✓ A reliable technique is described for producing chronic communicating hydrocephalus in experimental animals. This involves the injection of Silastic into the basilar cisterns by way of a cisterna magna puncture. This model proves to be very useful in studying the physiology of chronic communicating hydrocephalus and allows the evaluation of the condition by isotope cisternography.
A. Everette James Jr., William J. Flor, Mitchell Bush, Timothy Merz, and Berkley L. Rish Capt.
William R. Kennedy, Todd A. DeWees, Sahaja Acharya, Mustafaa Mahmood, Nels C. Knutson, S. Murty Goddu, James A. Kavanaugh, Timothy J. Mitchell, Keith M. Rich, Albert H. Kim, Eric C. Leuthardt, Joshua L. Dowling, Gavin P. Dunn, Michael R. Chicoine, Stephanie M. Perkins, Jiayi Huang, Christina I. Tsien, Clifford G. Robinson, and Christopher D. Abraham
The internal high-dose volume varies widely for a given prescribed dose during stereotactic radiosurgery (SRS) to treat brain metastases (BMs). This may be altered during treatment planning, and the authors have previously shown that this improves local control (LC) for non–small cell lung cancer BMs without increasing toxicity. Here, they seek to identify potentially actionable dosimetric predictors of LC after SRS for melanoma BM.
The records of patients with unresected melanoma BM treated with single-fraction Gamma Knife RS between 2006 and 2017 were reviewed. LC was assessed on a per-lesion basis, defined as stability or a decrease in lesion size. Outcome-oriented approaches were utilized to determine optimal dichotomization for dosimetric variables relative to LC. Univariable and multivariable Cox regression analysis was implemented to evaluate the impact of collected parameters on LC.
Two hundred eighty-seven melanoma BMs in 79 patients were identified. The median age was 56 years (range 31–86 years). The median follow-up was 7.6 months (range 0.5–81.6 months), and the median survival was 9.3 months (range 1.3–81.6 months). Lesions were optimally stratified by volume receiving at least 30 Gy (V30) greater than or equal to versus less than 25%. V30 was ≥ and < 25% in 147 and 140 lesions, respectively. For all patients, 1-year LC was 83% versus 66% for V30 ≥ and < 25%, respectively (p = 0.001). Stratifying by volume, lesions 2 cm or less (n = 215) had 1-year LC of 82% versus 70% (p = 0.013) for V30 ≥ and < 25%, respectively. Lesions > 2 to 3 cm (n = 32) had 1-year LC of 100% versus 43% (p = 0.214) for V30 ≥ and < 25%, respectively. V30 was still predictive of LC even after controlling for the use of immunotherapy and targeted therapy. Radionecrosis occurred in 2.8% of lesions and was not significantly associated with V30.
For a given prescription dose, an increased internal high-dose volume, as indicated by measures such as V30 ≥ 25%, is associated with improved LC but not increased toxicity in single-fraction SRS for melanoma BM. Internal dose escalation is an independent predictor of improved LC even in patients receiving immunotherapy and/or targeted therapy. This represents a dosimetric parameter that is actionable at the time of treatment planning and warrants further evaluation.