26 juni 2023: Bron: Journal of Clinical Oncology 41, no. 17_suppl (June 10, 2023) LBA4-LBA4. Published online June 07, 2023.

Wanneer bij patiënten met gevorderde ziekte van Hodgkin (stadium III en IV) als eerstelijns behandeling immuuntherapie met Nivolumab (Opdivo) wordt toegevoegd aan de standaard chemokuur van doxorubicinehydrochloride IV, vinblastinesulfaat IV, dacarbazine IV plus eventueel radiotherapie / bestraling in plaats van Brentuximab Vedotine dan verbetert de ziektevrije overleving op 1-jaar van 86 procent naar 94 procent. En met minder ernstige bijwerkingen. Dat blijkt uit de resultaten van de SWOG S1826 fase III studie en gepresenteerd op  ASCO 2023

De standaardgroep kreeg doxorubicinehydrochloride IV, vinblastinesulfaat IV, dacarbazine IV en Brentuximab Vedotine IV gedurende 30 minuten op dag 1 en 15. Patiënten kunnen pegfilgrastim SC krijgen op dag 2 en 16, of filgrastim SC of IV op dag 6-10 en 21- 25. De behandeling wordt elke 28 dagen gedurende 6 cycli herhaald bij afwezigheid van ziekteprogressie of onaanvaardbare toxiciteit. Na voltooiing van cyclus 6 kunnen patiënten 5 dagen per week bestraald worden gedurende ongeveer 4 weken naar goeddunken van de behandelend arts. Patiënten ondergaan ook perifere bloedmonsterafname en CT, PET/CT en MRI tijdens onderzoek.

De experimentele groep kreeg doxorubicinehydrochloride IV, vinblastinesulfaat IV, dacarbazine IV en Nivolumab (Opdivo) IV gedurende 30 minuten op dag 1 en 15. Patiënten kunnen pegfilgrastim SC krijgen op dag 2 en 16, of filgrastim SC of IV op dag 6-10 en 21-25 . De behandeling wordt elke 28 dagen gedurende 6 cycli herhaald bij afwezigheid van ziekteprogressie of onaanvaardbare toxiciteit. Na voltooiing van cyclus 6 kunnen patiënten 5 dagen per week bestraald worden gedurende ongeveer 4 weken naar goeddunken van de behandelend arts. Patiënten ondergaan ook perifere bloedmonsterafname en CT, PET/CT en MRI tijdens onderzoek.

Volgens de onderzoekers was het verschil in ziektevrije overleving op 1-jaars meting 94 procent versus 84 procent in het voordeel van Nivolumab (Opdivo). En minder dan 1 procent had nog radiotherapie / bestraling nodig.

Het abstract zoals gepresenteerd op  ASCO 2023

Meeting Abstract | 2023 ASCO Annual Meeting II

LBA4

Background: The addition of BV to initial chemotherapy improves overall survival (OS) in adults and PFS in pediatric patients (pts) with AS HL. However, frontline BV adds toxicity, most pediatric pts receive radiation therapy (RT), and 7-20% of pts still develop relapsed/refractory (RR) HL. The PD-1 pathway is central to the pathogenesis of HL and PD-1 blockade is effective in RR HL. The adult and pediatric cooperative groups of the National Clinical Trials Network (NCTN) conducted the randomized, phase 3 S1826 trial to evaluate N-AVD vs BV-AVD in pts with newly diagnosed AS HL. 

Methods: Eligible pts were ≥12 years (y) with stage 3-4 HL. Pts were randomized 1:1 to either 6 cycles of N-AVD or BV-AVD. Recipients of BV-AVD were required to receive G-CSF neutropenia prophylaxis vs optional with N-AVD. Pre-specified pts could receive RT to residually metabolically active lesions on end of treatment PET. Pts were stratified by age, international prognostic score (IPS), and intent to use RT. Response and disease progression were assessed by investigators using 2014 Lugano Classification. The primary endpoint was PFS; secondary endpoints included OS, event-free survival, patient-reported outcomes (PROs), and safety. 

Results: 994 pts were enrolled from 7/9/19 to 10/5/22; 976 were eligible and randomized to N-AVD (n=489) or BV-AVD (n=487). Median age was 27y (range, 12-83y), 56% of pts were male, 76% were white, 12% were black, and 13% were Hispanic. 24% of pts were < 18y, 10% were > 60y, and 32% had IPS 4-7. So far, < 1% of pts received RT. At the planned 2nd interim analysis (50% of total PFS events) the SWOG Data and Safety Monitoring Committee recommended to report the primary results because the primary PFS endpoint crossed the protocol-specified conservative statistical boundary. 30 PFS events occurred after N-AVD vs 58 events after BV-AVD. With a median follow-up of 12.1 months, PFS was superior in the N-AVD arm [HR 0.48, 99% CI 0.27-0.87, one-sided p=0.0005); 1y PFS: N-AVD, 94%, BV-AVD, 86%. 11 deaths (7 due to adverse events, AE) were observed after BV-AVD compared to 4 after N-AVD (3 due to AE). The rate of grade (gr) ≥ 3 hematologic AE was 48.4% (45.1% gr ≥ 3 neutropenia) after N-AVD compared to 30.5% (23.9% gr ≥ 3 neutropenia) after BV-AVD. Rates (any gr) of febrile neutropenia (5.6% N vs 6.4% BV), pneumonitis (2.0% N vs 3.2% BV), ALT elevation (30.7% N vs 39.8% BV), and colitis (1% N vs 1.3% BV) were similar. Hypo/hyperthyroidism was more frequent after N-AVD (7%/3% N vs <1% BV) while peripheral neuropathy (any gr) was more common after BV-AVD (sensory: 28.1% N vs 54.2% BV; motor: 4% N vs 6.8% BV). 

Conclusions: N-AVD improved PFS vs BV-AVD in pts with AS HL. Few immune AEs were observed and < 1% of pts received RT. Longer follow-up is needed to assess OS and PROs. S1826, the largest HL study in NCTN history, is a key step towards harmonizing the pediatric and adult treatment of AS HL. Funding provided by: National Cancer Institute of the National Institutes of Health U10CA180888 and U10CA180819 and Bristol-Myers Squibb. Clinical trial information: NCT03907488.

© 2023 by American Society of Clinical Oncology

Research Sponsor:

U.S. National Institutes of Health
Bristol Myers Squibb
NIH/NCI/NCTN: U10CA180888 and U10CA180819)

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