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AbstractPurpose: Isocitrate dehydrogenase (IDH) mutant gliomas are usually treated with radiotherapy and chemotherapy, which increases the risk for neurocognitive sequelae during patients’ most productive years. We report our experience using off-label first-inclass IDH1mut-inhibitor ivosidenib and its impact on tumor volume in IDHmut gliomas. Experimental Design: We retrospectively analyzed patients aged ≥18 years with radiation/chemotherapy-naïve, IDH1mut, non-enhancing, radiographically active, grade 2/3 gliomas, and ≥2 pretreatment and ≥2 on-ivosidenib MRIs. T2/FLAIR-based tumor volumes, growth rates and PFS were analyzed. Log-linear mixed-effect modeling of growth curves adjusted for grade, histology and age was performed. Results: We analyzed 116 MRIs of 12 patients (median age 46years range:26-60) 10 males, 8 astrocytomas (50% grade 3), 4 grade 2 oligodendrogliomas. Median on-drug follow-up was 13.2 months (interquartile rangeIQR:9.7-22.2). Tolerability was 100%. 50% of patients experienced ≥20% tumor volume reduction on treatment and absolute growth-rate was lower during treatment (-1.2±10.6cc/year) than before treatment (8.0±7.7cc/year; p≤0.05). Log-linear models in the Stable group (n=9) showed significant growth before treatment (53%/year; p=0.013), and volume reduction (- 34%/year; p=0.037) after 5-months on treatment. After-treatment volume curves were significantly lower than before treatment (after/before treatment ratio 0.5; p
Kamson et al. (Mon,) studied this question.
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