Abstract
BackgroundMelanoma patients with metastatic growth in the meninges have poor prognosis and few treatment options. Although treatment with BRAF inhibitors or immune checkpoint inhibitors has provided promising results, most patients with advanced melanoma are resistant to these treatments and develop severe side effects. Novel treatment strategies are needed for patients with meningeal melanoma metastases, and the potential of antiangiogenic therapy was investigated in this preclinical study.MethodsTwo GFP-transfected melanoma models (A-07 and D-12) differing substantially in VEGF-A expression were included in the study, and the anti-VEGF-A antibody bevacizumab was used as therapeutic agent. Meningeal metastases were initiated in BALB/c nu/nu mice by intracranial inoculation of melanoma cells, and bevacizumab treatment was given twice a week in i.p. doses of 10 mg/kg until the mice became moribund. Therapeutic effects were evaluated by determining tumor host survival time, assessing tumor growth and angiogenic activity by quantitative analyses of histological preparations, and measuring the expression of angiogenesis-related genes by quantitative PCR.ResultsMeningeal A-07 melanomas showed higher expression of VEGF-A than meningeal D-12 melanomas, whereas the expression of ANGPT2 and IL8, two important angiogenesis drivers in melanoma, was much higher in D-12 than in A-07 tumors. Bevacizumab treatment inhibited tumor angiogenesis and prolonged host survival in mice with A-07 tumors but not in mice with D-12 tumors. Meningeal A-07 tumors in bevacizumab-treated mice compensated for the reduced VEGF-A activity by up-regulating a large number of angiogenesis-related genes, including ANGPT2 and its receptors TIE1 and TIE2. Melanoma cells migrated from meningeal tumors into the cerebrum, where they initiated metastatic growth by vessel co-option. In the A-07 model, the density of cerebral micrometastases was higher in bevacizumab-treated than in untreated mice, either because bevacizumab treatment increased mouse survival or induced increased tumor gene expression.ConclusionsThe development of antiangiogenic strategies for the treatment of meningeal melanoma metastases is a challenging task because the outcome of treatment will depend on the angiogenic signature of the tumor tissue, treatment-induced alterations of the angiogenic signature, and the treatment sensitivity of metastatic lesions in other intracranial sites.
Highlights
Melanoma patients with metastatic growth in the meninges have poor prognosis and few treatment options
The present study showed that bevacizumab treatment prolonged the survival of mice bearing meningeal A-07 tumors, most likely because bevacizumab reduced the angiogenic activity and growth rate of the tumor tissue
Meningeal A-07 tumors compensated for reduced vascular endothelial growth factor A (VEGF-A)-mediated angiogenic activity by up-regulating the expression of a large number of other angiogenesis-related genes, including genes governing the ANGPT/TIE pathway
Summary
Melanoma patients with metastatic growth in the meninges have poor prognosis and few treatment options. Treatment with BRAF inhibitors or immune checkpoint inhibitors has provided promising results, most patients with advanced melanoma are resistant to these treatments and develop severe side effects. A majority of these patients show multiple brain lesions and/or meningeal involvement, and these factors are associated with poor prognosis [2, 5]. The introduction of molecularly targeted therapies and immunotherapy has given hope to patients with advanced melanoma [9, 10], and several trials are evaluating the effect of BRAF inhibitors and immune checkpoint inhibitors in patients with brain metastases [1, 11]. It is important to explore further treatment strategies to improve the dismal prognosis of this patient group
Sign-in/Register to view highlights & summary Sign-in/Register to access full text options 
Free) 
Talk to us
Join us for a 30 min session where you can share your feedback and ask us any queries you have
Schedule a call
