2022
DOI: 10.1182/blood-2022-170463
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Combination of Ibrutinib Plus Venetoclax with MRD-Driven Duration of Treatment Results in a Higher Rate of MRD Negativity in IGHV Unmutated Than Mutated CLL: Updated Interim Analysis of FLAIR Study

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Cited by 11 publications
(17 citation statements)
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“…However, if U-MRD4 was achieved at EOT+3, U-MRD4 was sustained in 80% of uIGHV patients and 76.9% of mIGHV patients (50). In the ClbO arm, just 12.2% of patients sustained U-MRD4 at EOT+18 (51). These findings reflect the durable responses seen in CLARITY, where 75% of the cohort had uIGHV (47), and demonstrate that while the addition of venetoclax increases U-MRD4 responses, the BTKi base still holds the preference for response in uIGHV disease.…”
Section: Mrd Outcomesmentioning
confidence: 61%
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“…However, if U-MRD4 was achieved at EOT+3, U-MRD4 was sustained in 80% of uIGHV patients and 76.9% of mIGHV patients (50). In the ClbO arm, just 12.2% of patients sustained U-MRD4 at EOT+18 (51). These findings reflect the durable responses seen in CLARITY, where 75% of the cohort had uIGHV (47), and demonstrate that while the addition of venetoclax increases U-MRD4 responses, the BTKi base still holds the preference for response in uIGHV disease.…”
Section: Mrd Outcomesmentioning
confidence: 61%
“…Of those in U-MRD4 at 6 months, this was sustained at either 26 or 38 months. Of note, 75% of this cohort had uIGHV disease, and the good rates of U-MRD4 and the durability of remission for U-MRD4 patients with IV have also been reflected in uIGHV patients in the later GLOW and FLAIR trials (47,50,51).…”
Section: Mrd Outcomesmentioning
confidence: 81%
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“…In treatment arms combining ibrutinib with rituximab or obinutuzumab, the PFS seems to be shorter in the IGHV unmutated than mutated subgroup, but direct comparisons are missing and results on the combination of acalabrutinib and obinutuzumab did not suggest a prognostic impact of the IGHV status ( 5 7 , 9 ). With regards to venetoclax-based fixed-duration therapy, unmutated IGHV status retained prognostic significance and one can speculate that as IGHV unmutated patients achieved high response rates and MRD negativity, shorter PFS may reflect the more proliferative nature of IGHV unmutated CLL cells potentially leading to a faster re-growth of the CLL clone after end of treatment ( 10 , 38 40 ).…”
mentioning
confidence: 99%