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Clinical Trial
. 2025 Aug;43(22):2527-2537.
doi: 10.1200/JCO-25-00744. Epub 2025 Jun 3.

Isatuximab Subcutaneous by On-Body Injector Versus Isatuximab Intravenous Plus Pomalidomide and Dexamethasone in Relapsed/Refractory Multiple Myeloma: Phase III IRAKLIA Study

Sikander Ailawadhi  1 Ivan Špička  2 Andrew Spencer  3 Jin Lu  4 Albert Oriol  5 Silvia Ling  6 Fredrik Schjesvold  7 Alejandro Berkovits  8 Marek Hus  9 Chunrui Li  10 Meletios-Athanasios Dimopoulos  11   12 Péter Rajnics  13   14 Sevgi Kalayoğlu Beşışık  15 Vania Hungria  16 Maria Del Rosario Custidiano  17 Gurdeep Parmar  18 Xavier Leleu  19 Fei Li  20 Claudio Cerchione  21 Cesar Gomez  22 Tadao Ishida  23 Maria Victoria Mateos  24 Tondre T Buck  25 Richard LeBlanc  26 Jiří Minařík  27 Hartmut Goldschmidt  28 Rick Zhang  29 Dorothée Sémiond  30 Florence Suzan  31 Maya Stefanova-Urena  29 Victorine Koch  31 Philippe Moreau  32
Affiliations
Clinical Trial

Isatuximab Subcutaneous by On-Body Injector Versus Isatuximab Intravenous Plus Pomalidomide and Dexamethasone in Relapsed/Refractory Multiple Myeloma: Phase III IRAKLIA Study

Sikander Ailawadhi et al. J Clin Oncol. 2025 Aug.

Erratum in

Abstract

Purpose: To report the results of the multicenter, open-label IRAKLIA trial (ClinicalTrials.gov identifier: NCT05405166) of isatuximab subcutaneous (SC) versus intravenous (IV), plus pomalidomide and dexamethasone, in relapsed/refractory multiple myeloma (MM), to our knowledge, the first phase III MM trial using an on-body injector (OBI).

Methods: Patients with ≥1 prior line of therapy were randomly assigned 1:1 to Isa OBI (1,400 mg) or IV (10 mg/kg) once weekly in cycle (C)1 and then every 2 weeks, plus pomalidomide (4 mg once daily, day [D]1-21) and dexamethasone (40 mg once weekly [age ≥75: 20 mg]) and treated until progression, unacceptable toxicity, or patient request. Coprimary end points were overall response rate (ORR; noninferiority margin, 0.839) and Isa Ctrough (C6D1 predose; noninferiority margin, 0.8). Noninferiority of OBI versus IV was demonstrated if both coprimary end points achieved noninferiority.

Results: IRAKLIA randomly assigned 531 patients (OBI, n=263; IV, n=268). After 12-month median follow-up, the ORR was 71.1% (OBI) and 70.5% (IV; relative risk, 1.008 [95% CI, 0.903 to 1.126]; lower CI exceeded noninferiority margin). The mean (standard deviation) C6D1 Ctrough was 499 (259) μg/mL (OBI) and 340 (169) μg/mL (IV). The Ctrough geometric mean ratio (90% CI) was 1.532 (1.316 to 1.784); lower CI exceeded noninferiority margin. Grade ≥3 treatment-emergent adverse event incidences were 81.7% (OBI) and 76.1% (IV); infusion reaction incidences were 1.5% and 25.0%. Injection site reactions occurred in 0.4% of OBI injections (all grade 1-2); 99.9% of injections completed without interruption.

Conclusion: IRAKLIA demonstrated efficacy and pharmacokinetic noninferiority between Isa OBI and IV. No unexpected safety signal was observed, with excellent local tolerability of Isa OBI. Efficacy and safety were comparable with Isa IV in ICARIA-MM, except the lower OBI infusion reaction rate. These results support potential use of the OBI, designed to improve practice efficiency.

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