A critical and often overlooked factor in managing hyperglycemia is hydration. Volume depletion from drug-induced diarrhea impairs the kidneys' ability to excrete glucose. This traps sugar in the body, creating a vicious cycle that dramatically elevates blood glucose levels.

While known for weight loss, GLP-1 agonists are also highly effective for managing hyperglycemia from both steroids and PI3K inhibitors. Using low or "micro" doses can be very helpful in cancer patients, providing glucose control while minimizing GI side effects like nausea.

Advances in drug design mean newer PI3K inhibitors are more targeted, resulting in significantly less off-target toxicity. For example, some investigational agents have a hyperglycemia risk under 15%, a substantial improvement over earlier drugs, making them easier to manage clinically.

Clinicians are hesitant to use insulin for PI3K inhibitor-induced hyperglycemia. The primary concern is that exogenous insulin, a potent growth factor, could theoretically counteract the therapy's anti-tumor effect by promoting cancer cell survival, although this risk remains unproven.

On-body glucose monitors give oncologists a richer understanding of a patient's glucose control, including 24-hour trends, time-in-range, and an A1c equivalent (GMI). This real-time data is critical for managing hyperglycemia from targeted therapies, offering more insight than periodic fasting tests.

A patient with normal baseline glucose on an AKT inhibitor can experience a sudden, severe spike in blood sugar when they get sick (e.g., fever, infection). The illness acts as a physiological stressor, creating a "perfect storm" that demands immediate attention and patient education.

For select patients who find frequent lab checks for hyperglycemia monitoring to be a significant barrier, a continuous glucose monitor (CGM) can be a practical alternative. While off-label, it provides valuable data for management in patients who might otherwise be non-adherent with monitoring.

Steroid-induced hyperglycemia is a primary driver of cancer-related high blood sugar. Patients with prediabetes (A1C 5.7-6.4%) are often overlooked but frequently develop hyperglycemia on high-dose dexamethasone, making proactive warnings and dietary guidance crucial for this group.

Testing for PI3K/AKT alterations at the initial diagnosis of metastatic disease, rather than waiting for progression, provides a crucial window of time. This allows clinicians to implement proactive dietary and medical strategies to mitigate future side effects like hyperglycemia before the targeted therapy is even started.