A key side effect of the FGFR inhibitor erdafitinib is central serous retinopathy, presenting as blurred vision. Standard of care involves a baseline ophthalmologic exam before starting treatment. If blurred vision occurs, treatment should be held immediately, but the condition is typically reversible and manageable with dose reduction.

Instead of automatically ruling out immunotherapy for cancer patients with co-existing autoimmune diseases like rheumatoid arthritis, oncologists collaborate with experienced rheumatologists. This specialist team can assess the patient's specific condition, manage risks, and confidently advise whether it is safe to proceed with anti-PD-1 therapy, enabling more patients to access effective treatments.

Due to significant ocular toxicity affecting most patients, the approved starting dose for belantumab is likely not optimal long-term. Effective management requires clinicians to proactively hold, delay, and reduce doses at the first sign of side effects, meaning real-world application will differ from the initial protocol.

The rapid and successful rollout of complex bispecific therapies into community settings is primarily driven by enhanced nursing staff skills and protocols for risk stratification. This combination allows for safe outpatient administration, preventing hospital admissions and broadening patient access beyond large academic centers.

Beyond patient comfort, the drug's favorable safety profile—lacking common GI issues or lab abnormalities—is a strategic advantage. It reduces the need for frequent patient monitoring and doctor visits, easing the logistical burden on clinicians compared to other therapies and making it an "easier to use" option.

Integrating next-gen SCLC treatments like T-cell engagers requires more than education; it demands a physical and operational overhaul. Community practices must build infrastructure for 24-hour observation and establish proactive partnerships with specialists like ophthalmologists to manage novel toxicities.

When managing ocular toxicity from the ADC mirvetuximab, clinicians advocate for delaying the subsequent dose to allow the cornea to heal naturally. This approach is often preferred over an immediate dose reduction, which might unnecessarily compromise the treatment's efficacy.

The ocular toxicity seen with the folate-targeted ADC mirvetuximab is not due to folate receptors in the eye. It is theorized to be caused by micropinocytosis, an alternative mechanism where the drug is non-specifically taken up by normal corneal cells, representing an off-target, off-tumor toxicity.

The KVA grading scale for Bellemaf's ocular side effects can trigger a grade 2 event based on an ophthalmologist's exam, even if the patient's functional vision (e.g., ability to read or drive) is unaffected. This disconnect between clinical grading and patient experience is crucial for managing treatment holds and counseling.