Standard RECIST criteria can misclassify a significant response as "stable disease." A desmoid tumor can shrink dramatically in volume (from a "softball" to a "pencil") but maintain its length, showing no change by RECIST. This suggests clinicians are likely underestimating the true benefit of therapies.

Even when desmoid tumor patients seem to tolerate niragacestat well, they often report a surprising improvement in well-being after discontinuing the drug. This reveals a subtle, cumulative quality-of-life impact from low-grade toxicities that may not be fully appreciated by patients or clinicians during active treatment.

As more effective treatments for desmoid tumors become available, a critical unmet need is emerging: knowing when to stop therapy. Future research must focus on identifying signals, such as radiologic changes on MRI, to guide treatment duration. This will help clinicians avoid both the risk of early relapse from stopping too soon and the toxicity of unnecessary overtreatment.

Desmoid tumors exhibit highly variable behavior, acting as a chronic disease in some patients while being manageable in others. This necessitates a personalized, long-term treatment strategy rather than a standard protocol, often requiring a diverse armamentarium of therapeutic options to be used over a patient's lifetime as needs change.

Desmoid tumors can shrink without treatment, a phenomenon seen in up to 35% of patients under observation. This inherent biological behavior makes it difficult to prove that continued tumor reduction during long-term therapy is solely due to the drug's effect.

Unlike traditional oncology where the goal is complete eradication, stable residual masses on imaging after successful desmoid tumor treatment are common and acceptable. Clinicians should not be compelled to operate or change therapy based on this finding alone, as it does not indicate active disease.

While continuous therapy remains the official standard of care for mHSPC, there's a growing consensus for individualized de-intensification. For patients with a sustained, undetectable PSA (e.g., for two years), clinicians are increasingly comfortable discussing stopping all treatments to improve quality of life and reduce toxicity.

Patients on niragacestat for desmoid tumors often experience rapid symptom improvement. However, this clinical benefit significantly precedes radiological response (tumor shrinkage on scans), which can take over five months to appear. This disconnect is crucial for managing patient expectations and assessing early treatment efficacy.

There is no standard duration for systemic therapies like niragacestat. Clinicians often aim for 6-12 months, potentially extending to two years. The decision to stop is subjective and arbitrary, balancing treatment side effects against disease symptoms, highlighting the need for individualized approaches rather than fixed protocols.