Nav1.8 complex not publicly disclosed. Selectivity ratios (Nav1.8 IC50 vs Nav1.5 IC50) not fully disclosed in indexed literature. Whether Nav1.8 inhibition differentially affects inflammatory vs neuropathic pain not established in human data.

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Clinical efficacy

Phase 3 RCTs — Confirmed

Abdominoplasty RCT (n=1,118):

• SPID48 (primary): LS mean difference vs placebo = 48.4 (95% CI: 33.6–63.1), P < 0.0001
• Source: PMID 40117446

Bunionectomy RCT (n=1,073):

• SPID48 (primary): LS mean difference vs placebo = 29.3 (95% CI: 14.0–44.6), P = 0.0002
• Source: PMID 40117446

Phase 3 — secondary endpoint vs hydrocodone/acetaminophen — Confirmed (non-superiority)

• Suzetrigine did NOT achieve superiority vs hydrocodone/acetaminophen 5/325 mg q6h on SPID48 (pre-specified key secondary endpoint)
• Pain reduction was numerically comparable between treatments
• Time to ≥2-point NPRS reduction was faster with suzetrigine
• Source: PMID 40117446

Supporting evidence — Supported

• Meta-analysis (n=1,584): pain reduction at 24h MD −0.93 NPRS (95% CI: −1.38 to −0.48) vs placebo; pain reduction at 48h also statistically significant
• Heterogeneity note: I² = 66% — suggests variable efficacy across surgical models
• Single-arm Phase 3 (n=256): 83.2% rated effectiveness as good/very good/excellent; most adverse events mild (27.7%) or moderate (8.2%); no new safety signals
• Sources: PMID 41790692, PMID 40165940

Evidence gaps — Contested / Gap

• Clinically modest effect: ~1-point NPRS improvement over placebo at 24h; FDA approval narrative (“first non-opioid in decades”) may create expectations of a transformative advance — actual data shows comparable efficacy to opioids, not superior efficacy
• No head-to-head data vs ibuprofen, acetaminophen, or celecoxib
• Only two surgical models (abdominoplasty, bunionectomy); generalizability to other acute pain causes (renal colic, fracture, burns) is unestablished
• No efficacy data in chronic pain (Phase 2/3 for diabetic peripheral neuropathy and lumbosacral radiculopathy are ongoing)
• Population was 92.3% female — demographic generalizability unknown
• Long-term efficacy beyond 14 days not established

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Pharmacokinetics — Supported

• Oral bioavailability confirmed; exact fraction not publicly disclosed in indexed literature (refer to FDA label)
• Dose-proportional PK across studied dose range (Phase 1 SAD study; PMID 41251403)
• Steady state reached in ~48 hours with twice-daily dosing (Phase 1 MAD; PMID 41251403)
• Primary metabolic pathway: CYP3A4 (PMID 41251403)
• No clinically significant CYP3A4 interactions at therapeutic concentrations in Phase 1 DDI assessments (PMID 41251403)

Gap: Exact half-life, protein binding %, food effect, Cmax/Tmax/clearance/Vd — not publicly disclosed in indexed literature. No dedicated renal/hepatic impairment PK study published. Active metabolites have not been clearly described.

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Safety profile

Confirmed safety advantages vs opioids and NSAIDs

Safety concern	Suzetrigine	Opioids	NSAIDs
Addiction risk	None (non-opioid)	High	None
Respiratory depression	None	Dose-dependent	None
GI ulceration	None	Constipation	Risk present
Cardiac (Nav1.5 cross-reactivity)	None detected	N/A	CV risk with COXibs

Confirmed safety findings

• Adverse events were mild-to-moderate in severity in both Phase 3 RCTs; no new safety signals identified up to 14 days
• No abuse potential identified in abuse liability studies (PMID 41481839)
• No clinically significant Nav1.5 (cardiac) cross-reactivity confirmed preclinically and in Phase 3 cardiac monitoring (PMID 41924085)

Adverse events in trials — Supported

• Mild AEs: 27.7% (71/256); moderate AEs: 8.2% (21/256) in single-arm Phase 3
• Most common: dizziness, nausea, headache
• Source: PMID 40165940

Contraindications and warnings — Reported

• Known hypersensitivity to suzetrigine or any excipients
• Concomitant use with strong CYP3A4 inhibitors may require dose adjustment or be contraindicated
• Use in pregnancy only if benefit justifies risk (confirm current pregnancy category with FDA label)
• Use with caution in severe renal or hepatic impairment (not studied)
• Long-term (>14 days) safety not established in clinical trials

Special populations — Gap (not studied)

• Elderly patients >75 years (limited enrollment in Phase 3)
• Pediatric patients
• Pregnancy and lactation
• Severe renal or hepatic impairment

Post-marketing surveillance — Gap

As of April 2026, suzetrigine has been FDA-approved for approximately 15 months. No post-marketing pharmacovigilance data is publicly available in indexed literature.

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Comparative landscape

Comparison	Key distinction
vs opioids	Comparable efficacy; suzetrigine has no addiction risk, no respiratory depression, no constipation — NOT a replacement for opioids in severe acute pain requiring opioid-level analgesia; non-inferiority suggested, superiority NOT confirmed
vs NSAIDs	No GI/renal/CV toxicity; no head-to-head data; NSAIDs are cheaper and well-characterized for mild-moderate pain; comparative value of branded suzetrigine vs OTC NSAIDs for mild-moderate pain is not established
vs acetaminophen	Likely more efficacious for moderate-to-severe pain; acetaminophen remains safer in liver disease and first-line for mild pain; no head-to-head data
vs lidocaine	Oral vs IV; Nav1.8 selectivity avoids CNS toxicity and arrhythmia risk of non-selective sodium channel blockade
vs gabapentinoids	Fundamentally different mechanisms and indications; suzetrigine for acute pain; gabapentin/pregabalin for neuropathic/chronic pain

Competitive position — Supported

Suzetrigine fills a specific niche as the first approved non-opioid, non-NSAID, non-acetaminophen option for moderate-to-severe acute pain. Value proposition is highest for:

1. Patients with NSAID contraindications (GI bleed history, renal impairment, on anticoagulation)
2. Patients at risk of or in recovery from opioid use disorder
3. Multimodal ERAS protocols aiming to reduce opioid requirements
4. Settings where addiction risk makes opioid prescribing undesirable

Not positioned as: replacement for OTC analgesics for mild pain.

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Formulation and delivery — Confirmed

• Oral tablet formulation (small molecule, not a biologic or peptide)
• Dosing: 100 mg loading dose orally, then 50 mg every 12 hours
• No device burden: no injection, IV infusion, pump, or cold chain required
• No immunogenicity risk (small molecule)
• Simple oral administration — no healthcare professional required for administration; suitable for outpatient and discharge prescribing

Limitations:

• Twice-daily dosing may reduce compliance vs once-daily analgesics
• Patients unable to take oral medications (post-surgical NPO, severe nausea) cannot use it
• Not suitable for patients requiring rapid-onset IV analgesia in hospital settings

Gap: Specific inactive ingredients, available tablet strengths, scoring for dose adjustment, storage conditions, and bioequivalence data for potential generic formulations — not in indexed literature.

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Vitals implementation guidance

⚠️ human_signoff_required — All Vitals coaching claims involving suzetrigine require clinical advisor review before user-facing use.

When to flag suzetrigine as an option (pending clinical review)

• User reports moderate-to-severe acute pain (post-procedure, injury) with NPRS ≥4
• NSAID contraindications present: GI bleed history, renal impairment, on anticoagulation, NSAID intolerance
• Opioid use disorder history or risk factors for opioid dependence
• ERAS/opioid-sparing multimodal protocol active

Not appropriate for Vitals coaching

• Mild acute pain (acetaminophen/ibuprofen remains first-line)
• Chronic pain (not approved; trials ongoing)
• Use in elderly >75, pediatric, pregnancy, severe organ impairment (not studied)
• Any specific HRV/wearable-based claims (no trial validation)

Theoretical wearable signal differentiation (speculative — requires clinical sign-off)

All of the following are mechanistic extrapolation. No wearable endpoints were measured in any suzetrigine trial.

Theoretical signal	Mechanism basis	Evidence grade
HRV preservation vs opioid protocol	Opioids suppress HRV; suzetrigine is non-opioid and theoretically preserves autonomic function	Low — not measured in trials
Respiratory preservation	Opioids cause dose-dependent respiratory depression; suzetrigine causes none	Moderate — mechanistically supported, not directly measured
Sleep architecture preservation	Opioids disrupt deep sleep and REM; reducing opioids with suzetrigine may preserve sleep	Low — no direct sleep endpoint data
Pain recovery trajectory	Pain improvement correlates with HRV recovery and RHR normalization post-surgery	Low — associative only, not validated for suzetrigine

Algorithm hooks

trigger_conditions:
  suzetrigine_candidate:
    when: "acute_pain_flag (NPRS 4+) AND (nsaid_contraindication OR opioid_risk OR opioid_sparing_goal)"
    confidence: "conditional"
    requires_clinical_review: true
    evidence_boundary: "No validated wearable endpoint exists for suzetrigine efficacy"
 
  opioid_sparing_coaching:
    when: "suzetrigine_prescribed AND opioid_reduction_goal"
    theoretical_signals: ["hrv_preserved", "resting_heart_rate_normal", "sleep_architecture_intact"]
    evidence_boundary: "No trial data validating HRV/pain correlation for suzetrigine — theoretical only"
    human_signoff_required: true
 
  autonomic_recovery_benchmark:
    when: "post_surgical AND analgesic_protocol"
    comparison: "suzetrigine_protocol vs opioid_protocol"
    theoretical_signals: ["hrv_trajectory", "rmssd_recovery", "step_count_progression"]
    evidence_boundary: "No published comparative wearable data — associative only"
    human_signoff_required: true
 
contraindications_absolute:
  - "known_hypersensitivity_suzetrigine"
  - "concomitant_strong_cyp3a4_inhibitor"
 
contraindications_relative:
  - "pregnancy_benefit_risk_unclear"
  - "severe_renal_impairment_not_studied"
  - "severe_hepatic_impairment_not_studied"
  - "elderly_over_75_limited_data"
  - "pediatric_not_studied"
 
evidence_boundaries:
  no_wearable_biomarker_validated: true
  no_head_to_head_nsaid_data: true
  no_long_term_safety_beyond_14_days: true
  no_real_world_effectiveness_data: true
  no_chronic_pain_efficacy: true
  no_pediatric_pregnancy_data: true
 
human_signoff_required:
  - "all_suzetrigine_coaching_recommendations"
  - "all_wearable_based_recovery_benchmarking"
  - "all_opioid_sparing_quantification_claims"

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Regulatory and access gaps

• EMA/MHRA status: Unknown — not confirmed in indexed literature as of April 2026
• Cost: Branded medication; high list price expected; insurance coverage varies; patient assistance programs may be available from Vertex
• Generics: Not expected for several years

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Evidence summary

Domain	Grade	Key Source
FDA approval	Confirmed	PMID 41771767
Phase 3 efficacy (SPID48)	Confirmed	PMID 40117446
Non-superiority vs opioids	Confirmed	PMID 40117446
Mechanism (Nav1.8 selectivity)	Confirmed	PMID 39775738, PMID 41977224
No abuse potential	Confirmed	PMID 41481839
No respiratory depression	Confirmed	PMID 40117446
No GI ulcer risk	Confirmed	PMID 40117446
Mild/moderate AE profile	Supported	PMID 40165940
CYP3A4 metabolism	Supported	PMID 41251403
Oral bioavailability	Supported	PMID 41251403
Meta-analysis efficacy (heterogeneity noted)	Supported	PMID 41790692
Opioid-sparing role	Supported	PMID 41481839
No Nav1.5 cross-reactivity	Supported	PMID 41924085
Single-arm effectiveness (83% good+)	Supported	PMID 40165940
HRV/autonomic preservation (wearable)	Gap (speculative)	Not measured in trials
Chronic pain efficacy	Gap	Phase 2/3 ongoing
Long-term (>14d) safety	Gap	Not studied
Real-world effectiveness	Gap	Post-marketing data not yet available
Head-to-head vs NSAIDs	Gap	No trials planned
Pediatric/pregnancy/elderly safety	Gap	Not studied

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Related notes

• Nav1.8 — voltage-gated sodium channel; primary mechanism target; no separate mechanism note yet (ghost link — create when a second compound targets this channel)
• Cluster Headache — pain condition note; suzetrigine not studied in this indication
• Body Systems MOC — pain management context

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Key references

• PMID 40117446 — Phase 3 RCTs (abdominoplasty + bunionectomy), primary efficacy evidence
• PMID 40165940 — Phase 3 single-arm study, broad acute pain
• PMID 41790692 — Meta-analysis of efficacy (I² = 66%)
• PMID 41785614 — Safety meta-analysis
• PMID 39775738 — Nav1.8 selectivity mechanism
• PMID 41977224 — Nav1.8 peripheral expression
• PMID 41924085 — Nav1.8 electrophysiology and selectivity vs Nav1.5
• PMID 41800743 — Activity-dependent DRG neuron effects
• PMID 41481839 — Abuse liability and opioid-sparing rationale
• PMID 41251403 — Phase 1 PK/ADME
• PMID 41182481 — Comparative landscape vs gabapentinoids
• PMID 41771767 — FDA approval announcement
• PMID 41779973 — Health economic/access analysis