Kyverna Therapeutics Announces Positive Phase 2 Interim Data for KYV-101 in Generalized Myasthenia Gravis

Analysis reveals significant industry trends and economic implications

Release Date

2025-10-29

Category

Clinical Trial Event

Reference

Source

Breakthrough Clinical Results

Kyverna Therapeutics announced positive interim Phase 2 data from the KYSA-6 study of KYV-101 in generalized myasthenia gravis (gMG). The data showed 100% of patients achieved clinically meaningful responses in MG-ADL and QMG, the co-primary endpoints of the Phase 3 trial, with mean reductions of -8.0 and -7.7 points at 24 weeks, respectively. KYV-101 was well-tolerated with no high-grade CRS or ICANS observed. These results reinforce confidence in the Company’s registrational KYSA-6 Phase 3 MG trial and KYV-101’s potential to deliver durable, drug-free, disease-free remission with a single dose.

Key Highlights

  • 100% of patients achieved clinically meaningful responses in MG-ADL and QMG with KYV-101 treatment.
  • KYV-101 demonstrated a consistent and manageable safety profile.
  • KYV-101 significantly reduced treatment burden, with 100% of patients free of nonsteroidal immunosuppressants, high-dose steroids, and FcRn and complement inhibitors.
  • Data reinforces confidence in the KYSA-6 Phase 3 trial design.

Incidence and Prevalence

Global Incidence and Prevalence of Myasthenia Gravis: Latest Estimates

Incidence Rates

Recent epidemiological studies worldwide suggest an incidence of acetylcholine receptor antibody-positive myasthenia gravis of up to 29 cases per 1 million people per year in the past 5-10 years. In the United States, the diagnosed incidence of MG in 2021 was calculated to be 3.1 per 100,000 persons (31 per million). Another US study reported an age-and sex-standardized incidence of 68.5 new cases per million person-years in the commercially/Medicare-insured cohort and 49.7 new cases per million person-years in the Medicaid-insured population.

In the East Midlands of the United Kingdom, the average annual incidence rate was 17.6/1,000,000 (95% CI 10.7-28.6). In South Korea, a nationwide population-based epidemiological study found the standardized incidence rate was 2.44 per 100,000 person-years (24.4 per million) in 2011.

In Cape Town, South Africa, the annual incidence rate for seropositive MG was 11.2 per million per year (95% confidence interval 8.7-14.3), and for South Africa overall, it was 2.6 per million/year (95% CI 2.2-2.9). After adjusting for those presumed to have seropositive MG without a confirmatory test, the annual incidence rate for Cape Town was 12.6 per million (95% CI 9.9-15.9).

Muscle-specific tyrosine kinase antibody-positive myasthenia gravis and Lambert-Eaton myasthenic syndrome are about 20 times less common than acetylcholine receptor antibody-positive myasthenia gravis.

Prevalence Rates

The diagnosed prevalence of Myasthenia Gravis in the United States in 2021 was calculated to be 37.0 per 100,000 persons. In Nordic countries (2000-2020), the overall prevalence per 100,000 was 18.56 (95% CI 18.31 to 18.81) in Denmark, 20.89 (95% CI 20.62 to 21.16) in Finland, and 23.42 (95% CI 23.21 to 23.64) in Sweden.

In South Korea, the standardized prevalence rates were 9.67 and 10.66 per 100,000 persons in 2010 and 2011, respectively.

Demographic Patterns

Incidence rates generally increase with age in both men and women, with higher rates observed in younger women (<50 years) compared to men of matching age, and higher rates in older men (≥65 years) compared to women of the same age group. In South Korea, the incidence and prevalence rates peaked in the elderly population aged 60 to 69 years for both sexes.

In Cape Town, the incidence rate in females was 15.3 per million/year (95% CI 11.2-20.4), and in males, 6.8 per million/year (95% CI 4.1-10.7). The incidence rate of seropositive MG in Cape Town was 6 times greater in those presenting after the age of 50 years than in those with earlier disease onset.

Trends

A global trend of increasing prevalence and incidence of MG has been observed in the last few decades. This increase in prevalence may be due, in part, to improvements in diagnostics but also to an aging global population and immunosenescence, as the largest increases in MG prevalence have been in patients ≥65 years old.

Over the past 120 years, mortality associated with myasthenia gravis has steadily decreased while the incidence of MG has increased. While mortality due to MG has been ≤5% for at least the past 25 years, the prevalence of MG has increased.

Study Design Parameters

Study Design Parameters and Endpoints in Key Myasthenia Gravis Trials

Study Designs

Randomized controlled trials dominate MG research with various designs:

  • Double-blind, placebo-controlled studies like the MycarinG trial of rozanolixizumab (200 patients)
  • Single-blinded trials comparing IVIG and PLEX (84 patients with worsening MG)
  • Open-labeled randomized controlled trials such as the 30-min walk or rest study (40 patients)
  • Phase 3 trials including ADAPT (167 patients across 56 centers in 15 countries), RAISE (174 patients at 75 sites), and CHAMPION MG (ravulizumab)

Recent innovations include telemedical solutions like the MyaLink platform (45 participants) enabling systematic symptom monitoring and wearable data collection.

Primary Endpoints

The most common primary endpoints include:

  • Myasthenia Gravis Activities of Daily Living (MG-ADL) score:

  • An 8-item outcome measure with good to excellent reliability

  • Primary efficacy endpoint in the rozanolixizumab trial (change from baseline to day 43)

  • Used in ADAPT where more efgartigimod patients were MG-ADL responders (68%) than placebo (30%)

  • In RAISE, zilucoplan showed greater MG-ADL reduction (-4.39) versus placebo (-2.30)

  • Quantitative Myasthenia Gravis Score (QMG):

  • Assesses functional status after IVIG/PLEX treatment

  • Measures efficacy of amifampridine phosphate

  • Evaluates core strength in exercise studies

  • Other Primary Endpoints:

  • MG Quality of Life (MG-QOL15) in exercise trials

  • Prednisone area under the dose-time curve in steroid-sparing studies

  • Percentage change in total IgG levels

Secondary Endpoints

Trials typically include multiple secondary measures:

  • Myasthenia Gravis Composite Score
  • Clinical Global Impression-Improvement
  • 3TUG (timed up and go) test
  • 6-minute walk test (6MWT)
  • Myasthenic Muscle Score (MMS)
  • Grip strength
  • Medication dosage changes
  • Treatment failures and clinical deterioration events

Safety Assessments

Treatment-emergent adverse events (TEAEs) are carefully monitored:

  • In the rozanolixizumab trial, common TEAEs included headache (38-45% vs 19% placebo), diarrhea (16-25% vs 13%), and pyrexia (13-20% vs 1%)
  • Efgartigimod was well tolerated with most frequent adverse events being headache (29%) and nasopharyngitis (12%)
  • Zilucoplan's most common adverse event was injection-site bruising (16% vs 9%)
  • Serious TEAEs occurred in 8-10% of patients across treatment groups

Recent Trial Outcomes

  • ADAPT: Efgartigimod demonstrated significant improvement with odds ratio of 4.95 for MG-ADL response
  • MycarinG: Rozanolixizumab showed greater MG-ADL reductions (-3.37 to -3.40) versus placebo (-0.78)
  • CHAMPION MG: Ravulizumab maintained MG-ADL improvements through 60 weeks (-4.0 from baseline)
  • RAISE: Zilucoplan demonstrated significant MG-ADL improvement versus placebo (difference: -2.09, p=0.0004)

Recent Studies

Recent Myasthenia Gravis Clinical Trials

RAISE Trial (2023)

  • Randomized, double-blind, placebo-controlled, phase 3 trial at 75 sites globally
  • Intervention: Zilucoplan (0.3 mg/kg once daily by self-injection) - a complement C5 inhibitor
  • Efficacy: Greater MG-ADL score reduction from baseline to week 12 compared to placebo (-4.39 vs -2.30; difference: -2.09; p=0.0004)
  • Safety: Treatment-emergent adverse events in 77% of zilucoplan patients vs 70% in placebo; most common was injection-site bruising (16%)

ADAPT+ Study (2023)

  • Open-label, single-arm, multicenter extension study for up to 3 years
  • Intervention: Efgartigimod (10 mg/kg) administered as 4 weekly intravenous infusions per cycle
  • Efficacy: For AChR-Ab+ participants, >90% had clinically meaningful improvement in MG-ADL scores across first 10 treatment cycles
  • Safety: 84.8% reported ≥1 treatment-emergent adverse event; most frequent: headache (24.8%), COVID-19 (15.2%), nasopharyngitis (13.8%)

MycarinG Study (2023)

  • Randomized, double-blind, placebo-controlled, phase 3 study at 81 centers globally
  • Intervention: Rozanolixizumab (7 mg/kg or 10 mg/kg) - a neonatal Fc receptor blocker given subcutaneously once weekly for 6 weeks
  • Efficacy: Clinically meaningful improvements in patient-reported and investigator-assessed outcomes
  • Safety: Most frequent adverse events were headache (45% in 7 mg/kg, 38% in 10 mg/kg), diarrhea and pyrexia; generally well tolerated

CHAMPION MG Trial (2024)

  • Ongoing open-label extension study
  • Intervention: Ravulizumab administered every 8 weeks based on body weight
  • Efficacy: Improvements maintained through 60 weeks; LS mean change from baseline in MG-ADL score was -4.0 (p<0.0001)
  • Safety: Well tolerated with no meningococcal infections reported

REGAIN Study (2021)

  • 26-week, phase 3, randomized, double-blind, placebo-controlled study with open-label extension
  • Intervention: Eculizumab for AChR+ refractory generalized myasthenia gravis
  • Efficacy: More eculizumab-treated patients achieved 'minimal symptom expression' versus placebo (21.4% vs 1.7%; p=0.0007)
  • Safety: Long-term tolerability consistent with previous reports

These recent clinical trials demonstrate significant advances in targeted therapies for myasthenia gravis, with multiple novel mechanisms showing clinically meaningful improvements in patient outcomes while maintaining favorable safety profiles. The development of these therapies represents important alternatives to traditional treatments like corticosteroids, which carry substantial risks of severe adverse effects with long-term use.