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  • QuickView: Sunvozertinib vs Chemotherapy in Advanced EGFR exon20ins NSCLC (WU-KONG28)

    WU-KONG28 ASCO 2026

    Sunvozertinib vs platinum-based chemotherapy · First-line advanced NSCLC with EGFR exon20ins · International randomized phase 3

    Total N
    324
    1:1 randomized
    Median PFS
    10.3 vs 7.5 mo
    Sunvo vs Chemo
    Hazard Ratio
    0.65
    95% CI 0.50–0.85 · P<0.001
    Confirmed ORR
    58.9% vs 31.1%
    Sunvo vs Chemo

    WU-KONG28 Study Design

    Key Eligibility
    • Locally advanced or metastatic non-squamous NSCLC
    • Documented EGFR exon20ins
    • Newly diagnosed or treatment-naïve
    • ECOG PS 0 or 1
    Randomization
    Ratio1:1
    StratificationBaseline brain metastasis (yes / no)
    Sites154 sites · 15 countries
    Data cutoffJanuary 16, 2026
    Sunvozertinib (N=163)
    300 mg once daily, oral
    Continuous until progression or unacceptable toxicity
    Platinum-based Chemotherapy (N=161)
    Carboplatin AUC5 + pemetrexed 500 mg/m² Q3W
    Up to 4 or 6 cycles (investigator discretion) → pemetrexed maintenance
    Crossover to sunvozertinib allowed at confirmed PD
    Endpoints
    Primary PFS assessed by BICR Key Secondary Overall Survival (OS) Secondary Investigator-assessed PFS · ORR · DCR · DoR · Tumor size change · Safety · PK Exploratory PFS2

    Efficacy

    Primary Endpoint: Median PFS (BICR)
    Sunvozertinib10.3 mo
    95% CI: 8.3, 14.0
    Chemotherapy7.5 mo
    95% CI: 6.7, 8.5
    HR (95% CI)0.65 (0.50, 0.85)
    P value<0.001
    PFS Landmark Rates
    12 months46.1% vs 26.7%
    18 months33.2% vs 17.1%
    24 months23.0% vs 10.3%
    Median follow-up: 24.0 mo (sunvo) · 18.0 mo (chemo)
    Objective Response Rate (BICR)
    Confirmed ORR
    Sunvozertinib58.9%
    95% CI: 50.9, 66.5
    Chemotherapy31.1%
    95% CI: 24.0, 38.8
    Odds Ratio (95% CI)3.2 (2.0, 5.0)
    Additional Response Data (from ASCO presentation)
    Best ORR68.1% vs 35.4%
    Disease Control Rate94.5% vs 85.7%
    Duration of Response
    Sunvozertinib11.2 mo
    95% CI: 8.2, 13.9
    Chemotherapy7.1 mo
    95% CI: 6.9, 11.1
    Median follow-up: 22.1 mo (sunvo) · 13.8 mo (chemo)
    Median Tumor Size Shrinkage
    Sunvozertinib-42.1%
    Range: -88.6 to 21.3
    Chemotherapy-24.7%
    Range: -85.6 to 362.2
    Crossover
    101 of 112 chemotherapy-arm patients (90.2%) with confirmed disease progression crossed over to receive sunvozertinib.
    Interim Overall Survival
    Sunvozertinib29.8 mo
    95% CI: 21.8, NE
    Chemotherapy28.8 mo
    95% CI: 20.7, NE
    HR (95% CI)0.99 (0.70, 1.40)
    P value0.48
    Data maturity38.9% (126/324 events)
    OS Landmark Rates
    18 months65.5% vs 67.2%
    24 months57.4% vs 56.2%
    30 months50.0% vs 49.1%
    Median OS follow-up: 26.1 mo (sunvo) · 26.7 mo (chemo). OS data immature; interpretation may be confounded by the crossover design. NE, not estimable.
    Subgroup Analysis: BICR-assessed PFS
    ← Favors sunvozertinib HR = 1.0 Favors chemotherapy →
    Overall(n=324)
    0.65 (0.50, 0.85)
    Age Group
    <65 years(n=182)
    0.62 (0.44, 0.87)
    ≥65 years(n=142)
    0.71 (0.46, 1.07)
    Sex
    Female(n=192)
    0.68 (0.48, 0.97)
    Male(n=132)
    0.58 (0.39, 0.85)
    Race
    Asian(n=204)
    0.56 (0.41, 0.77)
    Non-Asian(n=120)
    0.93 (0.58, 1.48)
    Region
    North America + EU(n=102)
    0.78 (0.47, 1.30)
    Others(n=222)
    0.62 (0.45, 0.84)
    Smoking History
    Never(n=208)
    0.61 (0.43, 0.85)
    Ever(n=116)
    0.73 (0.48, 1.11)
    Baseline ECOG
    0(n=89)
    0.77 (0.45, 1.31)
    ≥1(n=235)
    0.62 (0.46, 0.84)
    Brain Metastasis at Baseline
    With(n=41)
    0.96 (0.44, 2.08)
    Without(n=283)
    0.62 (0.47, 0.83)
    EGFR Exon20ins Subtype
    769_ASV(n=103)
    0.46 (0.29, 0.73)
    770_SVD(n=53)
    NR
    Other/Unknown(n=168)
    0.77 (0.53, 1.10)
    EGFR Exon20ins Region
    Near loop(n=220)
    0.59 (0.43, 0.82)
    Far loop(n=84)
    0.83 (0.49, 1.38)
    C-helix/Unknown(n=20)
    NR
    Disease-Related Surgery
    With(n=65)
    0.55 (0.29, 1.02)
    Without(n=259)
    0.69 (0.51, 0.92)
    X-axis range: 0.2 to 2.5. NR = not reported (insufficient events). Source: Heymach et al, ASCO 2026 LBA8500 (slide 7).

    Safety

    Sunvozertinib N=163; Chemotherapy N=150 (patients who received randomized treatment)
    Safety Overview
    ParameterSunvozertinib %Chemotherapy %
    Any adverse event100.099.3
    Any AE, Grade ≥375.556.7
    Any TRAE100.097.3
    Any TRAE, Grade ≥361.349.3
    Treatment-related SAE18.412.7
    TRAE leading to dose interruption45.427.3
    TRAE leading to dose reduction40.524.0
    TRAE leading to discontinuation7.411.3
    TRAE with fatal outcome0.00.7
    Top TRAEs leading to dose interruption and reduction with sunvozertinib: CPK increased and diarrhea (neither led to treatment discontinuation).
    Adverse Events ≥20% in Either Group (Any Grade)
    All-cause adverse events emerging during treatment (per NEJM Table 3). Grade ≥3 shown in adjacent column.
    Sunvo
    G≥3
    Chemo
    G≥3
    Diarrhea
    87.1%
    14.1%
    16.7%
    CPK increased
    58.3%
    20.9%
    4.0%
    0.7%
    Anemia
    57.1%
    9.2%
    62.7%
    11.3%
    Rash
    52.8%
    0.6%
    6.7%
    Paronychia
    48.5%
    3.7%
    0.7%
    Weight decreased
    43.6%
    3.7%
    11.3%
    0.7%
    Decreased appetite
    38.7%
    1.8%
    28.0%
    1.3%
    Creatinine increased
    33.7%
    0.6%
    9.3%
    Nausea
    28.2%
    1.8%
    46.0%
    1.3%
    Vomiting
    28.2%
    1.8%
    24.0%
    2.0%
    Hypokalemia
    25.2%
    3.7%
    7.3%
    0.7%
    Amylase increased
    23.3%
    1.2%
    11.3%
    Lipase increased
    23.3%
    5.5%
    7.3%
    1.3%
    AST increased
    22.1%
    2.5%
    37.3%
    0.7%
    Mouth ulceration
    20.2%
    1.2%
    3.3%
    ALT increased
    17.8%
    1.8%
    34.7%
    1.3%
    Fatigue
    15.3%
    1.2%
    20.0%
    2.7%
    Neutrophil ↓
    14.7%
    2.5%
    45.3%
    18.7%
    WBC ↓
    12.3%
    0.6%
    39.3%
    6.7%
    Constipation
    11.0%
    0.6%
    25.3%
    Platelet ↓
    9.2%
    2.5%
    22.0%
    6.7%
    Sunvozertinib AEs reflect wild-type EGFR inhibition (diarrhea, rash, paronychia, CPK elevation). Chemotherapy-associated myelosuppression (anemia, neutropenia, thrombocytopenia) predominates in the chemo arm.

    References

    1. Heymach JV, Liu G, Xing L, et al. Sunvozertinib monotherapy versus platinum-based chemotherapy as first-line treatment for advanced NSCLC with EGFR exon20ins: primary analysis of a multinational phase 3 randomized study (WU-KONG28). J Clin Oncol. 2026;44(suppl 17):LBA8500. doi:10.1200/JCO.2026.44.17_suppl.LBA8500. Presented at: 2026 ASCO Annual Meeting; May 29–June 2, 2026; Chicago, IL.
    2. Zhou C, Greillier L, Liu G, et al. First-line sunvozertinib in NSCLC with EGFR exon 20 insertion mutations. N Engl J Med. 2026. doi:10.1056/NEJMoa2604461.
    3. ClinicalTrials.gov identifier: NCT05668988.

    Abbreviations

    BICRBlinded Independent Central Review
    cORRConfirmed Objective Response Rate
    CPKCreatine phosphokinase
    DCRDisease Control Rate
    DoRDuration of Response
    ECOGEastern Cooperative Oncology Group
    EGFREpidermal Growth Factor Receptor
    Exon20insExon 20 Insertion Mutations
    HRHazard Ratio
    mPFSMedian Progression-Free Survival
    NSCLCNon-Small Cell Lung Cancer
    ORRObjective Response Rate
    OSOverall Survival
    PFSProgression-Free Survival
    PFS2Second Progression-Free Survival
    Q3WEvery 3 Weeks
    SAESerious Adverse Event
    TKITyrosine Kinase Inhibitor
    TRAETreatment-Related Adverse Event
    CANCER COMMUNICATOR · cancercommunicator.com
    Data sources: ASCO LBA8500 presentation · NEJM 10.1056/NEJMoa2604461 · Data cutoff: January 16, 2026