Mathematical prediction with pretreatment growth rate of metastatic cancer on outcomes: implications for the characterization of oligometastatic disease

Yerim Shin; Jee Suk Chang; Yeseul Kim; Sang Joon Shin; Jina Kim; Tae Hyung Kim; Mitchell Liu; Robert Olson; Jin Sung Kim; Wonmo Sung

doi:10.3389/fonc.2023.1061881

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Mathematical prediction with pretreatment growth rate of metastatic cancer on outcomes: implications for the characterization of oligometastatic disease

Authors: Yerim Shin ; Jee Suk Chang ; Yeseul Kim ; Sang Joon Shin ; Jina Kim ; Tae Hyung Kim ; Mitchell Liu ; Robert Olson ; Jin Sung Kim ; Wonmo Sung

Citation: FRONTIERS IN ONCOLOGY, Vol.13 : 1061881, 2023-05

Journal Title: FRONTIERS IN ONCOLOGY

Issue Date: 2023-05

Keywords: immune checkpoint inhabitor ; mathematical modeling ; melanoma ; oligometastasis ; tumor growth rate

Abstract: Background: Oligometastatic disease (OMD) represents an indolent cancer status characterized by slow tumor growth and limited metastatic potential. The use of local therapy in the management of the condition continues to rise. This study aimed to investigate the advantage of pretreatment tumor growth rate in addition to baseline disease burden in characterizing OMDs, generally defined by the presence of ≤ 5 metastatic lesions.

Methods: The study included patients with metastatic melanoma treated with pembrolizumab. Gross tumor volume of all metastases was contoured on imaging before (TP-1) and at the initiation of pembrolizumab (TP0). Pretreatment tumor growth rate was calculated by an exponential ordinary differential equation model using the sum of tumor volumes at TP-1 and TP0 and the time interval between TP-1. and TP0. Patients were divided into interquartile groups based on pretreatment growth rate. Overall survival, progression-free survival, and subsequent progression-free survival were the study outcomes.

Results: At baseline, median cumulative volume and number of metastases were 28.4 cc (range, 0.4-1194.8 cc) and 7 (range, 1-73), respectively. The median interval between TP-1 and TP0 was -90 days and pretreatment tumor growth rate (×10-2 days-1) was median 4.71 (range -0.62 to 44.1). The slow-paced group (pretreatment tumor growth rate ≤ 7.6 ×10-2 days-1, the upper quartile) had a significantly higher overall survival rate, progression-free survival, and subsequent progression-free survival compared to those of the fast-paced group (pretreatment tumor growth rate > 7.6 ×10-2 days-1). Notably, these differences were prominent in the subgroup with >5 metastases.

Conclusion: Pretreatment tumor growth rate is a novel prognostic metric associated with overall survival, progression-free survival, and subsequent progression-free survival among metastatic melanoma patients, especially patients with >5 metastases. Future prospective studies should validate the advantage of disease growth rate plus disease burden in better defining OMDs.