For elderly or comorbid patients, the high toxicity of powerful, time-limited combination therapies can outweigh their efficacy. A less harsh, continuous monotherapy is often preferable as it better preserves quality of life, even if it doesn't offer a treatment-free interval or a theoretical "100% life back."

Although continuous BTK inhibitors have the most prospective data for high-risk CLL (17p/TP53 mutations), some highly motivated patients still opt for fixed-duration treatment. This requires a detailed conversation where clinicians must explain the trade-off: achieving a treatment-free period may come at the cost of needing second-line therapy sooner.

A common assumption that older patients may prefer simpler, continuous medication regimens is often incorrect. Clinical experience shows that the vast majority of patients, regardless of age, are interested in a time-limited therapy option, provided it can be delivered conveniently without infusions.

When patients first choose an indefinite BTK inhibitor over a time-limited venetoclax regimen, they reveal underlying preferences (e.g., avoiding IV infusions, scheduling) that likely persist and should guide second-line treatment selection with pirtobrutinib.

The UK FLAIR trial demonstrated for the first time that a time-limited regimen (ibrutinib-venetoclax), guided by MRD to a median duration of 27 months, achieved superior progression-free and overall survival compared to continuous ibrutinib therapy in frontline CLL.

The CLL17 study reveals that continuous ibrutinib, fixed-duration venetoclax/obinutuzumab, and fixed-duration venetoclax/ibrutinib all yield identical progression-free survival rates at three years. This finding empowers clinicians to choose a strategy based on patient preference (continuous vs. fixed-duration) without compromising near-term efficacy.

Despite the appeal of stopping treatment, a key insight from clinical practice is that patients' most critical question remains which therapy offers the longest period of remission, often overriding factors like treatment duration and oral-only options.

While many CLL patients prefer fixed-duration therapy to avoid continuous medication, this preference is often overridden by practical logistics. The burden of increased monitoring and frequent clinic visits associated with fixed-duration regimens leads some patients to opt for continuous therapy instead.

The CLL17 trial revealed a counterintuitive finding: unfit patients had worse outcomes on continuous ibrutinib, likely due to toxicity-related discontinuations. The logistically harder venetoclax-obinutuzumab fixed-duration regimen produced equal efficacy in both fit and unfit patients, making it a better choice for the less fit.